Updated Reviewed

Drug-Drug Interactions

Table 24d. Drug Interactions Between Integrase Strand Transfer Inhibitors and Other Drugs

This table provides information on the known or predicted interactions between integrase strand transfer inhibitors (INSTIs) (bictegravir [BIC], dolutegravir [DTG], elvitegravir [EVG], or raltegravir [RAL]) and non-antiretroviral drugs. EVG is always coadministered with cobicistat (COBI or c). Cabotegravir (CAB) intramuscular (IM) plus rilpivirine (RPV) IM are co-packaged into a single product and are coadministered as a complete regimen; therefore, the dosing recommendations and clinical comments reflect the combination of CAB IM and RPV IM treatments. Because drug interaction studies were not conducted with either IM CAB or RPV, dosing recommendations for the IM formulations are based on drug interaction studies using oral CAB and RPV. For information regarding interactions between INSTIs and other antiretroviral (ARV) drugs, including dosing recommendations, refer to Tables 24c, 24e, 24f, and 25b.

Recommendations for managing a particular drug interaction may differ, depending on whether a new ARV drug is being initiated in a patient on a stable concomitant medication or whether a new concomitant medication is being initiated in a patient on a stable ARV regimen. The magnitude and significance of drug interactions are difficult to predict when several drugs with competing metabolic pathways are prescribed concomitantly. In cases where an interacting drug needs to be replaced with an alternative, providers should exercise their clinical judgment to select the most appropriate alternative medication.

Concomitant DrugINSTIEffect on INSTI or Concomitant Drug ConcentrationsDosing Recommendations and Clinical Comments
Acid Reducers

Al, Mg,

+/–

Ca-Containing Antacids

Please refer to the Miscellaneous Drugs section of this table for recommendations on use with other polyvalent cation products (e.g., Fe and Ca supplements, multivitamins).

BIC

Al/Mg Hydroxide Antacid

  • ↔ BIC AUC if antacid is administered 2 hours after BIC and under fasting conditions
  • BIC AUC ↓ 52% if antacid is administered 2 hours before BIC
  • BIC AUC ↓ 47% to 79% if administered simultaneously with antacid

CaCO3 Antacid

  • ↔ BIC AUC if administered with food
  • BIC AUC ↓ 33% if administered under fasting conditions

With Antacids That Contain Al/Mg

  • Administer antacids that contain Al/Mg at least 2 hours after or 6 hours before BIC.

With Antacids That Contain Ca

  • Administer BIC and antacids that contain Ca together with food.
  • Do not coadminister BIC simultaneously with antacids that contain Ca on an empty stomach.
CAB POCAB PO ↓ expected

With Antacids That Contain Polyvalent Cations (Al, Mg, or Ca)

  • Administer antacid products at least 2 hours before or 4 hours after taking CAB PO.
CAB IM↔ CAB IM expectedNo dose adjustment needed
DTG

DTG AUC ↓ 74% if administered simultaneously with antacid

DTG AUC ↓ 26% if administered 2 hours before antacid

Administer DTG at least 2 hours before or at least 6 hours after antacids that contain polyvalent cations.
EVG/c

EVG AUC ↓ 40% to 50% if administered simultaneously with antacid

EVG AUC ↓ 15% to 20% if administered 2 hours before or after antacid; ↔ with a 4‑hour interval

Separate EVG/c and antacid administration by more than 2 hours.
RAL

Al/Mg Hydroxide Antacid

  • RAL Cmin ↓ 49% to 63%

CaCO3 Antacid

  • RAL 400 mg twice daily: Cmin ↓ 32%
  • RAL 1,200 mg once daily: Cmin ↓ 48% to 57%

Do not coadminister RAL and Al/Mg hydroxide antacids. Use alternative acid-reducing agent.

With CaCO3 Antacids

  • RAL 1,200 mg once daily: Do not coadminister.
  • RAL 400 mg twice daily: No dose adjustment or separation needed
H2-Receptor AntagonistsBIC, CAB (PO and IM), DTG, EVG/c↔ INSTINo dose adjustment needed
RALRAL AUC ↑ 44% and Cmax ↑ 60%No dose adjustment needed
Proton Pump InhibitorsBIC, CAB (PO and IM), DTG, EVG/c↔ INSTINo dose adjustment needed
RALRAL AUC ↑ 37% and Cmin ↑ 24%No dose adjustment needed
Alpha-Adrenergic Antagonists for Benign Prostatic Hyperplasia
AlfuzosinBIC, CAB (PO and IM), DTG, RAL↔ alfuzosin expectedNo dose adjustment needed
EVG/c↑ alfuzosin expectedContraindicated
DoxazosinBIC, CAB (PO and IM), DTG, RAL↔ doxazosin expectedNo dose adjustment needed
EVG/c↑ doxazosin possibleInitiate doxazosin at lowest dose. Titrate based on doxazosin efficacy. Monitor blood pressure. Doxazosin dose reduction may be needed.
TamsulosinBIC, CAB (PO and IM), DTG, RAL↔ tamsulosin expectedNo dose adjustment needed
EVG/c↑ tamsulosin expectedDo not coadminister unless the benefits outweigh the risks. If coadministered, monitor blood pressure.
TerazosinBIC, CAB (PO and IM), DTG, RAL↔ terazosin expectedNo dose adjustment needed
EVG/c↑ terazosin possibleInitiate terazosin at lowest dose. Titrate based on terazosin efficacy. Monitor blood pressure. Terazosin dose reduction may be necessary.
SilodosinBIC, CAB (PO and IM), DTG, RAL↔ silodosin expectedNo dose adjustment needed
EVG/c↑ silodosin expectedContraindicated
Antibacterials—Antimycobacterials
BedaquilineBIC, CAB (PO and IM), DTG, RAL↔ bedaquilineNo dosage adjustment needed
EVG/c↑ bedaquiline possibleDo not coadminister unless benefits outweigh risks. If coadministered, consider therapeutic drug monitoring and monitor for bedaquiline-related adverse effects, including hepatotoxicity and QTc prolongation.
RifabutinBIC

Rifabutin 300 mg Once Daily

  • BIC AUC ↓ 38% and Cmin ↓ 56%
Do not coadminister.
CAB PO

CAB PO AUC ↓ 23% and Cmin ↓ 26%

↔ rifabutin

No dose adjustment needed
CAB IM

↓ CAB IM and RPV expected

↔ rifabutin expected

Contraindicated due to ↓ RPV, which is co-packaged and coadministered with CAB IM.
DTG

Rifabutin 300 mg Once Daily

  • ↔ DTG AUC and Cmin ↓ 30%
No dose adjustment needed
EVG/c

Rifabutin 150 mg Every Other Day With EVG/c Once Daily Compared to Rifabutin 300 mg Once Daily Alone

  • ↔ rifabutin AUC
  • 25-O-desacetyl-rifabutin AUC ↑ 625%
  • EVG AUC ↓ 21% and Cmin ↓ 67%
Do not coadminister.
RAL↔ RAL AUC and Cmin ↓ 20%No dose adjustment needed
RifampinBICBIC AUC ↓ 75%Contraindicated
CAB POCAB PO AUC ↓ 59% and Cmin ↓ 50%Contraindicated
CAB IMCAB IM ↓ expectedContraindicated
DTG

Rifampin With DTG 50 mg Twice Daily Compared to DTG 50 mg Twice Daily Alone

  • DTG AUC ↓ 54% and Cmin ↓ 72%

Rifampin With DTG 50 mg Twice Daily Compared to DTG 50 mg Once Daily Alone

  • DTG AUC ↑ 33% and Cmin ↑ 22%

Use DTG 50 mg twice daily (instead of DTG 50 mg once daily) in patients without suspected or documented INSTI-associated resistance mutations.

Consider an alternative to rifampin, such as rifabutin, in patients with certain suspected or documented INSTI-associated resistance mutations.

EVG/cSignificant ↓ EVG and COBI expectedContraindicated
RAL

RAL 400 mg

  • RAL AUC ↓ 40% and Cmin ↓ 61%

Rifampin With RAL 800 mg Twice Daily Compared to RAL 400 mg Twice Daily Alone

  • RAL AUC ↑ 27% and Cmin ↓ 53%

Use RAL 800 mg twice daily instead of 400 mg twice daily.

Do not coadminister RAL 1,200 mg once daily with rifampin.

Monitor closely for virologic response or consider using rifabutin as an alternative rifamycin.

RifapentineBIC, EVG/cSignificant ↓ BIC, EVG, and COBI expectedDo not coadminister.
CAB (PO and IM)Significant ↓ CAB (PO and IM) expectedContraindicated
DTG

Rifapentine 900 mg Once Weekly

  • DTG AUC ↓ 26% and Cmin ↓ 47%

Rifapentine 600 mg Once Daily With DTG 50 mg Twice Daily vs DTG 50 mg Once Daily Alone

  • ↔ DTG AUC and Cmin

With once-weekly rifapentine, DTG 50 mg daily may be used in patients with viral suppression on daily DTG. Monitor for virologic efficacy. Do not coadminister in patients who require twice-daily DTG.

With once-daily rifapentine for 4 weeks (1HP), use DTG 50 mg twice daily. See Tuberculosis/HIV Coinfection for more on rifapentine and DTG use.

RAL

Rifapentine 900 mg Once Weekly

  • RAL AUC ↑ 71% and Cmin ↓ 12%

Rifapentine 600 mg Once Daily

  • RAL Cmin ↓ 41%

For once-weekly rifapentine and RAL 400 mg twice daily, no dose adjustment is needed.

Do not coadminister with once-daily rifapentine.

Antibacterials—Macrolides
AzithromycinAll INSTIs↔ azithromycin expectedNo dose adjustment needed
ClarithromycinBIC↑ BIC possibleNo dose adjustment needed
CAB (PO and IM), DTG, RAL↔ clarithromycin expectedNo dose adjustment needed
EVG/c

↑ clarithromycin expected

↑ COBI possible

Reduce clarithromycin dose by 50% in patients with CrCl 50 to 60 mL/min.

Do not coadminister in patients with CrCl <50 mL/min. Consider alternative ARV or use azithromycin.

ErythromycinBIC↑ BIC possibleNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ erythromycin expected

No dose adjustment needed
EVG/c

↑ erythromycin expected

↑ COBI possible

No data available for dose recommendation. Consider alternative ARV or use azithromycin.
Anticoagulants
ApixabanBIC, CAB (PO and IM), DTG, RAL↔ apixaban expectedNo dose adjustment needed
EVG/c↑ apixaban expected

Do not coadminister in patients who require apixaban 2.5 mg twice daily.

Reduce apixaban dose by 50% in patients who require apixaban 5 mg or 10 mg twice daily.

DabigatranBIC, CAB (PO and IM), DTG, RAL↔ dabigatran expectedNo dose adjustment needed
EVG/c

↑ dabigatran expected

With COBI 150 mg Alone

  • Dabigatran AUC ↑ 110% to 127%

Reduction of Risk of Stroke and Systemic Embolism in Nonvalvular Atrial Fibrillation in Adult Patients

  • CrCl >30 mL/min: no dose adjustment needed
  • CrCl ≤30 mL/min: do not coadminister.

Treatment and Reduction in the Risk of Recurrence of DVT and PE or Prophylaxis of DVT and PE Following Hip Replacement Surgery in Adult Patients

  • CrCl ≥50 mL/min: no dose adjustment needed
  • CrCl <50 mL/min: do not coadminister.
EdoxabanBIC, CAB (PO and IM), DTG, RAL↔ edoxaban expectedNo dose adjustment needed
EVG/c↑ edoxaban expected

Stroke Prevention in Nonvalvular Atrial Fibrillation

  • No dose adjustment needed

DVT and PE

  • Administer edoxaban 30 mg once daily.
RivaroxabanBIC, CAB (PO and IM), DTG, RAL↔ rivaroxaban expectedNo dose adjustment needed
EVG/c↑ rivaroxaban expectedDo not coadminister.
WarfarinBIC, CAB (PO and IM), DTG, RAL↔ warfarin expectedNo dose adjustment needed
EVG/c↑ or ↓ warfarin possibleMonitor INR and adjust warfarin dose accordingly.
Antiseizure
CarbamazepineBIC↓ BIC possibleDo not coadminister.
CAB (PO and IM)↓ CAB expectedContraindicated
DTGDTG AUC ↓ 49%

Increase DTG dose to 50 mg twice daily in ART-naive or ART-experienced (but INSTI-naive) patients.

Do not coadminister in INSTI-experienced patients with known or suspected INSTI resistance.

EVG/c

Carbamazepine AUC ↑ 43%

EVG AUC ↓ 69% and Cmin ↓ >99%

↓ COBI expected

Contraindicated
RAL↓ or ↔ RAL possibleDo not coadminister.
EslicarbazepineAll INSTIs

↓ INSTI possible

↓ COBI possible

Consider alternative ARV or anticonvulsant.
EthosuximideBIC, CAB (PO and IM), DTG, RAL↔ ethosuximide expectedNo dose adjustment needed
EVG/c↑ ethosuximide possibleMonitor for ethosuximide-related adverse events.
LamotrigineBIC, CAB (PO and IM), DTG, RAL↔ lamotrigine expectedNo dose adjustment needed
EVG/cNo dataMonitor anticonvulsant concentrations and adjust dose accordingly.
OxcarbazepineBIC, DTG↓ BIC and DTG possibleDo not coadminister.
CAB (PO and IM)↓ CAB expectedContraindicated
EVG/c, RAL↓ EVG/c and RAL possibleConsider alternative ARV or anticonvulsant.
Phenobarbital, Phenytoin, PrimidoneBIC, DTG, RAL

↓ BIC and DTG possible

↓ or ↔ RAL possible

Do not coadminister.
CAB (PO and IM), EVG/c↓ CAB and EVG/c expectedContraindicated
Valproic AcidDTGDTG ↓ possibleNo dose adjustment needed. Take with food and monitor virologic response.
BIC, CAB (PO and IM), RALNo dataNo dose adjustment needed. Monitor virologic response.
Antidepressants, Anxiolytics, and Antipsychotics
Also see the Sedative/Hypnotics section below
Antidepressants, Anxiolytics
BupropionBIC, CAB (PO and IM), DTG, RAL↔ bupropion expectedNo dose adjustment needed
EVG/c↑ bupropion possibleTitrate bupropion dose based on clinical response.
BuspironeBIC, CAB (PO and IM), DTG, RAL↔ buspirone expectedNo dose adjustment needed
EVG/c↑ buspirone possibleInitiate buspirone at a low dose. Buspirone dose reduction may be needed.
DesvenlafaxineAll INSTIs↔ desvenlafaxine expectedNo dose adjustment needed
DuloxetineBIC, CAB (PO and IM), DTG, RAL↔ duloxetine expectedNo dose adjustment needed
EVG/c↑ duloxetine possibleNo dose adjustment needed
MirtazapineBIC, CAB (PO and IM), DTG, RAL↔ mirtazapine expectedNo dose adjustment needed
EVG/c↑ mirtazapine possibleMonitor for mirtazapine-related adverse events. Mirtazapine dose reduction may be necessary.
NefazodoneBIC, CAB (PO and IM), DTG, RAL↔ nefazodone expectedNo dose adjustment needed
EVG/c↑ nefazodone expectedConsider alternative ARV or antidepressant.
TrazodoneBIC, CAB (PO and IM), DTG, RAL↔ trazodone expectedNo dose adjustment needed
EVG/c↑ trazodone possibleTitrate dose based on antidepressant response and monitor for trazodone-related adverse events.

