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Synthetic Peptides Derived from the C-Terminal Region of Lys49 Phospholipase A_2 Homologues from Viperidae Snake Venoms: Biomimetic Activities and Potential Applications

机译:蛇毒蛇毒Lys49磷脂酶A_2同系物C端区域衍生的合成肽:仿生活性和潜在应用。

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摘要

Lys49-phospholipase A_2 homologues constitute a large family of toxins present in the venoms of viperid snake species, which despite lacking catalytic activity, cause significant skeletal muscle necrosis. The main structural determinants of this toxic effect have been experimentally mapped to a region near their C-terminus (115-129), which combines cationic and hydrophobic/aromatic amino acid residues. Short (13-mer) synthetic peptides representing this C-terminal region can mimick several of the effects of Lys49 PLA_2 homologues. In addition to their ability to damage muscle cells, these peptides display antibacterial, antiendotoxic, antifungal, antiparasite, and antitumor activities, as well as VEGF-receptor 2 (KDR)-binding and heparin-binding properties. Modifications of their sequences have shown possibilities to enhance their effects upon prokaryotic cells, while decreasing toxicity for eukaryotic cells. This review presents an updated summary on the biomimetic actions exerted by such peptides, and highlights their potential value as molecular tools or as drug leads in diverse biomedical areas.
机译:Lys49-磷脂酶A_2同源物构成了在蛇类蛇毒中存在的一大类毒素,尽管缺乏催化活性,但它们仍引起严重的骨骼肌坏死。已通过实验将这种毒性作用的主要结构决定因素定位在其C末端(115-129)附近,该区域结合了阳离子和疏水/芳族氨基酸残基。代表该C末端区域的短(13聚体)合成肽可以模仿Lys49 PLA_2同系物的几种作用。这些肽除了具有破坏肌肉细胞的能力外,还具有抗菌,抗内毒素,抗真菌,抗寄生虫和抗肿瘤的活性,以及​​VEGF受体2(KDR)和肝素的结合特性。其序列的修饰已显示出可能增强其对原核细胞的作用,同时降低对真核细胞的毒性。这篇综述提供了有关此类肽所发挥的仿生作用的最新摘要,并着重介绍了它们作为分子工具或在各种生物医学领域中作为药物的潜在价值。

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