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人类B细胞对蠕虫感染的致敏作用在子宫内就已形成。

B cell sensitization to helminthic infection develops in utero in humans.

作者信息

King C L, Malhotra I, Mungai P, Wamachi A, Kioko J, Ouma J H, Kazura J W

机构信息

Division of Geographic Medicine, Case Western Reserve University, University Hospitals of Cleveland, OH 44106, USA.

出版信息

J Immunol. 1998 Apr 1;160(7):3578-84.

PMID:9531321
Abstract

Human neonates are generally deficient in their ability to generate humoral immunity. This deficiency is thought to reflect physiologic immaturity of T and B cell function and lack of previous exposure to exogenous Ags. To determine whether neonatal humoral immunity can be modified by maternal helminth infection during pregnancy, we assessed Ig production by cord blood lymphocytes from healthy newborns of mothers living in an area of Kenya where schistosomiasis, bancroftian filariasis, and geohelminth infections are endemic. Twelve of 40 and 17 of 39 cord blood lymphocyte preparations from healthy newborns in Coast Province, Kenya, spontaneously made polyclonal IgE (range, 0.15-21 ng/ml) and IgG (1.6-10.1 ng/ml) in vitro. In vitro IgE synthesis by cord blood lymphocytes (CBL) was, on the average, 10-fold less than that of PBMC of Kenyan mothers (1.1-98 ng/ml) and was undetectable for CBL from newborns delivered in the United States. Schistosome and filarial Ags stimulated a 3- to > 100-fold increase in the production of polyclonal IgE and parasite-specific IgG Abs by lymphocytes from 10 of 40 and 6 of 39 Kenyan newborns, respectively. CBL observed to have helminth Ag-driven B cell responses were more likely to be from newborns of schistosome- or filaria-infected mothers than from uninfected mothers (p < 0.05). These data indicate that the human fetus can be sensitized in utero to produce helminth-specific B cells and that neonatal B cells are intrinsically capable of IgE and IgG production.

摘要

人类新生儿通常在产生体液免疫的能力方面存在缺陷。这种缺陷被认为反映了T和B细胞功能的生理不成熟以及缺乏先前对外源抗原的接触。为了确定孕期母体蠕虫感染是否能改变新生儿的体液免疫,我们评估了来自肯尼亚一个血吸虫病、班氏丝虫病和土源性蠕虫感染流行地区母亲所生健康新生儿的脐血淋巴细胞产生的免疫球蛋白。肯尼亚海岸省40份和39份健康新生儿脐血淋巴细胞制剂中,分别有12份和17份在体外自发产生多克隆IgE(范围为0.15 - 21 ng/ml)和IgG(1.6 - 10.1 ng/ml)。脐血淋巴细胞(CBL)体外IgE合成平均比肯尼亚母亲的外周血单个核细胞(PBMC)少10倍(1.1 - 98 ng/ml),而在美国出生的新生儿的CBL中未检测到。血吸虫和丝虫抗原分别刺激了40份肯尼亚新生儿中10份和39份新生儿中6份的淋巴细胞产生的多克隆IgE和寄生虫特异性IgG抗体增加3至>100倍。观察到有蠕虫抗原驱动的B细胞反应的CBL更有可能来自血吸虫或丝虫感染母亲的新生儿,而不是未感染母亲的新生儿(p < 0.05)。这些数据表明,人类胎儿可在子宫内被致敏以产生蠕虫特异性B细胞,并且新生儿B细胞本质上能够产生IgE和IgG。

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