首页> 外文期刊>Molecular pharmacology. >Three distinct D-amino acid substitutions confer potent antiangiogenic activity on an inactive peptide derived from a thrombospondin-1 type 1 repeat.
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Three distinct D-amino acid substitutions confer potent antiangiogenic activity on an inactive peptide derived from a thrombospondin-1 type 1 repeat.

机译:三个不同的D-氨基酸取代赋予源自血小板反应蛋白1型1重复序列的无活性肽有效的抗血管生成活性。

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摘要

Mal II, a 19-residue peptide derived from the second type 1 properdin-like repeat of the antiangiogenic protein thrombospondin-1 (TSP-1), was inactive in angiogenesis assays. Yet the substitution of any one of three L-amino acids by their D-enantiomers conferred on this peptide a potent antiangiogenic activity approaching that of the intact 450-kDa TSP-1. Substituted peptides inhibited the migration of capillary endothelial cells with an ED50 of 8.5 nM for the D-Ile-15 substitution, 10 nM for the D-Ser-4 substitution, and 0.75 nM for the D-Ser-5 substitution. A peptide with D-Ile at position 15 could be shortened to its last seven amino acids with little loss in activity. Like whole TSP-1, the Mal II D-Ile derivative inhibited a broad range of angiogenic inducers, was selective for endothelial cells, and required CD36 receptor binding for activity. A variety of end modifications further improved peptide potency. An ethylamide-capped heptapeptide was also active systemically in that when injected i.p. it rendered mice unable to mount a corneal angiogenic response, suggesting the potential usefulness of such peptides as antiangiogenic therapeutics.
机译:Mal II是一种19残基的肽,它来自抗血管生成蛋白thrombospondin-1(TSP-1)的第二个类型1备解素样重复序列,在血管生成测定中无效。然而,三个L-氨基酸中的任何一个被其D-对映体所取代,都赋予该肽以接近完整450-kDa TSP-1的有效抗血管生成活性。取代的肽抑制毛细血管内皮细胞的迁移,ED50的D-Ile-15取代为8.5 nM,D-Ser-4取代为10 nM,D-Ser-5取代为0.75 nM。在位置15处具有D-Ile的肽可以被缩短至其最后七个氨基酸,而活性几乎没有损失。像完整的TSP-1一样,Mal II D-Ile衍生物可抑制多种血管生成诱导剂,对内皮细胞具有选择性,并且需要CD36受体结合才能发挥活性。各种末端修饰进一步提高了肽效价。乙酰胺封端的七肽在注射时也具有全身活性。它使小鼠无法进行角膜血管生成反应,表明这种肽作为抗血管生成治疗剂的潜在用途。

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