Antiretroviral Associated Adverse Effects and Management Recommendations for Dyslipidemia

Adverse Effects	Associated ARVs	Onset/Clinical Manifestations	Estimated Frequency	Risk Factors	Prevention/ Monitoring	Management
Dyslipidemia	PIs All PIs, especially RTV-boosted PIs; lower incidence reported with DRV/r and ATV, with or without RTV NRTIs Lower incidence reported with TDF than with TAF NNRTIs Lower incidence reported with NVP, RPV, and ETR than with EFV INSTIs EVG/c	Onset As early as 2 weeks to months after beginning therapy Presentation PIs ↑ LDL-C, TC, and TG NRTIs ↑ LDL-C, TC, and TG. Significant increase in plasma lipid values was observed in adults switching from TDF to TAF, regardless of third agent or presence of a boosting agent. NNRTIs ↑ LDL-C, TC, and HDL-C	Reported frequency varies with specific ARV regimen, duration of ART, and the specific laboratory parameters used to diagnose lipid abnormalities. 10% to 20% of young children receiving LPV/r will have lipid abnormalities. 40% to 75% of older children and adolescents with prolonged ART history will have lipid abnormalities. Pooled dyslipidemia prevalence of 39.5% and an incidence of 32% (191 per 1,000 person-years) reported in a recent meta-analysis and a recent review of a large consortium of prospective observational cohorts, respectively.	Advanced-stage HIV disease High-fat, high‑cholesterol diet Sedentary lifestyle Obesity Hypertension Smoking Family history of dyslipidemia or premature ASCVD Metabolic syndrome Fat maldistribution	Prevention Low-fat diet Exercise Smoking-prevention counseling Use of ARVs is associated with a lower prevalence of dyslipidemia, such as INSTIs, and to a lesser extent, newer PIs (e.g., ATV, DRV). When considering a TDF-based or TAF-based regimen, the lipid-lowering beneficial effect of TDF should be weighed against its potential for increased renal and bone toxicities. Monitoring^a Obtain fasting (or non‑fasting) lipid profile (TC, HDL-C, non-HDL-C, LDL-C, and TG) twice (>2 weeks but ≤3 months apart) and average these results. Monitor every 6 months (for abnormal results) or every 12 months (for normal results). If TG or LDL-C is elevated or if a patient has additional risk factors, obtain FLP. Children With Lipid Abnormalities and/or Additional Risk Factors Obtain 12-hour FLP before initiating or changing therapy and every 6 months thereafter (more often if indicated). Children Receiving Lipid-Lowering Therapy With Statins or Fibrates Obtain 12-hour FLP, LFT, and CK at 4 weeks, 8 weeks, and 3 months after starting lipid therapy. If minimal alterations in AST, ALT, and CK are indicated, monitor every 3–4 months during the first year and every 6 months thereafter (or as clinically indicated). Repeat FLP 4 weeks after increasing doses of antihyperlipidemic agents.	Assess all patients for additional ASCVD risk factors. Patients with HIV are considered to be at moderate risk for ASCVD.^b ARV regimen changes should be considered, especially when the patient is receiving older PIs (e.g., LPV/r) and/or RTV boosting. Switching to a PI-sparing regimen, a PI-based regimen with a more favorable lipid profile, or COBI boosting causes a decline in LDL‑C or TG values. The lipid-lowering effect of an ARV regimen switch on LDL-C is less pronounced than with statin therapy but may be enough to re-establish a healthy lipid profile. Refer patients to a lipid specialist early if LDL-C is ≥250 mg/dL or TG is ≥500 mg/dL. If LDL-C is ≥130 mg/dL but <250 mg or TG is ≥150 mg/dL but <500 mg/dL, the following staged treatment approach is recommended by the NHLBI guidelines^b: Implement diet, nutrition, and lifestyle management for 6‍–‍9 months. Consult with a dietician if one is available. If a 6- to 9-month trial of lifestyle modification fails and the patient is aged ≥10 years, consider implementing lipid-lowering therapy after consulting a lipid specialist. Statin therapy should be considered for patients with elevated LDL-C levels. NHLBI guidelines provide recommendations for statin therapy in patients with specific LDL-C levels and risk factors.^bConcurrent substitution—preferably to ARVs with no inhibitory or inducing effect on CYP3A4 or OATP1B1 (e.g., INSTI)—also should be considered as appropriate to limit drug–drug interaction potential. Drug therapy can be considered in cases of severe hypertriglyceridemia (TG ≥500 mg/dL). Fibrates (gemfibrozil and fenofibrate) may be used. The long-term risks of lipid abnormalities in children who are receiving ART are unclear. However, persistent dyslipidemia in children may lead to premature ASCVD.
^a Because of the burden of collecting fasting blood samples, some practitioners routinely measure cholesterol and TG from nonfasting blood samples and follow-up abnormal values with a test done in the fasted state. ^b Refer to the NHLBI guidelines: Expert Panel on Integrated Guidelines for Cardiovascular Health and Risk Reduction in Children and Adolescents. Key to Symbol: ↑ = increase Key: ALT = alanine aminotransferase; ART = antiretroviral therapy; ARV = antiretroviral; ASCVD = atherosclerotic cardiovascular disease; AST = aspartate aminotransferase; ATV = atazanavir; CK = creatine kinase; COBI = cobicistat; CYP3A4 = cytochrome P450 3A4; DRV = darunavir; DRV/r = darunavir/ritonavir; EFV = efavirenz; ETR = etravirine; EVG/c = elvitegravir/cobicistat; FLP = fasting lipid profile; HDL-C = high-density lipoprotein cholesterol; INSTI = integrase strand transfer inhibitor; LDLC = low-density lipoprotein cholesterol; LFT = liver function test; LPV/r = lopinavir/ritonavir; NHLBI = National Heart, Lung, and Blood Institute; NNRTI = non-nucleoside reverse transcriptase inhibitor; NRTI = nucleoside reverse transcriptase inhibitor; NVP = nevirapine; OATP1B1 = organic anion transporter polypeptide 1B1; PI = protease inhibitor; PUFA = polyunsaturated fatty acid; RPV = rilpivirine; RTV = ritonavir; TAF = tenofovir alafenamide; TC = total cholesterol; TDF = tenofovir disoproxil fumarate; TG = triglycerides