Tricyclic Antidepressants

(e.g., amitriptyline, desipramine, doxepin, imipramine, nortriptyline)

BIC, CAB (PO and IM), DTG, RAL↔ TCA expectedNo dose adjustment needed
EVG/cDesipramine AUC ↑ 65%Initiate with lowest dose of TCA and titrate dose carefully.
↑ TCA expectedInitiate with lowest dose of TCA. Titrate dose carefully based on antidepressant response and/or drug concentrations.

Selective Serotonin Reuptake Inhibitors

(e.g., citalopram, escitalopram, fluoxetine, fluvoxamine, paroxetine, sertraline, vortioxetine)

EVG/c↔ sertralineNo dose adjustment needed
EVG/c↑ other SSRIs possibleInitiate with lowest dose of SSRI. Titrate dose carefully based on antidepressant response.
BIC, CAB (PO and IM), DTG, RAL↔ SSRI expectedNo dose adjustment needed
VenlafaxineBIC, CAB (PO and IM), DTG, RAL↔ venlafaxine expectedNo dose adjustment needed
EVG/c↑ venlafaxine possibleMonitor for venlafaxine-related adverse events.
Antipsychotics
AripiprazoleBIC, CAB (PO and IM), DTG, RAL↔ aripiprazole expectedNo dose adjustment needed
EVG/c↑ aripiprazole expectedAdminister 25% of the usual aripiprazole dose. Titrate based on aripiprazole effectiveness and adverse events. Refer to aripiprazole label for dosing recommendations in patients who are known to be CYP2D6-poor metabolizers or who have major depressive disorder.
BrexpiprazoleBIC, CAB (PO and IM), DTG, RAL↔ brexpiprazole expectedNo dose adjustment needed
EVG/c↑ brexpiprazole expectedAdminister 25% of the usual brexpiprazole dose. Titrate based on brexpiprazole effectiveness and adverse events. Refer to brexpiprazole label for dosing recommendations in patients who are known to be CYP2D6-poor metabolizers or who have major depressive disorder.
CariprazineBIC, CAB (PO and IM), DTG, RAL↔ cariprazine expectedNo dose adjustment needed
EVG/c↑ cariprazine expected

Starting Cariprazine in a Patient Who Is Already Receiving EVG/c

  • Administer cariprazine 1.5 mg on Day 1 and Day 3, with no dose given on Day 2. From Day 4 onward, administer cariprazine 1.5 mg daily. Dose can be increased to a maximum of cariprazine 3 mg daily. If EVG/c is withdrawn, cariprazine dose may need to be increased.

Starting EVG/c in a Patient Who Is Already Receiving Cariprazine

  • For patients receiving cariprazine 3 mg or cariprazine 6 mg daily, reduce the dose by half. For patients receiving cariprazine 4.5 mg daily, reduce dose to cariprazine 1.5 mg or cariprazine 3 mg daily. For patients receiving cariprazine 1.5 mg daily, change to cariprazine 1.5 mg every other day. If EVG/c is withdrawn, cariprazine dose may need to be increased
IloperidoneBIC, CAB (PO and IM), DTG, RAL↔ iloperidone expectedNo dose adjustment needed
EVG/c↑ iloperidone expectedDecrease iloperidone dose by 50%.
LumateperoneBIC, CAB (PO and IM), DTG, RAL↔ lumateperone expectedNo dose adjustment needed
EVG/c↑ lumateperone expectedDo not coadminister.
LurasidoneBIC, CAB (PO and IM), DTG, RAL↔ lurasidone expectedNo dose adjustment needed
EVG/c↑ lurasidone expectedContraindicated
Olanzapine, Olanzapine/ SamidorphanAll INSTIs↔ olanzapine expectedNo dose adjustment needed.
EVG/c

↔ olanzapine expected

↑ samidorphan possible

No dose adjustment needed

Other Antipsychotics

CYP3A4 and/or CYP2D6 substrates (e.g., perphenazine, risperidone, thioridazine)

EVG/c↑ antipsychotic possibleInitiate antipsychotic at a low dose. Antipsychotic dose reduction may be needed.
PimavanserinBIC, CAB (PO and IM), DTG, RAL↔ pimavanserin expectedNo dose adjustment needed
EVG/c↑ pimavanserin expectedReduce pimavanserin dose to 10 mg.
PimozideBIC, CAB (PO and IM), DTG, RAL↔ pimozide expectedNo dose adjustment needed
EVG/c↑ pimozide expectedContraindicated
QuetiapineBIC, CAB (PO and IM), DTG, RAL↔ quetiapine expectedNo dose adjustment needed
EVG/c↑ quetiapine AUC expected

Starting Quetiapine in a Patient Receiving EVG/c

  • Start quetiapine at the lowest dose and titrate up as needed. Monitor for quetiapine efficacy and adverse events.

Starting EVG/c in a Patient Receiving a Stable Dose of Quetiapine

  • Reduce quetiapine dose to 1/6 of the current dose. Closely monitor for quetiapine efficacy and adverse events.
ZiprasidoneBIC, CAB (PO and IM), DTG, RAL↔ ziprasidone expectedNo dose adjustment needed
EVG/c↑ ziprasidone possibleMonitor for ziprasidone-related adverse events.
Antimigraine
Ergot DerivativesBIC, CAB (PO and IM), DTG, RAL↔ dihydroergotamine, ergotamine, and methylergonovine expectedNo dose adjustment needed
EVG/c↑ dihydroergotamine, ergotamine, and methylergonovine expectedContraindicated
Calcitonin Gene-Related Peptide (CGRP) Receptor Antagonists
AtogepantBIC, CAB (PO and IM), DTG, RAL

↔ atogepant expected

↑ atogepant expected

No dose adjustment needed
EVG/c↑ atogepant expected

Chronic migraine: Do not coadminister.

Episodic migraine: Administer atogepant at a dose of 10 mg once daily.

RimegepantBIC, CAB (PO and IM), DTG, RAL↔ rimegepant expectedNo dose adjustment needed
EVG/c↑ rimegepant expectedDo not coadminister.
UbrogepantBIC, CAB (PO and IM), DTG, RAL↔ ubrogepant expectedNo dose adjustment needed
EVG/c↑ ubrogepant expectedContraindicated
ZavegepantBIC, CAB (PO and IM), DTG, RAL↔ zavegepant expectedNo dose adjustment needed
EVG/c↑ zavegepant expectedDo not coadminister.
Serotonin 5-HT1B, 1D Receptor Agonist
AlmotriptanBIC, CAB (PO and IM), DTG, RAL↔ almotriptan expectedNo dose adjustment needed
EVG/c↑ almotriptan expectedAdminister single dose of almotriptan 6.25 mg. Maximum dose should not exceed 12.5 mg in a 24-hour period.
EletriptanBIC, CAB (PO and IM), DTG, RAL↔ eletriptan expectedNo dose adjustment needed
EVG/c↑ eletriptan expectedContraindicated
Frovatriptan, Naratriptan, Rizatriptan, Sumatriptan ZolmitriptanAll INSTIs↔ triptan expectedNo dose adjustment needed
Antifungals
IbrexafungerpBIC, CAB (PO and IM), DTG, RAL↔ ibrexafungerp expectedNo dose adjustment needed
EVG/c↑ ibrexafungerp expectedReduce ibrexafungerp dose to 150 mg twice daily.
IsavuconazoleBIC, CAB (PO and IM), DTG, RAL↑ INSTI possibleNo dose adjustment needed
EVG/c

↑ isavuconazole expected

↑ or ↓ EVG and COBI possible

Contraindicated
ItraconazoleBIC↑ BIC expectedNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ itraconazole expected

No dose adjustment needed
EVG/c

↑ itraconazole expected

↑ EVG and COBI possible

Consider monitoring itraconazole concentrations to guide dose adjustments. Do not coadminister with high itraconazole doses (>200 mg/day) unless guided by itraconazole concentrations.
PosaconazoleBIC↑ BIC expectedNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ posaconazole expected

No dose adjustment needed
EVG/c

↑ EVG and COBI possible

↑ posaconazole possible

If coadministered, monitor posaconazole concentrations.
VoriconazoleBIC↑ BIC possibleNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ voriconazole expected

No dose adjustment needed
EVG/c

↑ voriconazole expected

↑ EVG and COBI possible

Do not coadminister voriconazole and COBI, unless the benefit outweighs the risk. If coadministered, consider monitoring voriconazole concentrations and adjust dose accordingly.
Antimalarials
Artemether/LumefantrineBIC↔ antimalarial expectedNo dose adjustment needed
CAB (PO and IM), DTG, RAL↔ antimalarial expectedNo dose adjustment needed
EVG/c↑ artemether and lumefantrine possibleMonitor for artemether and lumefantrine-related adverse events, including QTc prolongation.
ArtesunateAll INSTIs↔ dihydroartemisinin expectedNo dose adjustment needed
Atovaquone/ProguanilAll INSTIs↔ atovaquone/proguanil expectedNo dose adjustment needed
MefloquineCAB (PO and IM), DTG, RAL↔ mefloquine expectedNo dose adjustment needed
EVG/c↑ mefloquine possibleMonitor for mefloquine-related adverse events, including psychiatric symptoms and QTc prolongation.
Glucose-Lowering
MetforminBICMetformin AUC ↑ 39%Monitor for adverse events of metformin.
CAB (PO and IM), RAL↔ metformin expectedNo dose adjustment needed.
DTG

DTG 50 mg Once Daily Plus Metformin 500 mg Twice Daily

  • Metformin AUC ↑ 79% and Cmax ↑ 66%

DTG 50 mg Twice Daily Plus Metformin 500 mg Twice Daily

  • Metformin AUC ↑ 2.4-fold and Cmax ↑ 2-fold

Start metformin at the lowest dose and titrate based on glycemic control. Monitor for adverse events of metformin.

When starting/stopping DTG in patients on metformin, dose adjustment of metformin may be necessary to maintain optimal glycemic control and/or minimize adverse events of metformin.

EVG/c↑ metformin possibleNo dose adjustment needed
SaxagliptinBIC, CAB (PO and IM), DTG, RAL↔ saxagliptin expectedNo dose adjustment needed
EVG/c↑ saxagliptin expectedLimit saxagliptin dose to 2.5 mg once daily.
Dapagliflozin/
Saxagliptin
BIC, CAB (PO and IM), DTG, RAL↔ dapagliflozin or saxagliptin expectedNo dose adjustment needed
EVG/c↑ saxagliptin expectedDo not coadminister. Dapagliflozin is available only as a coformulated drug that contains 5 mg of saxagliptin. When coadministered with EVG/c, the dose of saxagliptin should not exceed 2.5 mg once daily; thus, this combination is not recommended.
Antiplatelets
ClopidogrelBIC, CAB (PO and IM), DTG, RAL↔ clopidogrel expectedNo dose adjustment needed
EVG/c↓ clopidogrel active metabolite, with impaired platelet inhibition expectedDo not coadminister.
PrasugrelBIC, CAB (PO and IM), DTG, RAL↔ prasugrel expectedNo dose adjustment needed
EVG/c↓ prasugrel active metabolite, with no impairment of platelet inhibition expectedNo dose adjustment needed
TicagrelorBIC, CAB (PO and IM), DTG, RAL↔ ticagrelor expectedNo dose adjustment needed
EVG/c↑ ticagrelor expectedDo not coadminister.
VorapaxarBIC, CAB (PO and IM) DTG, RAL↔ vorapaxar expectedNo dose adjustment needed
EVG/c↑ vorapaxar expectedDo not coadminister.
Antipneumocystis and Antitoxoplasmosis
AtovaquoneAll INSTIs↔ atovaquone expectedNo dose adjustment needed
Antivirals—Hepatitis C
Elbasvir/GrazoprevirBIC↔ BIC expectedNo dose adjustment needed
CAB (PO and IM)↔ CAB, elbasvir, and grazoprevir expectedNo dose adjustment needed
DTG

↔ DTG

↔ elbasvir

↔ grazoprevir

No dose adjustment needed
EVG/c

↑ elbasvir expected

↑ grazoprevir expected

Do not coadminister.
RAL

↔ RAL with elbasvir

RAL AUC ↑ 43% with grazoprevir

↔ elbasvir

↔ grazoprevir

No dose adjustment needed
Glecaprevir/PibrentasvirBIC, CAB (PO and IM)↔ BIC or CAB expectedNo dose adjustment needed
DTG↔ DTG and glecaprevir/ pibrentasvirNo dose adjustment needed
RAL

No significant effect

RAL AUC ↑ 47%

 
EVG/c

Glecaprevir AUC ↑ 3-fold

Pibrentasvir AUC ↑ 57%

EVG AUC ↑ 47%

No dose adjustment needed.

