HIV Clinical Trial
Official title:
A Double-Blind, Randomized, Controlled Trial to Evaluate the Safety, Immunogenicity, and Efficacy of Standard Dose Quadrivalent Inactivated Influenza Vaccine, and Double Dose Quadrivalent Inactivated Influenza Vaccine in HIV-Infected and HIV-Uninfected Pregnant Women in a Malaria-Endemic Area of Rural Western Kenya
In 2012, the WHO Strategic Advisory Group of Experts (SAGE) concluded that pregnant women are the most important risk group for season influenza vaccination based upon "compelling evidence of substantial risk of severe disease in this group and evidence that seasonal influenza vaccine is safe and effective in preventing disease in pregnant women as well as their young infants, in whom disease burden is also high". Recent data from Kenya, similarly suggest rates of influenza-associated hospitalizations in children under age 1 to be as high, or higher, than those observed in the United States. However, TIV may have reduced immunogenicity in HIV-infected adults, and HIV infection has been shown to reduce placental transfer of both tetanus and measles antibodies. Therefore, we propose to conduct a double-blind randomized controlled trial of influenza vaccines stratified by HIV status in up to 720 pregnant women in their second and third trimesters and their infants residing in health and demographic surveillance sites (HDSS) in Nyanza Province, Western Kenya. We propose to assess the safety, immunogenicity, and efficacy of standard dose QIV and double dose QIV in HIV-infected and HIV-uninfected pregnant women. Findings will inform maternal influenza vaccination policies in Kenya and other African countries.
Recent investments in influenza surveillance in many African countries confirm results from
other countries that young children, pregnant women, and those with chronic medical
conditions are at increased risk of hospitalization and death from influenza infection.
Annual influenza vaccination is the most effective method for preventing influenza virus
infection and its complications. Vaccination is currently recommended in high risk groups in
many developed countries and the WHO Strategic Advisory Group of Experts (SAGE) on
Immunization made a recommendation for vaccination of pregnant women in their 2005 position
paper on influenza vaccine. In 2012, the SAGE further concluded that pregnant women are the
most important risk group for inactivated seasonal influenza vaccination based upon
"compelling evidence of substantial risk of severe disease in this group and evidence that
seasonal influenza vaccine is safe and effective in preventing disease in pregnant women as
well as their young infants, in whom disease burden is also high".
Maternal influenza immunization is viewed as the most effective way to protect infants less
than 6 months of age who are not yet eligible for immunization. In the United States,
children under 6 months experience very high rates of influenza-associated hospitalization
and are among those most at risk of severe outcomes. Recent data from Kenya, similarly
suggest rates of influenza-associated hospitalizations in children under age 1 to be as
high, or higher, than those observed in the United States. Vaccination of pregnant women
provides protection to their infants against laboratory-confirmed influenza illness in the
first months of life. Furthermore, vaccination of pregnant women has been associated with a
decreased risk of pre-term birth and small for gestational age in Canada and the state of
Georgia in the US, and increased birth weight in infants during periods of high transmission
in Bangladesh. However, traditional TIV may have reduced immunogenicity in HIV-infected
adults, and HIV infection has been shown to reduce placental transfer of both tetanus and
measles antibodies. The high prevalence of other diseases, including malaria and
malnutrition, may also impact the effectiveness of influenza vaccination for pregnant women
and their infants in sub-Saharan Africa.
Use of double dose QIV may produce a greater immune response in pregnant women and increased
antibody production may improve transplacental transfer of influenza antibodies to the
developing fetus, conferring a better or possibly longer duration of protection from
influenza infection. Therefore, we propose to conduct a randomized controlled trial of
influenza vaccines in a high HIV-prevalence, malaria-endemic setting in Kenya, using
inactivated polio vaccine (IPV) as a comparator/control. We propose to assess the safety,
immunogenicity, and efficacy of standard dose (15 µg) QIV (FLUARIX® (GlaxoSmithKline
Biologicals, Dresden, Germany) and double dose (30 µg) QIV in HIV-infected and
HIV-uninfected pregnant women.
