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可消除细菌黏附并引发免疫的百日咳抗原。

Pertussis antigens that abrogate bacterial adherence and elicit immunity.

作者信息

Brennan M J, Shahin R D

机构信息

Center for Biologics Evaluation and Research, Food and Drug Administration, Bethesda, Maryland 20852-1448, USA.

出版信息

Am J Respir Crit Care Med. 1996 Oct;154(4 Pt 2):S145-9. doi: 10.1164/ajrccm/154.4_Pt_2.S145.

Abstract

Infectious disease processes follow the initial steps of adherence of the organism to host tissues and subsequent colonization of the target tissues that can occur through specific adhesion-receptor systems. Bordetella pertussis, the human pathogen that causes whooping cough, has evolved a genetically controlled system whereby adhesins are expressed when they enter the human host. Two adhesins, filamentous hemagglutinin (FHA) and pertactin, mediate the adherence of the bacterium to eukaryotic cells through varied attachment mechanisms, including lectin-like binding sites that interact with sulfated sugars on cell surface glycoconjugates and the ARG-GLY-ASP binding sequence, which recognizes a family of integrins found on the cell surface. The differential expression of relevant receptors by various eukaryotic cells likely plays a role in the pathogenesis and immune response to the bacterium by the host, directing the organism to specific cell types and to specific tissue sites. Substantial evidence exists that the B. pertussis adhesins, FHA and pertactin, elicit immune responses that are protective in animal models for the disease, including serum antibody production and local immune responses in the respiratory tract following nasal administration of encapsulated antigens. Both of these adhesins are components of new acellular pertussis vaccines that have proven safe and highly effective for prevention of serious disease in infants.

摘要

传染病进程始于病原体黏附于宿主组织的初始步骤,随后通过特定的黏附受体系统在靶组织中定殖。引起百日咳的人类病原体百日咳博德特氏菌进化出一种基因控制系统,使得黏附素在进入人类宿主时得以表达。两种黏附素,丝状血凝素(FHA)和百日咳杆菌黏附素,通过多种附着机制介导细菌与真核细胞的黏附,这些机制包括与细胞表面糖缀合物上的硫酸化糖相互作用的凝集素样结合位点以及识别细胞表面发现的一类整合素的ARG-GLY-ASP结合序列。各种真核细胞对相关受体的差异表达可能在宿主对该细菌的发病机制和免疫反应中发挥作用,引导病原体趋向特定的细胞类型和特定的组织部位。大量证据表明,百日咳博德特氏菌黏附素FHA和百日咳杆菌黏附素在该疾病的动物模型中引发具有保护作用的免疫反应,包括血清抗体产生以及经鼻给予包封抗原后呼吸道中的局部免疫反应。这两种黏附素都是新型无细胞百日咳疫苗的成分,已证明对预防婴儿严重疾病安全且高效。

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