Supplemental Table 1. Results of Major Studies on Antiretroviral Interventions to Prevent Perinatal HIV Transmission

Body
Supplemental Table 1. Results of Major Studies on Antiretroviral Interventions to Prevent Perinatal HIV Transmission
Study Name;
Location(s);
Mode of Infant Feeding 		Antiretroviral Drugs Antepartum and Intrapartum Interventions Postpartum Interventions Perinatal Transmission Rate and Efficacy
PACTG 076;
United States, France;1
Formula feeding		 ZDV vs. placebo Long (from 14 weeks)

IV IP		 Long (6 weeks); infant only Perinatal transmission at 18 months was 8.3% in ZDV arm vs. 25.5% in placebo arm (68% efficacy).
CDC Short-Course ZDV Trial;
Thailand;12
Formula feeding		 ZDV vs. placebo Short (from 36 weeks)

Oral IP		 None Perinatal transmission at 6 months was 9.4% in ZDV arm vs. 18.9% in placebo arm (50% efficacy).
DITRAME (ANRS 049a) Trial;
Ivory Coast, Burkina Faso;11,39 
Breastfeeding		 ZDV vs. placebo Short (from 36 weeks)

Oral IP		 Short (1 week); mother only Perinatal transmission at 6 months was 18.0% in ZDV arm vs. 27.5% in placebo arm (38% efficacy).

Perinatal transmission at 15 months was 21.5% in ZDV arm vs. 30.6% in placebo arm (30% efficacy).

Perinatal transmission was 22.5% in ZDV arm vs. 30.2% in placebo arm in pooled analysis at 24 months (26% efficacy).
CDC Short-Course ZDV Trial;
Ivory Coast;10,11
Breastfeeding		 ZDV vs. placebo Short (from 36 weeks)

Oral IP		 None Perinatal transmission at 3 months was 16.5% in ZDV arm vs. 26.1% in placebo arm (37% efficacy).

Perinatal transmission was 22.5% in ZDV arm vs. 30.2% in placebo arm in pooled analysis at 24 months (26% efficacy).
PETRA Trial;
South Africa, Tanzania, Uganda;5
Breastfeeding and formula feeding		 AP/IP/PP ZDV plus 3TC

vs.

IP/PP ZDV plus 3TC

vs.

IP-only ZDV plus 3TC

vs.

Placebo		 Short (from 36 weeks)

Oral IP		 Short (1 week); mother and infant Perinatal transmission at 6 weeks was 5.7% for AP/IP/PP ZDV plus 3TC, 8.9% for IP/PP ZDV plus 3TC, 14.2% for IP-only ZDV plus 3TC, and 15.3% for placebo (efficacy compared with placebo: 63%, 42%, and 0%, respectively).

Perinatal transmission at 18 months was 14.9% for AP/IP/PP ZDV plus 3TC, 18.1% for IP/PP ZDV plus 3TC, 20.0% for IP-only ZDV plus 3TC, and 22.2% for placebo (efficacy compared with placebo: 34%, 18%, and 0%, respectively).
HIVNET 012 Trial;
Uganda;4
Breastfeeding		 SD NVP vs. ZDV No AP ARV drugs

Oral IP:
  • SD NVP vs. oral ZDV
 SD NVP within 72 hours of birth; infant only

vs.

ZDV for 1 week; infant only		 Perinatal transmission at 6–8 weeks was 11.8% in NVP arm vs. 20.0% in ZDV arm (42% efficacy) and 15.7% in NVP arm vs. 25.8% in ZDV arm at 18 months (41% efficacy).
 
SAINT Trial;
South Africa;6
Breastfeeding and formula feeding		 SD NVP vs. ZDV plus 3TC No AP ARV drugs

Oral IP:
  • SD NVP vs. ZDV plus 3TC
 SD NVP within 48 hours of birth; mother and infant

vs.