If coadministered with TDF, monitor for TDF-related adverse events. Consider monitoring for hepatotoxicity if coadministered with TDF or TAF.

Ledipasvir/SofosbuvirBIC, DTG, RAL↔ BIC, DTG, and RALNo dose adjustment needed
CAB (PO and IM)↔ CAB expectedNo dose adjustment needed
EVG/c/TDF/
FTC

↑ TDF expected

↑ ledipasvir expected

Do not coadminister.
EVG/c/TAF/
FTC
↔ EVG/c/TAF/FTC expectedNo dose adjustment needed
SofosbuvirBIC, CAB (PO and IM), DTG, EVG/C

↔ INSTI expected

↔ sofosbuvir expected

No dose adjustment needed
RAL↔ RAL and sofosbuvirNo dose adjustment needed
Sofosbuvir/VelpatasvirBIC, DTG, RAL↔ sofosbuvir and velpatasvirNo dose adjustment needed. If coadministered with TDF, monitor for TDF‑related adverse events.
CAB (PO and IM)

↔ CAB expected

↔ sofosbuvir and velpatasvir expected

EVG/c

↔ EVG/c/TAF/FTC

Velpatasvir AUC ↑ 50%

Sofosbuvir/
Velpatasvir/
Voxilaprevir
BIC

When Administered With Sofosbuvir/
Velpatasvir/
Voxilaprevir (400 mg/100 mg/100 mg) plus Voxilaprevir 100 mg

  • ↔ BIC, sofosbuvir, velpatasvir, voxilaprevir
No dose adjustment needed
EVG/c

When Administered With Sofosbuvir/
Velpatasvir/
Voxilaprevir (400 mg/100 mg/100 mg) plus Voxilaprevir 100 mg

  • Sofosbuvir AUC ↑ 22%
  • ↔ velpatasvir
  • Voxilaprevir AUC ↑ 2-fold
No dose adjustment needed. If coadministered with TDF, monitor for TDF-related adverse events. Consider monitoring for hepatotoxicity if coadministered with TDF or TAF.
BIC, CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ sofosbuvir, velpatasvir, and voxilaprevir expected

No dose adjustment needed
Antivirals—Miscellaneous (e.g., for CMV, Mpox)
BrincidofovirBIC, CAB (PO and IM), DTG, RAL↔ INSTI expectedNo dose adjustment needed
EVG/c

↑ brincidofovir possible

↑ EVG possible

Administer EVG/c dose at least 3 hours after administering brincidofovir and monitor for brincidofovir-related adverse events, including elevations in ALT/AST and bilirubin and GI adverse events.
CidofovirBIC, CAB (PO and IM), DTG, EVG/c, RAL

↔ INSTI expected

↔ cidofovir expected

No dose adjustment needed
TecovirimatCAB (IM)↔ CAB expected

No dose adjustment needed.

Do not initiate CAB/RPV IM during or within 2 weeks after tecovirimat treatment. (Refer to Table 24b for interaction with RPV.)

BIC, CAB (PO), DTG, EVG/c, RAL↔ INSTI expectedNo dose adjustment needed
Antivirals—SARS-CoV-2
MolnupiravirBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ INSTI and molnupiravir expectedNo dose adjustment needed
Ritonavir-boosted NirmatrelvirBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ INSTI and ritonavir-boosted nirmatrelvir expectedNo dose adjustment needed
EVG/c/FTC/TAF

↑ TAF possible

↔ ritonavir-boosted nirmatrelvir expected

No dose adjustment needed
RemdesivirBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ INSTI and remdesivir expectedNo dose adjustment needed
Beta-Agonists, Long-Acting Inhaled
Arformoterol,
Formoterol
All INSTIs↔ arformoterol or formoterol expectedNo dose adjustment needed
IndacaterolBIC, CAB (PO and IM), DTG, RAL↔ indacaterol expectedNo dose adjustment needed
EVG/c↑ indacaterol expected
OlodaterolBIC, CAB (PO and IM), DTG, RAL↔ olodaterol expectedNo dose adjustment needed
EVG/c↑ olodaterol expected
SalmeterolBIC, CAB (PO and IM), DTG, RAL↔ salmeterol expectedNo dose adjustment needed
EVG/c↑ salmeterol possibleDo not coadminister due to the potential for increased risk of salmeterol-associated cardiovascular events.
Cardiac Medications
Antiarrhythmics
AmiodaroneBIC, CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ amiodarone expected

No dose adjustment needed
EVG/c↑ amiodarone expectedDo not coadminister unless the benefits outweigh the risks. If coadministration is necessary, monitor for amiodarone-related adverse events and consider monitoring ECG and amiodarone concentrations.
DigoxinBIC, CAB (PO and IM), RAL↔ digoxin expectedNo dose adjustment needed
EVG/cDigoxin Cmax ↑ 41% and ↔ AUCTherapeutic drug monitoring for digoxin is recommended if available.
DofetilideCAB (PO and IM)↔ dofetilide expectedNo dose adjustment needed
BIC, DTG↑ dofetilide expectedContraindicated
EVG/c↑ dofetilide possibleDo not coadminister.
DisopyramideBIC, CAB (PO and IM), RAL↔ disopyramide expectedNo dose adjustment needed
DTG↑ disopyramide possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor disopyramide concentrations and for antiarrhythmic-related adverse events.
EVG/c↑ disopyramide expectedDo not coadminister.
DronedaroneBIC, CAB (PO and IM), DTG, RAL↔ dronedarone expectedNo dose adjustment needed
EVG/c↑ dronedarone expectedContraindicated
FlecainideBIC, CAB (PO and IM), DTG, RAL↔ flecainide expectedNo dose adjustment needed
EVG/c↑ flecainide possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor flecainide concentrations and for antiarrhythmic-related adverse events.
PropafenoneBIC, CAB (PO and IM), DTG, RAL↔ propafenone expectedNo dose adjustment needed
EVG/c↑ propafenone possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor propafenone concentrations and for antiarrhythmic-related adverse events.
MexiletineBIC, CAB (PO and IM), DTG, RAL↔ mexiletine expectedNo dose adjustment needed
EVG/c↑ mexiletine possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor mexiletine concentrations and for antiarrhythmic-related adverse events.
Systemic LidocaineBIC, CAB (PO and IM), DTG, RAL↔ lidocaine expectedNo dose adjustment needed
EVG/c↑ lidocaine possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor lidocaine concentrations and for antiarrhythmic-related adverse events.
QuinidineBIC, CAB (PO and IM), DTG, RAL↔ quinidine expectedNo dose adjustment needed
EVG/c↑ quinidine possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor lidocaine concentrations and for antiarrhythmic-related adverse events.
Beta-Blockers
Atenolol, Bisoprolol, Carvedilol, Metoprolol, Nadolol, Nebivolol, SotalolCAB (PO and IM), RAL↔ beta-blocker expectedNo dose adjustment needed
BIC, DTG, EVG/c↑ beta-blocker possibleBeta-blocker dose may need to be decreased; adjust dose based on clinical response.
Calcium Channel Blockers
Calcium Channel BlockersBIC

↑ BIC possible with diltiazem

↔ expected for all other CCBs

No dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ CCB expected

No dose adjustment needed
EVG/c↑ CCB possibleTitrate CCB dose and monitor for CCB efficacy and adverse events.
Cardiac—Other
BosentanBIC, DTG↓ BIC and DTG possibleNo dose adjustment needed
CAB (PO and IM)↔ bosentan expectedConsider using alternative ARV or an alternative to bosentan because bosentan may ↓ RPV, which is co-packaged and coadministered with CAB IM. If bosentan is used with RPV, monitor virologic response to ART.
RAL↔ bosentan expectedNo dose adjustment needed
EVG/c↑ bosentan possible

In Patients on EVG/c ≥10 Days

  • Start bosentan at 62.5 mg once daily or every other day based on individual tolerability.

In Patients on Bosentan Who Require EVG/c

  • Stop bosentan ≥36 hours before EVG/c initiation. At least 10 days after initiation of EVG/c, resume bosentan at 62.5 mg once daily or every other day based on individual tolerability.
EplerenoneBIC, CAB (PO and IM), DTG, RAL↔ eplerenone expectedNo dose adjustment needed
EVG/c↑ eplerenone expectedContraindicated
IvabradineBIC, CAB (PO and IM), DTG, RAL↔ ivabradine expectedNo dose adjustment needed
EVG/c↑ ivabradine expectedContraindicated
MavacamtenBIC, CAB (PO and IM), DTG, RAL↔ mavacamten expectedNo dose adjustment needed
EVG/c↑ mavacamten expectedContraindicated
RanolazineBIC, CAB (PO and IM), DTG, RAL↔ ranolazine expectedNo dose adjustment needed
EVG/c↑ ranolazine expectedContraindicated
Corticosteroids

Beclomethasone

Inhaled or intranasal

BIC, CAB (PO and IM), DTG, EVG/c, RAL↔ glucocorticoid expectedNo dose adjustment needed

Budesonide, Ciclesonide, Fluticasone, Mometasone

Inhaled or intranasal

BIC, CAB (PO and IM), DTG, RAL↔ glucocorticoid expectedNo dose adjustment needed
EVG/c↑ glucocorticoid possibleDo not coadminister unless the potential benefits of inhaled or intranasal corticosteroid outweigh the risks of systemic corticosteroid adverse effects. Coadministration can result in adrenal insufficiency and Cushing’s syndrome. Consider using an alternative corticosteroid (e.g., beclomethasone).

Betamethasone, Budesonide

Systemic

BIC, CAB (PO and IM), DTG, RAL

↔ INSTI expected

 ↔ glucocorticoid expected

No dose adjustment needed
EVG/c

↑ glucocorticoid possible

↓ EVG possible

Do not coadminister unless the potential benefits of systemic budesonide outweigh the risks of systemic corticosteroid adverse effects. Coadministration can result in adrenal insufficiency and Cushing’s syndrome.

Dexamethasone

Systemic

BIC↓ BIC possibleConsider alternative corticosteroid for long-term use or alternative ARV. If coadministration is necessary, monitor virologic response to ART.
CAB (PO and IM), DTG, RAL↔ INSTI expectedNo dose adjustment needed
EVG/c↓ EVG and COBI possibleConsider alternative corticosteroid for long-term use or alternative ARV. If coadministration is necessary, monitor virologic response to ART.

Prednisone, Prednisolone

Systemic

BIC, CAB (PO and IM), DTG, RAL↔ glucocorticoid expectedNo dose adjustment needed
EVG/c↑ prednisolone possibleCoadministration may be considered if the potential benefits outweigh the risks of systemic corticosteroid adverse effects. If coadministration is necessary, monitor for adrenal insufficiency and Cushing’s syndrome.

Betamethasone, Methylprednisolone,

Prednisolone, Triamcinolone

Local injections, including intra-articular, epidural, or intra-orbital

BIC, CAB (PO and IM), DTG, RAL↔ glucocorticoid expectedNo dose adjustment needed
EVG/c↑ glucocorticoid expectedDo not coadminister. Coadministration may result in adrenal insufficiency and Cushing’s syndrome.
Herbal Products
St. John’s WortBIC, CAB (PO and IM), DTG↓ BIC and DTG possibleDo not coadminister.
EVG/c↓ EVG and COBI expectedContraindicated
Hormonal Therapies

Injectable Contraceptives

Depot MPA

BIC, CAB (PO and IM), DTG, RAL↔ INSTI and injectable contraceptive expectedNo dose adjustment needed
EVG/c↑ MPA possibleNo dose adjustment needed

Oral Contraceptives

(e.g., desogestrel, drospirenone, ethinyl estradiol, levonorgestrel, norethindrone, norgestimate) 

BIC, CAB (PO, IM), DTG, RAL

↔ ethinyl estradiol and norgestimate with DTG 

↔ ethinyl estradiol and levonorgestrel with CAB PO 

↔ ethinyl estradiol and norgestimate expected with BIC, RAL 

↔ norgestimate expected with CAB PO and IM 

↔ levonorgestrel expected 

↔ drospirenone expected 

↔ norethindrone expected 

No dose adjustment needed
EVG/c

Norgestimate AUC, Cmax, and Cmin ↑ > 2-fold 

Ethinyl estradiol AUC ↓ 25% and Cmin ↓ 44% 

↑ drospirenone possible 

The effects of increases in progestin (norgestimate) are not fully known and may include insulin resistance, dyslipidemia, acne, and venous thrombosis. Decreased ethinyl estradiol may lead to more intermenstrual bleeding. Weigh the risks and benefits of using the drug and consider using an alternative ARV or contraceptive method.

Clinical monitoring is recommended due to the potential for hyperkalemia. Consider using alternative ARV or contraceptive method.

↑ levonorgestrel possible

↑ norethindrone expected

No dose adjustment needed

Subdermal Implant Contraceptives

(e.g., etonogestrel, levonorgestrel)

BIC, CAB (PO and IM), DTG, RAL

Etonogestrel ↑ 27% with DTG

↔ etonogestrel or levonorgestrel expected with BIC, CAB, RAL

No dose adjustment needed
EVG/c

↑ etonogestrel expected

↑ levonorgestrel expected

No dose adjustment needed

Transdermal Contraceptives

(e.g., ethinyl estradiol/norelgestromin, ethinyl estradiol/levonorgestrel)  

BIC, CAB (PO and IM), DTG, RAL↔ contraceptive expectedNo dose adjustment needed
EVG/c

↑ progestin possible 

↓ ethinyl estradiol possible 

No dose adjustment needed

Vaginal Ring Contraceptives

(e.g., etonogestrel/ethinyl estradiol, segesterone/ethinyl estradiol) 

BIC, CAB (PO and IM), DTG, RAL↔ contraceptive expected No dose adjustment needed
EVG/c

↑ progestin possible 

↓ ethinyl estradiol possible 

For segesterone/ethinyl estradiol vaginal rings, use alternative ARV or contraceptive methods.

