Brown Spider Venom Phospholipases D: From Potent Molecules Involved in Pathogenesis of Brown Spider Bites to Molecular Tools for Studying Ectosomes, Ectocytosis, and Its Applications.

IF 3.9 3区 医学 Q2 FOOD SCIENCE & TECHNOLOGY
Toxins Pub Date : 2025-02-05 DOI:10.3390/toxins17020070
Ana Carolina Martins Wille, Mariana Izabele Machado, Samira Hajjar Souza, Hanna Câmara da Justa, Maria Eduarda de Fraga-Ferreira, Eloise de Souza Mello, Luiza Helena Gremski, Silvio Sanches Veiga
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引用次数: 0

Abstract

Accidents caused by Loxosceles spiders, commonly known as brown spiders, are frequent in warm and temperate regions worldwide, with a higher prevalence in South America and the southern United States. In the venoms of species clinically associated with accidents, phospholipases D (PLDs) are the most expressed toxins. This classification is based on the toxins' ability to cleave various phospholipids, with a preference for sphingomyelin. Studies using purified PLDs have demonstrated that these enzymes cleave phospholipids from cells, producing derivatives that can activate leukocytes. A dysregulated inflammatory response is the primary effect following envenomation, leading to dermonecrosis, which is histopathologically characterized by aseptic coagulative necrosis-a key feature of envenomation. Although advances in understanding the structure-function relationship of enzymes have been achieved through molecular biology, heterologous expression, site-directed mutations, crystallography, and bioinformatic analyses-describing PLDs in the venoms of various species and highlighting the conservation of amino acid residues involved in catalysis, substrate binding, and magnesium stabilization-little is known about the cellular biology of these PLDs. Studies have shown that the treatment of various cells with recombinant PLDs stimulates the formation of ectosomes and ectocytosis, events that initiate a cascade of intracellular signaling in PLD-binding cells and lead to the release of extracellular microvesicles. These microvesicles may act as signalosomes for other target cells, thereby triggering an inflammatory response and dermonecrosis. In this review, we will discuss the biochemical properties of PLDs, the target cells that bind to them, and the ectocytosis-dependent pathophysiology of envenoming.

褐蜘蛛毒液磷脂酶D:从参与褐蜘蛛咬伤发病机制的有效分子到研究外胞体、外胞功能及其应用的分子工具。
由Loxosceles蜘蛛引起的事故,通常被称为棕色蜘蛛,在全球温暖和温带地区经常发生,在南美洲和美国南部发病率较高。在临床上与事故相关的物种的毒液中,磷脂酶D (PLDs)是表达最多的毒素。这种分类是基于毒素切割各种磷脂的能力,尤其是鞘磷脂。使用纯化pld的研究表明,这些酶从细胞中切割磷脂,产生可以激活白细胞的衍生物。炎症反应失调是中毒后的主要影响,导致皮肤坏死,其组织病理学特征为无菌性凝固性坏死,这是中毒的主要特征。尽管通过分子生物学、异源表达、位点定向突变、晶体学和生物信息学分析,在理解酶的结构-功能关系方面取得了进展——描述了各种物种毒液中的pld,并强调了催化、底物结合和镁稳定中涉及的氨基酸残基的保护——但对这些pld的细胞生物学知之甚少。研究表明,用重组pld处理各种细胞会刺激外泌体和外胞量的形成,这些事件在pld结合的细胞中启动细胞内信号的级联反应,并导致细胞外微泡的释放。这些微泡可能作为其他靶细胞的信号体,从而引发炎症反应和皮肤坏死。在这篇综述中,我们将讨论pld的生化特性,与它们结合的靶细胞,以及外生细胞依赖的病理生理。
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来源期刊
Toxins
Toxins TOXICOLOGY-
CiteScore
7.50
自引率
16.70%
发文量
765
审稿时长
16.24 days
期刊介绍: Toxins (ISSN 2072-6651) is an international, peer-reviewed open access journal which provides an advanced forum for studies related to toxins and toxinology. It publishes reviews, regular research papers and short communications. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced.
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