首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Sj7170 a Unique Dual-function Peptide with a Specific α-Chymotrypsin Inhibitory Activity and a Potent Tumor-activating Effect from Scorpion Venom
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Sj7170 a Unique Dual-function Peptide with a Specific α-Chymotrypsin Inhibitory Activity and a Potent Tumor-activating Effect from Scorpion Venom

机译:Sj7170一种独特的双重功能肽具有特定的α-胰凝乳蛋白酶抑制活性并具有蝎毒的有效肿瘤激活作用

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摘要

A new peptide precursor, termed Sj7170, was characterized from the venomous gland cDNA library of the scorpion Scorpiops jendeki. Sj7170 was deduced to be a 62-amino acid peptide cross-linked by five disulfide bridges. The recombinant Sj7170 peptide (rSj7170) with chromatographic purity was produced by a prokaryotic expression system. Enzyme inhibition assay in vitro and in vivo showed that rSj7170 specifically inhibited the activity of α-chymotrypsin at micromole concentrations. In addition, Sj7170 not only promoted cell proliferation and colony formation by up-regulating the expression of cyclin D1 in vitro but also enhanced tumor growth in nude mice. Finally, Sj7170 accelerated cellular migration and invasion by increasing the expression of the transcription factor Snail and then inducing the epithelial-mesenchymal transition. Moreover, Sj7170 changed cell morphology and cytoskeleton of U87 cells by the GTPase pathway. Taken together, Sj7170 is a unique dual-function peptide, i.e. a specific α-chymotrypsin inhibitor and a potent tumorigenesis/metastasis activator. Our work not only opens an avenue of developing new modulators of tumorigenesis/metastasis from serine protease inhibitors but also strengthens the functional link between protease inhibitors and tumor activators.
机译:一种新的肽前体,称为Sj7170,是从蝎子Scorpiops jendeki的有毒腺cDNA文库中表征的。推测Sj7170是通过五个二硫键交联的62个氨基酸的肽。通过原核表达系统生产具有色谱纯度的重组Sj7170肽(rSj7170)。体内外酶抑制试验表明,rSj7170在微摩尔浓度下特异性抑制α-胰凝乳蛋白酶的活性。此外,Sj7170不仅通过在体外上调细胞周期蛋白D1的表达来促进细胞增殖和集落形成,而且还增强了裸鼠的肿瘤生长。最后,Sj7170通过增加转录因子Snail的表达并诱导上皮-间质转化来加速细胞迁移和侵袭。此外,Sj7170通过GTPase途径改变了U87细胞的细胞形态和细胞骨架。综上所述,Sj7170是独特的双重功能肽,即特定的α-胰凝乳蛋白酶抑制剂和有效的肿瘤发生/转移激活剂。我们的工作不仅为从丝氨酸蛋白酶抑制剂开发新的肿瘤发生/转移调节剂开辟了道路,而且还加强了蛋白酶抑制剂与肿瘤激活剂之间的功能联系。

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