Emergency Contraceptives

Levonorgestrel (PO)

BIC, CAB (PO and IM), DTG, RAL↔ levonorgestrel expectedNo dose adjustment needed
EVG/c↑ levonorgestrel possibleNo dose adjustment needed
Hormonal Therapies—Gender-Affirming and Menopause
Gender-Affirming TherapyBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ goserelin, leuprolide acetate, and spironolactone expectedNo dose adjustment needed
BIC, CAB (PO and IM), DTG, RAL↔ estrogen expectedNo dose adjustment needed
↔ testosterone expectedNo dose adjustment needed
EVG/c

↑ or ↓ estradiol possible

↑ cyproterone, dutasteride, and finasteride possible

Adjust dutasteride dose as needed based on clinical effects and endogenous hormone concentrations.
↑ testosterone possibleMonitor masculinizing effects of testosterone and monitor for adverse effects. Adjust testosterone dose as necessary.
Menopausal Replacement TherapyBIC, CAB (PO and IM), DTG, RAL

↔ estrogen expected with estradiol or conjugated estrogen (equine and synthetic)

↔ drospirenone, MPA, and micronized progesterone expected

No dose adjustment needed
EVG/c

↓ or ↑ estrogen possible

↑ drospirenone possible

↑ oral MPA possible

↑ oral micronized progesterone possible

Adjust estrogen and progestin dose as needed based on clinical effects.
Immunosuppressants
Cyclosporine, Everolimus, Sirolimus, TacrolimusBIC, CAB (PO and IM), DTG, RAL↔ immunosuppressant expectedNo dose adjustment needed
EVG/c↑ immunosuppressant possibleInitiate with an adjusted dose of immunosuppressant to account for potential increased concentrations of the immunosuppressant. Monitor for immunosuppressant-related adverse events. Therapeutic drug monitoring of immunosuppressant is recommended. Consult with a specialist as necessary.
Lipid-Modifying
AtorvastatinBIC, CAB (PO and IM), DTG, RAL↔ atorvastatin expectedNo dose adjustment needed
EVG/cAtorvastatin AUC ↑ 2.6-fold and Cmax ↑ 2.3-foldAdminister the lowest effective dose while monitoring for adverse events. Do not exceed 20 mg atorvastatin daily.
FluvastatinBIC, CAB (PO and IM), DTG, RAL↔ fluvastatin expectedNo dose adjustment needed
EVG/c↑ fluvastatin possibleAdminister the lowest effective fluvastatin dose while monitoring for adverse events.
LomitapideBIC, CAB (PO and IM), DTG, RAL↔ lomitapide expectedNo dose adjustment needed
EVG/c↑ lomitapide expectedContraindicated
LovastatinBIC, CAB (PO and IM), DTG, RAL↔ lovastatin expectedNo dose adjustment needed
EVG/cSignificant ↑ lovastatin expectedContraindicated
Pitavastatin,
Pravastatin
BIC, CAB (PO and IM), DTG, RAL↔ statin expectedNo dose adjustment needed
EVG/cNo dataNo dose adjustment needed. Monitor for adverse events.
RosuvastatinBIC, CAB (PO and IM), DTG, RAL↔ rosuvastatin expectedNo dose adjustment needed
EVG/cRosuvastatin AUC ↑ 38% and Cmax ↑ 89%Administer the lowest effective dose while monitoring for adverse events.
SimvastatinBIC, CAB (PO and IM), DTG, RAL↔ simvastatin expectedNo dose adjustment needed
EVG/cSignificant ↑ simvastatin expectedContraindicated
Narcotics and Treatment for Opioid Dependence

Buprenorphine

Sublingual, buccal, or implant

BIC, CAB (PO and IM), DTG↔ buprenorphine and norbuprenorphine (active metabolite) expectedNo dose adjustment needed
EVG/c

Buprenorphine AUC ↑ 35% and Cmin ↑ 66%

Norbuprenorphine (active metabolite) AUC ↑ 42% and Cmin ↑ 57%

No dose adjustment needed. Monitor for adverse events of buprenorphine. When transferring buprenorphine from transmucosal administration to implantation, monitor to ensure buprenorphine effect is adequate and not excessive.
RAL

↔ buprenorphine and norbuprenorphine (active metabolite) (sublingual)

↔ buprenorphine or norbuprenorphine (active metabolite) expected (implant)

No dose adjustment needed
FentanylBIC, CAB (PO and IM), DTG, RAL↔ fentanyl expectedNo dose adjustment needed
EVG/c↑ fentanylMonitor for fentanyl efficacy and adverse events, including potentially fatal respiratory depression.
LofexidineBIC, CAB (PO and IM), DTG, RAL↔ lofexidine expectedNo dose adjustment needed
EVG/c↑ lofexidine possibleMonitor for lofexidine-related adverse events, including symptoms of orthostasis and bradycardia.
MethadoneAll INSTIs↔ methadoneNo dose adjustment needed
TramadolBIC, CAB (PO and IM), DTG, RAL↔ tramadol and M1 (active metabolite) expectedNo dose adjustment needed
EVG/c

↑ tramadol expected

↓ M1 (active metabolite) possible

Tramadol dose adjustments may be necessary. Monitor for clinical response and tramadol-related adverse events.
PDE5 Inhibitors
AvanafilBIC, CAB (PO and IM), DTG, RAL↔ avanafil expectedNo dose adjustment needed
EVG/cNo dataDo not coadminister.
SildenafilBIC, CAB (PO and IM), DTG, RAL↔ sildenafil expectedNo dose adjustment needed
EVG/c↑ sildenafil expected

For Treatment of Erectile Dysfunction

  • Start with sildenafil 25 mg every 48 hours and monitor for sildenafil-related adverse events.

Contraindicated for treatment of PAH.

TadalafilBIC, CAB (PO and IM), DTG, RAL↔ tadalafil expectedNo dose adjustment needed
EVG/c↑ tadalafil expected

For Treatment of Erectile Dysfunction

  • Start with tadalafil 5 mg. Do not exceed a single dose of tadalafil 10 mg every 72 hours. Monitor for tadalafil-related adverse events.

For Treatment of PAH

In Patients on EVG/c >7 Days

  • Start with tadalafil 20 mg once daily. Increase to tadalafil 40 mg once daily based on tolerability.

In Patients on Tadalafil who Require EVG/c

  • Stop tadalafil ≥24 hours before EVG/c initiation. Seven days after EVG/c initiation, restart tadalafil at 20 mg once daily and increase to tadalafil 40 mg once daily based on tolerability.
VardenafilBIC, CAB (PO and IM), DTG, RAL↔ vardenafil expectedNo dose adjustment needed
EVG/c↑ vardenafil expectedStart with vardenafil 2.5 mg every 72 hours and monitor for vardenafil-related adverse events.
Sedative/Hypnotics
Benzodiazepines
Alprazolam, Clonazepam, Clorazepate, Diazepam, Estazolam, FlurazepamBIC, CAB (PO and IM), DTG, RAL↔ benzodiazepine expectedNo dose adjustment needed
EVG/c↑ benzodiazepine possible

Dose reduction of benzodiazepine may be necessary. Initiate with a low dose and monitor for benzodiazepine-related adverse events.

Consider using an alternative benzodiazepine, such as lorazepam, oxazepam, or temazepam.

Midazolam, TriazolamBIC, CAB (PO and IM), RAL↔ benzodiazepine expectedNo dose adjustment needed
DTG

With DTG 25 mg

  • ↔ midazolam AUC
No dose adjustment needed
EVG/c

↑ midazolam expected

↑ triazolam expected

Contraindicated

Do not coadminister triazolam or oral midazolam and EVG/c.

Parenteral midazolam can be administered in a closely monitored setting. Consider dose reduction, especially if >1 dose is administered.

Orexin Receptor Antagonists
Daridorexant,
Lemborexant,
Suvorexant
BIC, CAB (PO and IM), DTG, RAL↔ daridorexant, lemborexant, suvorexant expectedNo dose adjustment needed
EVG/c↑ daridorexant, lemborexant, suvorexant expectedDo not coadminister.
Other Sedatives
EszopicloneBIC, CAB (PO and IM), DTG, RAL↔ eszopiclone expectedNo dose adjustment needed
EVG/c↑ eszopiclone expectedStart with lowest dose and increase to a max of 2 mg daily. Monitor for eszopiclone-related adverse events.
ZolpidemBIC, CAB (PO and IM), DTG, RAL↔ zolpidem expectedNo dose adjustment needed
EVG/c↑ zolpidem expectedInitiate zolpidem at a low dose. Dose reduction of zolpidem may be necessary.
Miscellaneous Drugs
CalcifediolBIC, CAB (PO and IM), DTG, RAL↔ calcifediol expectedNo dose adjustment needed
EVG/c↑ calcifediol possibleDose adjustment of calcifediol may be required. Monitor serum 25-hydroxyvitamin D, intact PTH, and serum Ca concentrations.
CisaprideBIC, CAB (PO and IM), DTG, RAL↔ cisapride expectedNo dose adjustment needed
EVG/c↑ cisapride expectedContraindicated
ColchicineBIC, CAB (PO and IM), DTG, RAL↔ colchicine expectedNo dose adjustment needed
EVG/c↑ colchicine expected

Do not coadminister in patients with hepatic or renal impairment.

For Treatment of Gout Flares

  • Administer a single dose of colchicine 0.6 mg, followed by colchicine 0.3 mg 1 hour later. Do not repeat dose for at least 3 days.

For Prophylaxis of Gout Flares

  • If original dose was colchicine 0.6 mg twice daily, decrease to colchicine 0.3 mg once daily. If dose was 0.6 mg once daily, decrease to 0.3 mg every other day.

For Treatment of Familial Mediterranean Fever

  • Do not exceed colchicine 0.6 mg once daily or 0.3 mg twice daily.
DronabinolBIC, CAB (PO and IM), DTG, RAL↔ dronabinol expectedNo dose adjustment needed
EVG/c↑ dronabinol possibleMonitor for dronabinol-related adverse events.
EluxadolineBIC, CAB (PO and IM), DTG, RAL↔ eluxadoline expectedNo dose adjustment needed
EVG/c↑ eluxadoline possibleMonitor for eluxadoline-related adverse events.
Ergot DerivativesBIC, CAB (PO and IM), DTG, RAL↔ dihydroergotamine, ergotamine, and methylergonovine expectedNo dose adjustment needed
EVG/c↑ dihydroergotamine, ergotamine, and methylergonovine expectedContraindicated
FinerenoneBIC, CAB (PO and IM), DTG, RAL↔ finerenone expectedNo dose adjustment needed
EVG/c↑ finerenone expectedContraindicated
FlibanserinBIC, CAB (PO and IM), DTG, RAL↔ flibanserin expectedNo dose adjustment needed
EVG/c↑ flibanserin expectedContraindicated
NaloxegolBIC, CAB (PO and IM), DTG, RAL↔ naloxegol expectedNo dose adjustment needed
EVG/c↑ naloxegol expectedContraindicated

Polyvalent Cation Supplements

Mg, Al, Fe, Ca, Zn, including multivitamins with minerals

Note: Please refer to the Acid Reducers section in this table for recommendations on use with Al-, Mg-, and Ca-containing antacids.

BIC

↔ BIC AUC if administered simultaneously with Fe or Ca and food

BIC AUC ↓ 33% if administered simultaneously with CaCO3 under fasting conditions

BIC AUC ↓ 63% if administered simultaneously with Fe under fasting conditions

With Supplements That Contain Ca or Fe

  • Administer BIC and supplements that contain Ca or Fe together with food.

Do not coadminister BIC under fasting conditions simultaneously with, or 2 hours after, supplements that contain Ca or Fe.

CAB↓ INSTI possible

If coadministration is necessary, administer INSTI at least 2 hours before or at least 4 hours after supplements that contain polyvalent cations, including but not limited to the following products: cation-containing laxatives; Fe, Ca, or Mg supplements; and sucralfate. Monitor for virologic response.

Many oral multivitamins also contain varying amounts of polyvalent cations; the extent and significance of chelation is unknown.

DTG

DTG AUC ↓ 39% if administered simultaneously with CaCO3 under fasting conditions

DTG AUC ↓ 54% if administered simultaneously with Fe under fasting conditions

↔ DTG when administered with Ca or Fe supplement simultaneously with food

With Supplements That Contain Ca or Fe

  • Administer DTG and supplements that contain Ca or Fe together with food, or administer DTG at least 2 hours before or at least 6 hours after supplement.

Do not coadminister DTG under fasting conditions simultaneously with, or 2 hours after, supplements that contain Ca or Fe.

EVG/c, RAL↓ INSTI possible

If coadministration is necessary, administer INSTI at least 2 hours before or at least 6 hours after supplements that contain polyvalent cations, including but not limited to the following products: cation-containing laxatives; Fe, Ca, or Mg supplements; and sucralfate. Monitor for virologic response.

Many oral multivitamins also contain varying amounts of polyvalent cations; the extent and significance of chelation is unknown.

PraziquantelBIC, CAB (PO and IM), DTG, RAL↔ praziquantel and INSTI expectedNo dose adjustment needed
EVG/c↑ praziquantel possibleConsider alternative ARV. If coadministration is necessary, monitor for praziquantel-related adverse events.
Key to Symbols:
↑ = increase
↓ = decrease
↔ = less than 20% change in AUC

Key: Al = aluminum; ALT = alanine aminotransferase; ART = antiretroviral therapy; ARV = antiretroviral; AST = aspartate aminotransferase; AUC = area under the curve; BIC = bictegravir; Ca = calcium; CAB = cabotegravir; CaCO3 = calcium carbonate; CCB = calcium channel blocker; Cmax = maximum plasma concentration; Cmin = minimum plasma concentration; CMV = cytomegalovirus; COBI = cobicistat; CrCl = creatinine clearance; CYP = cytochrome P450; DTG = dolutegravir; DVT = deep vein thrombosis; ECG = electrocardiogram; EVG = elvitegravir; EVG/c = elvitegravir/cobicistat; Fe = iron; FTC = emtricitabine; GI = gastrointestinal; IM = intramuscular; INR = international normalized ratio; INSTI = integrase strand transfer inhibitor; Mg = magnesium; MPA = medroxyprogesterone acetate; PAH = pulmonary arterial hypertension; PDE5 = phosphodiesterase type 5; PE = pulmonary embolism; PO = orally; PTH = parathyroid hormone; QTc = QT corrected for heart rate; RAL = raltegravir; RPV = rilpivirine; SSRI = selective serotonin reuptake inhibitors; TAF = tenofovir alafenamide; TCA = tricyclic antidepressants; TDF = tenofovir disoproxil fumarate; Zn = zinc

Drug-Drug Interactions

Table 24d. Drug Interactions Between Integrase Strand Transfer Inhibitors and Other Drugs

Concomitant DrugINSTIEffect on INSTI or Concomitant Drug ConcentrationsDosing Recommendations and Clinical Comments
Acid Reducers

Al, Mg,

+/–

Ca-Containing Antacids

Please refer to the Miscellaneous Drugs section of this table for recommendations on use with other polyvalent cation products (e.g., Fe and Ca supplements, multivitamins).

