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乳杆菌和双歧杆菌增强黏膜 B 细胞反应,并在新生无菌猪疾病模型中差异调节对口服人轮状病毒疫苗的全身抗体反应。

Lactobacilli and Bifidobacteria enhance mucosal B cell responses and differentially modulate systemic antibody responses to an oral human rotavirus vaccine in a neonatal gnotobiotic pig disease model.

机构信息

a Food Animal Health Research Program; Department of Veterinary Preventive Medicine; Ohio Agricultural Research and Development Center; The Ohio State University ; Wooster , OH USA.

出版信息

Gut Microbes. 2014;5(5):639-51. doi: 10.4161/19490976.2014.969972.

Abstract

B cells play a key role in generation of protective immunity against rotavirus infection, a major cause of gastroenteritis in children. Current RV vaccines are less effective in developing countries compared to developed countries. Commensals/probiotics influence mucosal immunity, but the role of early gut colonizing bacteria in modulating intestinal B cell responses to RV vaccines is largely unknown. We co-colonized neonatal gnotobiotic pigs, the only animal model susceptible to HRV diarrhea, with 2 dominant bacterial species present in the gut of breastfed infants, Lactobacillus rhamnosus strain GG and Bifidobacterium animalis lactis Bb12 to evaluate their impact on B cell responses to an attenuated (Att) human rotavirus (HRV) Wa strain vaccine. Following HRV challenge, probiotic-colonized, AttHRV vaccinated piglets had significantly lower fecal scores and reduced HRV shedding titers compared to uncolonized, AttHRV vaccinated pigs. The reduction in HRV diarrhea was significantly correlated with higher intestinal IgA HRV antibody titers and intestinal HRV-specific IgA antibody secreting cell (ASC) numbers in probiotic-colonized, AttHRV vaccinated pigs compared to uncolonized, vaccinated pigs. The significantly higher small intestinal HRV IgA antibody responses coincided with higher IL-6, IL-10 and APRIL responses of ileal mononuclear cells (MNCs) and the immunomodulatory effects of probiotics genomic DNA on TGF-β and IL-10 responses. However, serum RV IgG antibody titers and total IgG titers were significantly lower in probiotic-colonized, AttHRV vaccinated pigs compared to uncolonized, vaccinated pigs, both pre- and post-challenge. In summary, LGG and Bb12 beneficially modulated intestinal B cell responses to HRV vaccine.

摘要

B 细胞在产生针对轮状病毒(RV)感染的保护性免疫方面发挥着关键作用,轮状病毒是导致儿童肠胃炎的主要原因。与发达国家相比,目前的 RV 疫苗在发展中国家的效果较差。共生菌/益生菌会影响黏膜免疫,但早期定植于肠道的细菌在调节肠道 B 细胞对 RV 疫苗的反应方面的作用在很大程度上尚未可知。我们将两种在母乳喂养婴儿肠道中存在的优势细菌种属(鼠李糖乳杆菌 GG 株和动物双歧杆菌 Bb12 株)共同定植于新生无菌猪,这些无菌猪是唯一对 HRV 腹泻易感的动物模型,以评估它们对减毒(Att)人轮状病毒(HRV)Wa 株疫苗的 B 细胞反应的影响。在 HRV 攻毒后,与未定植、AttHRV 疫苗接种的猪相比,定植了益生菌、AttHRV 疫苗接种的仔猪粪便评分更低,HRV 脱落滴度更低。HRV 腹泻的减少与定植了益生菌、AttHRV 疫苗接种的猪的肠道 HRV 特异性 IgA 抗体分泌细胞(ASC)数量和肠道 IgA HRV 抗体滴度显著升高显著相关,而与未定植、AttHRV 疫苗接种的猪相比。小肠 HRV IgA 抗体反应显著升高与回肠单核细胞(MNC)中更高的 IL-6、IL-10 和 APRIL 反应以及益生菌基因组 DNA 对 TGF-β和 IL-10 反应的免疫调节作用一致。然而,与未定植、AttHRV 疫苗接种的猪相比,定植了益生菌、AttHRV 疫苗接种的猪的血清 RV IgG 抗体滴度和总 IgG 滴度在攻毒前后均显著降低。综上所述,LGG 和 Bb12 有益地调节了 HRV 疫苗对肠道 B 细胞的反应。

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