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含天然存在的卡替他汀变体的人嗜铬粒蛋白A的蛋白水解切割:纤溶酶在卡替他汀区域的差异加工

Proteolytic cleavage of human chromogranin a containing naturally occurring catestatin variants: differential processing at catestatin region by plasmin.

作者信息

Biswas Nilima, Vaingankar Sucheta M, Mahata Manjula, Das Madhusudan, Gayen Jiaur R, Taupenot Laurent, Torpey Justin W, O'Connor Daniel T, Mahata Sushil K

机构信息

Department of Medicine, University of California San Diego School of Medicine and Veteran's Affairs San Diego Healthcare System, La Jolla, CA 92093-0838, USA.

出版信息

Endocrinology. 2008 Feb;149(2):749-57. doi: 10.1210/en.2007-0838. Epub 2007 Nov 8.

Abstract

The plasma level of chromogranin A (CgA) is elevated in genetic hypertension. Conversely, the plasma level of the CgA peptide catestatin is diminished in individuals with established hypertension and those with a genetic risk of this disease. Resequencing of the human CHGA gene identified three naturally occurring variants of catestatin (Gly364Ser, Pro370Leu, and Arg374Gln) that exhibit different potencies in inhibiting catecholamine secretion. Here, we have examined whether there is any differential processing of the three CHGA variants to catestatin by the endoproteolytic enzyme plasmin. Plasmin digestion of the purified CgA proteins generated a stable biologically active 14-amino acid peptide (human CgA(360-373)) from the wild-type, Gly364Ser, and Arg374Gln proteins despite the disruption of the dibasic site (Arg(373)Arg(374)) in the Arg374Gln variant. Unexpectedly, the action of plasmin in generating the catestatin peptide from the Pro370Leu protein was less efficient. The efficiency of cleavage at the dibasic Arg(373) downward arrowArg(374) site in synthetic human CgA(360-380) was 3- to 4-fold less in Pro370Leu CgA, compared with the wild type. Circular dichroism of the synthetic CgA(352-372) suggested a difference in the amount of alpha-helix and beta-sheet between the wild-type and Pro370Leu CgA peptides. Because the Pro(370) residue is in the P4 position, the local secondary structure in the vicinity of the cleavage site may enforce the specificity or accessibility to plasmin. The less efficient proteolytic processing of the Pro370Leu protein by plasmin, coupled with the strong association of this variant with ethnicity, suggests that the Pro370Leu CHGA gene variant may contribute to the differential prevalence of cardiovascular disease across ethnic groups.

摘要

嗜铬粒蛋白A(CgA)的血浆水平在遗传性高血压中升高。相反,在已确诊的高血压患者以及有该疾病遗传风险的个体中,CgA肽癌抑素的血浆水平降低。对人类CHGA基因进行重测序,鉴定出癌抑素的三种天然存在的变体(Gly364Ser、Pro370Leu和Arg374Gln),它们在抑制儿茶酚胺分泌方面表现出不同的效力。在此,我们研究了三种CHGA变体被内切蛋白酶纤溶酶加工成癌抑素的过程是否存在差异。对纯化的CgA蛋白进行纤溶酶消化,尽管Arg374Gln变体中的双碱性位点(Arg(373)Arg(374))被破坏,但仍从野生型、Gly364Ser和Arg374Gln蛋白中产生了一种稳定的具有生物活性的14个氨基酸的肽(人CgA(360 - 373))。出乎意料的是,纤溶酶从Pro370Leu蛋白生成癌抑素肽的作用效率较低。与野生型相比,Pro370Leu CgA中合成的人CgA(360 - 380)在双碱性Arg(373)↓Arg(374)位点的切割效率低3至4倍。合成的CgA(352 - 372)的圆二色性表明,野生型和Pro370Leu CgA肽之间的α-螺旋和β-折叠数量存在差异。由于Pro(370)残基处于P4位置,切割位点附近的局部二级结构可能会增强对纤溶酶的特异性或可及性。纤溶酶对Pro370Leu蛋白的蛋白水解加工效率较低,再加上该变体与种族的强烈关联,表明Pro370Leu CHGA基因变体可能导致心血管疾病在不同种族中的患病率存在差异。

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