BIC

Al/Mg Hydroxide Antacid

  • ↔ BIC AUC if antacid is administered 2 hours after BIC and under fasting conditions
  • BIC AUC ↓ 52% if antacid is administered 2 hours before BIC
  • BIC AUC ↓ 47% to 79% if administered simultaneously with antacid

CaCO3 Antacid

  • ↔ BIC AUC if administered with food
  • BIC AUC ↓ 33% if administered under fasting conditions

With Antacids That Contain Al/Mg

  • Administer antacids that contain Al/Mg at least 2 hours after or 6 hours before BIC.

With Antacids That Contain Ca

  • Administer BIC and antacids that contain Ca together with food.
  • Do not coadminister BIC simultaneously with antacids that contain Ca on an empty stomach.
CAB POCAB PO ↓ expected

With Antacids That Contain Polyvalent Cations (Al, Mg, or Ca)

  • Administer antacid products at least 2 hours before or 4 hours after taking CAB PO.
CAB IM↔ CAB IM expectedNo dose adjustment needed
DTG

DTG AUC ↓ 74% if administered simultaneously with antacid

DTG AUC ↓ 26% if administered 2 hours before antacid

Administer DTG at least 2 hours before or at least 6 hours after antacids that contain polyvalent cations.
EVG/c

EVG AUC ↓ 40% to 50% if administered simultaneously with antacid

EVG AUC ↓ 15% to 20% if administered 2 hours before or after antacid; ↔ with a 4‑hour interval

Separate EVG/c and antacid administration by more than 2 hours.
RAL

Al/Mg Hydroxide Antacid

  • RAL Cmin ↓ 49% to 63%

CaCO3 Antacid

  • RAL 400 mg twice daily: Cmin ↓ 32%
  • RAL 1,200 mg once daily: Cmin ↓ 48% to 57%

Do not coadminister RAL and Al/Mg hydroxide antacids. Use alternative acid-reducing agent.

With CaCO3 Antacids

  • RAL 1,200 mg once daily: Do not coadminister.
  • RAL 400 mg twice daily: No dose adjustment or separation needed
H2-Receptor AntagonistsBIC, CAB (PO and IM), DTG, EVG/c↔ INSTINo dose adjustment needed
RALRAL AUC ↑ 44% and Cmax ↑ 60%No dose adjustment needed
Proton Pump InhibitorsBIC, CAB (PO and IM), DTG, EVG/c↔ INSTINo dose adjustment needed
RALRAL AUC ↑ 37% and Cmin ↑ 24%No dose adjustment needed
Alpha-Adrenergic Antagonists for Benign Prostatic Hyperplasia
AlfuzosinBIC, CAB (PO and IM), DTG, RAL↔ alfuzosin expectedNo dose adjustment needed
EVG/c↑ alfuzosin expectedContraindicated
DoxazosinBIC, CAB (PO and IM), DTG, RAL↔ doxazosin expectedNo dose adjustment needed
EVG/c↑ doxazosin possibleInitiate doxazosin at lowest dose. Titrate based on doxazosin efficacy. Monitor blood pressure. Doxazosin dose reduction may be needed.
TamsulosinBIC, CAB (PO and IM), DTG, RAL↔ tamsulosin expectedNo dose adjustment needed
EVG/c↑ tamsulosin expectedDo not coadminister unless the benefits outweigh the risks. If coadministered, monitor blood pressure.
TerazosinBIC, CAB (PO and IM), DTG, RAL↔ terazosin expectedNo dose adjustment needed
EVG/c↑ terazosin possibleInitiate terazosin at lowest dose. Titrate based on terazosin efficacy. Monitor blood pressure. Terazosin dose reduction may be necessary.
SilodosinBIC, CAB (PO and IM), DTG, RAL↔ silodosin expectedNo dose adjustment needed
EVG/c↑ silodosin expectedContraindicated
Antibacterials—Antimycobacterials
BedaquilineBIC, CAB (PO and IM), DTG, RAL↔ bedaquilineNo dosage adjustment needed
EVG/c↑ bedaquiline possibleDo not coadminister unless benefits outweigh risks. If coadministered, consider therapeutic drug monitoring and monitor for bedaquiline-related adverse effects, including hepatotoxicity and QTc prolongation.
RifabutinBIC

Rifabutin 300 mg Once Daily

  • BIC AUC ↓ 38% and Cmin ↓ 56%
Do not coadminister.
CAB PO

CAB PO AUC ↓ 23% and Cmin ↓ 26%

↔ rifabutin

No dose adjustment needed
CAB IM

↓ CAB IM and RPV expected

↔ rifabutin expected

Contraindicated due to ↓ RPV, which is co-packaged and coadministered with CAB IM.
DTG

Rifabutin 300 mg Once Daily

  • ↔ DTG AUC and Cmin ↓ 30%
No dose adjustment needed
EVG/c

Rifabutin 150 mg Every Other Day With EVG/c Once Daily Compared to Rifabutin 300 mg Once Daily Alone

  • ↔ rifabutin AUC
  • 25-O-desacetyl-rifabutin AUC ↑ 625%
  • EVG AUC ↓ 21% and Cmin ↓ 67%
Do not coadminister.
RAL↔ RAL AUC and Cmin ↓ 20%No dose adjustment needed
RifampinBICBIC AUC ↓ 75%Contraindicated
CAB POCAB PO AUC ↓ 59% and Cmin ↓ 50%Contraindicated
CAB IMCAB IM ↓ expectedContraindicated
DTG

Rifampin With DTG 50 mg Twice Daily Compared to DTG 50 mg Twice Daily Alone

  • DTG AUC ↓ 54% and Cmin ↓ 72%

Rifampin With DTG 50 mg Twice Daily Compared to DTG 50 mg Once Daily Alone

  • DTG AUC ↑ 33% and Cmin ↑ 22%

Use DTG 50 mg twice daily (instead of DTG 50 mg once daily) in patients without suspected or documented INSTI-associated resistance mutations.

Consider an alternative to rifampin, such as rifabutin, in patients with certain suspected or documented INSTI-associated resistance mutations.

EVG/cSignificant ↓ EVG and COBI expectedContraindicated
RAL

RAL 400 mg

  • RAL AUC ↓ 40% and Cmin ↓ 61%

Rifampin With RAL 800 mg Twice Daily Compared to RAL 400 mg Twice Daily Alone

  • RAL AUC ↑ 27% and Cmin ↓ 53%

Use RAL 800 mg twice daily instead of 400 mg twice daily.

Do not coadminister RAL 1,200 mg once daily with rifampin.

Monitor closely for virologic response or consider using rifabutin as an alternative rifamycin.

RifapentineBIC, EVG/cSignificant ↓ BIC, EVG, and COBI expectedDo not coadminister.
CAB (PO and IM)Significant ↓ CAB (PO and IM) expectedContraindicated
DTG

Rifapentine 900 mg Once Weekly

  • DTG AUC ↓ 26% and Cmin ↓ 47%

Rifapentine 600 mg Once Daily With DTG 50 mg Twice Daily vs DTG 50 mg Once Daily Alone

  • ↔ DTG AUC and Cmin

With once-weekly rifapentine, DTG 50 mg daily may be used in patients with viral suppression on daily DTG. Monitor for virologic efficacy. Do not coadminister in patients who require twice-daily DTG.

With once-daily rifapentine for 4 weeks (1HP), use DTG 50 mg twice daily. See Tuberculosis/HIV Coinfection for more on rifapentine and DTG use.

RAL

Rifapentine 900 mg Once Weekly

  • RAL AUC ↑ 71% and Cmin ↓ 12%

Rifapentine 600 mg Once Daily

  • RAL Cmin ↓ 41%

For once-weekly rifapentine and RAL 400 mg twice daily, no dose adjustment is needed.

Do not coadminister with once-daily rifapentine.

Antibacterials—Macrolides
AzithromycinAll INSTIs↔ azithromycin expectedNo dose adjustment needed
ClarithromycinBIC↑ BIC possibleNo dose adjustment needed
CAB (PO and IM), DTG, RAL↔ clarithromycin expectedNo dose adjustment needed
EVG/c

↑ clarithromycin expected

↑ COBI possible

Reduce clarithromycin dose by 50% in patients with CrCl 50 to 60 mL/min.

Do not coadminister in patients with CrCl <50 mL/min. Consider alternative ARV or use azithromycin.

ErythromycinBIC↑ BIC possibleNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ erythromycin expected

No dose adjustment needed
EVG/c

↑ erythromycin expected

↑ COBI possible

No data available for dose recommendation. Consider alternative ARV or use azithromycin.
Anticoagulants
ApixabanBIC, CAB (PO and IM), DTG, RAL↔ apixaban expectedNo dose adjustment needed
EVG/c↑ apixaban expected

Do not coadminister in patients who require apixaban 2.5 mg twice daily.

Reduce apixaban dose by 50% in patients who require apixaban 5 mg or 10 mg twice daily.

DabigatranBIC, CAB (PO and IM), DTG, RAL↔ dabigatran expectedNo dose adjustment needed
EVG/c

↑ dabigatran expected

With COBI 150 mg Alone

  • Dabigatran AUC ↑ 110% to 127%

Reduction of Risk of Stroke and Systemic Embolism in Nonvalvular Atrial Fibrillation in Adult Patients

  • CrCl >30 mL/min: no dose adjustment needed
  • CrCl ≤30 mL/min: do not coadminister.

Treatment and Reduction in the Risk of Recurrence of DVT and PE or Prophylaxis of DVT and PE Following Hip Replacement Surgery in Adult Patients

  • CrCl ≥50 mL/min: no dose adjustment needed
  • CrCl <50 mL/min: do not coadminister.
EdoxabanBIC, CAB (PO and IM), DTG, RAL↔ edoxaban expectedNo dose adjustment needed
EVG/c↑ edoxaban expected

Stroke Prevention in Nonvalvular Atrial Fibrillation

  • No dose adjustment needed

DVT and PE

  • Administer edoxaban 30 mg once daily.
RivaroxabanBIC, CAB (PO and IM), DTG, RAL↔ rivaroxaban expectedNo dose adjustment needed
EVG/c↑ rivaroxaban expectedDo not coadminister.
WarfarinBIC, CAB (PO and IM), DTG, RAL↔ warfarin expectedNo dose adjustment needed
EVG/c↑ or ↓ warfarin possibleMonitor INR and adjust warfarin dose accordingly.
Antiseizure
CarbamazepineBIC↓ BIC possibleDo not coadminister.
CAB (PO and IM)↓ CAB expectedContraindicated
DTGDTG AUC ↓ 49%

Increase DTG dose to 50 mg twice daily in ART-naive or ART-experienced (but INSTI-naive) patients.

Do not coadminister in INSTI-experienced patients with known or suspected INSTI resistance.

EVG/c

Carbamazepine AUC ↑ 43%

EVG AUC ↓ 69% and Cmin ↓ >99%

↓ COBI expected

Contraindicated
RAL↓ or ↔ RAL possibleDo not coadminister.
EslicarbazepineAll INSTIs

↓ INSTI possible

↓ COBI possible

Consider alternative ARV or anticonvulsant.
EthosuximideBIC, CAB (PO and IM), DTG, RAL↔ ethosuximide expectedNo dose adjustment needed
EVG/c↑ ethosuximide possibleMonitor for ethosuximide-related adverse events.
LamotrigineBIC, CAB (PO and IM), DTG, RAL↔ lamotrigine expectedNo dose adjustment needed
EVG/cNo dataMonitor anticonvulsant concentrations and adjust dose accordingly.
OxcarbazepineBIC, DTG↓ BIC and DTG possibleDo not coadminister.
CAB (PO and IM)↓ CAB expectedContraindicated
EVG/c, RAL↓ EVG/c and RAL possibleConsider alternative ARV or anticonvulsant.
Phenobarbital, Phenytoin, PrimidoneBIC, DTG, RAL

↓ BIC and DTG possible

↓ or ↔ RAL possible

Do not coadminister.
CAB (PO and IM), EVG/c↓ CAB and EVG/c expectedContraindicated
Valproic AcidDTGDTG ↓ possibleNo dose adjustment needed. Take with food and monitor virologic response.
BIC, CAB (PO and IM), RALNo dataNo dose adjustment needed. Monitor virologic response.
Antidepressants, Anxiolytics, and Antipsychotics
Also see the Sedative/Hypnotics section below
Antidepressants, Anxiolytics
BupropionBIC, CAB (PO and IM), DTG, RAL↔ bupropion expectedNo dose adjustment needed
EVG/c↑ bupropion possibleTitrate bupropion dose based on clinical response.
BuspironeBIC, CAB (PO and IM), DTG, RAL↔ buspirone expectedNo dose adjustment needed
EVG/c↑ buspirone possibleInitiate buspirone at a low dose. Buspirone dose reduction may be needed.
DesvenlafaxineAll INSTIs↔ desvenlafaxine expectedNo dose adjustment needed
DuloxetineBIC, CAB (PO and IM), DTG, RAL↔ duloxetine expectedNo dose adjustment needed
EVG/c↑ duloxetine possibleNo dose adjustment needed
MirtazapineBIC, CAB (PO and IM), DTG, RAL↔ mirtazapine expectedNo dose adjustment needed
EVG/c↑ mirtazapine possibleMonitor for mirtazapine-related adverse events. Mirtazapine dose reduction may be necessary.
NefazodoneBIC, CAB (PO and IM), DTG, RAL↔ nefazodone expectedNo dose adjustment needed
EVG/c↑ nefazodone expectedConsider alternative ARV or antidepressant.
TrazodoneBIC, CAB (PO and IM), DTG, RAL↔ trazodone expectedNo dose adjustment needed
EVG/c↑ trazodone possibleTitrate dose based on antidepressant response and monitor for trazodone-related adverse events.