ZDV plus 3TC for 1 week; mother and infant		 Perinatal transmission at 8 weeks was 12.3% in SD NVP arm vs. 9.3% in ZDV plus 3TC arm (difference not statistically significant, P = 0.11).
PHPT-1;
Thailand;13
Formula feeding		 4 ZDV regimens with different durations of AP and infant PP administration; no placebo Long (from 28 weeks) or short (from 36 weeks)

Oral IP
 
 Long (6 weeks) or short (3 days); infant only Perinatal transmission rate was 10.5% in the short-short arm. This arm was stopped at interim analysis.

Perinatal transmission at 6 months was 6.5% in long-long arm vs. 4.7% in long-short arm and 8.6% in short-long arm (no statistical difference). In utero transmission was significantly higher with short vs. long maternal therapy regimens (5.1% vs. 1.6%).
PACTG 316 Trial;
Bahamas, Belgium, Brazil, France, Germany, Italy, Spain, Sweden, Switzerland, United Kingdom, United States;21
Formula feeding		 SD NVP vs. placebo among women already receiving ZDV alone (23%) or ZDV plus other ARV drugs (77% combination therapy) Nonstudy ARV regimen

Oral IP:
  • Placebo vs. SD NVP plus IV ZDV
     
 Placebo vs. SD NVP within 72 hours of birth plus nonstudy ARV drugs (ZDV); infant only 77% of women received dual- or triple-combination ARV regimens during pregnancy.

Trial stopped early because of very low perinatal transmission in both arms: 1.4% in SD NVP arm vs. 1.6% in placebo arm (53% of perinatal transmission was in utero).
PHPT-2;
Thailand;40
Formula feeding		 ZDV alone

vs.

ZDV plus maternal and infant SD NVP

vs.

ZDV plus maternal SD NVP		 ZDV from 28 weeks

Oral IP:
  • ZDV alone, or
  • ZDV plus SD NVP
 ZDV for 1 week with or without SD NVP; infant only ZDV-alone arm was stopped because the rate of perinatal transmission was higher in this arm than in the ZDV/NVP arm (6.3% vs. 1.1%, respectively). In arms in which the mother received SD NVP, the perinatal transmission rate did not differ significantly whether the infant received SD NVP or not (2.0% vs. 2.8%, respectively).
DITRAME Plus (ANRS 1201.0) Trial;
Ivory Coast;15
Breastfeeding and formula feeding		 Open label, ZDV plus SD NVP ZDV from 36 weeks

Oral IP:
  • ZDV plus SD NVP
 SD NVP plus ZDV for 1 week; infant only Perinatal transmission at 6 weeks was 6.5% (95% CI, 3.9% to 9.1%); perinatal transmission for historical control group receiving short ZDV (98% of whom were breastfed) was 12.8%. 
DITRAME Plus (ANRS 1201.1) Trial;
Ivory Coast;15
Breastfeeding and formula feeding 		Open label, ZDV plus 3TC plus SD NVP ZDV plus 3TC from 32 weeks (stopped at 3 days PP)

Oral IP:
  • ZDV plus 3TC plus SD NVP
 SD NVP plus ZDV for 1 week; infant only Perinatal transmission at 6 weeks was 4.7% (95% CI, 2.4% to 7.0%); perinatal transmission for historical control group receiving short ZDV (98% of whom were breastfed) was 12.8%.
NVAZ Trial;
Malawi;7
Breastfeeding		 Neonatal SD NVP

vs.

SD NVP plus ZDV
 
 No AP or IP ARV drugs SD NVP with or without ZDV for 1 week; infant only Perinatal transmission at 6–8 weeks was 15.3% in SD NVP plus ZDV arm vs. 20.9% in SD NVP-only arm. 

Perinatal transmission rates at 6–8 weeks among infants without HIV at birth were 7.7% and 12.1%, respectively (36% efficacy).
Postnatal NVP plus ZDV Trial;
Malawi;8
Breastfeeding		 Neonatal SD NVP

vs.

SD NVP plus ZDV		 No AP ARV drugs

Oral IP:
  • SD NVP
 SD NVP with or without ZDV for 1 week; infant only
 
 Perinatal transmission at 6–8 weeks was 16.3% in NVP plus ZDV arm vs. 14.1% in SD NVP-only arm (difference not statistically significant). 