Adverse Effects

Associated ARVs

Onset/Clinical Manifestations

Estimated Frequency

Risk Factors

Prevention/ Monitoring

Management

Dyslipidemia

PIs

All PIs, especially RTV-boosted PIs; lower incidence reported with DRV/r and ATV, with or without RTV

NRTIs

Lower incidence reported with TDF than with TAF

NNRTIs

Lower incidence reported with NVP, RPV, and ETR than with EFV

INSTIs

EVG/c

Onset

As early as 2 weeks to months after beginning therapy

Presentation

PIs

↑ LDL-C, TC, and TG

NRTIs

↑ LDL-C, TC, and TG. Significant increase in plasma lipid values was observed in adults switching from TDF to TAF, regardless of third agent or presence of a boosting agent.

NNRTIs

↑ LDL-C, TC, and HDL-C

Reported frequency varies with specific ARV regimen, duration of ART, and the specific laboratory parameters used to diagnose lipid abnormalities.

10% to 20% of young children receiving LPV/r will have lipid abnormalities.

40% to 75% of older children and adolescents with prolonged ART history will have lipid abnormalities.

Pooled dyslipidemia prevalence of 39.5% and an incidence of 32% (191 per 1,000 person-years) reported in a recent meta-analysis and a recent review of a large consortium of prospective observational cohorts, respectively.

Advanced-stage HIV disease

High-fat, high‑cholesterol diet

Sedentary lifestyle

Obesity

Hypertension

Smoking

Family history of dyslipidemia or premature ASCVD

Metabolic syndrome

Fat maldistribution

Prevention

Low-fat diet
Exercise
Smoking-prevention counseling
Use of ARVs is associated with a lower prevalence of dyslipidemia, such as INSTIs, and to a lesser extent, newer PIs (e.g., ATV, DRV).
When considering a TDF-based or TAF-based regimen, the lipid-lowering beneficial effect of TDF should be weighed against its potential for increased renal and bone toxicities.

Monitoring^a

Obtain fasting (or non‑fasting) lipid profile (TC, HDL-C, non-HDL-C, LDL-C, and TG) twice (>2 weeks but ≤3 months apart) and average these results. Monitor every 6 months (for abnormal results) or every 12 months (for normal results).
If TG or LDL-C is elevated or if a patient has additional risk factors, obtain FLP.