Tricyclic Antidepressants

(e.g., amitriptyline, desipramine, doxepin, imipramine, nortriptyline)

BIC, CAB (PO and IM), DTG, RAL↔ TCA expectedNo dose adjustment needed
EVG/cDesipramine AUC ↑ 65%Initiate with lowest dose of TCA and titrate dose carefully.
↑ TCA expectedInitiate with lowest dose of TCA. Titrate dose carefully based on antidepressant response and/or drug concentrations.

Selective Serotonin Reuptake Inhibitors

(e.g., citalopram, escitalopram, fluoxetine, fluvoxamine, paroxetine, sertraline, vortioxetine)

EVG/c↔ sertralineNo dose adjustment needed
EVG/c↑ other SSRIs possibleInitiate with lowest dose of SSRI. Titrate dose carefully based on antidepressant response.
BIC, CAB (PO and IM), DTG, RAL↔ SSRI expectedNo dose adjustment needed
VenlafaxineBIC, CAB (PO and IM), DTG, RAL↔ venlafaxine expectedNo dose adjustment needed
EVG/c↑ venlafaxine possibleMonitor for venlafaxine-related adverse events.
Antipsychotics
AripiprazoleBIC, CAB (PO and IM), DTG, RAL↔ aripiprazole expectedNo dose adjustment needed
EVG/c↑ aripiprazole expectedAdminister 25% of the usual aripiprazole dose. Titrate based on aripiprazole effectiveness and adverse events. Refer to aripiprazole label for dosing recommendations in patients who are known to be CYP2D6-poor metabolizers or who have major depressive disorder.
BrexpiprazoleBIC, CAB (PO and IM), DTG, RAL↔ brexpiprazole expectedNo dose adjustment needed
EVG/c↑ brexpiprazole expectedAdminister 25% of the usual brexpiprazole dose. Titrate based on brexpiprazole effectiveness and adverse events. Refer to brexpiprazole label for dosing recommendations in patients who are known to be CYP2D6-poor metabolizers or who have major depressive disorder.
CariprazineBIC, CAB (PO and IM), DTG, RAL↔ cariprazine expectedNo dose adjustment needed
EVG/c↑ cariprazine expected

Starting Cariprazine in a Patient Who Is Already Receiving EVG/c

  • Administer cariprazine 1.5 mg on Day 1 and Day 3, with no dose given on Day 2. From Day 4 onward, administer cariprazine 1.5 mg daily. Dose can be increased to a maximum of cariprazine 3 mg daily. If EVG/c is withdrawn, cariprazine dose may need to be increased.

Starting EVG/c in a Patient Who Is Already Receiving Cariprazine

  • For patients receiving cariprazine 3 mg or cariprazine 6 mg daily, reduce the dose by half. For patients receiving cariprazine 4.5 mg daily, reduce dose to cariprazine 1.5 mg or cariprazine 3 mg daily. For patients receiving cariprazine 1.5 mg daily, change to cariprazine 1.5 mg every other day. If EVG/c is withdrawn, cariprazine dose may need to be increased
IloperidoneBIC, CAB (PO and IM), DTG, RAL↔ iloperidone expectedNo dose adjustment needed
EVG/c↑ iloperidone expectedDecrease iloperidone dose by 50%.
LumateperoneBIC, CAB (PO and IM), DTG, RAL↔ lumateperone expectedNo dose adjustment needed
EVG/c↑ lumateperone expectedDo not coadminister.
LurasidoneBIC, CAB (PO and IM), DTG, RAL↔ lurasidone expectedNo dose adjustment needed
EVG/c↑ lurasidone expectedContraindicated
Olanzapine, Olanzapine/ SamidorphanAll INSTIs↔ olanzapine expectedNo dose adjustment needed.
EVG/c

↔ olanzapine expected

↑ samidorphan possible

No dose adjustment needed

Other Antipsychotics

CYP3A4 and/or CYP2D6 substrates (e.g., perphenazine, risperidone, thioridazine)

EVG/c↑ antipsychotic possibleInitiate antipsychotic at a low dose. Antipsychotic dose reduction may be needed.
PimavanserinBIC, CAB (PO and IM), DTG, RAL↔ pimavanserin expectedNo dose adjustment needed
EVG/c↑ pimavanserin expectedReduce pimavanserin dose to 10 mg.
PimozideBIC, CAB (PO and IM), DTG, RAL↔ pimozide expectedNo dose adjustment needed
EVG/c↑ pimozide expectedContraindicated
QuetiapineBIC, CAB (PO and IM), DTG, RAL↔ quetiapine expectedNo dose adjustment needed
EVG/c↑ quetiapine AUC expected

Starting Quetiapine in a Patient Receiving EVG/c

  • Start quetiapine at the lowest dose and titrate up as needed. Monitor for quetiapine efficacy and adverse events.

Starting EVG/c in a Patient Receiving a Stable Dose of Quetiapine

  • Reduce quetiapine dose to 1/6 of the current dose. Closely monitor for quetiapine efficacy and adverse events.
ZiprasidoneBIC, CAB (PO and IM), DTG, RAL↔ ziprasidone expectedNo dose adjustment needed
EVG/c↑ ziprasidone possibleMonitor for ziprasidone-related adverse events.
Antimigraine
Ergot DerivativesBIC, CAB (PO and IM), DTG, RAL↔ dihydroergotamine, ergotamine, and methylergonovine expectedNo dose adjustment needed
EVG/c↑ dihydroergotamine, ergotamine, and methylergonovine expectedContraindicated
Calcitonin Gene-Related Peptide (CGRP) Receptor Antagonists
AtogepantBIC, CAB (PO and IM), DTG, RAL

↔ atogepant expected

↑ atogepant expected

No dose adjustment needed
EVG/c↑ atogepant expected

Chronic migraine: Do not coadminister.

Episodic migraine: Administer atogepant at a dose of 10 mg once daily.

RimegepantBIC, CAB (PO and IM), DTG, RAL↔ rimegepant expectedNo dose adjustment needed
EVG/c↑ rimegepant expectedDo not coadminister.
UbrogepantBIC, CAB (PO and IM), DTG, RAL↔ ubrogepant expectedNo dose adjustment needed
EVG/c↑ ubrogepant expectedContraindicated
ZavegepantBIC, CAB (PO and IM), DTG, RAL↔ zavegepant expectedNo dose adjustment needed
EVG/c↑ zavegepant expectedDo not coadminister.
Serotonin 5-HT1B, 1D Receptor Agonist
AlmotriptanBIC, CAB (PO and IM), DTG, RAL↔ almotriptan expectedNo dose adjustment needed
EVG/c↑ almotriptan expectedAdminister single dose of almotriptan 6.25 mg. Maximum dose should not exceed 12.5 mg in a 24-hour period.
EletriptanBIC, CAB (PO and IM), DTG, RAL↔ eletriptan expectedNo dose adjustment needed
EVG/c↑ eletriptan expectedContraindicated
Frovatriptan, Naratriptan, Rizatriptan, Sumatriptan ZolmitriptanAll INSTIs↔ triptan expectedNo dose adjustment needed
Antifungals
IbrexafungerpBIC, CAB (PO and IM), DTG, RAL↔ ibrexafungerp expectedNo dose adjustment needed
EVG/c↑ ibrexafungerp expectedReduce ibrexafungerp dose to 150 mg twice daily.
IsavuconazoleBIC, CAB (PO and IM), DTG, RAL↑ INSTI possibleNo dose adjustment needed
EVG/c

↑ isavuconazole expected

↑ or ↓ EVG and COBI possible

Contraindicated
ItraconazoleBIC↑ BIC expectedNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ itraconazole expected

No dose adjustment needed
EVG/c

↑ itraconazole expected

↑ EVG and COBI possible

Consider monitoring itraconazole concentrations to guide dose adjustments. Do not coadminister with high itraconazole doses (>200 mg/day) unless guided by itraconazole concentrations.
PosaconazoleBIC↑ BIC expectedNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ posaconazole expected

No dose adjustment needed
EVG/c

↑ EVG and COBI possible

↑ posaconazole possible

If coadministered, monitor posaconazole concentrations.
VoriconazoleBIC↑ BIC possibleNo dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ voriconazole expected

No dose adjustment needed
EVG/c

↑ voriconazole expected

↑ EVG and COBI possible

Do not coadminister voriconazole and COBI, unless the benefit outweighs the risk. If coadministered, consider monitoring voriconazole concentrations and adjust dose accordingly.
Antimalarials
Artemether/LumefantrineBIC↔ antimalarial expectedNo dose adjustment needed
CAB (PO and IM), DTG, RAL↔ antimalarial expectedNo dose adjustment needed
EVG/c↑ artemether and lumefantrine possibleMonitor for artemether and lumefantrine-related adverse events, including QTc prolongation.
ArtesunateAll INSTIs↔ dihydroartemisinin expectedNo dose adjustment needed
Atovaquone/ProguanilAll INSTIs↔ atovaquone/proguanil expectedNo dose adjustment needed
MefloquineCAB (PO and IM), DTG, RAL↔ mefloquine expectedNo dose adjustment needed
EVG/c↑ mefloquine possibleMonitor for mefloquine-related adverse events, including psychiatric symptoms and QTc prolongation.
Glucose-Lowering
MetforminBICMetformin AUC ↑ 39%Monitor for adverse events of metformin.
CAB (PO and IM), RAL↔ metformin expectedNo dose adjustment needed.
DTG

DTG 50 mg Once Daily Plus Metformin 500 mg Twice Daily

  • Metformin AUC ↑ 79% and Cmax ↑ 66%

DTG 50 mg Twice Daily Plus Metformin 500 mg Twice Daily

  • Metformin AUC ↑ 2.4-fold and Cmax ↑ 2-fold

Start metformin at the lowest dose and titrate based on glycemic control. Monitor for adverse events of metformin.

When starting/stopping DTG in patients on metformin, dose adjustment of metformin may be necessary to maintain optimal glycemic control and/or minimize adverse events of metformin.

EVG/c↑ metformin possibleNo dose adjustment needed
SaxagliptinBIC, CAB (PO and IM), DTG, RAL↔ saxagliptin expectedNo dose adjustment needed
EVG/c↑ saxagliptin expectedLimit saxagliptin dose to 2.5 mg once daily.
Dapagliflozin/
Saxagliptin
BIC, CAB (PO and IM), DTG, RAL↔ dapagliflozin or saxagliptin expectedNo dose adjustment needed
EVG/c↑ saxagliptin expectedDo not coadminister. Dapagliflozin is available only as a coformulated drug that contains 5 mg of saxagliptin. When coadministered with EVG/c, the dose of saxagliptin should not exceed 2.5 mg once daily; thus, this combination is not recommended.
Antiplatelets
ClopidogrelBIC, CAB (PO and IM), DTG, RAL↔ clopidogrel expectedNo dose adjustment needed
EVG/c↓ clopidogrel active metabolite, with impaired platelet inhibition expectedDo not coadminister.
PrasugrelBIC, CAB (PO and IM), DTG, RAL↔ prasugrel expectedNo dose adjustment needed
EVG/c↓ prasugrel active metabolite, with no impairment of platelet inhibition expectedNo dose adjustment needed
TicagrelorBIC, CAB (PO and IM), DTG, RAL↔ ticagrelor expectedNo dose adjustment needed
EVG/c↑ ticagrelor expectedDo not coadminister.
VorapaxarBIC, CAB (PO and IM) DTG, RAL↔ vorapaxar expectedNo dose adjustment needed
EVG/c↑ vorapaxar expectedDo not coadminister.
Antipneumocystis and Antitoxoplasmosis
AtovaquoneAll INSTIs↔ atovaquone expectedNo dose adjustment needed
Antivirals—Hepatitis C
Elbasvir/GrazoprevirBIC↔ BIC expectedNo dose adjustment needed
CAB (PO and IM)↔ CAB, elbasvir, and grazoprevir expectedNo dose adjustment needed
DTG

↔ DTG

↔ elbasvir

↔ grazoprevir

No dose adjustment needed
EVG/c

↑ elbasvir expected

↑ grazoprevir expected

Do not coadminister.
RAL

↔ RAL with elbasvir

RAL AUC ↑ 43% with grazoprevir

↔ elbasvir

↔ grazoprevir

No dose adjustment needed
Glecaprevir/PibrentasvirBIC, CAB (PO and IM)↔ BIC or CAB expectedNo dose adjustment needed
DTG↔ DTG and glecaprevir/ pibrentasvirNo dose adjustment needed
RAL

No significant effect

RAL AUC ↑ 47%

 
EVG/c

Glecaprevir AUC ↑ 3-fold

Pibrentasvir AUC ↑ 57%

EVG AUC ↑ 47%

No dose adjustment needed.

If coadministered with TDF, monitor for TDF-related adverse events. Consider monitoring for hepatotoxicity if coadministered with TDF or TAF.

