A REVIEW OF GROUP B STREPTOCOCCUS (GBS) VAGINAL COLONIZATION AND ASCENDING INTRAUTERINE INFECTION: INTERACTION BETWEEN HOST IMMUNE RESPONSES AND GBS VIRULENCE FACTORS

Hanan H. Wahid, Puteri F. D. Mustapha Rounal, Ayesha Bahez, M. I. A. Mustafa Mahmud, N. Kamarudin, Arvind R. Selvakumaran, A. M. Ahmad Mustafa, Hamizah Ismail
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Abstract

Vaginal colonization with Group B streptococcus (GBS) or Streptococcus agalactiae can potentially cause ascending intrauterine infection among pregnant women, and hence it is known as one of the risk factors for preterm delivery. Ascending intrauterine infection may also cause the transmission of GBS to the fetus in utero and the newborn during delivery, leading to the development of early onset of neonatal infection. GBS are β-hemolytic, gram-positive bacteria that are opportunistic commensal of the gastrointestinal and urogenital tract of approximately 18% of pregnant women globally. Intrapartum antibiotic prophylaxis (IAP) only reduces the rate of early onset neonatal infection, but not the late onset neonatal infection. Thus, the development of GBS vaccine is thought to be important to decrease the rate of preterm delivery and neonatal infections particularly in low-and-middle income countries where IAP program is not feasible. Vaccination can also be cost-effective for the healthcare system when executed together with IAP program. The aim of the current review is to summarize the mechanisms on how the GBS virulence factors interact with host immune components in the gestational tissues, leading to cervicovaginal colonization and ascending intrauterine infection. The elucidation of these mechanisms is essential for expediting the development of vaccines and novel therapeutic measures targeting these GBS virulence factors that will hamper the vaginal colonization, ascending intrauterine infection and conceptus tissue invasion by GBS. These strategies are crucial to potentially reduce the rate of preterm delivery and subsequent serious complications in the newborn.
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b族链球菌阴道定植与宫内感染的进展:宿主免疫反应与gbs毒力因子的相互作用
阴道定植B族链球菌(GBS)或无乳链球菌可能导致孕妇宫内感染上升,因此被认为是早产的危险因素之一。上升宫内感染也可能导致GBS在宫内胎儿和分娩过程中传播给新生儿,导致新生儿感染的早发性发展。GBS是一种β-溶血性革兰氏阳性细菌,是全球约18%孕妇胃肠道和泌尿生殖道的机会共生菌。产时抗生素预防(IAP)只能降低早发型新生儿感染率,但不能降低晚发型新生儿感染率。因此,开发GBS疫苗被认为对降低早产率和新生儿感染率非常重要,特别是在IAP计划不可行的中低收入国家。如果与IAP计划一起实施,疫苗接种对卫生保健系统也具有成本效益。本文的目的是总结GBS毒力因子如何与妊娠组织中的宿主免疫成分相互作用,导致宫颈阴道定植和升高宫内感染的机制。阐明这些机制对于加快针对这些GBS毒力因子的疫苗和新治疗措施的开发至关重要,这些毒力因子将阻碍GBS阴道定植,增加宫内感染和子宫组织入侵。这些策略对于潜在地降低新生儿早产率和随后的严重并发症至关重要。
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