Perinatal transmission rates at 6–8 weeks among infants without HIV at birth were 6.5% and 16.9%, respectively.
Post-Exposure Infant Prophylaxis;
South Africa;9
Breastfeeding and formula feeding		 Neonatal SD NVP

vs.

ZDV for 6 weeks		 No AP or IP ARV drugs SD NVP vs. ZDV for 6 weeks For formula-fed infants only, perinatal transmission at 6 weeks was 14.3% in SD NVP arm vs. 14.1% in ZDV arm (not significant, P = 0.30). For breastfed infants only, perinatal transmission was 12.2% in SD NVP arm vs. 19.6% in ZDV arm (P = 0.03).
Mashi;
Botswana;41,42
Breastfeeding and formula feeding		 Initial:
  • Short-course ZDV with/without maternal and infant SD NVP and with/without breastfeeding
Revised:
  • Short-course ZDV plus infant SD NVP with/without maternal SD NVP and with/without breastfeeding; women with CD4 counts <200 cells/mmreceived combination therapy.
 First Randomization:
  • ZDV from 34 weeks
Oral IP:
  • ZDV plus either SD NVP or placebo
 Second Randomization:
  • Breastfeeding plus ZDV (infant) 6 months plus SD NVP; infant only, vs.
  • Formula feeding plus ZDV (infant) 4 weeks plus SD NVP; infant only
     
 Initial Design:
  • In formula-feeding arm, perinatal transmission at 1 month was 2.4% in maternal and infant SD NVP arm vs. 8.3% in placebo arm (P = 0.05). 
  • In breastfeeding plus infant ZDV arm, perinatal transmission at 1 month was 8.4% in SD NVP arm vs. 4.1% in placebo arm (difference not statistically significant).
     
Revised Design:
  • Perinatal transmission at 1 month was 4.3% in maternal plus infant SD NVP arm vs. 3.7% in maternal placebo plus infant SD NVP arm (no significant difference; no interaction with mode of infant feeding).
Perinatal transmission at 7 months was 9.1% in breastfeeding plus ZDV arm vs. 5.6% in formula-feeding arm; mortality at 7 months was 4.9% in breastfeeding plus ZDV arm vs. 9.3% in formula-feeding arm; HIV-free survival at 18 months was 15.6% in the breastfeeding plus ZDV arm vs. 14.2% in the formula-feeding arm.
SWEN;
Uganda, Ethiopia, India;24
Breastfeeding		 SD NVP

vs.

NVP for 6 weeks

 		 No AP ARV drugs

Oral IP:
  • SD NVP
 Infant SD NVP vs. NVP for 6 weeks Postnatal Infection in Infants Without HIV at Birth:
  • Perinatal transmission at 6 weeks was 5.3% in SD NVP arm vs. 2.5% in extended NVP arm (risk ratio 0.54, P = 0.009).
  • Perinatal transmission at 6 months was 9.0% in SD NVP arm vs. 6.9% in extended NVP arm (risk ratio 0.80, P = 0.16).
     
HIV-free survival was significantly lower in extended NVP arm at both 6 weeks and 6 months of age.
PEPI-Malawi Trial;
Malawi;23
Breastfeeding		 SD NVP plus ZDV for 1 week (control)

vs.

2 extended infant regimens (NVP or NVP/ZDV) for 14 weeks		 No AP ARV drugs

Oral IP:
  • SD NVP (if mother presents in time)
 Infant SD NVP plus ZDV for 1 week (control)

vs.

Control plus NVP for 14 weeks

vs.

