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人类和小牛中出现的产志贺毒素和肠致病性杂交血清型O80:H2

Emerging hybrid shigatoxigenic and enteropathogenic serotype O80:H2 in humans and calves.

作者信息

Mainil Jacques G, Nakamura Keiji, Ikeda Rie, Crombé Florence, Diderich Jacob, Saulmont Marc, Piérard Denis, Thiry Damien, Hayashi Tetsuya

机构信息

Veterinary Bacteriology, Department of Infectious and Parasitic Diseases, Faculty of Veterinary Medicine and Centre for Fundamental and Applied Research for Animals and Health (FARAH), University of Liège (ULiège), Liège, Belgium.

Department of Bacteriology, Faculty of Medical Sciences, Kyushu University, Fukuoka, Japan.

出版信息

Clin Microbiol Rev. 2025 Sep 11;38(3):e0001125. doi: 10.1128/cmr.00011-25. Epub 2025 May 29.

Abstract

SUMMARYAttaching-effacing (AE) lesion- and Shiga toxin-producing (.) (AE-STEC), previously known as "enterohemorrhagic " (EHEC), are responsible for (hemorrhagic) enterocolitis (HC) and hemolytic uremic syndrome (HUS) in humans. The most frequent and pathogenic AE-STEC belong to a few O:H major serotypes that are responsible for the majority of cases and outbreaks worldwide. From time to time, one or another non-major O:H serotype can emerge, causing either local outbreaks or a a progressive increase in clinical cases. One of these minor serotypes is O80:H2, which has been progressively emerging in Western Europe, especially in France, since 2010. AE-STEC O80:H2 are responsible for not only HC and HUS but also invasive infections with bacteremia and internal organ infection. In parallel to their emergence in humans, AE-STEC and enteropathogenic (EPEC) O80:H2 have also been emerging in young calves suffering diarrhea and enteritis and, more rarely septicemia, in Belgium since 2009. In this manuscript, an overview of AE-STEC and EPEC O80:H2 infections in humans and calves is presented, with particular focus on the clinical manifestations, the prevalence and incidence in Western Europe, and the identification of the potential reservoir(s). In addition, the results of a large-scale whole genome-based phylogenetic analysis of 417 published and unpublished genome sequences currently available in the literature and in the NCBI and EnteroBase databases are presented with hypotheses on the origin and evolution of this new hybrid AE-STEC and EPEC serotype.

摘要

摘要

黏附-蚀损性(AE)病变型和产志贺毒素(STEC)型(AE-STEC),以前被称为“肠出血性大肠杆菌”(EHEC),可导致人类患出血性小肠结肠炎(HC)和溶血尿毒综合征(HUS)。最常见且具有致病性的AE-STEC属于少数几种主要的O:H血清型,它们导致了全球大多数病例和疫情的发生。时不时会出现一种或另一种非主要的O:H血清型,引发局部疫情或临床病例的逐渐增加。其中一种次要血清型是O80:H2,自2010年以来在西欧,尤其是法国逐渐出现。AE-STEC O80:H2不仅会导致HC和HUS,还会引发伴有菌血症的侵袭性感染和内脏器官感染。与它们在人类中出现的同时,自2009年以来,AE-STEC和肠致病性大肠杆菌(EPEC)O80:H2也在比利时患有腹泻和肠炎的幼犊中出现,较少情况下还会导致败血症。在本手稿中,对人类和犊牛中AE-STEC和EPEC O80:H2感染进行了概述,特别关注临床表现、西欧的患病率和发病率,以及潜在宿主的识别。此外,还展示了对文献、NCBI和EnteroBase数据库中目前可用的417个已发表和未发表的基因组序列进行的大规模全基因组系统发育分析结果,并对这种新的杂交AE-STEC和EPEC血清型的起源和进化提出了假设。

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