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首页> 外文期刊>Journal of proteomics >Dracula's children: Molecular evolution of vampire bat venom
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Dracula's children: Molecular evolution of vampire bat venom

机译:德古拉的孩子:吸血蝙蝠毒液的分子进化

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While vampire bat oral secretions have been the subject of intense research, efforts have concentrated only on two components: DSPA (Desmodus rotundus salivary plasminogen activator) and Draculin. The molecular evolutionary history of DSPA has been elucidated, while conversely draculin has long been known from only a very small fragment and thus even the basic protein class was not even established. Despite the fact that vampire bat venom has a multitude of effects unaccounted by the documented bioactivities of DSPA and draculin, efforts have not been made to establish what other bioactive proteins are secreted by their submaxillary gland. In addition, it has remained unclear whether the anatomically distinct anterior and posterior lobes of the submaxillary gland are evolving on separate gene expression trajectories or if they remain under the shared genetic control. Using a combined proteomic and transcriptomic approach, we show that identical proteins are simultaneously expressed in both lobes. In addition to recovering the known structural classes of DSPA, we recovered a novel DSPA isoform as well as obtained a very large sequence stretch of draculin and thus established that it is a mutated version of the lactotransferrin scaffold. This study reveals a much more complex secretion profile than previously recognised. In addition to obtaining novel versions of scaffolds convergently recruited into other venoms (allergen-like, CRiSP, kallikrein, Kunitz, lysozyme), we also documented novel expression of small peptides related to calcitonin, PACAP, and statherin. Other overexpressed protein types included BPI-fold, lacritin, and secretoglobin. Further, we investigate the molecular evolution of various vampire bat venom-components and highlight the dominant role of positive selection in the evolution of these proteins. Conspicuously many of the proteins identified in the proteome were found to be homologous to proteins with known activities affecting vasodilation and platelet aggregation. We show that vampire bat venom proteins possibly evade host immune response by the mutation of the surface chemistry through focal mutagenesis under the guidance of positive Darwinian selection. These results not only contribute to the body of knowledge regarding haematophagous venoms but also provide a rich resource for novel lead compounds for use in drug design and development. Biological significance: These results have direct implications in understanding the molecular evolutionary history of vampire bat venom. The unusual peptides discovered reinforce the value of studying such neglected taxon for biodiscovery.
机译:尽管吸血蝙蝠的口腔分泌物一直是研究的重点,但研究工作仅集中在两个部分:DSPA(圆形腐烂唾液纤溶酶原激活剂)和Draculin。已经阐明了DSPA的分子进化史,而相反地,从很小的片段中就知道了draraculin,因此甚至连基本的蛋白质类别也没有建立。尽管事实上吸血蝙蝠毒液具有多种作用,但文献记载的DSPA和draculin的生物活性无法说明这些作用,但尚未做出努力来确定其上颌下腺分泌的其他生物活性蛋白。此外,尚不清楚上颌下腺在解剖学上不同的前叶和后叶是否在独立的基因表达轨迹上进化,或者是否仍处于共同的遗传控制之下。使用蛋白质组学和转录组学相结合的方法,我们表明相同的蛋白质同时在两个叶中表达。除了回收已知的DSPA结构类别外,我们还回收了新型的DSPA同工型,并获得了非常大的德拉科林序列延伸序列,因此确定它是乳运铁蛋白支架的突变形式。这项研究揭示了比以前认识的复杂得多的分泌特征。除了获得会集到其他毒液(类似过敏原,CRiSP,激肽释放酶,Kunitz,溶菌酶)的新型支架外,我们还记录了与降钙素,PACAP和斯坦汀相关的小肽的新型表达。其他过表达的蛋白质类型包括BPI折叠,催乳素和分泌球蛋白。此外,我们调查了各种吸血蝙蝠毒液成分的分子进化,并强调了阳性选择在这些蛋白质进化中的主导作用。显然,发现在蛋白质组中鉴定出的许多蛋白质与具有已知影响血管舒张和血小板聚集的活性的蛋白质同源。我们显示吸血蝙蝠毒蛋白可能逃避宿主免疫反应,通过在积极的达尔文选择的指导下通过局部诱变的表面化学突变。这些结果不仅有助于了解关于食血性毒液的知识,而且还为用于药物设计和开发的新型先导化合物提供了丰富的资源。生物学意义:这些结果对了解吸血蝙蝠毒液的分子进化历史具有直接的意义。发现的非同寻常的肽增强了研究这种被忽视的生物分类用于生物发现的价值。

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