Control plus NVP/ZDV for 14 weeks		 Postnatal Infection in Infants Without HIV at Birth:
  • Perinatal transmission at 6 weeks was 5.1% in control arm vs. 1.7% in extended NVP arm (67% efficacy) and 1.6% in extended NVP/ZDV arm (69% efficacy).
  • Perinatal transmission at 9 months was 10.6% in control arm vs. 5.2% in extended NVP arm (51% efficacy) and 6.4% in extended NVP/ZDV arm (40% efficacy).
No significant difference in perinatal transmission between the extended prophylaxis arms; however, more hematologic toxicity with NVP/ZDV.
MITRA;
Tanzania;26 
Breastfeeding		 Infant 3TC for 6 months (observational) ZDV/3TC from 36 weeks through labor Maternal ZDV/3TC for 1 week; infant 3TC for 6 months Perinatal transmission at 6 months was 4.9% (postnatal perinatal transmission between 6 weeks and 6 months was 1.2%).
Kisumu Breastfeeding Study;
Kenya;29
Breastfeeding		 Maternal triple-drug prophylaxis (observational) ZDV/3TC/NVP (NFV if CD4 count >250 cells/mm3) from 34 weeks through labor Maternal ZDV/3TC/NVP (NFV if CD4 count >250 cells/mm3) for 6 months, infant SD NVP Perinatal transmission at 6 months was 5.0% (postnatal perinatal transmission between 7 days and 6 months was 2.6%).
MITRA-PLUS;
Tanzania;25
Breastfeeding		 Maternal triple-drug prophylaxis (observational) ZDV/3TC/NVP (NFV if CD4 count >200 cells/mm3) from 34 weeks through labor Maternal ZDV/3TC/NVP (NFV if CD4 count >200 cells/mm3) for 6 months, infant ZDV/3TC for 1 week Perinatal transmission at 6 months was 5.0% (postnatal perinatal transmission between 6 weeks and 6 months was 0.9%), not significantly different from 6-month infant prophylaxis in MITRA.
Kesho Bora;
Multi-African;28
Breastfeeding primarily		 AP ZDV/SD NVP with no postnatal prophylaxis

vs.

Maternal triple-drug prophylaxis in women with CD4 counts 200–500 cells/mm3		 Arm 1:
  • ZDV/3TC/LPV/r
Arm 2:
  • ZDV plus SD NVP
From 28 weeks through labor
 		 Arm 1:
  • Maternal ZDV/3TC/LPV/r for 6 months, infant SD NVP plus ZDV for 1 week
Arm 2:
  • Maternal ZDV/3TC for 1 week (no further postnatal prophylaxis), infant SD NVP plus ZDV for 1 week (no further postnatal prophylaxis)
 Perinatal transmission at birth was 1.8% with maternal triple-drug prophylaxis (Arm 1) vs. 2.5% with ZDV/SD NVP (Arm 2), not significantly different. In women with CD4 counts 350–500 cells/mm3, perinatal transmission at birth was 1.7% in both arms.

Perinatal transmission at 12 months was 5.4% with maternal triple-drug prophylaxis (Arm 1) vs. 9.5% with ZDV/SD NVP (with no further postnatal prophylaxis after 1 week) (Arm 2) (P = 0.029).
 
Mma Bana;
Botswana;2
Breastfeeding		 Compared 2 maternal triple-drug prophylaxis regimens in women with CD4 counts >200 cells/mm3 Arm 1:
  • ZDV/3TC/ABC
Arm 2:
  • ZDV/3TC/LPV/r
From 26 weeks through labor

 

 Arm 1:
  • Maternal ZDV/3TC/ABC for 6 months, infant SD NVP plus ZDV for 4 weeks
Arm 2:
  • Maternal ZDV/3TC/LPV/r for 6 months, infant SD NVP plus ZDV for 4 weeks
 Perinatal transmission at 6 months overall was 1.3%: 2.1% in ZDV/3TC/ABC Arm 1 vs. 0.4% in ZDV/3TC/LPV/r Arm 2 (P = 0.53).
BAN;
Malawi;27,43
Breastfeeding		 Postpartum maternal triple-drug prophylaxis vs. infant NVP in women with CD4 counts ≥250 cells/mm3  No AP drugs

IP Regimens
Arm 1 (Control):
  • ZDV/3TC plus SD NVP
Arm 2:
  • ZDV/3TC plus SD NVP
Arm 3:
  • ZDV/3TC plus SD NVP
 Arm 1 (Control):
  • Maternal ZDV/3TC for 1 week; infant SD NVP plus ZDV/3TC for 1 week
Arm 2:
  • Control as above, then maternal ZDV/3TC/LPV/r for 6 months
Arm 3:
  • Control as above, then infant NVP for 6 months
 Postnatal Infection in Infants Without HIV at 2 Weeks:
  • Perinatal transmission at 28 weeks was 5.7% in control Arm 1, 2.9% in maternal triple-drug prophylaxis Arm 2 (P = 0.009 vs. control), and 1.7% in infant NVP Arm 3 (P < 0.001 vs. control).
  • Perinatal transmission at 48 weeks was 7.0% in control Arm 1, 4.0% in maternal triple-drug prophylaxis Arm 2 (P = 0.0273 vs. control), and 4% in infant NVP Arm 3 (P = 0.0027 vs. control).
     
