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白色念珠菌分泌天冬氨酸蛋白酶在毒力和发病机制中的作用。

Candida albicans secreted aspartyl proteinases in virulence and pathogenesis.

作者信息

Naglik Julian R, Challacombe Stephen J, Hube Bernhard

机构信息

Department of Oral Medicine, Pathology & Immunology, GKT Dental Institute, Kings College London, London, United Kingdom.

出版信息

Microbiol Mol Biol Rev. 2003 Sep;67(3):400-28, table of contents. doi: 10.1128/MMBR.67.3.400-428.2003.

Abstract

Candida albicans is the most common fungal pathogen of humans and has developed an extensive repertoire of putative virulence mechanisms that allows successful colonization and infection of the host under suitable predisposing conditions. Extracellular proteolytic activity plays a central role in Candida pathogenicity and is produced by a family of 10 secreted aspartyl proteinases (Sap proteins). Although the consequences of proteinase secretion during human infections is not precisely known, in vitro, animal, and human studies have implicated the proteinases in C. albicans virulence in one of the following seven ways: (i) correlation between Sap production in vitro and Candida virulence, (ii) degradation of human proteins and structural analysis in determining Sap substrate specificity, (iii) association of Sap production with other virulence processes of C. albicans, (iv) Sap protein production and Sap immune responses in animal and human infections, (v) SAP gene expression during Candida infections, (vi) modulation of C. albicans virulence by aspartyl proteinase inhibitors, and (vii) the use of SAP-disrupted mutants to analyze C. albicans virulence. Sap proteins fulfill a number of specialized functions during the infective process, which include the simple role of digesting molecules for nutrient acquisition, digesting or distorting host cell membranes to facilitate adhesion and tissue invasion, and digesting cells and molecules of the host immune system to avoid or resist antimicrobial attack by the host. We have critically discussed the data relevant to each of these seven criteria, with specific emphasis on how this proteinase family could contribute to Candida virulence and pathogenesis.

摘要

白色念珠菌是人类最常见的真菌病原体,它已形成了一系列广泛的假定毒力机制,使其能够在合适的易感条件下成功定殖并感染宿主。细胞外蛋白水解活性在念珠菌致病性中起核心作用,由一个包含10种分泌天冬氨酸蛋白酶(Sap蛋白)的家族产生。尽管蛋白酶在人类感染过程中的分泌后果尚不完全清楚,但体外、动物和人体研究已表明蛋白酶在白色念珠菌毒力中以以下七种方式之一发挥作用:(i)体外Sap产生与念珠菌毒力之间的相关性;(ii)人类蛋白质的降解以及确定Sap底物特异性的结构分析;(iii)Sap产生与白色念珠菌其他毒力过程的关联;(iv)动物和人类感染中的Sap蛋白产生及Sap免疫反应;(v)念珠菌感染期间的SAP基因表达;(vi)天冬氨酸蛋白酶抑制剂对白色念珠菌毒力的调节;(vii)使用SAP基因缺失突变体分析白色念珠菌毒力。Sap蛋白在感染过程中发挥多种特殊功能,包括为获取营养而消化分子的简单作用、消化或扭曲宿主细胞膜以促进黏附和组织侵袭,以及消化宿主免疫系统的细胞和分子以避免或抵抗宿主的抗菌攻击。我们对与这七个标准相关的数据进行了批判性讨论,特别强调了这个蛋白酶家族如何促进念珠菌的毒力和发病机制。

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