Tuberculosis (TB) is a leading cause of death among HIV-infected persons in low-income settings and can be a serious complication for HIV-infected pregnant women and their infants. Isoniazid (INH) preventive therapy (IPT) is effective in preventing TB infection in HIV-infected adults, but the safety of IPT in pregnant women is unknown. This study evaluated the safety of IPT among HIV-infected pregnant women.
TB disease is the most common HIV-related opportunistic infection and is a leading cause of death among HIV-infected persons in low-income settings. When TB occurs during or soon after pregnancy, it can cause complications for the mother as well as infant TB or death. Infant TB is very difficult to diagnose, and up to half of infant TB cases are caused by maternal TB. It has been shown that treatment for active TB is safe and effective during pregnancy and that IPT is safe and effective in preventing TB infection in HIV-infected adults. However, the safety of IPT in HIV-infected pregnant women is not known, especially in regard to its combination with highly active retroviral therapy (HAART). This study evaluated the safety of immediate (antepartum, or before delivery) versus deferred (postpartum, or after delivery) IPT among HIV-infected pregnant women in high TB incidence settings. HIV-infected pregnant women were randomly assigned (1:1) to one of two arms: Arm A (immediate/antepartum INH) and Arm B (deferred/postpartum INH group). Women in both arms received oral prenatal multivitamins and pyridoxine (vitamin B6) once daily from study entry through Week 40 postpartum. Study visits for women occurred at screening, entry, every 4 weeks until labor and delivery, at labor and delivery, and every 4 weeks after delivery until 48 weeks postpartum. Visits consisted of giving a medical history and undergoing a physical exam and blood collection; all visits through the delivery visit also included an obstetrical exam. Presence of HIV infection was documented at screening and a tuberculin skin test (TST) was administered at the delivery visit and at the Week 44 postpartum visit. Study visits for infants occurred at birth and at several time points through Week 48. These visits included a medical history, physical exam, and blood collection. Intensive pharmacokinetic (PK) samples, that is, samples taken at many different time points within a 24-hour test period, were collected from a small subset of women, one test period at antepartum and one at postpartum. Sparse PK samples, that is, samples taken at fewer time points within the test period, were collected on all women, once each at antepartum and postpartum.
Study Type
INTERVENTIONAL
300-mg tablet once daily by mouth, either from entry through Week 28 antepartum (Arm A) or from Week 12 postpartum through Week 40 postpartum (Arm B)
Placebo tablet once daily by mouth, either from Week 28 visit through Week 40 postpartum (Arm A) or from entry until Week 12 postpartum visit (Arm B)
Gaborone CRS
Gaborone, Botswana
Molepolole CRS
Gaborone, Botswana
Les Centres GHESKIO Clinical Research Site (GHESKIO-INLR) CRS
Port-au-Prince, Haiti
Incidence Rate of Combined Endpoint: Grade 3 or Higher Adverse Events (AEs) Related to Treatment, or AE Causing Discontinuation of Treatment
Incidence rate, calculated by Mantel-Haenszel (MH), weighted by gestational age strata 1) gestational age at entry less than 24 weeks or 2) gestational age at entry greater than or equal to 24 weeks. AE's include laboratory results, signs/symptoms, or diagnoses; graded as per Division of AIDS (DAIDS) or by protocol-defined hepatotoxicity measures. Related to treatment indicates possibly, probably, or definitely related to INH or Placebo for INH as judged by Independent Endpoint Review Committee. Discontinuation refers to permanent discontinuation of study treatment.
Time frame: Measured from study entry through Week 48 after birth
Number of Mothers With a Fetal Death
Fetal deaths include both stillbirths and spontaneous abortions; in case of a multiple birth, mothers who had at least one fetal death
Time frame: Measured from study entry through end of pregnancy
Number of Mothers With a Fetus Small for Gestational Age
Small for gestational age was determined by physician at site
Time frame: Measured at delivery
Number of Mothers With an Infant Born Prematurely
Premature birth is defined as gestational age of \< 37 weeks at delivery.
Time frame: Measured at delivery
Number of Mothers With a Low Birth-weight Infant
Low birth weight is defined as weight \< 2500 mg
Time frame: Measured on day of birth
Number of Mothers With an Infant With a Congenital Anomaly
Includes congenital anomalies meeting the Metropolitan Atlanta Congenital Defects Program criteria.
