Disease Transmission, Vertical, Vertical Human Immunodeficiency Virus Transmission, HIV Infections
Conditions
Keywords
HIV, Perinatal, Prevention, Transmission, Nevirapine, Epivir, Zidovudine, Nelfinavir, ZDV, NVP, 3TC, NFV, Viracept, Viramune, HIV Seronegativity, Treatment Naive
Brief summary
Giving anti-HIV medications to babies born of HIV positive mothers right after birth can lower the babies' risk of contracting HIV. This study will assess the safety and efficacy of two different combinations of anti-HIV medications compared to a one drug standard regimen in preventing mother to baby transmission. The one drug standard treatment and two combinations to be studied are: 1) zidovudine, 2) zidovudine/nevirapine and 3) zidovudine/lamivudine/nelfinavir.
Detailed description
Despite the notable reductions in perinatal transmission of HIV-1 with antiretroviral therapy and other interventions, perinatal transmission continues to occur at rates of 20-30% among pregnant women who are not identified as HIV-1-infected and/or are not provided with antiretroviral therapy. The optimum treatment strategy for prevention of transmission of HIV-1 to infants born to these women is unknown. No trials have evaluated the efficacy of neonatal antiretroviral therapy alone but observational data suggest benefit from zidovudine (ZDV) therapy given to the infant beginning within 48 hours of birth and continued for six weeks. This protocol will compare the safety and efficacy of three antiretroviral regimens administered in the neonatal period: Arm A- ZDV, Arm B- ZDV plus nevirapine (NVP), and Arm C- ZDV plus nelfinavir (NFV) and lamivudine (3TC). Two regimens were selected based on expected antiretroviral activity, pharmacokinetic data, and toxicity profiles. Standard of care (6 weeks of ZDV) alone will be compared to the 6 weeks of ZDV plus either 3 doses of NVP or 2 weeks of 3TC and NFV. Arm B (ZDV + NVP) is the regimen expected to provide the best profile when factors of efficacy, safety, cost, acceptability and convenience are considered. The comparison of Arms B and C is also of considerable interest since the 2-drug Arm B is easier to implement and less expensive than the triple drug Arm C. Although triple drug therapies have been recommended for post-exposure prophylaxis for needle-stick injuries in high-risk circumstances, it is unknown whether the triple drug arm will provide better efficacy than the 2-drug arm for post-exposure prophylaxis of the infant. This open-label study is expected to accrue 1731 infants of women identified in labor as being HIV positive or who are HIV positive but have not received antiretroviral medication during the pregnancy. If eligible the infant will be randomized at birth to one of three aforementioned treatment arms. Medical history, social, demographic, physical exam, RNA and T- lymphocyte data are collected on the mother during the delivery visit. The infant will have a birth visit and then return for 1-week, 2-week, 4-week, 3-month and a final 6-month visit. Infant evaluations will include: a medical history and physical exam, DNA testing, CBC and liver function tests, cells for long-term storage and RNA/CD4/CD8 testing if HIV positive. The initial study drug doses will be given to the infant while in the hospital. Mothers will administer the infants' remaining treatment doses at home depending on ability.
