Tuberculosis Preventive Treatment for Pregnant People With Human Immunodeficiency Virus in South Africa: A Modeling Analysis of Clinical Benefits and Risks.

IF 8.2 1区 医学 Q1 IMMUNOLOGY Clinical Infectious Diseases Pub Date : 2024-11-15 DOI:10.1093/cid/ciae508
Linzy V Rosen, Acadia M Thielking, Caitlin M Dugdale, Grace Montepiedra, Emma Kalk, Soyeon Kim, Sylvia M LaCourse, Jyoti S Mathad, Kenneth A Freedberg, C Robert Horsburgh, A David Paltiel, Robin Wood, Andrea L Ciaranello, Krishna P Reddy
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Abstract

Background: Although prior studies of tuberculosis-preventive treatment (TPT) for pregnant people with human immunodeficiency virus (PPWH) report conflicting adverse pregnancy outcome (APO) risks, international guidelines recommend TPT for PPWH.

Methods: We used a microsimulation model to evaluate 5 TPT strategies among PPWH receiving antiretroviral therapy in South Africa: No TPT; 6 months of isoniazid (6H) or 3 months of isoniazid-rifapentine (3HP) during pregnancy (Immediate 6H or Immediate 3HP) or post partum (Deferred 6H or Deferred 3HP). The primary outcomes were maternal, fetal/infant, and combined deaths from causes potentially influenced by TPT (maternal tuberculosis, maternal hepatotoxicity, stillbirth, low birth weight [LBW], and infant tuberculosis). Tuberculosis during pregnancy confers 250% and 81% higher modeled risks of stillbirth and LBW, respectively. In lower-risk or higher-risk scenarios, immediate TPT confers 38% lower or 92% higher risks of stillbirth and 16% lower or 35% higher risks of LBW.

Results: Immediate TPT would minimize deaths among PPWH. When TPT confers higher stillbirth and LBW risks, immediate TPT would produce the most combined maternal and fetal/infant deaths, even with low maternal CD4 cell count and high tuberculosis incidence. If immediate TPT yields a <4% or <20% increase in stillbirth or LBW, immediate TPT would produce fewer combined deaths than deferred TPT (sensitivity analysis range, <2%-22% and <11%-120%, respectively).

Conclusions: If APO risks are below identifiable thresholds, TPT during pregnancy could decrease combined maternal and fetal/infant deaths. Given uncertainty around isoniazid's risks, and the low threshold at which APO risks could outweigh benefits from tuberculosis deaths averted, studies of newer TPT regimens among PPWH are warranted to inform guidelines.

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南非人类免疫缺陷病毒孕妇的结核病预防治疗:临床效益和风险的模型分析。
背景:尽管之前对人类免疫缺陷病毒感染者(PPWH)孕妇进行的结核病预防治疗(TPT)研究报告了相互矛盾的不良妊娠结局(APO)风险,但国际指南仍建议对PPWH进行TPT治疗:我们使用微观模拟模型对南非接受抗逆转录病毒治疗的 PPWH 的 5 种 TPT 策略进行了评估:方法:我们使用微观模拟模型对南非接受抗逆转录病毒治疗的 PPWH 的 5 种 TPT 策略进行了评估:无 TPT;孕期 6 个月异烟肼 (6H) 或 3 个月异烟肼-利福喷丁 (3HP)(立即 6H 或立即 3HP)或产后(推迟 6H 或推迟 3HP)。主要结果是产妇、胎儿/婴儿以及可能受 TPT 影响的原因(产妇结核病、产妇肝中毒、死胎、出生体重不足 [LBW] 和婴儿结核病)导致的合并死亡。孕期结核病导致死产和出生体重不足的模型风险分别高出 250% 和 81%。在风险较低或风险较高的情况下,立即进行 TPT 可使死胎风险降低 38%或提高 92%,使婴儿出生体重不足风险降低 16%或提高 35%:结果:立即 TPT 将最大限度地减少 PPWH 的死亡。当 TPT 带来更高的死产和低出生体重儿风险时,即使产妇的 CD4 细胞计数较低且结核病发病率较高,立即 TPT 也会造成最多的产妇和胎儿/婴儿合并死亡。如果立即 TPT 产生结论:如果 APO 风险低于可识别的阈值,孕期 TPT 可减少孕产妇和胎儿/婴儿的合并死亡。鉴于异烟肼风险的不确定性,以及APO风险可能超过避免结核病死亡所带来的益处的低阈值,有必要在 PPWH 中对较新的 TPT 方案进行研究,以便为指南提供参考。
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来源期刊
Clinical Infectious Diseases
Clinical Infectious Diseases 医学-传染病学
CiteScore
25.00
自引率
2.50%
发文量
900
审稿时长
3 months
期刊介绍: Clinical Infectious Diseases (CID) is dedicated to publishing original research, reviews, guidelines, and perspectives with the potential to reshape clinical practice, providing clinicians with valuable insights for patient care. CID comprehensively addresses the clinical presentation, diagnosis, treatment, and prevention of a wide spectrum of infectious diseases. The journal places a high priority on the assessment of current and innovative treatments, microbiology, immunology, and policies, ensuring relevance to patient care in its commitment to advancing the field of infectious diseases.
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