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Allocation
RANDOMIZED
Purpose
PREVENTION
Masking
DOUBLE
Enrollment
956
Byramjee Jeejeebhoy Medical College (BJMC) CRS
Pune, Maharashtra, India
Soweto IMPAACT CRS
Johannesburg, Gauteng, South Africa
Desmond Tutu TB Centre - Stellenbosch University (DTTC-SU) CRS
Cape Town, Western Cape, South Africa
Fam-Cru Crs
Cape Town, Western Cape, South Africa
Kilimanjaro Christian Medical Centre (KCMC)
Moshi, Tanzania
Chiang Mai University HIV Treatment (CMU HIV Treatment) CRS
Chiang Mai, Thailand
MU-JHU Research Collaboration (MUJHU CARE LTD) CRS
Kampala, Uganda
...and 3 more locations
Time frame: Measured from study entry through Week 48 after birth
Number of Mothers With an Adverse Pregnancy Outcome: Spontaneous Abortion, Stillbirth, Premature Birth, Low Birth Weight, or Congenital Anomaly
In case of a multiple birth, mothers who had at least one adverse pregnancy outcome. Spontaneous abortion is intra-uterine fetal death prior to 20 weeks of gestational age; stillbirth, the same, \>= 20 weeks; preterm delivery, \< 37 weeks of gestational age; low birth weight, \< 2,500 grams, and congenital anomalies meeting the Metropolitan Atlanta Congenital Defects Program criteria.
Time frame: Measured from study entry through Week 48 after birth
Number of Infants With Grade 3 or Higher Clinical or Laboratory AE
Laboratory, sign/symptom, or diagnoses graded as 3 or higher by DAIDS criteria.
Time frame: Measured from study entry through Week 48 after birth
Number of Infants With Grade 3 or Higher Clinical or Laboratory AE Related to Treatment
As before, but AE is judged to be possibly, probably, or definitely related to INH or Placebo for INH, by clinic medical staff
Time frame: Measured from study entry through Week 48 after birth
Number of Infants Which Are HIV-infected
HIV infection determined during follow-up period. Infection at birth or during breastfeeding
Time frame: Measured from study entry through study Week 44
Number of Infants Hospitalized
Hospitalization due to reasons other than birth
Time frame: Measured from study entry through Week 48 after birth
Incidence Rate of TB Infection Among Mothers
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata. Probable or confirmed TB infection, as judged by Secondary Endpoint Review Committee
Time frame: Measured from study entry to Week 48 after birth
Incidence Rate of Tuberculosis (TB) Among Infants
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata. Probable or confirmed TB, or congenital TB as defined using the Cantwell criteria (see reference), judged by the Secondary Endpoint Review Committee. Includes an infant death due to unknown cause.
Time frame: Measured from study entry through Week 48 after birth
Incidence Rate of Infant Death
Incidence rate was calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through Week 48 after birth
Incidence Rate of Maternal Deaths
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through Week 48 postpartum
Incidence Rate of Combined Endpoints: Maternal TB or Maternal Death
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through Week 48 after birth
Incidence Rate of Combined Endpoints: Infant TB or Infant Death
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through Week 48 after birth
Incidence Rate of Combined Endpoints: Maternal TB, Maternal Death, Infant TB, or Infant Death
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through Week 48 after birth
Incidence Rate of Combined Endpoint, Antepartum: Grade 3 or Higher AE Related to Treatment, or Discontinuation of Treatment Due to AE
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata
Time frame: Measured from study entry through end of pregnancy
Incidence Rate of Combined Endpoint, up to 12 Weeks Postpartum: Grade 3 or Higher AE Related to Treatment, or Discontinuation of Treatment Due to AE
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through 12 weeks after birth
Incidence Rate, Antepartum, of Grade 3 or Higher AE
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through end of pregnancy
Incidence Rate, up to 12 Weeks Postpartum, of Grade 3 or Higher AE
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through 12 weeks postpartum
Incidence Rate, Antepartum, of Hepatotoxicity, Defined by Protocol-specific Definition of Hepatotoxicity, Related to Treatment
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata. Protocol-specific definition of hepatotoxicity: Any one of the following: 1) Alanine aminotransferase (ALT) or aspartate aminotransferase (AST) greater than 5 times the upper limit of normal (ULN), where ULN is specified by the clinic physician; 2) Total bilirubin \> 3 X ULN; 3) ALT greater than 3 X ULN and total bilirubin greater than 2 X ULN; or 4) ALT \> 3 X ULN and persistent symptomatic clinical hepatitis
Time frame: Measured from study entry through delivery
Incidence Rate, to 12 Weeks Postpartum, of Hepatotoxicity, Protocol-specific Definition, Related to Treatment
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata
Time frame: Measured from study entry through 12 weeks postpartum
Incidence Rate, Antepartum, of Hepatotoxicity, Protocol-specific Definition, Any Cause
Incidence rate calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through delivery
Incidence Rate, to 12 Weeks Postpartum, of Hepatotoxicity, Protocol-specific Definition, Any Cause
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through 12 weeks postpartum
Incidence Rate, Antepartum, of Hepatotoxicity, Defined by DAIDS, Related to Treatment
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata. Hepatotoxicity definition as defined by DAIDS AE grading criteria 1.0.
