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The crystal structure of carnitine palmitoyltransferase 2 and implications for diabetes treatment

机译:肉碱棕榈酰转移酶2的晶体结构及其对糖尿病的治疗意义

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摘要

Carnitine palmitoyltransferases 1 and 2 (CPTs) facilitate the import of long-chain fatty acids into mitochondria. Modulation of the catalytic activity of the CPT system is currently under investigation for the development of novel drags against diabetes mellitus. We report here the 1.6 angstrom resolution structure of the full-length mitochondrial membrane protein CPT-2. The structure of CPT-2 in complex with the generic CPT inhibitor ST1326 ([R]-N-[tetradecylcarbamoyl]-aminocarnitine), a substrate analog mimicking palmitoylcarnitine and currently in clinical trials for diabetes mellitus treatment, was solved at 2.5 angstrom resolution. These structures of CPT-2 provide insight into the function of residues involved in substrate binding and determination of substrate specificity, thereby facilitating the rational design of antidiabetic drugs. We identify a sequence insertion found in CPT-2 that mediates membrane localization. Mapping of mutations described for CPT-2 deficiency, a hereditary disorder of lipid metabolism, implies effects on substrate recognition and structural integrity of CPT-2.
机译:肉碱棕榈酰转移酶1和2(CPT)有助于将长链脂肪酸导入线粒体。当前正在研究CPT系统的催化活性的调节,以开发抗糖尿病的新型药物。我们在这里报告全长线粒体膜蛋白CPT-2的1.6埃分辨率结构。与CPT通用抑制剂ST1326([R] -N- [十四烷基氨基甲酰基]-氨基肉碱)(一种模仿棕榈酰肉碱的底物类似物,目前正在糖尿病治疗的临床试验)复合的CPT-2的结构分辨率为2.5埃。 CPT-2的这些结构提供了对参与底物结合和确定底物特异性的残基功能的洞察力,从而促进了抗糖尿病药物的合理设计。我们确定在CPT-2中发现的介导膜定位的序列插入。针对CPT-2缺乏症(一种脂类代谢的遗传性疾病)描述的突变图意味着对CPT-2的底物识别和结构完整性有影响。

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