Interventions
DRUGZidovudine
Given for 6 weeks. 12mg PO BID if birthweight (BW) \> 2000 grams 8 mg PO BID if BW \< 2000 grams
DRUGNevirapine (NVP)
Standard of Care (Zidovudine) plus NVP, first dose initiated within 48 hrs of birth, second dose 48 hrs (+ 4 hours) after the first dose, and third dose 96 hours (+ 4 hours) after the second dose : 12 mg PO per dose if BW \> 2000 grams, 8 mg PO per dose if BW \< 2000 grams
DRUGEpivir (3TC)
Stand of care (Zidovudine) plus 3TC, given for 2 weeks: 6 mg po bid if BW \> 2000 grams 4 mg po bid if BW \< 2000 grams AND NFV, given for 2 weeks: 200 mg po bid if BW \> 3000 grams 150 mg po bid if BW \> 2,000 - 3000 grams 100 mg PO BID if BW \< 2000 grams
DRUGNelfinavir (NFV)
200 mg BID if birth weight (BW) \> 3000 grams for 2 weeks;150 mg BID if BW \> 2000-3000 grams for 2 weeks; 100 mg BID BW \</= 2000 grams for 2 weeks
Sponsors
National Institute of Allergy and Infectious Diseases (NIAID)
Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)
Study design
Allocation
RANDOMIZED
Intervention model
PARALLEL
Primary purpose
PREVENTION
Masking
NONE
Eligibility
Sex/Gender
ALL
Age
No minimum to 2 Days
Healthy volunteers
Yes
Inclusion criteria
Infants who meet all of the following criteria are eligible for the study: * Mother known to be HIV-1-infected prior to labor or identified at the time of labor or \<48 hours postpartum. HIV-1 infection for the purposes of enrollment into this study is defined as: (a) Single positive HIV-1 rapid test in mother or her infant; or (b) Historical documentation of a positive HIV-1 diagnostic test confirmed by repeat diagnostic testing for HIV-1 according to country guidelines in mother (written documentation of test results must be present in the medical record). * Maternal written informed consent for study participation. * Mother has not received any antiretroviral therapy during the current pregnancy prior to the onset of labor and delivery; women may have received intravenous or oral ZDV during labor. Women may have received any antiretroviral therapy in previous pregnancies for prevention of vertical HIV-1 transmission. * Infant is \<48 hours old. Infant may have received up to 48 hours of ZDV as standard care before study enrollment.
Exclusion criteria
Infants who meet any of the following criteria will be excluded from the study: * Extreme prematurity (\< 32 weeks of gestation). * Birth weight \<1500 grams. * Presence of life-threatening conditions. * Inability to take oral medication throughout the first 48 hours of life (must be able to receive oral medication by age 48 hours). * Maternal inability to provide informed consent because of a lack of a conscious state, psychiatric conditions, or language barriers. * Mother received any antiretroviral therapy during labor and delivery other than intravenous or oral ZDV.
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Infant HIV Infection Status | 3 months | Intrapartum HIV infection at 3 Months |
| Participants With Serious Adverse Events | through age 6 months. | Serious Adverse Events by System Organ Class=Blood and lymphatic system disorders |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Participant Deaths | through age 6 months | — |
| 3TC and NFV Pharmacokinetics | through age 14 days | Descriptive study of 3TC and NFV pharmacokinetics during first two weeks of life using weight band dosing regimen in a subset of enrolled infants. |
| Clinical Covariates of HIV-1 Infection | through age 3 months | Compare HIV-1 RNA levels; CD4+ lymphocyte counts; and rates of genotypic and phenotypic resistance among the three treatment regimens. |
| NVP Pharmacokinetics | 14 days | Descriptive study of NVP pharmacokinetics during first two weeks of life using weight band dosing in a subset of enrolled infants. |
| Risk Factors for Perinatal HIV-1 Transmission | through age 3 months | Risk factors to be assessed include maternal HIV-1 RNA levels at delivery, maternal syphilis and other infections, obstetrical factors such as duration of membrane rupture, and adherence to neonatal medication. |
| Infant HIV-1 Infection Status | birth | In utero HIV-1 infection rate |
Countries
Argentina, Brazil, Puerto Rico, South Africa, United States
Participant flow
Recruitment details
The first subject was enrolled on 02/27/2004 and the study ended 02/28/2011. A total of 17 sites in Brazil, South Africa, Argentina and the U.S. participated in the study.