Time frame: Measured from study entry through delivery
Incidence Rate, up to 12 Weeks Postpartum, of Hepatotoxicity, Defined by DAIDS, Related to Treatment
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata
Time frame: Measured from study start through 12 weeks postpartum
Incidence Rate, Antepartum, of Hepatotoxicity, Defined by DAIDS, Any Cause
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study entry through delivery
Incidence Rate, up to 12 Weeks Postpartum, of Hepatotoxicity, Defined by DAIDS, Any Cause
Incidence rates calculated by Mantel-Haenszel, weighted by gestational age strata.
Time frame: Measured from study start through 12 weeks postpartum
Number of Mothers With Tuberculosis Resistant to INH
Resistance to INH from isolates of Mycobacterium tuberculosis, as a percentage of mothers who develop culture-confirmed TB
Time frame: Measured from study entry through Week 48 postpartum
Number of Infants With Tuberculosis Resistant to INH
Resistance to INH from isolates of Mycobacterium tuberculosis, as a percentage of infants who develop culture-confirmed TB
Time frame: Measured from study entry through Week 48 after birth
Pharmacokinetic (PK) Parameter: Adjusted Mean of Area Under the Curve of Plasma Concentration Versus Time (AUC24h), for INH
Pharmacokinetic parameter was estimated from population PK modeling fitted to the intensive PK data. AUC0-24h was predicted using population pharmacokinetic model using the NONMEM software program. A 2-compartment model with first-order absorption with transit compartment and first-order elimination with well-stirred liver model to capture hepatic clearance and first-pass extraction with 1 parameter (hepatic intrinsic clearance) was used,
Time frame: Measured at antepartum (third trimester and >= 2 weeks after starting study drug) and week 16 postpartum (+/-) 4 weeks) while on active INH; blood samples were drawn pre-dose and at 1, 2, 4, 6, 8, and 12 hours post-dosing.
Pharmacokinetic (PK) Parameter: Adjusted Mean of Area Under the Curve (AUC24h), for EFV
Pharmacokinetic parameter was estimated from population PK modeling fitted to the intensive PK data. AUC0-24h was predicted using population pharmacokinetic model using the NONMEM software program. A 2-compartment model with first-order absorption with transit compartment and first-order elimination with well-stirred liver model to capture hepatic clearance and first-pass extraction with 1 parameter (hepatic intrinsic clearance) was used,
Time frame: Measured at antepartum (third trimester and >= 2 weeks after starting study drug) and week 16 postpartum (+/-) 4 weeks) while on active INH; blood samples were drawn pre-dose and at 1, 2, 4, 6, 8, and 12 hours post-dosing.
Agreement Between Interferon-gamma Release Assay (IGRA) TB Test and Tuberculin Skin Test (TST) Results, Women at Delivery
IGRA done by Quantiferon Gold Test (QGIT). For women, TST is considered positive if greater than or equal to 5 mm
Time frame: Measured at delivery
Agreement Between IGRA and TST TB Test Results, Infant
The TST result was positive if greater than or equal to 10 mm in HIV-negative infants, or greater than or equal to 5 mm in HIV-positive infants.
Time frame: Measured at week 44 after birth
Agreement Between IGRA and TST TB Tests, Women at 44 Weeks Postpartum
IGRA done by Quantiferon Gold Test (QGIT). For women, TST is considered positive if greater than or equal to 5 mm
Time frame: Measured at Week 44 postpartum
Number of Women by Level of Adherence to Prescribed Regimen, as Assessed by Self-report
Adherence is the percentage of expected doses taken during the 28 week active treatment period, categorized as poor (\<60%), reasonable (\>= 60%, \<80%), good (\>=80%, \<90%), or excellent (\>= 90%). Measured by participant's self-report of doses taken within the last 3 days.
Time frame: Adherence reported every 4 weeks during active treatment; study entry through week 28 for Arm A, week 12 postpartum through week 40 postpartum for Arm B
Number of Women by Level of Adherence to Prescribed Regimen, as Assessed by Pill Count
Adherence is the percentage of expected doses taken during the 28 week active treatment period. Pill count: participants returned their prescription pill containers, and the remaining (unused) pills were counted.
Time frame: Adherence reported every 4 weeks during active treatment; study entry through week 28 for Arm A, week 12 postpartum through week 40 postpartum for Arm B