No significant difference between maternal triple-drug prophylaxis (Arm 2) and infant NVP (Arm 3) (P = 0.12 at 28 weeks and P = 0.426 at 48 weeks).
HPTN 046;
South Africa, Tanzania, Uganda, Zimbabwe;38,44
Breastfeeding		 Postpartum prophylaxis to prevent breast milk transmission of HIV with 6 weeks of infant NVP vs. 6 months of infant NVP AP drugs allowed if required for maternal health All infants received daily NVP from birth through age 6 weeks.

Arm 1:
  • Daily infant NVP from 6 weeks through 6 months
Arm 2:
  • Daily infant placebo from 6 weeks through 6 months
 In infants without HIV at age 6 weeks, the 6-month infant HIV infection rate was 1.1% (0.3% to 1.8%) in the extended NVP arm vs. 2.4% (1.3% to 3.6%) in the placebo arm (P = 0.048). 

18-month postnatal infection rates were 2.2% (1.1% to 3.3%) in the extended NVP arm vs. 3.1% (1.9% to 4.4%) in the placebo arm (P = 0.28). HIV infection and mortality rates did not differ between arms at any age through 18 months.

At infant randomization at age 6 weeks, 29% of mothers in each arm were receiving a triple-drug ARV regimen for the treatment of HIV.

For mothers receiving triple-drug ARV regimens at the time of randomization, in infants without HIV at age 6 weeks, the 6-month infant HIV infection rate was 0.2% and not statistically different from the rates seen in the extended NVP arm (0.5%) and placebo arm (0%). 

For mothers with CD4 counts >350 cells/mm3 who were not receiving triple-drug ARV regimens, in infants without HIV at age 6 weeks, the 6-month infant HIV infection rate was 0.7% (0% to 1.5%) in the extended NVP arm vs. 2.8% (1.3% to 4.4%) in the placebo arm (P = 0.014).
 
NICHD-HPTN 040/PACTG 1043 Trial;
Brazil, Argentina, South Africa, United States;45
Formula feeding		 Infant prophylaxis with 6 weeks of ZDV

vs.

6 weeks of infant ZDV plus 3 doses of NVP in first week of life

vs.

6 weeks of infant ZDV plus 2 weeks 3TC/NFV		 No AP drugs

If mother presented early enough, IV ZDV during labor through delivery		 Arm 1 (Control):
  • Infant ZDV for 6 weeks
Arm 2:
  • Control as above plus NVP, with first dose within 48 hours of birth, second dose 48 hours later, and third dose 96 hours after second dose
Arm 3:
  • Control as above, plus 3TC and NFV from birth through age 2 weeks
 IP HIV transmission among infants with negative HIV test at birth: 4.8% (3.2% to 7.1%) with ZDV (Arm 1) vs. 2.2% (1.2% to 3.9%) with ZDV plus NVP (Arm 2) (P = 0.046 compared with Arm 1) vs. 2.4% (1.4% to 4.3%) with ZDV plus 3TC/NFV (Arm 3) (P = 0.046 compared with Arm 1).

Overall HIV transmission rates, including in utero infection: 11.0% (8.7% to 14.0%) with ZDV (Arm 1) vs. 7.1% (5.2% to 9.6%) with ZDV plus NVP (Arm 2) (P = 0.035 compared with Arm 1) vs. 7.4% (5.4% to 9.9%) with ZDV plus 3TC/NFV (Arm 3) (P = 0.035 compared with Arm 1).