Ledipasvir/SofosbuvirBIC, DTG, RAL↔ BIC, DTG, and RALNo dose adjustment needed
CAB (PO and IM)↔ CAB expectedNo dose adjustment needed
EVG/c/TDF/
FTC

↑ TDF expected

↑ ledipasvir expected

Do not coadminister.
EVG/c/TAF/
FTC
↔ EVG/c/TAF/FTC expectedNo dose adjustment needed
SofosbuvirBIC, CAB (PO and IM), DTG, EVG/C

↔ INSTI expected

↔ sofosbuvir expected

No dose adjustment needed
RAL↔ RAL and sofosbuvirNo dose adjustment needed
Sofosbuvir/VelpatasvirBIC, DTG, RAL↔ sofosbuvir and velpatasvirNo dose adjustment needed. If coadministered with TDF, monitor for TDF‑related adverse events.
CAB (PO and IM)

↔ CAB expected

↔ sofosbuvir and velpatasvir expected

EVG/c

↔ EVG/c/TAF/FTC

Velpatasvir AUC ↑ 50%

Sofosbuvir/
Velpatasvir/
Voxilaprevir
BIC

When Administered With Sofosbuvir/
Velpatasvir/
Voxilaprevir (400 mg/100 mg/100 mg) plus Voxilaprevir 100 mg

  • ↔ BIC, sofosbuvir, velpatasvir, voxilaprevir
No dose adjustment needed
EVG/c

When Administered With Sofosbuvir/
Velpatasvir/
Voxilaprevir (400 mg/100 mg/100 mg) plus Voxilaprevir 100 mg

  • Sofosbuvir AUC ↑ 22%
  • ↔ velpatasvir
  • Voxilaprevir AUC ↑ 2-fold
No dose adjustment needed. If coadministered with TDF, monitor for TDF-related adverse events. Consider monitoring for hepatotoxicity if coadministered with TDF or TAF.
BIC, CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ sofosbuvir, velpatasvir, and voxilaprevir expected

No dose adjustment needed
Antivirals—Miscellaneous (e.g., for CMV, Mpox)
BrincidofovirBIC, CAB (PO and IM), DTG, RAL↔ INSTI expectedNo dose adjustment needed
EVG/c

↑ brincidofovir possible

↑ EVG possible

Administer EVG/c dose at least 3 hours after administering brincidofovir and monitor for brincidofovir-related adverse events, including elevations in ALT/AST and bilirubin and GI adverse events.
CidofovirBIC, CAB (PO and IM), DTG, EVG/c, RAL

↔ INSTI expected

↔ cidofovir expected

No dose adjustment needed
TecovirimatCAB (IM)↔ CAB expected

No dose adjustment needed.

Do not initiate CAB/RPV IM during or within 2 weeks after tecovirimat treatment. (Refer to Table 24b for interaction with RPV.)

BIC, CAB (PO), DTG, EVG/c, RAL↔ INSTI expectedNo dose adjustment needed
Antivirals—SARS-CoV-2
MolnupiravirBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ INSTI and molnupiravir expectedNo dose adjustment needed
Ritonavir-boosted NirmatrelvirBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ INSTI and ritonavir-boosted nirmatrelvir expectedNo dose adjustment needed
EVG/c/FTC/TAF

↑ TAF possible

↔ ritonavir-boosted nirmatrelvir expected

No dose adjustment needed
RemdesivirBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ INSTI and remdesivir expectedNo dose adjustment needed
Beta-Agonists, Long-Acting Inhaled
Arformoterol,
Formoterol
All INSTIs↔ arformoterol or formoterol expectedNo dose adjustment needed
IndacaterolBIC, CAB (PO and IM), DTG, RAL↔ indacaterol expectedNo dose adjustment needed
EVG/c↑ indacaterol expected
OlodaterolBIC, CAB (PO and IM), DTG, RAL↔ olodaterol expectedNo dose adjustment needed
EVG/c↑ olodaterol expected
SalmeterolBIC, CAB (PO and IM), DTG, RAL↔ salmeterol expectedNo dose adjustment needed
EVG/c↑ salmeterol possibleDo not coadminister due to the potential for increased risk of salmeterol-associated cardiovascular events.
Cardiac Medications
Antiarrhythmics
AmiodaroneBIC, CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ amiodarone expected

No dose adjustment needed
EVG/c↑ amiodarone expectedDo not coadminister unless the benefits outweigh the risks. If coadministration is necessary, monitor for amiodarone-related adverse events and consider monitoring ECG and amiodarone concentrations.
DigoxinBIC, CAB (PO and IM), RAL↔ digoxin expectedNo dose adjustment needed
EVG/cDigoxin Cmax ↑ 41% and ↔ AUCTherapeutic drug monitoring for digoxin is recommended if available.
DofetilideCAB (PO and IM)↔ dofetilide expectedNo dose adjustment needed
BIC, DTG↑ dofetilide expectedContraindicated
EVG/c↑ dofetilide possibleDo not coadminister.
DisopyramideBIC, CAB (PO and IM), RAL↔ disopyramide expectedNo dose adjustment needed
DTG↑ disopyramide possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor disopyramide concentrations and for antiarrhythmic-related adverse events.
EVG/c↑ disopyramide expectedDo not coadminister.
DronedaroneBIC, CAB (PO and IM), DTG, RAL↔ dronedarone expectedNo dose adjustment needed
EVG/c↑ dronedarone expectedContraindicated
FlecainideBIC, CAB (PO and IM), DTG, RAL↔ flecainide expectedNo dose adjustment needed
EVG/c↑ flecainide possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor flecainide concentrations and for antiarrhythmic-related adverse events.
PropafenoneBIC, CAB (PO and IM), DTG, RAL↔ propafenone expectedNo dose adjustment needed
EVG/c↑ propafenone possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor propafenone concentrations and for antiarrhythmic-related adverse events.
MexiletineBIC, CAB (PO and IM), DTG, RAL↔ mexiletine expectedNo dose adjustment needed
EVG/c↑ mexiletine possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor mexiletine concentrations and for antiarrhythmic-related adverse events.
Systemic LidocaineBIC, CAB (PO and IM), DTG, RAL↔ lidocaine expectedNo dose adjustment needed
EVG/c↑ lidocaine possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor lidocaine concentrations and for antiarrhythmic-related adverse events.
QuinidineBIC, CAB (PO and IM), DTG, RAL↔ quinidine expectedNo dose adjustment needed
EVG/c↑ quinidine possibleConsider alternative ARV or antiarrhythmics. If coadministered, monitor lidocaine concentrations and for antiarrhythmic-related adverse events.
Beta-Blockers
Atenolol, Bisoprolol, Carvedilol, Metoprolol, Nadolol, Nebivolol, SotalolCAB (PO and IM), RAL↔ beta-blocker expectedNo dose adjustment needed
BIC, DTG, EVG/c↑ beta-blocker possibleBeta-blocker dose may need to be decreased; adjust dose based on clinical response.
Calcium Channel Blockers
Calcium Channel BlockersBIC

↑ BIC possible with diltiazem

↔ expected for all other CCBs

No dose adjustment needed
CAB (PO and IM), DTG, RAL

↔ INSTI expected

↔ CCB expected

No dose adjustment needed
EVG/c↑ CCB possibleTitrate CCB dose and monitor for CCB efficacy and adverse events.
Cardiac—Other
BosentanBIC, DTG↓ BIC and DTG possibleNo dose adjustment needed
CAB (PO and IM)↔ bosentan expectedConsider using alternative ARV or an alternative to bosentan because bosentan may ↓ RPV, which is co-packaged and coadministered with CAB IM. If bosentan is used with RPV, monitor virologic response to ART.
RAL↔ bosentan expectedNo dose adjustment needed
EVG/c↑ bosentan possible

In Patients on EVG/c ≥10 Days

  • Start bosentan at 62.5 mg once daily or every other day based on individual tolerability.

In Patients on Bosentan Who Require EVG/c

  • Stop bosentan ≥36 hours before EVG/c initiation. At least 10 days after initiation of EVG/c, resume bosentan at 62.5 mg once daily or every other day based on individual tolerability.
EplerenoneBIC, CAB (PO and IM), DTG, RAL↔ eplerenone expectedNo dose adjustment needed
EVG/c↑ eplerenone expectedContraindicated
IvabradineBIC, CAB (PO and IM), DTG, RAL↔ ivabradine expectedNo dose adjustment needed
EVG/c↑ ivabradine expectedContraindicated
MavacamtenBIC, CAB (PO and IM), DTG, RAL↔ mavacamten expectedNo dose adjustment needed
EVG/c↑ mavacamten expectedContraindicated
RanolazineBIC, CAB (PO and IM), DTG, RAL↔ ranolazine expectedNo dose adjustment needed
EVG/c↑ ranolazine expectedContraindicated
Corticosteroids

Beclomethasone

Inhaled or intranasal

BIC, CAB (PO and IM), DTG, EVG/c, RAL↔ glucocorticoid expectedNo dose adjustment needed

Budesonide, Ciclesonide, Fluticasone, Mometasone

Inhaled or intranasal

BIC, CAB (PO and IM), DTG, RAL↔ glucocorticoid expectedNo dose adjustment needed
EVG/c↑ glucocorticoid possibleDo not coadminister unless the potential benefits of inhaled or intranasal corticosteroid outweigh the risks of systemic corticosteroid adverse effects. Coadministration can result in adrenal insufficiency and Cushing’s syndrome. Consider using an alternative corticosteroid (e.g., beclomethasone).

Betamethasone, Budesonide

Systemic

BIC, CAB (PO and IM), DTG, RAL

↔ INSTI expected

 ↔ glucocorticoid expected

No dose adjustment needed
EVG/c

↑ glucocorticoid possible

↓ EVG possible

Do not coadminister unless the potential benefits of systemic budesonide outweigh the risks of systemic corticosteroid adverse effects. Coadministration can result in adrenal insufficiency and Cushing’s syndrome.

Dexamethasone

Systemic

BIC↓ BIC possibleConsider alternative corticosteroid for long-term use or alternative ARV. If coadministration is necessary, monitor virologic response to ART.
CAB (PO and IM), DTG, RAL↔ INSTI expectedNo dose adjustment needed
EVG/c↓ EVG and COBI possibleConsider alternative corticosteroid for long-term use or alternative ARV. If coadministration is necessary, monitor virologic response to ART.

Prednisone, Prednisolone

Systemic

BIC, CAB (PO and IM), DTG, RAL↔ glucocorticoid expectedNo dose adjustment needed
EVG/c↑ prednisolone possibleCoadministration may be considered if the potential benefits outweigh the risks of systemic corticosteroid adverse effects. If coadministration is necessary, monitor for adrenal insufficiency and Cushing’s syndrome.

Betamethasone, Methylprednisolone,

Prednisolone, Triamcinolone

Local injections, including intra-articular, epidural, or intra-orbital

BIC, CAB (PO and IM), DTG, RAL↔ glucocorticoid expectedNo dose adjustment needed
EVG/c↑ glucocorticoid expectedDo not coadminister. Coadministration may result in adrenal insufficiency and Cushing’s syndrome.
Herbal Products
St. John’s WortBIC, CAB (PO and IM), DTG↓ BIC and DTG possibleDo not coadminister.
EVG/c↓ EVG and COBI expectedContraindicated
Hormonal Therapies

Injectable Contraceptives

Depot MPA

BIC, CAB (PO and IM), DTG, RAL↔ INSTI and injectable contraceptive expectedNo dose adjustment needed
EVG/c↑ MPA possibleNo dose adjustment needed

Oral Contraceptives

(e.g., desogestrel, drospirenone, ethinyl estradiol, levonorgestrel, norethindrone, norgestimate) 

BIC, CAB (PO, IM), DTG, RAL

↔ ethinyl estradiol and norgestimate with DTG 

↔ ethinyl estradiol and levonorgestrel with CAB PO 

↔ ethinyl estradiol and norgestimate expected with BIC, RAL 

↔ norgestimate expected with CAB PO and IM 

↔ levonorgestrel expected 

↔ drospirenone expected 

↔ norethindrone expected 

No dose adjustment needed
EVG/c

Norgestimate AUC, Cmax, and Cmin ↑ > 2-fold 

Ethinyl estradiol AUC ↓ 25% and Cmin ↓ 44% 

↑ drospirenone possible 

The effects of increases in progestin (norgestimate) are not fully known and may include insulin resistance, dyslipidemia, acne, and venous thrombosis. Decreased ethinyl estradiol may lead to more intermenstrual bleeding. Weigh the risks and benefits of using the drug and consider using an alternative ARV or contraceptive method.

Clinical monitoring is recommended due to the potential for hyperkalemia. Consider using alternative ARV or contraceptive method.

↑ levonorgestrel possible

↑ norethindrone expected

No dose adjustment needed

Subdermal Implant Contraceptives

(e.g., etonogestrel, levonorgestrel)

BIC, CAB (PO and IM), DTG, RAL

Etonogestrel ↑ 27% with DTG

↔ etonogestrel or levonorgestrel expected with BIC, CAB, RAL

No dose adjustment needed
EVG/c

↑ etonogestrel expected

↑ levonorgestrel expected

No dose adjustment needed

Transdermal Contraceptives

(e.g., ethinyl estradiol/norelgestromin, ethinyl estradiol/levonorgestrel)  

BIC, CAB (PO and IM), DTG, RAL↔ contraceptive expectedNo dose adjustment needed
EVG/c

↑ progestin possible 

↓ ethinyl estradiol possible 

No dose adjustment needed

Vaginal Ring Contraceptives

(e.g., etonogestrel/ethinyl estradiol, segesterone/ethinyl estradiol) 

BIC, CAB (PO and IM), DTG, RAL↔ contraceptive expected No dose adjustment needed
EVG/c

↑ progestin possible 

↓ ethinyl estradiol possible 

For segesterone/ethinyl estradiol vaginal rings, use alternative ARV or contraceptive methods.

