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ITPase-deficient mice show growth retardation and die before weaning.

机译:缺乏ITPase的小鼠表现出生长迟缓,并在断奶前死亡。

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Inosine triphosphate pyrophosphatase (ITPase), the enzyme that hydrolyzes ITP and other deaminated purine nucleoside triphosphates to the corresponding purine nucleoside monophosphate and pyrophosphate, is encoded by the Itpa gene. In this study, we established Itpa knockout (KO) mice and used them to show that ITPase is required for the normal organization of sarcomeres in the heart. Itpa(-/-) mice died about 2 weeks after birth with features of growth retardation and cardiac myofiber disarray, similar to the phenotype of the cardiac alpha-actin KO mouse. Inosine nucleotides were found to accumulate in both the nucleotide pool and RNA of Itpa(-/-) mice. These data suggest that the role of ITPase in mice is to exclude ITP from the ATP pool, and the main target substrate of this enzyme is rITP. Our data also suggest that cardiomyopathy, which is mainly caused by mutations in sarcomeric protein-encoding genes, is also caused by a defect in maintaining the quality of the ATP pool, which is an essential requirement for sarcomere function.
机译:肌苷三磷酸焦磷酸酶(ITPase)是将ITP和其他脱氨基嘌呤核苷三磷酸水解为相应的嘌呤核苷单磷酸和焦磷酸的酶,由Itpa基因编码。在这项研究中,我们建立了Itpa基因敲除(KO)小鼠,并用它们来证明ITPase是心脏肉瘤正常组织所必需的。 Itpa(-/-)小鼠出生后约2周死亡,具有生长迟缓和心肌肌纤维紊乱的特征,类似于心脏α-肌动蛋白KO小鼠的表型。发现肌苷核苷酸积累在Itpa(-/-)小鼠的核苷酸库和RNA中。这些数据表明,ITPase在小鼠中的作用是将ITP从ATP库中排除,该酶的主要靶标底物是rITP。我们的数据还表明,心肌病主要由肌节蛋白编码基因的突变引起,也由维持ATP库质量的缺陷引起,这是肌节功能的基本要求。

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