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通过给母鼠静脉注射抗F41单克隆抗体对哺乳幼鼠进行被动保护,使其免受F41阳性产肠毒素大肠杆菌菌株的侵害。

Passive protection of suckling infant mice against F41-positive enterotoxigenic Escherichia coli strains by intravenous inoculation of the dams with monoclonal antibodies against F41.

作者信息

Duchet-Suchaux M, Menanteau P, van Zijderveld F G

机构信息

Unite de Pathologie Infectieuse et Immunologie, Institut National de la Recherche Agronomique, Centre de Tours, Nouzilly, France.

出版信息

Infect Immun. 1992 Jul;60(7):2828-34. doi: 10.1128/iai.60.7.2828-2834.1992.

Abstract

Ten monoclonal antibodies (MAbs) against five different epitope clusters of adhesion factor F41 (two MAbs per cluster) were tested for protection of infant mice against an oral challenge with F41-positive enterotoxigenic Escherichia coli (ETEC) B2C and B41M. Infant mice suckling dams intravenously inoculated with MAbs were orally challenged, and the survival rates were measured for 12 days after inoculation and challenge. Irrespective of their epitope specificity, all F41 MAbs given in a single dose of 4 mg per dam had a protective effect against both ETEC strains. In contrast, one K99 MAb of the same isotype and given in the same dose as the F41 MAbs did not protect infant mice at all. A reduction in the dose of F41 MAbs to 0.032 mg per dam resulted in a decrease in protection. Two different MAbs against the same epitope cluster were not necessarily equally protective. Combining MAbs two by two, whether the MAbs recognized the same epitope cluster or not, resulted in protective activity essentially similar to that obtained with each MAb separately, without any improvement. Therefore, one MAb against any epitope may be sufficient for protection. Enzyme-linked immunosorbent assay (ELISA) titers of MAbs in the serum of dams were similar, irrespective of the epitope specificity of the MAbs, and gradually decreased from day 1 to day 12 after inoculation. We found a good correlation between colostrum and milk ELISA titers of MAbs and serum ELISA titers of MAbs. Colostrum and milk MAb titers were 10-fold lower than corresponding serum MAb titers and stayed high until day 5 after inoculation. The most protective MAb had the highest ELISA titers in colostrum and milk for the first 5 days after inoculation. ETEC strain B2C colonized the intestines of infant mice suckling MAb-inoculated mothers until day 12 after challenge. Intestinal levels of the challenge strain were high on day 2 but never reached the very high numbers (10(9) to 10(10)) described previously in a diarrheic infant mouse model. MAbs did not eliminate the challenge ETEC strain from the intestines of infant mice.

摘要

针对粘附因子F41的五个不同表位簇的十种单克隆抗体(MAb)(每个簇两种MAb),进行了保护幼鼠免受F41阳性产肠毒素大肠杆菌(ETEC)B2C和B41M口服攻击的测试。给静脉接种MAb的哺乳母鼠的幼鼠进行口服攻击,并在接种和攻击后12天测量存活率。无论其表位特异性如何,以每只母鼠4毫克的单剂量给予的所有F41 MAb对两种ETEC菌株均具有保护作用。相比之下,相同同种型且与F41 MAb剂量相同的一种K99 MAb根本没有保护幼鼠。将F41 MAb的剂量降低至每只母鼠0.032毫克会导致保护作用降低。针对同一表位簇的两种不同MAb不一定具有同等的保护作用。将MAb两两组合,无论MAb是否识别相同的表位簇,产生的保护活性与分别使用每种MAb获得的保护活性基本相似,没有任何改善。因此,针对任何表位的一种MAb可能足以提供保护。母鼠血清中MAb的酶联免疫吸附测定(ELISA)滴度相似,与MAb的表位特异性无关,并且在接种后第1天至第12天逐渐降低。我们发现MAb的初乳和乳汁ELISA滴度与血清ELISA滴度之间具有良好的相关性。初乳和乳汁MAb滴度比相应的血清MAb滴度低10倍,并且在接种后第5天之前一直保持较高水平。在接种后的前5天,最具保护作用的MAb在初乳和乳汁中的ELISA滴度最高。ETEC菌株B2C在攻击后12天内定殖于接种MAb的母鼠所哺乳的幼鼠肠道中。攻击菌株在第2天的肠道水平很高,但从未达到先前在腹泻幼鼠模型中描述的非常高的数量(10⁹至10¹⁰)。MAb并未从幼鼠肠道中清除攻击的ETEC菌株。

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