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鉴定人丙氨酸-乙醛酸氨基转移酶配体作为与 1 型原发性高草酸尿症相关变体的药理学伴侣。

Identification of Human Alanine-Glyoxylate Aminotransferase Ligands as Pharmacological Chaperones for Variants Associated with Primary Hyperoxaluria Type 1.

机构信息

Department of Medicine and Surgery, University of Perugia, P.le L. Severi 1, 06132 Perugia, Italy.

Department of Food and Drug, University of Parma, Parco Area delle Scienze 27/A, 43124 Parma, Italy.

出版信息

J Med Chem. 2022 Jul 28;65(14):9718-9734. doi: 10.1021/acs.jmedchem.2c00142. Epub 2022 Jul 13.

Abstract

Primary hyperoxaluria type I (PH1) is a rare kidney disease due to the deficit of alanine:glyoxylate aminotransferase (AGT), a pyridoxal-5'-phosphate-dependent enzyme responsible for liver glyoxylate detoxification, which in turn prevents oxalate formation and precipitation as kidney stones. Many PH1-associated missense mutations cause AGT misfolding. Therefore, the use of pharmacological chaperones (PCs), small molecules that promote correct folding, represents a useful therapeutic option. To identify ligands acting as PCs for AGT, we first performed a small screening of commercially available compounds. We tested each molecule by a dual approach aimed at defining the inhibition potency on purified proteins and the chaperone activity in cells expressing a misfolded variant associated with PH1. We then performed a chemical optimization campaign and tested the resulting synthetic molecules using the same approach. Overall, the results allowed us to identify a promising hit compound for AGT and draw conclusions about the requirements for optimal PC activity.

摘要

I 型原发性高草酸尿症(PH1)是一种罕见的肾脏疾病,其病因是丙氨酸:乙醛酸氨基转移酶(AGT)缺乏,该酶是一种依赖吡哆醛-5'-磷酸的酶,负责肝脏乙醛酸解毒,从而防止草酸形成和沉淀为肾结石。许多与 PH1 相关的错义突变导致 AGT 错误折叠。因此,使用药理学伴侣(PCs),即促进正确折叠的小分子,代表了一种有用的治疗选择。为了鉴定作为 AGT 的 PC 的配体,我们首先对市售化合物进行了小规模筛选。我们通过双重方法测试每种分子,旨在确定对纯化蛋白的抑制效力和在表达与 PH1 相关的错误折叠变体的细胞中的伴侣活性。然后,我们进行了化学优化运动,并使用相同的方法测试了所得的合成分子。总体而言,这些结果使我们能够鉴定出一种有前途的 AGT 命中化合物,并得出关于最佳 PC 活性要求的结论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dd07/9340776/09e756d33156/jm2c00142_0002.jpg

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