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NCT05705427 Clinical Trial

The COMBAT HBV Feasibility Trial

Hepatitis B Clinical Trial

COMBAT-HBV

Official title:
Simplifying Hepatitis B Care in Pregnancy by Combining Birth-dose Vaccine and Tenofovir: The COMBAT HBV Feasibility Trial

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT05705427
Other study ID # 22-1492
Secondary ID
Status Recruiting
Phase Phase 4
First received
Last updated
Start date August 17, 2023
Est. completion date June 2025

Study information
Verified date October 2023
Source University of North Carolina, Chapel Hill
Contact Peyton J Thompson, MD, MSCR
Phone 919-445-0854
Email peyton_thompson@med.unc.edu
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a double-blind, randomized placebo-controlled trial (RCT) of a prophylaxis-for-all approach to prevention of mother-to-child transmission (PMTCT) of hepatitis B virus (HBV) in the Democratic Republic of Congo (DRC). HBV-infected pregnant women will be randomized to either receive tenofovir or placebo beginning at 28-32 weeks' gestation and continuing through 4 weeks' postpartum. Women will be followed every 4-6 weeks throughout the prenatal and postpartum period to evaluate for side effects related to the medication. Infants will receive a birth-dose of HBV vaccine, ideally within 24 hours. Participants will be followed longitudinally through 6 months' postpartum.

Description:

The overall study design is a randomized, double-blind, placebo-controlled trial among two groups of mother-infant dyads: women who receive TDF vs placebo in late pregnancy and the postpartum period (beginning at 28-32 weeks' gestation and continuing through 4 weeks' postpartum). While official World Health Organization (WHO) recommendations are to continue TDF at least through delivery, a range from delivery through 12 weeks' postpartum is possible; the investigators will continue therapy through 4 weeks' postpartum in this study. This feasibility trial will evaluate the acceptability, safety and preliminary effectiveness of a TDF-for-all approach to prevent MTCT of HBV in low-resource settings. HBsAg-positive pregnant women will be enrolled at 28-32 weeks' gestation, and will present for regular medication checks, with a study closeout visit at 24 weeks' postpartum. Study activities at monthly medication checks will include medication refills, assessment of adherence (via pill counts and verbal surveys), and evaluation for side effects. All infants will receive a birth-dose of HBV vaccine within 24 hours of life. MTCT of HBV will be defined as the proportion of infants with positive HBsAg testing at 6 months. This pilot study will provide preliminary data for sample size calculations, including safety and effectiveness data, to prepare for larger RCTs to determine the effectiveness of a tenofovir-for-all approach, as well as the added benefit of tenofovir over birth-dose vaccination.

Recruitment information / eligibility
Status Recruiting
Enrollment 560
Est. completion date June 2025
Est. primary completion date June 2025
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: - Pregnant women =18 years of age who present for routine prenatal care between 28-32 weeks' gestation and who test HBV-positive by point-of-care hepatitis B surface antigen test. Women must intend to seek maternity and postpartum care exclusively at one of the Kinshasa-based study maternity centers. - Infants born to enrolled women will be included in the study Exclusion Criteria: - Individuals with abnormal creatinine by point-of-care testing - Any woman who plans to move outside of Kinshasa Province during the study period. - Any HIV-positive individual, determined by routine point-of-care screening at antenatal care visits

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
Tenofovir Disoproxil Fumarate 300 MG
Pregnant women in the experimental arm will receive TDF daily beginning in the 3rd trimester of pregnancy and continuing through 1 month postpartum.
Biological:
Hepatitis B monovalent vaccine
All infants born to women in the study will receive a birth-dose hepatitis B vaccine.
Drug:
Placebo
Pregnant women in the placebo arm will receive a placebo pill daily beginning in the 3rd trimester of pregnancy and continuing through 1 month postpartum.

Locations
Country Name City State
Congo, The Democratic Republic of the Université Protestant au Congo Kinshasa

Sponsors (5)
Lead Sponsor Collaborator
University of North Carolina, Chapel Hill Abbott, Albert Einstein College of Medicine, Doris Duke Charitable Foundation, Université Protestant au Congo

Country where clinical trial is conducted

Congo, The Democratic Republic of the, 

Outcome
Type Measure Description Time frame Safety issue
Primary Safety (Pregnant Women): Number of Pregnant Women With Adverse Effects Related to Study Medications Safety of TDF prophylaxis in pregnant women, defined as a composite of adverse events (# mild adverse events [AEs], # moderate-to-severe AEs), presence of side effects and alanine aminotransferase elevations = 5x upper limit of normal Up to study close-out visit, or up to 12 months
Primary Safety (Infants): Number of Infants with Adverse Effects Related to Study Medications Safety of maternal TDF for infants, defined as a composite of: Birth weight (grams), mid-upper arm circumference (centimeters), gestational age at delivery (weeks and days), delivery mode (vaginal vs C-section), APGAR scores (0-10), # of adverse events At delivery
Primary Feasibility (Recruitment): Number of Eligible Participants Who Were Enrolled in the Study Recruitment is indicative of the number of pregnant women who are screened versus those actually enrolled in the study. Up to study close-out visit, or up to 12 months
Primary Feasibility (Refusal): Number of Eligible Participants Who Refused to Enroll in the Study Refusal will be defined as the number of individuals who refuse enrollment upon initial recruitment. Up to study close-out visit, or up to 12 months
Primary Feasibility (Withdrawal): Number of Enrolled Participants Who Withdraw from the Study Withdrawal is indicative of the number of enrolled participants who choose not to continue study activities after having been enrolled. Up to study close-out visit, or up to 12 months
Primary Feasibility (Retention): Number of Enrolled Participants Who Remain in the Study Through 6 Months Postpartum Retention is defined as the number of participants who remain in the study through the 6-month postpartum visit. Up to study close-out visit, or up to 12 months
Primary Feasibility (Maintenance): Proportion of Study Visits Completed Per Participant Adherence to study visits and procedures, defined as proportion of the actual number of visits attended divided by the expected study visits (8) and multiplied by 100. Up to study close-out visit (12 months)
Primary Acceptability (Lab Testing): Number of Mothers With Lab Testing Acceptability Scores >80% Number of mothers who report the process of undergoing lab draws as "acceptable" in the exit survey. Range 0-100%, with 0% being unacceptable and 100% being acceptable. Upon study close-out visit, or up to 12 months
Primary Acceptability (Medication): Number of Mothers With Medication Acceptability Scores >80% Number of mothers who report the process of taking the study medication as "acceptable" in the exit survey. Range 0-100%, with 0% being unacceptable and 100% being acceptable. Upon study close-out visit, or up to 12 months
Primary Preliminary Effectiveness: Number of Infants With HBV Positivity by Rapid Diagnostic Testing at 6 Months of Life to Indicate Mother-to-Child Transmission of HBV Mother-to-child transmission of HBV is defined as HBsAg positivity in the infant at 6 months of life. Measured at 6 months after birth
Secondary Sensitivity of the Hepatitis B Core-Related Antigen Test Sensitivity will be defined as the number of true positive tests divided by the sum of the true positives and false negatives. Measured at Enrollment
Secondary Specificity of the Hepatitis B Core-Related Antigen Test Specificity will be defined as the number of true negative tests divided by the sum of the true negatives and the false positives. Measured at Enrollment
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