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系统方法定义志贺氏菌感染的体液免疫相关性。

Systems approach to define humoral correlates of immunity to Shigella.

机构信息

Ragon Institute of MGH, Harvard and MIT, Cambridge, MA, USA.

Department of Pediatrics, Center for Vaccine Development and Global Health, University of Maryland School of Medicine, Baltimore, MD, USA.

出版信息

Cell Rep. 2022 Aug 16;40(7):111216. doi: 10.1016/j.celrep.2022.111216.

Abstract

Shigella infection is the second leading cause of death due to diarrheal disease in young children worldwide. With the rise of antibiotic resistance, initiatives to design and deploy a safe and effective Shigella vaccine are urgently needed. However, efforts to date have been hindered by the limited understanding of immunological correlates of protection against shigellosis. We applied systems serology to perform a comprehensive analysis of Shigella-specific antibody responses in sera obtained from volunteers before and after experimental infection with S. flexneri 2a in a series of controlled human challenge studies. Polysaccharide-specific antibody responses are infrequent prior to infection and evolve concomitantly with disease severity. In contrast, pre-existing antibody responses to type 3 secretion system proteins, particularly IpaB, consistently associate with clinical protection from disease. Linked to particular Fc-receptor binding patterns, IpaB-specific antibodies leverage neutrophils and monocytes, and complement and strongly associate with protective immunity. IpaB antibody-mediated functions improve with a subsequent rechallenge resulting in complete clinical protection. Collectively, our systems serological analyses indicate protein-specific functional correlates of immunity against Shigella in humans.

摘要

志贺氏菌感染是全球导致幼儿腹泻病死亡的第二大原因。随着抗生素耐药性的出现,迫切需要设计和部署安全有效的志贺氏菌疫苗。然而,迄今为止,由于对志贺氏菌病保护的免疫相关因素的了解有限,这些努力受到了阻碍。我们应用系统血清学方法,在一系列志贺氏菌人工感染的人体挑战研究中,对志愿者在感染 S. flexneri 2a 前后获得的血清中的志贺氏菌特异性抗体反应进行了全面分析。多糖特异性抗体反应在感染前很少发生,并与疾病严重程度同时发生演变。相比之下,针对 III 型分泌系统蛋白(尤其是 IpaB)的预先存在的抗体反应与疾病的临床保护始终相关。与特定的 Fc 受体结合模式相关联,IpaB 特异性抗体利用中性粒细胞和单核细胞以及补体,并与保护性免疫强烈相关。IpaB 抗体介导的功能在随后的再挑战中得到改善,从而实现完全的临床保护。总的来说,我们的系统血清学分析表明,针对人类志贺氏菌的免疫具有蛋白质特异性功能相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/161e/9396529/435b2abf0728/fx1.jpg

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