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首页> 外文期刊>Nature chemical biology >An allosteric switch for pro-HGF/Met signaling using zymogen activator peptides
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An allosteric switch for pro-HGF/Met signaling using zymogen activator peptides

机译:使用酶原激活剂肽的促HGF / Met信号转导的变构开关

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Stimulation of hepatocyte growth factor (HGF) signaling through the Met receptor is an attractive approach for promoting tissue repair and preventing fibrosis. Using structure-guided peptide phage display combined with an activity-based sorting strategy, we engineered allosteric activators of zymogen-like pro-HGF to bypass proteolytic activation and reversibly stimulate pro-HGF signaling through Met. Biochemical, structural and biological data showed that zymogen activator peptides (ZAPtides) potently and selectively bind the activation pocket within the serine protease-like b-chain of pro-HGF and display titratable activation of pro-HGF-dependent Met signaling, leading to cell survival and migration. To further demonstrate the versatility of our ZAPtide platform, we identified allosteric activators for pro-macrophage stimulating protein and a zymogen serine protease, Protein C, which also provides evidence for target selectivity. These studies reveal that ZAPtides use molecular mimicry of the trypsin-like N-terminal insertion mechanism and establish a new paradigm for selective pharmacological activation of plasminogen-related growth factors and zymogen serine proteases.
机译:通过Met受体刺激肝细胞生长因子(HGF)信号传导是促进组织修复和预防纤维化的一种有吸引力的方法。使用结构指导的肽噬菌体展示结合基于活动的排序策略,我们设计了酶原样前HGF的变构活化剂,以绕过蛋白水解激活并通过Met可逆地刺激前HGF信号传导。生化,结构和生物学数据表明,酶原激活剂肽(ZAPtides)有效地并选择性地结合前HGF的丝氨酸蛋白酶样b链内的激活口袋,并显示出可滴定的前HGF依赖性Met信号传导,导致细胞生存和迁移。为了进一步证明我们的ZAPtide平台的多功能性,我们鉴定了促巨噬细胞刺激蛋白和酶原丝氨酸蛋白酶蛋白C的变构活化剂,这也为靶标选择性提供了证据。这些研究表明ZAPtides使用类胰蛋白酶N末端插入机制的分子模拟,并为纤溶酶原相关生长因子和酶原丝氨酸蛋白酶的选择性药理激活建立了新的范例。

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