探究钠偶联中性氨基酸转运体 SNAT2 结合袋的氨基酸类似物的结构-活性关系

IF 3 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Sebastian Jakobsen, Maria Pedersen, Carsten Uhd Nielsen
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引用次数: 0

摘要

钠偶联中性氨基酸转运体 SNAT2(SLC38A2)已被证明具有重要的生理功能,并与癌症等多种疾病有关。然而,针对这种转运体的化合物很少被发现,人们对 SNAT2 结合的结构要求也知之甚少。本研究旨在利用氨基酸类似物建立 SNAT2 的基本结构-活性关系。首先研究了这些类似物在高渗处理的 PC-3 细胞中抑制 SNAT2 介导的 3H 甘氨酸摄取的能力。然后使用 FLIPR 膜电位测定法和邻苯二甲醛衍生化细胞内氨基,随后使用 HPLC-Fl 进行定量,以确定底物。结果表明,C 端的酯类衍生物能保持 SNAT2 的亲和力,这表明负电荷并不那么重要。另一方面,底物 N 端的正电荷以及能向结合位点提供至少两个氢键的能力对于 SNAT2 识别胺似乎很重要。带侧链电荷的氨基酸一般对 SNAT2 没有亲和力,但其不带电荷的衍生物能够抑制 SNAT2 介导的 3H 甘氨酸摄取,同时也表明长度相当的氨基酸对 SNAT2 仍有亲和力。几种氨基酸类似物似乎是 SNAT2 的新型底物,而 γ-苄基 L-谷氨酸似乎不能被 SNAT2 有效转运。对这一结构的深入研究可能有助于发现 SNAT2 的非转运抑制剂。因此,本研究为了解 SNAT2 的基本结构结合要求提供了有价值的见解,有助于今后发现靶向 SNAT2 的化合物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Structure-activity relationship of amino acid analogs to probe the binding pocket of sodium-coupled neutral amino acid transporter SNAT2

The sodium-coupled neutral amino acid transporter SNAT2 (SLC38A2) has been shown to have important physiological functions and is implicated in various diseases like cancer. However, few compounds targeting this transporter have been identified and little is known about the structural requirements for SNAT2 binding. In this study, the aim was to establish the basic structure-activity relationship for SNAT2 using amino acid analogs. These analogs were first studied for their ability to inhibit SNAT2-mediated 3H-glycine uptake in hyperosmotically treated PC-3 cells. Then to identify substrates a FLIPR membrane potential assay and o-phthalaldehyde derivatization of intracellular amino with subsequent quantification using HPLC-Fl was used. The results showed that ester derivatives of the C-terminus maintained SNAT2 affinity, suggesting that the negative charge was less important. On the other hand, the positive charge at the N-terminus of the substrate and the ability to donate at least two hydrogen bonds to the binding site appeared important for SNAT2 recognition of the amine. Side chain charged amino acids generally had no affinity for SNAT2, but their non-charged derivatives were able to inhibit SNAT2-mediated 3H-glycine uptake, while also showing that amino acids of a notable length still had affinity for SNAT2. Several amino acid analogs appeared to be novel substrates of SNAT2, while γ-benzyl L-glutamate seemed to be inefficiently translocated by SNAT2. Elaborating on this structure could lead to the discovery of non-translocated inhibitors of SNAT2. Thus, the present study provides valuable insights into the basic structural binding requirements for SNAT2 and can aid the future discovery of compounds that target SNAT2.

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来源期刊
Amino Acids
Amino Acids 生物-生化与分子生物学
CiteScore
6.40
自引率
5.70%
发文量
99
审稿时长
2.2 months
期刊介绍: Amino Acids publishes contributions from all fields of amino acid and protein research: analysis, separation, synthesis, biosynthesis, cross linking amino acids, racemization/enantiomers, modification of amino acids as phosphorylation, methylation, acetylation, glycosylation and nonenzymatic glycosylation, new roles for amino acids in physiology and pathophysiology, biology, amino acid analogues and derivatives, polyamines, radiated amino acids, peptides, stable isotopes and isotopes of amino acids. Applications in medicine, food chemistry, nutrition, gastroenterology, nephrology, neurochemistry, pharmacology, excitatory amino acids are just some of the topics covered. Fields of interest include: Biochemistry, food chemistry, nutrition, neurology, psychiatry, pharmacology, nephrology, gastroenterology, microbiology
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