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霍乱样肠毒素对免疫反应的调节作用。

Modulation of the immune response by the cholera-like enterotoxins.

作者信息

Plant Andrea, Williams Neil A

机构信息

University of Bristol, Department of Pathology and Microbiology, School of Medical Sciences, University Walk, Bristol, BS8 1TD, UK.

出版信息

Curr Top Med Chem. 2004;4(5):509-19. doi: 10.2174/1568026043451230.

Abstract

Cholera toxins and heat labile enterotoxin from E. coli differ from most soluble proteins in eliciting systemic immunity both against themselves and unrelated admixed antigens, rather than tolerance following administration to a mucosal surface. Several reports have also demonstrated preferential induction of Th2-type responses when these molecules are used as adjuvants. Conversely, these proteins and their non-toxic derivatives, including the B sub-units are also able prevent and alleviate autoimmune diseases in naïve and systemically immune hosts demonstrating wide-ranging effects on the immune system. The recent observation that amelioration of autoimmune disease is associated with the generation of regulatory T cells which inhibit pathogenic Th1 responses may also help to consolidate these two apparently contradictory outcomes of exposure to the cholera-like enterotoxins. Furthermore, the observation that EtxB is able to alleviate autoimmune disease in the absence of conjugation to autoantigen highlights its potential for use in the clinical setting where the target antigen is often unknown. Direct effects on T cells, B cells and APC have been demonstrated in vitro which have provided insights into how these molecules may elicit these diverse effects. Further investigation is required for elucidation of the mechanisms of action of adjuvanticity and tolerance induction by these molecules to realise their potential for use in vaccines and therapies for autoimmune disease in humans.

摘要

霍乱毒素和大肠杆菌热不稳定肠毒素与大多数可溶性蛋白质不同,它们在经黏膜表面给药后,引发的是针对自身和无关混合抗原的全身免疫,而非耐受性。一些报告还表明,当这些分子用作佐剂时,会优先诱导Th2型反应。相反,这些蛋白质及其无毒衍生物,包括B亚基,也能够预防和减轻初免和全身免疫宿主的自身免疫疾病,表明它们对免疫系统具有广泛影响。最近的观察结果表明,自身免疫疾病的改善与抑制致病性Th1反应的调节性T细胞的产生有关,这也可能有助于巩固接触霍乱样肠毒素的这两个明显矛盾的结果。此外,观察到EtxB在未与自身抗原结合的情况下能够减轻自身免疫疾病,这突出了其在临床环境中的应用潜力,因为在临床环境中目标抗原往往未知。已在体外证明了其对T细胞、B细胞和抗原呈递细胞的直接作用,这为了解这些分子如何引发这些不同效应提供了见解。需要进一步研究以阐明这些分子的佐剂作用和耐受性诱导机制,从而实现它们在人类自身免疫疾病疫苗和治疗中的应用潜力。

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