Children With Lipid Abnormalities and/or Additional Risk Factors

Obtain 12-hour FLP before initiating or changing therapy and every 6 months thereafter (more often if indicated).

Children Receiving Lipid-Lowering Therapy With Statins or Fibrates

Obtain 12-hour FLP, LFT, and CK at 4 weeks, 8 weeks, and 3 months after starting lipid therapy.
If minimal alterations in AST, ALT, and CK are indicated, monitor every 3–4 months during the first year and every 6 months thereafter (or as clinically indicated).
Repeat FLP 4 weeks after increasing doses of antihyperlipidemic agents.

Assess all patients for additional ASCVD risk factors. Patients with HIV are considered to be at moderate risk for ASCVD.^b

ARV regimen changes should be considered, especially when the patient is receiving older PIs (e.g., LPV/r) and/or RTV boosting. Switching to a PI-sparing regimen, a PI-based regimen with a more favorable lipid profile, or COBI boosting causes a decline in LDL‑C or TG values. The lipid-lowering effect of an ARV regimen switch on LDL-C is less pronounced than with statin therapy but may be enough to re-establish a healthy lipid profile.

Refer patients to a lipid specialist early if LDL-C is ≥250 mg/dL or TG is ≥500 mg/dL.

If LDL-C is ≥130 mg/dL but <250 mg or TG is ≥150 mg/dL but <500 mg/dL, the following staged treatment approach is recommended by the NHLBI guidelines^b:

Implement diet, nutrition, and lifestyle management for 6‍–‍9 months. Consult with a dietician if one is available.
If a 6- to 9-month trial of lifestyle modification fails and the patient is aged ≥10 years, consider implementing lipid-lowering therapy after consulting a lipid specialist.
Statin therapy should be considered for patients with elevated LDL-C levels. NHLBI guidelines provide recommendations for statin therapy in patients with specific LDL-C levels and risk factors.^bConcurrent substitution—preferably to ARVs with no inhibitory or inducing effect on CYP3A4 or OATP1B1 (e.g., INSTI)—also should be considered as appropriate to limit drug–drug interaction potential.
Drug therapy can be considered in cases of severe hypertriglyceridemia (TG ≥500 mg/dL). Fibrates (gemfibrozil and fenofibrate) may be used.

The long-term risks of lipid abnormalities in children who are receiving ART are unclear. However, persistent dyslipidemia in children may lead to premature ASCVD.

^a Because of the burden of collecting fasting blood samples, some practitioners routinely measure cholesterol and TG from nonfasting blood samples and follow-up abnormal values with a test done in the fasted state.

^b Refer to the NHLBI guidelines: Expert Panel on Integrated Guidelines for Cardiovascular Health and Risk Reduction in Children and Adolescents.

Key to Symbol:
↑ = increase

Key: ALT = alanine aminotransferase; ART = antiretroviral therapy; ARV = antiretroviral; ASCVD = atherosclerotic cardiovascular disease; AST = aspartate aminotransferase; ATV = atazanavir; CK = creatine kinase; COBI = cobicistat; CYP3A4 = cytochrome P450 3A4; DRV = darunavir; DRV/r = darunavir/ritonavir; EFV = efavirenz; ETR = etravirine; EVG/c = elvitegravir/cobicistat; FLP = fasting lipid profile; HDL-C = high-density lipoprotein cholesterol; INSTI = integrase strand transfer inhibitor; LDLC = low-density lipoprotein cholesterol; LFT = liver function test; LPV/r = lopinavir/ritonavir; NHLBI = National Heart, Lung, and Blood Institute; NNRTI = non-nucleoside reverse transcriptase inhibitor; NRTI = nucleoside reverse transcriptase inhibitor; NVP = nevirapine; OATP1B1 = organic anion transporter polypeptide 1B1; PI = protease inhibitor; PUFA = polyunsaturated fatty acid; RPV = rilpivirine; RTV = ritonavir; TAF = tenofovir alafenamide; TC = total cholesterol; TDF = tenofovir disoproxil fumarate; TG = triglycerides

References

Table 17b. Antiretroviral Therapy–Associated Adverse Effects and Management Recommendations—Dyslipidemia