A human-specific cytotoxic neopeptide generated by the deafness gene Cingulin.

IF 6.6 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Yuhang Huang, Linqing Zhang, Yuecen Sun, Qing Liu, Jie Chen, Xiaoyun Qian, Xia Gao, Guang-Jie Zhu, Guoqiang Wan
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Abstract

Accumulation of mutant proteins in cells can induce proteinopathies and cause functional damage to organs. Recently, the Cingulin (CGN) protein has been shown to maintain the morphology of cuticular plates of inner ear hair cells and a frameshift mutation in CGN causes autosomal dominant non-syndromic hearing loss. Here, we find that the mutant CGN proteins form insoluble aggregates which accumulate intracellularly and lead to cell death. Expression of the mutant CGN in the inner ear results in severe hair cell death and hearing loss in mice, resembling the auditory phenotype in human patients. Interestingly, a human-specific residue (V1112) in the neopeptide generated by the frameshift mutation is critical for the aggregation and cytotoxicity of the mutant human CGN. Moreover, the expression of heat shock factor 1 (HSF1) decreases the accumulation of insoluble mutant CGN aggregates and rescues cell death. In summary, these findings identify mutant-specific toxic polypeptides as a disease-causing mechanism of the deafness mutation in CGN, which can be targeted by the expression of the cell chaperone response regulator HSF1.

由耳聋基因 Cingulin 生成的人类特异性细胞毒性新肽。
突变蛋白质在细胞中的积累可诱发蛋白质病,并对器官造成功能性损害。最近,Cingulin(CGN)蛋白被证明能维持内耳毛细胞角质板的形态,CGN的框架移位突变会导致常染色体显性非综合征性听力损失。在这里,我们发现突变型 CGN 蛋白会形成不溶性的聚集体,聚集在细胞内导致细胞死亡。在小鼠内耳中表达突变型 CGN 会导致严重的毛细胞死亡和听力损失,这与人类患者的听觉表型相似。有趣的是,框架移位突变产生的新肽中的一个人类特异残基(V1112)对于突变型人类 CGN 的聚集和细胞毒性至关重要。此外,热休克因子1(HSF1)的表达可减少不溶性突变型CGN聚集体的积累并挽救细胞死亡。总之,这些发现确定了突变体特异性毒性多肽是 CGN 中耳聋突变的致病机制,而细胞伴侣反应调节因子 HSF1 的表达可以针对这一机制。
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来源期刊
Journal of Genetics and Genomics
Journal of Genetics and Genomics 生物-生化与分子生物学
CiteScore
8.20
自引率
3.40%
发文量
4756
审稿时长
14 days
期刊介绍: The Journal of Genetics and Genomics (JGG, formerly known as Acta Genetica Sinica ) is an international journal publishing peer-reviewed articles of novel and significant discoveries in the fields of genetics and genomics. Topics of particular interest include but are not limited to molecular genetics, developmental genetics, cytogenetics, epigenetics, medical genetics, population and evolutionary genetics, genomics and functional genomics as well as bioinformatics and computational biology.
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