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H⁺/氨基酸转运体大鼠PAT2(Slc36a2)的底物特异性及功能表征

Substrate specificity and functional characterisation of the H+/amino acid transporter rat PAT2 (Slc36a2).

作者信息

Kennedy David J, Gatfield Kelly M, Winpenny John P, Ganapathy Vadivel, Thwaites David T

机构信息

Institute for Cell & Molecular Biosciences, Faculty of Medical Sciences, University of Newcastle upon Tyne, Framlington Place, Newcastle upon Tyne NE2 4HH, UK.

出版信息

Br J Pharmacol. 2005 Jan;144(1):28-41. doi: 10.1038/sj.bjp.0706029.

Abstract

Functional characteristics and substrate specificity of the rat proton-coupled amino acid transporter 2 (rat PAT2 (rPAT2)) were determined following expression in Xenopus laevis oocytes using radiolabelled uptake measurements, competition experiments and measurements of substrate-evoked current using the two-electrode voltage-clamp technique. The aim of the investigation was to determine the structural requirements and structural limitations of potential substrates for rPAT2. Amino (and imino) acid transport via rPAT2 was pH-dependent, Na(+)-independent and electrogenic. At extracellular pH 5.5 (in Na(+)-free conditions) proline uptake was saturable (Km 172+/-41 muM), demonstrating that rPAT2 is, relative to PAT1, a high-affinity transporter.PAT2 preferred substrates are L-alpha-amino acids with small aliphatic side chains (e.g. the methyl group in alanine) and 4- or 5-membered heterocyclic amino and imino acids such as 2-azetidine-carboxylate, proline and cycloserine, where both D- and L-enantiomers are transported. The major restrictions on transport are side chain size (the ethyl group of alpha-aminobutyric acid is too large) and backbone length, where the separation of the carboxyl and amino groups by only two CH(2) groups, as in beta-alanine, is enough to reduce transport. Methylation of the amino group is tolerated (e.g. sarcosine) but increasing methylation, as in betaine, decreases transport. A free carboxyl group is preferred as O-methyl esters show either reduced transport (alanine-O-methyl ester) or are excluded. The structural characteristics that determine the substrate specificity of rPAT2 have been identified. This information should prove valuable in the design of selective substrates/inhibitors for PAT1 and PAT2.

摘要

利用放射性标记摄取测量、竞争实验以及采用双电极电压钳技术测量底物诱发电流等方法,在非洲爪蟾卵母细胞中表达大鼠质子偶联氨基酸转运体2(大鼠PAT2,即rPAT2)后,测定了其功能特性和底物特异性。该研究的目的是确定rPAT2潜在底物的结构要求和结构限制。通过rPAT2进行的氨基酸(和亚氨基酸)转运是pH依赖性、Na⁺非依赖性且生电性的。在细胞外pH 5.5(无Na⁺条件下)时,脯氨酸摄取呈饱和状态(Km为172±41 μM),表明相对于PAT1,rPAT2是一种高亲和力转运体。PAT2的优选底物是具有小脂肪族侧链的L-α-氨基酸(例如丙氨酸中的甲基)以及4或5元杂环氨基酸和亚氨基酸,如2-氮杂环丁烷羧酸、脯氨酸和环丝氨酸,D型和L型对映体均可被转运。转运的主要限制因素是侧链大小(α-氨基丁酸的乙基太大)和主链长度,其中像β-丙氨酸那样仅由两个CH₂基团分隔羧基和氨基就足以降低转运。氨基的甲基化是可以耐受的(例如肌氨酸),但像甜菜碱那样甲基化程度增加则会降低转运。优选游离羧基,因为O-甲酯要么转运减少(丙氨酸-O-甲酯),要么被排除在外。已确定了决定rPAT2底物特异性的结构特征。该信息在设计PAT1和PAT2的选择性底物/抑制剂方面应具有重要价值。

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