Treating Genital Herpes Infection to Reduce Racial Disparities in the Risk of Severe Maternal Morbidity
NCT ID: NCT05429346
Last Updated: 2024-04-24
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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RECRUITING
339000 participants
OBSERVATIONAL
2023-01-08
2026-04-30
Brief Summary
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Detailed Description
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Recent studies have shown that pregnant women with genital herpes simplex virus (GHSV) infection are at higher risk of pregnancy complications, including SMM. This reported association is supported by strong biological plausibility. Once infected, the virus remains in the body permanently, shedding the virus periodically and causing inflammation in the reproductive tract. The virus is often reactivated during pregnancy due to stress, hormonal changes, and weakened immunity, exacerbating existing inflammation and leading to pregnancy complications, including SMM. At the same time, CDC reports have repeatedly shown that the rate of GHSV infection is 4 times higher in AA women than in White women. Thus, the combination of (a) an increased risk of SMM associated with GHSV infection with (b) high GHSV infection rate in AA makes GHSV a likely contributing factor to the persistently observed racial disparities in SMM. More importantly, recent studies, including a pilot study conducted by the investigators, have shown that treating women with GHSV infection using existing anti-herpes medications could lead to reduction in the risk of SMM. Given that it would benefit AA women more because of their higher GHSV infection rate, the treatment could consequently lead to reduction in racial disparities in SMM. Currently, there is a significant knowledge gap regarding the benefit of treating GHSV infection to reduce the risk of SMM and its racial disparities. Thus, pregnant women with GHSV infection, including many AA women, are not being treated during pregnancy. The current CDC guidelines for treating GHSV infection at 36 weeks of gestation are focused on reducing vertical transmission to newborns; thus, the treatment timing is too late to prevent SMM. Thus, a potentially effective treatment in reducing racial disparities in SMM is not being implemented because of the lack of evidence and the knowledge gap which urgently need to be addressed.
To investigate the comparative effectiveness of treating women with GHSV infection, in comparison to not treating or treating too late, to reduce racial disparities in SMM, the investigators will conduct a large cohort study by leveraging their experience and expertise in studying GHSV infection during pregnancy. The study will consist of pregnant women in four cohorts: (1) women with GHSV infection who received treatment early in pregnancy (before the 3rd trimester); (2) women with GHSV infection who received treatment later in pregnancy (during the 3rd trimester); (3) women with GHSV infection without treatment during pregnancy (untreated); and (4) women without GHSV infection (unexposed controls). Data on GHSV infection and its treatment, SMM diagnosis, and potential confounders are available for all included women from electronic medical records (EMRs). In addition, the study will consist of a sub-cohort of 1,200 participants, selected from each of the four cohorts, who will be interviewed to collect data on additional confounders not available from the EMR. These data will allow the investigators to assess the existence of unmeasured confounders and whether they will impact the results, if any.
The specific aims will address these questions:
Aim 1: Is treating GHSV infection in pregnancy effective in mitigating the racial disparities in SMM? Aim 2: Is treating GHSV infection early in pregnancy more effective than later in pregnancy to mitigate the racial disparities in SMM? Aim 3: Does GHSV infection, if untreated, contribute to racial disparities in the risk of SMM?
The proposed study will address not only one of PCORI research priorities (SAE) in relation to severe maternal morbidity, but also another PCORI priority: reducing racial disparities in health outcomes. The study is also rooted in, and supported by, promising preliminary results and emerging literature with biological plausibility (scientific premise). Unlikely other factors that may contribute to racial disparities that are either very difficult to modify (e.g. sociodemographic factors) or impossible to modify (e.g., genetic factors), if the findings of the pilot study are confirmed, GHSV infection is a modifiable factor that can be treated by existing anti-herpes medications. Thus, the study will fill a knowledge gap which could lead to reduction in racial disparities in SMM through changes in clinical practice of how GHSV infection is treated among pregnant women.
Conditions
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Study Design
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COHORT
PROSPECTIVE
Study Groups
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Genital herpes treated before third trimester
Pregnant women with genital herpes infection receiving treatment before the 3rd trimester.
No interventions assigned to this group
Genital herpes treated during third trimester
Pregnant women with genital herpes infection receiving treatment during the 3rd trimester.
No interventions assigned to this group
Genital herpes untreated
Pregnant women with untreated genital herpes infection.
No interventions assigned to this group
Control Group
Pregnant women (controls) with neither genital herpes infection nor treatment.
No interventions assigned to this group
Eligibility Criteria
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Inclusion Criteria
* Pregnant women
Exclusion Criteria
* Non-pregnant women
18 Years
55 Years
FEMALE
No
Sponsors
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Patient-Centered Outcomes Research Institute
OTHER
Kaiser Permanente
OTHER
Responsible Party
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Principal Investigators
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De-Kun Li, MD, PhD
Role: PRINCIPAL_INVESTIGATOR
Division of Research, Kaiser Permanente Northern California
Locations
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Division of Research, Kaiser Permanente Northern California
Oakland, California, United States
Countries
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Central Contacts
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Facility Contacts
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Other Identifiers
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1873689
Identifier Type: -
Identifier Source: org_study_id
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