OBJECTIVES:
1. To evaluate the immunogenicity of standard dose (15 µg) QIV and double dose (30 µg) QIV
in HIV-infected and uninfected pregnant women
2. To evaluate the level of vaccine-induced influenza antibody transfer to infants of
HIV-infected and uninfected pregnant women who receive standard dose (15 µg) QIV or
double dose (30 µg) QIV
3. To evaluate the safety of standard dose (15 µg) QIV and double dose (30 µg) QIV in
HIV-infected and HIV-uninfected pregnant women and fetus
DESIGN:
This trial will be conducted as a double-blind, randomized, controlled trial stratified by
HIV status in up to 720 pregnant women in their second and third trimesters and their
infants residing in health and demographic surveillance sites (HDSS) around Siaya District
Hospital and Lwak Mission Hospital in Nyanza Province, Western Kenya. The study will be
conducted in accordance with International Conference on Harmonization Good Clinical
Practice (GCP) standards. Mothers must agree to be counseled and tested for HIV at the time
of screening and enrollment unless there is written documentation of HIV infection or a
negative HIV test in the last 3 months. After initial screening for eligibility and informed
consent, enrolled women will be stratified by HIV status (infected, uninfected) and block
randomized in a 1:1:1:1 ratio to receive standard dose (15 µg) QIV, double dose (30 µg) QIV
or IPV. The day of vaccination will be considered study Day 0 for each subject. Each subject
will receive a single vaccination. For the first 240 enrolled women, study personnel will
visit their homes on Days 1, 2, and 3 to do active surveillance for adverse events following
vaccination. Pregnancy outcomes will be recorded for all subjects (live birth, still birth,
or spontaneous abortion). HIV testing will be repeated at birth for all women with negative
results at screening. Live and still born infants will be examined by trained study
personnel in the first 24 hours after delivery to determine birth weight, length, assess
gestational age, and identify possible congenital anomalies associated with vaccination.
All enrolled subjects will be asked to return to the antenatal study clinic on Study Day 7,
Day 28, Day 56 (if not delivered), for delivery, and for any febrile or respiratory illness
or other concern. During the enrollment process, their mobile telephone number will be
recorded (or a number will be recorded for someone they identify in the village with a
mobile telephone who will be willing to transmit information to them). Participants will be
contacted by phone or in person every 2 weeks to determine if they have had fever and/or
cough during the prior 2 weeks. Subjects with fever only will receive a malaria smear and
other treatment as appropriate per Kenya Ministry of Health (MOH) guidelines. Subjects with
fever or cough will have respiratory specimens collected via placement of NP/OP swabs by
trained clinical personnel for influenza testing. After delivery, subjects will be asked to
bring infants to the study clinic for evaluation on Days 7, 42, and 70 of life and when the
child is approximately 6 months of age. Infants will also be under surveillance for fever,
history of fever, hypothermia and/or cough for the first 6 months of life. All febrile,
hypothermic, and/or coughing infants will receive testing for malaria and nasopharyngeal
(NP)and oropharyngeal (OP) swabs for influenza. Febrile infants under 2 months of age will
receive additional testing and treatment per national guidelines. Any infant admitted to the
hospital with any respiratory symptom, hypothermia, apnea or fever will receive testing for
influenza by real-time reverse transcriptase-polymerase chain reaction (rRT-PCR) of NP/OP
specimens.
Vaccine immunogenicity will be evaluated by comparing hemagglutination inhibition (HI)
titers on Day 0 and Day 28 and at delivery in the mother, in cord blood, in the mother and
infant at infant Day 70 of life, and in the infant at approximately 6 months of age. We will
determine the proportion of vaccinated women who achieve a fourfold rise in HI titers
post-vaccination compared to pre-vaccination or an HI titer ≥40 for subjects with baseline
HI titer <10, compared to the same outcome in controls. The proportion of HI titers ≥40 in
cord blood and in infants will also be measured and compared among vaccine recipients and
controls. Geometric means of HI titers will also be compared.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Prevention
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