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Perinatal Antibiotic Exposure Affects the Transmission between Maternal and Neonatal Microbiota and Is Associated with Early-Onset Sepsis

机译:围产期抗生素暴露会影响母体和新生儿微生物群系之间的传播,与早期发病败血症相关联

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Intrapartum antibiotic prophylaxis reduces the risk of infection to a mother and neonate, but antibiotic-mediated maternal and neonatal microbiota dysbiosis increases other health risks to newborn infants. We studied the impact of perinatal antibiotic prophylaxis on the microbiota in mothers and newborns with full-term or preterm delivery. Ninety-eight pregnant women and their neonates were divided into the following four groups: full term without antibiotic exposure (FT), full term with antibiotic exposure (FTA), preterm without antibiotic exposure (PT), and preterm with antibiotic exposure (PTA). Bacterial composition was analyzed by sequencing the 16S rRNA gene from maternal vaginal swabs (V) and neonatal meconium (F). The results showed that in maternal vaginal and neonatal meconium microbiota, FT and PT groups had a higher load of Lactobacillus spp. than did the FTA and PTA groups. In addition, whether in the mother or newborn, the dissimilarity in microbiota between FT and PT was the lowest compared to that between other groups. Compared to the FT and PT groups, the dissimilarity in microbial structures between the vagina and meconium decreased in the FTA and PTA groups. The health outcome of infants reveals an association between early-onset sepsis and antibiotic-mediated microbiota dysbiosis. In conclusion, perinatal antibiotic exposure is related to the establishment of gut microbiota and health risks in newborns. Promoting the rational usage of antibiotics with pregnant women will improve neonatal health. IMPORTANCE Perinatal antibiotic prophylaxis is an effective method for preventing group B Streptococcus (GBS) infection in newborns. Antibiotic exposure unbalances women’s vaginal microbiota, which is associated with the establishment of the newborn gut microbiota. However, the influence of perinatal antibiotic exposure on neonatal gut microbiota colonization and health outcomes remains unclear. In this study, we found that perinatal antibiotic exposure induced microbiota dysbiosis in a woman’s vagina and the neonatal gut, and we highlight a significant decrease in the abundance of Lactobacillus spp. The influence of antibiotic use on the microbiota was greater than that from gestational age. Additionally, full-term newborns without antibiotic exposure had no evidence of early-onset sepsis, whereas in full-term or preterm newborns with antibiotic exposure before birth, at least one infant was diagnosed with early-onset sepsis. These results suggest an association between perinatal antibiotic exposure and microbial dysbiosis in maternal vaginal and neonatal gut environments, which may be related to the occurrence of early-onset sepsis.
机译:抗生素抗生素预防性降低了对母亲和新生儿感染的风险,但抗生素介导的孕产妇和新生儿微生物症失育症会增加新生儿的其他健康风险。我们研究了围产期抗生素预防对母亲和新生儿的微生物生物的影响,全术语或早产。九十八名孕妇及其新生儿分为以下四组:无抗生素暴露(FT)的全术语,抗生素暴露(FTA),早产,没有抗生素暴露(PT),和抗生素暴露的早产(PTA) 。通过测序来自母体阴道拭子(V)和新生儿型(F)的16S rRNA基因分析细菌组合物。结果表明,在孕产妇阴道和新生儿型微生物群中,FT和PT基团具有更高的乳杆菌SPP。而不是FTA和PTA组。此外,无论是在母亲还是新生儿中,与其他组之间的FT和PT之间的微生物群之间的异化性最低。与FT和Pt组相比,在FTA和PTA基团中,阴道和胎膜之间的微生物结构中的微生物结构的异化性。婴儿的健康结果显示出早期发病败血症和抗生素介导的微生物菌症之间的关联。总之,围产期抗生素暴露与在新生儿中建立肠道微生物肿瘤和健康风险有关。促进孕妇抗生素的理性使用将改善新生儿健康。围产期抗生素预防性是预防新生儿B组链球菌(GBS)感染的有效方法。抗生素暴露不平衡女性的阴道微生物群,与建立新生肠道微生物群。然而,围产期抗生素暴露对新生儿肠道微生物群殖民化和健康结果的影响仍不清楚。在这项研究中,我们发现围产期抗生素暴露诱导女性阴道和新生儿肠道中的微生物菌脱敏,并且我们突出了乳酸杆菌的丰度显着降低。抗生素对微生物酵母的影响大于孕龄的影响。此外,没有抗生素暴露的全术语新生儿没有证据表明早发败血症,而在出生前以抗生素暴露的全术语或早产新生儿,至少有一个婴儿被诊断出患有早期发病败血症。这些结果表明妇幼的抗生素暴露和微生物暴露和新生儿肠道环境中的微生物消带病之间的关联,这可能与早发败血症的发生有关。

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