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蛇毒透明质酸酶对透明质酸的降解作用:从毒素传递到免疫病理学

Hyaluronan breakdown by snake venom hyaluronidases: From toxins delivery to immunopathology.

作者信息

Silva de França Felipe, Tambourgi Denise V

机构信息

Immunochemistry Laboratory, Instituto Butantan, São Paulo, Brazil.

出版信息

Front Immunol. 2023 Mar 17;14:1125899. doi: 10.3389/fimmu.2023.1125899. eCollection 2023.

Abstract

Snake venom enzymes have a broad range of molecular targets in plasma, tissues, and cells, among which hyaluronan (HA) is outstanding. HA is encountered in the extracellular matrix of diverse tissues and in the bloodstream, and its different chemical configurations dictate the diverse morphophysiological processes in which it participates. Hyaluronidases are highlighted among the enzymes involved in HA metabolism. This enzyme has been detected along the phylogenetic tree, suggesting that hyaluronidases exert multiple biological effects on different organisms. Hyaluronidases have been described in tissues, blood and snake venoms. Snake venom hyaluronidases (SVHYA) contribute to tissue destruction in envenomations and are called spreading factors since their action potentiates venom toxin delivery. Interestingly, SVHYA are clustered in Enzyme Class 3.2.1.35 together with mammalian hyaluronidases (HYAL). Both HYAL and SVHYA of Class 3.2.1.35 act upon HA, generating low molecular weight HA fragments (LMW-HA). LMW-HA generated by HYAL becomes a damage-associated molecular pattern that is recognized by Toll-like receptors 2 and 4, triggering cell signaling cascades culminating in innate and adaptive immune responses that are characterized by lipid mediator generation, interleukin production, chemokine upregulation, dendritic cell activation and T cell proliferation. In this review, aspects of the structures and functions of HA and hyaluronidases in both snake venoms and mammals are presented, and their activities are compared. In addition, the potential immunopathological consequences of HA degradation products generated after snakebite envenoming and their use as adjuvant to enhance venom toxin immunogenicity for antivenom production as well as envenomation prognostic biomarker are also discussed.

摘要

蛇毒酶在血浆、组织和细胞中有广泛的分子靶点,其中透明质酸(HA)尤为突出。HA存在于多种组织的细胞外基质和血液中,其不同的化学结构决定了它所参与的各种形态生理过程。透明质酸酶是参与HA代谢的酶中备受关注的一类。这种酶在系统发育树上均有发现,表明透明质酸酶对不同生物体发挥多种生物学作用。透明质酸酶已在组织、血液和蛇毒中被描述。蛇毒透明质酸酶(SVHYA)在蛇咬伤中毒时会导致组织破坏,因其作用能增强毒液毒素的传递,所以被称为扩散因子。有趣的是,SVHYA与哺乳动物透明质酸酶(HYAL)一起被归为3.2.1.35酶类。3.2.1.35类的HYAL和SVHYA都作用于HA,产生低分子量HA片段(LMW - HA)。由HYAL产生的LMW - HA成为一种损伤相关分子模式,可被Toll样受体2和4识别,触发细胞信号级联反应,最终导致以脂质介质生成、白细胞介素产生、趋化因子上调、树突状细胞活化和T细胞增殖为特征的先天性和适应性免疫反应。在本综述中,介绍了蛇毒和哺乳动物中HA及透明质酸酶的结构和功能方面,并对它们的活性进行了比较。此外,还讨论了蛇咬伤中毒后HA降解产物潜在的免疫病理后果,以及它们作为佐剂增强毒液毒素免疫原性用于抗蛇毒血清生产和蛇咬伤中毒预后生物标志物的用途。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d03/10064005/42c9775e58ff/fimmu-14-1125899-g001.jpg

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