Participants by arm
| Arm | Count |
|---|---|
| Arm A (ZDV Only) Standard of care ( Zidovudine only). 12 mg PO BID if BW\>2000 grams ; 8 mg PO BID if BW\</= 2000 grams | 581 |
| ARM B (ZDV + NVP) Standard of care (Zidovudine) plus Nevirapine (NVP)
NVP, first dose initiated within 48 hrs of birth, second dose 48 hrs (+ 4 hours) after the first dose, and third dose 96 hours (+ 4 hours) after the second dose :
12 mg PO per dose if BW \> 2000 grams, 8 mg PO per dose if BW \< 2000 grams | 580 |
| ARM C (ZDV + 3TC + NFV) Standard of Care (Zidovudine) plus 2 weeks of Epivir (3TC) and Nelfinavir (NFV) 3TC, given for 2 weeks: 6 mg po bid if BW \> 2000 grams 4 mg po bid if BW \< 2000 grams AND
NFV, given for 2 weeks:
200 mg po bid if BW \> 3000 grams 150 mg po bid if BW \> 2,000 - 3000 grams 100 mg PO BID if BW \< 2000 grams | 574 |
| Total | 1,735 |
Withdrawals & dropouts
| Period | Reason | FG000 | FG001 | FG002 |
|---|---|---|---|---|
| Overall Study | Death | 11 | 15 | 17 |
| Overall Study | Lost to Follow-up | 15 | 24 | 24 |
| Overall Study | moved out of area | 9 | 7 | 4 |
| Overall Study | Withdrawal by Subject | 19 | 19 | 23 |
Baseline characteristics
| Characteristic | Arm A (ZDV Only) | ARM B (ZDV + NVP) | ARM C (ZDV + 3TC + NFV) | Total |
|---|---|---|---|---|
| Age Continuous Gestational Age in Weeks | 39 weeks STANDARD_DEVIATION 1.7 | 39 weeks STANDARD_DEVIATION 1.5 | 39 weeks STANDARD_DEVIATION 1.7 | 39 weeks STANDARD_DEVIATION 1.7 |
| Region of Enrollment Argentina | 10 participants | 6 participants | 11 participants | 27 participants |
| Region of Enrollment Brazil | 409 participants | 408 participants | 402 participants | 1219 participants |
| Region of Enrollment Puerto Rico | 0 participants | 1 participants | 1 participants | 2 participants |
| Region of Enrollment South Africa | 158 participants | 161 participants | 156 participants | 475 participants |
| Region of Enrollment United States | 4 participants | 4 participants | 4 participants | 12 participants |
| Sex: Female, Male Female | 298 Participants | 303 Participants | 281 Participants | 882 Participants |
| Sex: Female, Male Male | 283 Participants | 277 Participants | 293 Participants | 853 Participants |
Adverse events
| Event type | EG000 affected / at risk | EG001 affected / at risk | EG002 affected / at risk |
|---|---|---|---|
| deaths Total, all-cause mortality | — / — | — / — | — / — |
| other Total, other adverse events | 492 / 581 | 482 / 580 | 480 / 574 |
| serious Total, serious adverse events | 219 / 581 | 211 / 580 | 252 / 574 |
Outcome results
Primary
Infant HIV Infection Status
Intrapartum HIV infection at 3 Months
Time frame: 3 months
Population: All infants with HIV-1 test results except infants infected at birth (i.e. in utero infections) were included in these analysis.
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| ARM A (ZDV - Standard of Care) | Infant HIV Infection Status | 24 participants |
| ARM B (ZDV + NVP) | Infant HIV Infection Status | 11 participants |
| ARM C (ZDV +3TC+NFV) | Infant HIV Infection Status | 12 participants |
p-value: 0.046multiple comparison
Primary
Participants With Serious Adverse Events
Serious Adverse Events by System Organ Class=Blood and lymphatic system disorders
Time frame: through age 6 months.
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| ARM A (ZDV - Standard of Care) | Participants With Serious Adverse Events | 86 participants |
| ARM B (ZDV + NVP) | Participants With Serious Adverse Events | 59 participants |
| ARM C (ZDV +3TC+NFV) | Participants With Serious Adverse Events | 110 participants |
p-value: 0.0001Chi-squared
Secondary
3TC and NFV Pharmacokinetics
Descriptive study of 3TC and NFV pharmacokinetics during first two weeks of life using weight band dosing regimen in a subset of enrolled infants.
Time frame: through age 14 days
Population: This was a descriptive study. A total of 26 infants were analyzed with 14 at age 4-7 days and 12 at 10-14 days.Plasma samples were collected prior to first AM dose and then at 1,2,4,8 and 12 hours.
| Arm | Measure | Group | Value (MEDIAN) | Dispersion |
|---|---|---|---|---|
| ARM A (ZDV - Standard of Care) | 3TC and NFV Pharmacokinetics | (NFV-AUC-12h) 4-7 day | 20.7 ug*h/mL | Full Range 46.57 |
| ARM A (ZDV - Standard of Care) | 3TC and NFV Pharmacokinetics | (NFV-AUC-12h) 10-14 day | 25.5 ug*h/mL | Full Range 13.1 |
| ARM A (ZDV - Standard of Care) | 3TC and NFV Pharmacokinetics | (3TC-AUC-12 h) 4-7 day | 4.0 ug*h/mL | Full Range 4.5 |
| ARM A (ZDV - Standard of Care) | 3TC and NFV Pharmacokinetics | (3TC-AUC-12h) 10-14 day | 7.9 ug*h/mL | Full Range 4.12 |
Secondary
Clinical Covariates of HIV-1 Infection
Compare HIV-1 RNA levels; CD4+ lymphocyte counts; and rates of genotypic and phenotypic resistance among the three treatment regimens.