Grade 3 or 4 neutropenia more frequent in ZDV/3TC/NFV Arm 3 (70 infants) than in ZDV-alone Arm 1 (33 infants) or ZDV/NVP Arm 2 (32 infants) (P < 0.001).
ANRS 12174 Trial;
Burkina Faso, South Africa, Uganda, Zambia;30,31
Breastfeeding		 Compared 2 infant ARV prophylaxis regimens during breastfeeding; infants tested PCR-negative at birth and were born to mothers with CD4 counts >350 cells/mm As per standard of care Arm 1:
  • Daily infant LPV/r from 1 week through 50 weeks of age
Arm 2:
  • Daily infant 3TC from 1 week through 50 weeks of age
 Postnatal Infection in Infants Without HIV at Birth:
  • Postnatal transmission at age 50 weeks was 1.4% (0.70–2.76) in Arm 1 vs.1.5% (0.80–2.91) in Arm 2 (P = 0.83).
  • HIV-free survival was 96.5% (84.6–97.7) in Arm 1 vs. 96.3% (94.4–97.5) in Arm 2 (P = 0.85). 
     
PROMOTE;
Uganda;46
Breastfeeding		 Compared 2 triple-ARV regimens; no CD4 restriction Arm 1:
  • ZDV/3TC/LPV/r
Arm 2:
  • ZDV/3TC/EFV 
  • ARVs started at 12–28 weeks’ gestation and continued through labor
     
 Randomized regimen continued postpartum through 1 year of breastfeeding HIV-free survival was 92.9% in the LPV/r arm vs. 97.2% in the EFV arm (P = 0.10). Only 2 of 374 liveborn infants acquired infection, both in the LPV/r arm.
 
 
PROMISE;
India, Malawi, South Africa, Tanzania, Uganda, Zambia, Zimbabwe;18
Breastfeeding and formula feeding (antepartum component)		 Compared ZDV prophylaxis and 2 ART regimens during pregnancy among women at >14 weeks' gestation and with CD4 counts ≥350 cells/mm3  Arm 1:
  • ZDV during pregnancy plus SD NVP plus TDF plus FTC at delivery
Arm 2:
  • ZDV plus 3TC plus LPV/r
Arm 3:
  • TDF plus FTC plus LPV/r
 Arm 1:
  • TDF/FTC tail continued for 6–14 days postpartum
Arms 2 and 3:
  • ART regimen continued for 6–14 days postpartum
Infants received once-daily NVP for 6 weeks.		 Infant HIV Infection Rates by Age 14 Days
Arm 1:
  • 1.8% (25/1,386)
Arm 2:
  • 0.5% (7/1,385)
Arm 3:
  • 0.6% (2/325)
Combined ART arms vs. ZDV arm difference in perinatal transmission risk:
-1.3% (95% CI, -2.1% to -0.4%)
PROMISE;
India, Malawi, South Africa, Tanzania, Uganda, Zambia, Zimbabwe;18
Breastfeeding (postpartum component)		 Compared infant NVP and maternal ART during breastfeeding among infants born to women with CD4 counts ≥350 cells/mm3 This was a postpartum study. intervention only. Eligible women included women enrolled in PROMISE antepartum (see above) and women who received no ARV drugs during pregnancy. Arm 1:
  • Mothers received TDF plus FTC plus LPV/r
Arm 2:
  • Once-daily infant NVP
Regimens were continued until 42 days after last breastmilk exposure or age 18 months, whichever came first.		 Infant Infection Rates
Arm 1:
  • 0.57% (7/1,219)
Arm 2:
  • 0.58% (7/1,211)
Rates of Infant HIV-1–Free Survival at 24 Months
Arm 1:
  • 97.1%
Arm 2:
  • 97.7%
Key to Acronyms: 3TC = lamivudine; ABC = abacavir; AP = antepartum; ARV = antiretroviral; ART = antiretroviral therapy; CD4 = CD4 T lymphocyte; CDC = Centers for Disease Control and Prevention; CI = confidence interval; EFV = efavirenz; FTC = emtricitabine; IP = intrapartum; IV = intravenous; LPV/r = lopinavir/ritonavir; NFV = nelfinavir; NVP = nevirapine; PCR = polymerase chain reaction; PP = postpartum; SD = single-dose; TDF = tenofovir disoproxil fumarate; ZDV = zidovudine