赖氨酸117残基对肝细胞核因子1α的功能至关重要。

Lysine 117 Residue Is Essential for the Function of the Hepatocyte Nuclear Factor 1α.

作者信息

Chu Yuan, Zhao Long, Liu Xian, Chen Hui, Zhao Chen, Chen Sicong, Xiang Shensi, Lu Jun, Wang Xiaofang, Wan Yue, Dong Diandian, Yao Songhui, Li Changyan, Yin Ronghua, Ren Guangming, Yang Xiaoming, Yu Miao

机构信息

State Key Laboratory of Proteomics, Beijing Institute of Radiation Medicine, Beijing, China.

State Key Laboratory of Proteomics, Beijing Proteome Research Center, National Center for Protein Sciences (Beijing), Beijing Institute of Lifeomics, Beijing, China.

出版信息

Diabetes. 2023 Oct 1;72(10):1502-1516. doi: 10.2337/db22-0672.

DOI:10.2337/db22-0672

PMID:37440709

Abstract

UNLABELLED

Hepatocyte nuclear factor 1α (HNF1α) plays essential roles in controlling development and metabolism; its mutations are clearly linked to the occurrence of maturity-onset diabetes of the young (MODY3) in humans. Lysine 117 (K117) to glutamic acid (E117) mutation in the HNF1α gene has been clinically associated with MODY3, but no functional data on this variant are available. Here, we addressed the role of lysine 117 in HNF1α function using a knock-in animal model and site-directed mutagenesis. HNF1α K117E homozygous mice exhibited dwarfism, hepatic dysfunction, renal Fanconi syndrome, and progressive wasting syndrome. These phenotypes were very similar to those of mice with complete HNF1α deficiency, suggesting that K117 is critical to HNF1α functions. K117E homozygotes developed diabetes in the early postnatal period. The relative deficiency of serum insulin levels and the normal response to insulin treatment in homozygous mice were markedly similar to those in the MODY3 disorder in humans. Moreover, K117E heterozygous mutant causes age-dependent glucose intolerance, which is similar to the pathogenesis of MODY3 as well. K117 mutants significantly reduced the overall transactivation and DNA binding capacity of HNF1α by disrupting dimerization. Collectively, our findings reveal a previously unappreciated role of POU domain of HNF1α in homodimerization and provide important clues for identifying the molecular basis of HNF1α-related diseases such as MODY3.

ARTICLE HIGHLIGHTS

HNF1α K117E homozygous mice exhibited dwarfism, hepatic dysfunction, renal Fanconi syndrome, and progressive wasting syndrome. K117E homozygotes developed diabetes in the early postnatal period. K117E heterozygous mutant causes age-dependent glucose intolerance, which is similar to the pathogenesis of maturity-onset diabetes of the young. K117 mutants significantly reduced the overall transactivation and DNA binding capacity of HNF1α by disrupting dimerization.

摘要

未标注

肝细胞核因子1α（HNF1α）在控制发育和代谢中起关键作用；其突变与人类青年发病型糖尿病（MODY3）的发生明显相关。HNF1α基因中赖氨酸117（K117）突变为谷氨酸（E117）在临床上与MODY3相关，但关于该变体的功能数据尚无可用信息。在此，我们使用基因敲入动物模型和定点诱变来研究赖氨酸117在HNF1α功能中的作用。HNF1α K117E纯合小鼠表现出侏儒症、肝功能障碍、肾范科尼综合征和进行性消瘦综合征。这些表型与完全缺乏HNF1α的小鼠非常相似，表明K117对HNF1α功能至关重要。K117E纯合子在出生后早期即发生糖尿病。纯合小鼠血清胰岛素水平相对不足以及对胰岛素治疗的正常反应与人类MODY3疾病中的情况明显相似。此外，K117E杂合突变导致年龄依赖性葡萄糖不耐受，这也与MODY3的发病机制相似。K117突变体通过破坏二聚化显著降低了HNF1α的整体反式激活和DNA结合能力。