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半胱天冬酶-6中与肿瘤相关的突变对催化效率产生负面影响。

Tumor-Associated Mutations in Caspase-6 Negatively Impact Catalytic Efficiency.

作者信息

Dagbay Kevin B, Hill Maureen E, Barrett Elizabeth, Hardy Jeanne A

机构信息

Department of Chemistry, University of Massachusetts Amherst , Amherst, Massachusetts 01003, United States.

出版信息

Biochemistry. 2017 Aug 29;56(34):4568-4577. doi: 10.1021/acs.biochem.7b00357. Epub 2017 Aug 16.

Abstract

Unregulated, particularly suppressed programmed cell death is one of the distinguishing features of many cancer cells. The cysteine protease caspase-6, one of the executioners of apoptotic cell death, plays a crucial role in regulation of apoptosis. Several somatic mutations in the CASP6 gene in tumor tissues have been reported. This work explores the effect of CASP6 tumor-associated mutations on the catalytic efficiency and structure of caspase-6. In general, these mutations showed decreased overall rates of catalytic turnover. Mutations within 8 Å of the substrate-binding pocket of caspase-6 were found to be the most catalytically deactivating. Notably, the R259H substitution decreased activity by 457-fold. This substitution disrupts the cation-π stacking interaction between Arg-259 and Trp-227, which is indispensable for proper assembly of the substrate-binding loops in caspase-6. Sequence conservation analysis at the homologous position across the caspase family suggests a role for this cation-π stacking in the catalytic function of caspases generally. These data suggest that caspase-6 deactivating mutations may contribute to multifactorial carcinogenic transformations.

摘要

不受调控,尤其是受抑制的程序性细胞死亡是许多癌细胞的显著特征之一。半胱氨酸蛋白酶caspase-6是凋亡性细胞死亡的执行者之一,在细胞凋亡调控中起关键作用。已有报道称肿瘤组织中的CASP6基因存在若干体细胞突变。这项工作探讨了CASP6肿瘤相关突变对caspase-6催化效率和结构的影响。总体而言,这些突变显示出催化周转的总体速率降低。发现caspase-6底物结合口袋8 Å范围内的突变是最具催化失活作用的。值得注意的是,R259H替代使活性降低了457倍。这种替代破坏了Arg-259与Trp-227之间的阳离子-π堆积相互作用,而这种相互作用对于caspase-6中底物结合环的正确组装是必不可少的。对caspase家族同源位置的序列保守性分析表明,这种阳离子-π堆积通常在caspases的催化功能中起作用。这些数据表明,caspase-6失活突变可能促成多因素致癌转化。

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