Emergency Contraceptives

Levonorgestrel (PO)

BIC, CAB (PO and IM), DTG, RAL↔ levonorgestrel expectedNo dose adjustment needed
EVG/c↑ levonorgestrel possibleNo dose adjustment needed
Hormonal Therapies—Gender-Affirming and Menopause
Gender-Affirming TherapyBIC, CAB (PO and IM), DTG, EVG/c, RAL↔ goserelin, leuprolide acetate, and spironolactone expectedNo dose adjustment needed
BIC, CAB (PO and IM), DTG, RAL↔ estrogen expectedNo dose adjustment needed
↔ testosterone expectedNo dose adjustment needed
EVG/c

↑ or ↓ estradiol possible

↑ cyproterone, dutasteride, and finasteride possible

Adjust dutasteride dose as needed based on clinical effects and endogenous hormone concentrations.
↑ testosterone possibleMonitor masculinizing effects of testosterone and monitor for adverse effects. Adjust testosterone dose as necessary.
Menopausal Replacement TherapyBIC, CAB (PO and IM), DTG, RAL

↔ estrogen expected with estradiol or conjugated estrogen (equine and synthetic)

↔ drospirenone, MPA, and micronized progesterone expected

No dose adjustment needed
EVG/c

↓ or ↑ estrogen possible

↑ drospirenone possible

↑ oral MPA possible

↑ oral micronized progesterone possible

Adjust estrogen and progestin dose as needed based on clinical effects.
Immunosuppressants
Cyclosporine, Everolimus, Sirolimus, TacrolimusBIC, CAB (PO and IM), DTG, RAL↔ immunosuppressant expectedNo dose adjustment needed
EVG/c↑ immunosuppressant possibleInitiate with an adjusted dose of immunosuppressant to account for potential increased concentrations of the immunosuppressant. Monitor for immunosuppressant-related adverse events. Therapeutic drug monitoring of immunosuppressant is recommended. Consult with a specialist as necessary.
Lipid-Modifying
AtorvastatinBIC, CAB (PO and IM), DTG, RAL↔ atorvastatin expectedNo dose adjustment needed
EVG/cAtorvastatin AUC ↑ 2.6-fold and Cmax ↑ 2.3-foldAdminister the lowest effective dose while monitoring for adverse events. Do not exceed 20 mg atorvastatin daily.
FluvastatinBIC, CAB (PO and IM), DTG, RAL↔ fluvastatin expectedNo dose adjustment needed
EVG/c↑ fluvastatin possibleAdminister the lowest effective fluvastatin dose while monitoring for adverse events.
LomitapideBIC, CAB (PO and IM), DTG, RAL↔ lomitapide expectedNo dose adjustment needed
EVG/c↑ lomitapide expectedContraindicated
LovastatinBIC, CAB (PO and IM), DTG, RAL↔ lovastatin expectedNo dose adjustment needed
EVG/cSignificant ↑ lovastatin expectedContraindicated
Pitavastatin,
Pravastatin
BIC, CAB (PO and IM), DTG, RAL↔ statin expectedNo dose adjustment needed
EVG/cNo dataNo dose adjustment needed. Monitor for adverse events.
RosuvastatinBIC, CAB (PO and IM), DTG, RAL↔ rosuvastatin expectedNo dose adjustment needed
EVG/cRosuvastatin AUC ↑ 38% and Cmax ↑ 89%Administer the lowest effective dose while monitoring for adverse events.
SimvastatinBIC, CAB (PO and IM), DTG, RAL↔ simvastatin expectedNo dose adjustment needed
EVG/cSignificant ↑ simvastatin expectedContraindicated
Narcotics and Treatment for Opioid Dependence

Buprenorphine

Sublingual, buccal, or implant

BIC, CAB (PO and IM), DTG↔ buprenorphine and norbuprenorphine (active metabolite) expectedNo dose adjustment needed
EVG/c

Buprenorphine AUC ↑ 35% and Cmin ↑ 66%

Norbuprenorphine (active metabolite) AUC ↑ 42% and Cmin ↑ 57%

No dose adjustment needed. Monitor for adverse events of buprenorphine. When transferring buprenorphine from transmucosal administration to implantation, monitor to ensure buprenorphine effect is adequate and not excessive.
RAL

↔ buprenorphine and norbuprenorphine (active metabolite) (sublingual)

↔ buprenorphine or norbuprenorphine (active metabolite) expected (implant)

No dose adjustment needed
FentanylBIC, CAB (PO and IM), DTG, RAL↔ fentanyl expectedNo dose adjustment needed
EVG/c↑ fentanylMonitor for fentanyl efficacy and adverse events, including potentially fatal respiratory depression.
LofexidineBIC, CAB (PO and IM), DTG, RAL↔ lofexidine expectedNo dose adjustment needed
EVG/c↑ lofexidine possibleMonitor for lofexidine-related adverse events, including symptoms of orthostasis and bradycardia.
MethadoneAll INSTIs↔ methadoneNo dose adjustment needed
TramadolBIC, CAB (PO and IM), DTG, RAL↔ tramadol and M1 (active metabolite) expectedNo dose adjustment needed
EVG/c

↑ tramadol expected

↓ M1 (active metabolite) possible

Tramadol dose adjustments may be necessary. Monitor for clinical response and tramadol-related adverse events.
PDE5 Inhibitors
AvanafilBIC, CAB (PO and IM), DTG, RAL↔ avanafil expectedNo dose adjustment needed
EVG/cNo dataDo not coadminister.
SildenafilBIC, CAB (PO and IM), DTG, RAL↔ sildenafil expectedNo dose adjustment needed
EVG/c↑ sildenafil expected

For Treatment of Erectile Dysfunction

  • Start with sildenafil 25 mg every 48 hours and monitor for sildenafil-related adverse events.

Contraindicated for treatment of PAH.

TadalafilBIC, CAB (PO and IM), DTG, RAL↔ tadalafil expectedNo dose adjustment needed
EVG/c↑ tadalafil expected

For Treatment of Erectile Dysfunction

  • Start with tadalafil 5 mg. Do not exceed a single dose of tadalafil 10 mg every 72 hours. Monitor for tadalafil-related adverse events.

For Treatment of PAH

In Patients on EVG/c >7 Days

  • Start with tadalafil 20 mg once daily. Increase to tadalafil 40 mg once daily based on tolerability.

In Patients on Tadalafil who Require EVG/c

  • Stop tadalafil ≥24 hours before EVG/c initiation. Seven days after EVG/c initiation, restart tadalafil at 20 mg once daily and increase to tadalafil 40 mg once daily based on tolerability.
VardenafilBIC, CAB (PO and IM), DTG, RAL↔ vardenafil expectedNo dose adjustment needed
EVG/c↑ vardenafil expectedStart with vardenafil 2.5 mg every 72 hours and monitor for vardenafil-related adverse events.
Sedative/Hypnotics
Benzodiazepines
Alprazolam, Clonazepam, Clorazepate, Diazepam, Estazolam, FlurazepamBIC, CAB (PO and IM), DTG, RAL↔ benzodiazepine expectedNo dose adjustment needed
EVG/c↑ benzodiazepine possible

Dose reduction of benzodiazepine may be necessary. Initiate with a low dose and monitor for benzodiazepine-related adverse events.

Consider using an alternative benzodiazepine, such as lorazepam, oxazepam, or temazepam.

Midazolam, TriazolamBIC, CAB (PO and IM), RAL↔ benzodiazepine expectedNo dose adjustment needed
DTG

With DTG 25 mg

  • ↔ midazolam AUC
No dose adjustment needed
EVG/c

↑ midazolam expected

↑ triazolam expected

Contraindicated

Do not coadminister triazolam or oral midazolam and EVG/c.

Parenteral midazolam can be administered in a closely monitored setting. Consider dose reduction, especially if >1 dose is administered.

Orexin Receptor Antagonists
Daridorexant,
Lemborexant,
Suvorexant
BIC, CAB (PO and IM), DTG, RAL↔ daridorexant, lemborexant, suvorexant expectedNo dose adjustment needed
EVG/c↑ daridorexant, lemborexant, suvorexant expectedDo not coadminister.
Other Sedatives
EszopicloneBIC, CAB (PO and IM), DTG, RAL↔ eszopiclone expectedNo dose adjustment needed
EVG/c↑ eszopiclone expectedStart with lowest dose and increase to a max of 2 mg daily. Monitor for eszopiclone-related adverse events.
ZolpidemBIC, CAB (PO and IM), DTG, RAL↔ zolpidem expectedNo dose adjustment needed
EVG/c↑ zolpidem expectedInitiate zolpidem at a low dose. Dose reduction of zolpidem may be necessary.
Miscellaneous Drugs
CalcifediolBIC, CAB (PO and IM), DTG, RAL↔ calcifediol expectedNo dose adjustment needed
EVG/c↑ calcifediol possibleDose adjustment of calcifediol may be required. Monitor serum 25-hydroxyvitamin D, intact PTH, and serum Ca concentrations.
CisaprideBIC, CAB (PO and IM), DTG, RAL↔ cisapride expectedNo dose adjustment needed
EVG/c↑ cisapride expectedContraindicated
ColchicineBIC, CAB (PO and IM), DTG, RAL↔ colchicine expectedNo dose adjustment needed
EVG/c↑ colchicine expected

Do not coadminister in patients with hepatic or renal impairment.

For Treatment of Gout Flares

  • Administer a single dose of colchicine 0.6 mg, followed by colchicine 0.3 mg 1 hour later. Do not repeat dose for at least 3 days.

For Prophylaxis of Gout Flares

  • If original dose was colchicine 0.6 mg twice daily, decrease to colchicine 0.3 mg once daily. If dose was 0.6 mg once daily, decrease to 0.3 mg every other day.

For Treatment of Familial Mediterranean Fever

  • Do not exceed colchicine 0.6 mg once daily or 0.3 mg twice daily.
DronabinolBIC, CAB (PO and IM), DTG, RAL↔ dronabinol expectedNo dose adjustment needed
EVG/c↑ dronabinol possibleMonitor for dronabinol-related adverse events.
EluxadolineBIC, CAB (PO and IM), DTG, RAL↔ eluxadoline expectedNo dose adjustment needed
EVG/c↑ eluxadoline possibleMonitor for eluxadoline-related adverse events.
Ergot DerivativesBIC, CAB (PO and IM), DTG, RAL↔ dihydroergotamine, ergotamine, and methylergonovine expectedNo dose adjustment needed
EVG/c↑ dihydroergotamine, ergotamine, and methylergonovine expectedContraindicated
FinerenoneBIC, CAB (PO and IM), DTG, RAL↔ finerenone expectedNo dose adjustment needed
EVG/c↑ finerenone expectedContraindicated
FlibanserinBIC, CAB (PO and IM), DTG, RAL↔ flibanserin expectedNo dose adjustment needed
EVG/c↑ flibanserin expectedContraindicated
NaloxegolBIC, CAB (PO and IM), DTG, RAL↔ naloxegol expectedNo dose adjustment needed
EVG/c↑ naloxegol expectedContraindicated

Polyvalent Cation Supplements

Mg, Al, Fe, Ca, Zn, including multivitamins with minerals

Note: Please refer to the Acid Reducers section in this table for recommendations on use with Al-, Mg-, and Ca-containing antacids.

BIC

↔ BIC AUC if administered simultaneously with Fe or Ca and food

BIC AUC ↓ 33% if administered simultaneously with CaCO3 under fasting conditions

BIC AUC ↓ 63% if administered simultaneously with Fe under fasting conditions

With Supplements That Contain Ca or Fe

  • Administer BIC and supplements that contain Ca or Fe together with food.

Do not coadminister BIC under fasting conditions simultaneously with, or 2 hours after, supplements that contain Ca or Fe.

CAB↓ INSTI possible

If coadministration is necessary, administer INSTI at least 2 hours before or at least 4 hours after supplements that contain polyvalent cations, including but not limited to the following products: cation-containing laxatives; Fe, Ca, or Mg supplements; and sucralfate. Monitor for virologic response.

Many oral multivitamins also contain varying amounts of polyvalent cations; the extent and significance of chelation is unknown.

DTG

DTG AUC ↓ 39% if administered simultaneously with CaCO3 under fasting conditions

DTG AUC ↓ 54% if administered simultaneously with Fe under fasting conditions

↔ DTG when administered with Ca or Fe supplement simultaneously with food

With Supplements That Contain Ca or Fe

  • Administer DTG and supplements that contain Ca or Fe together with food, or administer DTG at least 2 hours before or at least 6 hours after supplement.

Do not coadminister DTG under fasting conditions simultaneously with, or 2 hours after, supplements that contain Ca or Fe.

EVG/c, RAL↓ INSTI possible

If coadministration is necessary, administer INSTI at least 2 hours before or at least 6 hours after supplements that contain polyvalent cations, including but not limited to the following products: cation-containing laxatives; Fe, Ca, or Mg supplements; and sucralfate. Monitor for virologic response.

Many oral multivitamins also contain varying amounts of polyvalent cations; the extent and significance of chelation is unknown.

PraziquantelBIC, CAB (PO and IM), DTG, RAL↔ praziquantel and INSTI expectedNo dose adjustment needed
EVG/c↑ praziquantel possibleConsider alternative ARV. If coadministration is necessary, monitor for praziquantel-related adverse events.
Key to Symbols:
↑ = increase
↓ = decrease
↔ = less than 20% change in AUC

Key: Al = aluminum; ALT = alanine aminotransferase; ART = antiretroviral therapy; ARV = antiretroviral; AST = aspartate aminotransferase; AUC = area under the curve; BIC = bictegravir; Ca = calcium; CAB = cabotegravir; CaCO3 = calcium carbonate; CCB = calcium channel blocker; Cmax = maximum plasma concentration; Cmin = minimum plasma concentration; CMV = cytomegalovirus; COBI = cobicistat; CrCl = creatinine clearance; CYP = cytochrome P450; DTG = dolutegravir; DVT = deep vein thrombosis; ECG = electrocardiogram; EVG = elvitegravir; EVG/c = elvitegravir/cobicistat; Fe = iron; FTC = emtricitabine; GI = gastrointestinal; IM = intramuscular; INR = international normalized ratio; INSTI = integrase strand transfer inhibitor; Mg = magnesium; MPA = medroxyprogesterone acetate; PAH = pulmonary arterial hypertension; PDE5 = phosphodiesterase type 5; PE = pulmonary embolism; PO = orally; PTH = parathyroid hormone; QTc = QT corrected for heart rate; RAL = raltegravir; RPV = rilpivirine; SSRI = selective serotonin reuptake inhibitors; TAF = tenofovir alafenamide; TCA = tricyclic antidepressants; TDF = tenofovir disoproxil fumarate; Zn = zinc

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