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从棕色蜘蛛(中间型洛氏蛛)毒液中鉴定、克隆并对一种新型皮肤坏死毒素(磷脂酶D)进行功能表征。

Identification, cloning and functional characterization of a novel dermonecrotic toxin (phospholipase D) from brown spider (Loxosceles intermedia) venom.

作者信息

Appel Marcia Helena, da Silveira Rafael Bertoni, Chaim Olga Meiri, Paludo Kátia Sabrina, Silva Dilza Trevisan, Chaves Daniele M, da Silva Paulo Henrique, Mangili Oldemir C, Senff-Ribeiro Andrea, Gremski Waldemiro, Nader Helena B, Veiga Silvio Sanches

机构信息

Department of Cell Biology, Federal University of Paraná, Jardim das Américas, 81531-990, Curitiba, Paraná, Brazil.

出版信息

Biochim Biophys Acta. 2008 Feb;1780(2):167-78. doi: 10.1016/j.bbagen.2007.11.007. Epub 2007 Nov 26.

Abstract

Brown spider bites are associated with lesions including dermonecrosis, gravitational spreading and a massive inflammatory response, along with systemic problems that may include hematological disturbances and renal failure. The mechanisms by which the venom exerts its noxious effects are currently under investigation. It is known that the venom contains a major toxin (dermonecrotic toxin, biochemically a phospholipase D) that can experimentally induce dermonecrosis, inflammatory response, animal mortality and platelet aggregation. Herein, we describe cloning, heterologous expression, purification and functionality of a novel isoform of the 33 kDa dermonecrotic toxin. Circular dichroism analysis evidenced correct folding for the toxin. The recombinant toxin was recognized by whole venom serum antibodies and by a specific antibody to a previously described dermonecrotic toxin. The identified toxin was found to display phospholipase activity and dermonecrotic properties. Additionally, the toxin caused a massive inflammatory response in rabbit skin dermis, evoked platelet aggregation, increased vascular permeability, caused edema and death in mice. These characteristics in combination with functional studies for other dermonecrotic toxins illustrate that a family of dermonecrotic toxins exists, and includes a novel member with high activity that may be useful for future structural and functional studies.

摘要

棕色蜘蛛叮咬会引发包括皮肤坏死、重力性扩散和大规模炎症反应在内的损伤,以及可能包括血液系统紊乱和肾衰竭的全身问题。毒液发挥其有害作用的机制目前正在研究中。已知毒液含有一种主要毒素(皮肤坏死毒素,生化上是一种磷脂酶D),它可以在实验中诱导皮肤坏死、炎症反应、动物死亡和血小板聚集。在此,我们描述了一种33 kDa皮肤坏死毒素新亚型的克隆、异源表达、纯化及其功能。圆二色性分析证明该毒素折叠正确。重组毒素被全毒液血清抗体和针对先前描述的皮肤坏死毒素的特异性抗体识别。所鉴定的毒素显示出磷脂酶活性和皮肤坏死特性。此外,该毒素在兔皮肤真皮中引发了大规模炎症反应,诱发了血小板聚集,增加了血管通透性,导致小鼠出现水肿和死亡。这些特征与对其他皮肤坏死毒素的功能研究相结合,表明存在一个皮肤坏死毒素家族,其中包括一个具有高活性的新成员,这可能对未来的结构和功能研究有用。

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