Time frame: through age 3 months
Secondary
Infant HIV-1 Infection Status
In utero HIV-1 infection rate
Time frame: birth
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| ARM A (ZDV - Standard of Care) | Infant HIV-1 Infection Status | 37 participants |
| ARM B (ZDV + NVP) | Infant HIV-1 Infection Status | 28 participants |
| ARM C (ZDV +3TC+NFV) | Infant HIV-1 Infection Status | 28 participants |
p-value: 0.2432multiple comparison
Secondary
NVP Pharmacokinetics
Descriptive study of NVP pharmacokinetics during first two weeks of life using weight band dosing in a subset of enrolled infants.
Time frame: 14 days
| Arm | Measure | Group | Value (MEDIAN) |
|---|---|---|---|
| ARM A (ZDV - Standard of Care) | NVP Pharmacokinetics | NVP conc prior to 3rd dose | 362 ng/mL |
| ARM A (ZDV - Standard of Care) | NVP Pharmacokinetics | NVP peak conc (Cmax) post 3rd dose | 2286 ng/mL |
| ARM A (ZDV - Standard of Care) | NVP Pharmacokinetics | NVP conc 3-5 day post 3rd dose | 459 ng/mL |
| ARM A (ZDV - Standard of Care) | NVP Pharmacokinetics | NVP conc 7 day post 3rd dose | 76 ng/mL |
Secondary
Participant Deaths
Time frame: through age 6 months
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| ARM A (ZDV - Standard of Care) | Participant Deaths | 11 participants |
| ARM B (ZDV + NVP) | Participant Deaths | 15 participants |
| ARM C (ZDV +3TC+NFV) | Participant Deaths | 17 participants |
p-value: 0.49Chi-squared
Secondary
Risk Factors for Perinatal HIV-1 Transmission
Risk factors to be assessed include maternal HIV-1 RNA levels at delivery, maternal syphilis and other infections, obstetrical factors such as duration of membrane rupture, and adherence to neonatal medication.
Time frame: through age 3 months
Population: All available demographic and clinical variables were tested for association with transmission rate. All variables that were significant at p ≤ 0.20 were included in the multivariable regression model. Variables that were not significant were then removed from the model. The backward elimination method was used to select the final model.
| Arm | Measure | Group | Value (NUMBER) |
|---|---|---|---|
| ARM A (ZDV - Standard of Care) | Risk Factors for Perinatal HIV-1 Transmission | Treatment Arm C (ZDV+3TC/NFV) | 12 participants |
| ARM A (ZDV - Standard of Care) | Risk Factors for Perinatal HIV-1 Transmission | Treatment Arm A (ZDV only) | 24 participants |
| ARM A (ZDV - Standard of Care) | Risk Factors for Perinatal HIV-1 Transmission | Treatment Arm B (ZDV+NFV) | 11 participants |
| ARM A (ZDV - Standard of Care) | Risk Factors for Perinatal HIV-1 Transmission | Illegal Substance Abuse during pregnancy | 7 participants |
| ARM B (ZDV + NVP) | Risk Factors for Perinatal HIV-1 Transmission | Treatment Arm B (ZDV+NFV) | 523 participants |
| ARM B (ZDV + NVP) | Risk Factors for Perinatal HIV-1 Transmission | Treatment Arm C (ZDV+3TC/NFV) | 516 participants |
| ARM B (ZDV + NVP) | Risk Factors for Perinatal HIV-1 Transmission | Illegal Substance Abuse during pregnancy | 130 participants |
| ARM B (ZDV + NVP) | Risk Factors for Perinatal HIV-1 Transmission | Treatment Arm A (ZDV only) | 505 participants |
p-value: 0.0595% CI: [0.24, 1.01]Regression, Logistic
p-value: 0.0195% CI: [0.19, 0.82]Regression, Logistic
p-value: 0.0395% CI: [1.08, 5.86]Regression, Logistic
p-value: <0.000195% CI: [1.56, 3.35]Regression, Logistic