首页> 外文OA文献 >Use of the transport specificity ratio and cysteine-scanning mutagenesis to detect multiple substrate specificity determinants in the consensus amphipathic region of the Escherichia coli GABA (gamma-aminobutyric acid) transporter encoded by gabP.
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Use of the transport specificity ratio and cysteine-scanning mutagenesis to detect multiple substrate specificity determinants in the consensus amphipathic region of the Escherichia coli GABA (gamma-aminobutyric acid) transporter encoded by gabP.

机译:使用转运特异性比和半胱氨酸扫描诱变来检测由gabP编码的大肠杆菌GABA(γ-氨基丁酸)转运蛋白的共有两亲性区域中的多个底物特异性决定簇。

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摘要

The Escherichia coli GABA (gamma-aminobutyric acid) permease, GabP, and other members of the APC (amine/polyamine/choline) transporter superfamily share a CAR (consensus amphipathic region) that probably contributes to solute translocation. If true, then the CAR should contain structural features that act as determinants of substrate specificity ( k (cat)/ K (m)). In order to address this question, we have developed a novel, expression-independent TSR (transport specificity ratio) analysis, and applied it to a series of 69 cysteine-scanning (single-cysteine) variants. The results indicate that GabP has multiple specificity determinants (i.e. residues at which an amino acid substitution substantially perturbs the TSR). Specificity determinants were found: (i) on a hydrophobic surface of the CAR (from Leu-267 to Ala-285), (ii) on a hydrophilic surface of the CAR (from Ser-299 to Arg-318), and (iii) in a cytoplasmic loop (His-233) between transmembrane segments 6 and 7. Overall, these observations show that (i) structural features within the CAR have a role in substrate discrimination (as might be anticipated for a transport conduit) and, interestingly, (ii) the substrate discrimination task is shared among specificity determinants that appear too widely dispersed across the GabP molecule to be in simultaneous contact with the substrates. We conclude that GabP exhibits behaviour consistent with a broadly applicable specificity delocalization principle, which is demonstrated to follow naturally from the classical notion that translocation occurs synchronously with conformational transitions that change the chemical potential of the bound ligand [Tanford (1982) Proc. Natl. Acad. Sci. U.S.A. 79, 2882-2884].
机译:大肠杆菌GABA(γ-氨基丁酸)通透酶,GabP和APC(胺/多胺/胆碱)转运蛋白超家族的其他成员共享一个CAR(共有两亲性区域),可能有助于溶质易位。如果为true,则CAR应该包含充当底物特异性决定因素的结构特征(k(cat)/ K(m))。为了解决这个问题,我们开发了一种新颖的,与表达无关的TSR(运输特异性比)分析,并将其应用于一系列69个半胱氨酸扫描(单半胱氨酸)变体。结果表明,GabP具有多个特异性决定簇(即,氨基酸取代基本上干扰TSR的残基)。发现了特异性决定因素:(i)在CAR的疏水表面(从Leu-267到Ala-285),(ii)在CAR的亲水表面(从Ser-299到Arg-318),和(iii )在跨膜区段6和7之间的胞质环(His-233)中。总体而言,这些观察结果表明(i)CAR内的结构特征在底物识别中起着作用(对于运输导管可能是预期的),有趣的是,(ii)底物识别任务由特异性决定因素共同承担,这些决定因素似乎在GabP分子中分布得太广,无法与底物同时接触。我们得出的结论是,GabP表现出与广泛适用的特异性离域原理一致的行为,这从经典观念自然而然地遵循,即易位与构象转变同步发生,该构象转变改变了结合配体的化学势[Tanford(1982)Proc.Natl.Acad.Sci.USA,88:3587-8404]。 Natl。学院科学[U.S.A. 79,2882-2884]。

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