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首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Positive and Negative Allosteric Modulation of an α1β3γ2 γ-Aminobutyric Acid Type A (GABAA) Receptor by Binding to a Site in the Transmembrane Domain at the γ+-β− Interface
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Positive and Negative Allosteric Modulation of an α1β3γ2 γ-Aminobutyric Acid Type A (GABAA) Receptor by Binding to a Site in the Transmembrane Domain at the γ+-β− Interface

机译:通过与跨膜域中的γ+-β-界面上的位点结合对α1β3γ2γ-氨基丁酸A型(GABAA)受体进行正向和负向变构调节

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In the process of developing safer general anesthetics, isomers of anesthetic ethers and barbiturates have been discovered that act as convulsants and inhibitors of γ-aminobutyric acid type A receptors (GABAARs) rather than potentiators. It is unknown whether these convulsants act as negative allosteric modulators by binding to the intersubunit anesthetic-binding sites in the GABAAR transmembrane domain (Chiara, D. C., Jayakar, S. S., Zhou, X., Zhang, X., Savechenkov, P. Y., Bruzik, K. S., Miller, K. W., and Cohen, J. B. (2013) J. Biol. Chem. 288, 19343–19357) or to known convulsant sites in the ion channel or extracellular domains. Here, we show that S-1-methyl-5-propyl-5-(m-trifluoromethyl-diazirynylphenyl) barbituric acid (S-mTFD-MPPB), a photoreactive analog of the convulsant barbiturate S-MPPB, inhibits α1β3γ2 but potentiates α1β3 GABAAR responses. In the α1β3γ2 GABAAR, S-mTFD-MPPB binds in the transmembrane domain with high affinity to the γ+ subunit interface site with negative energetic coupling to GABA binding in the extracellular domain at the β+ subunit interfaces. GABA inhibits S-[3H]mTFD-MPPB photolabeling of γ2Ser-280 (γM2–15′) in this site. In contrast, within the same site GABA enhances photolabeling of β3Met-227 in βM1 by an anesthetic barbiturate, R-[3H]methyl-5-allyl-5-(m-trifluoromethyl-diazirynylphenyl)barbituric acid (mTFD-MPAB), which differs from S-mTFD-MPPB in structure only by chirality and two hydrogens (propyl versus allyl). S-mTFD-MPPB and R-mTFD-MPAB are predicted to bind in different orientations at the γ+ site, based upon the distance in GABAAR homology models between γ2Ser-280 and β3Met-227. These results provide an explanation for S-mTFD-MPPB inhibition of α1β3γ2 GABAAR function and provide a first demonstration that an intersubunit-binding site in the GABAAR transmembrane domain binds negative and positive allosteric modulators.
机译:在开发更安全的全身麻醉剂的过程中,已发现麻醉性醚和巴比妥酸酯的异构体可充当γ-氨基丁酸A型受体(GABAARs)而不是增强剂的惊厥剂和抑制剂。尚不清楚这些惊厥剂是否通过与GABAAR跨膜结构域中的亚基间麻醉结合位点结合而充当负变构调节剂(Chiara,DC,Jayakar,SS,Zhou,X.,Zhang,X.,Savechenkov,PY,Bruzik, KS,Miller,KW和Cohen,JB(2013)J. Biol。Chem。288,19343–19357)或离子通道或胞外域中已知的惊厥位点。在这里,我们显示S-1-甲基-5-丙基-5-(间三氟甲基-二氮杂苯基)巴比妥酸(S-mTFD-MPPB)是惊厥性巴比妥酸盐S-MPPB的光反应类似物,可抑制α1β3γ2但增强α1β3 GABAAR回应。在α1β3γ2GABAAR中,S-mTFD-MPPB在跨膜结构域中以高亲和力与γ + -亚基界面位点结合,与GABA结合负能量耦合。 β + -亚基界面处的胞外域。 GABA抑制了该位点的S-[ 3 H] mTFD-MPPB光标记γ2Ser-280(γM2-15')。相反,在同一位点,GABA增强了麻醉性巴比妥酸盐R-[ 3 H]甲基-5-烯丙基-5-(间三氟甲基-二氮烯基苯基)巴比妥利对βM1中β3Met-227的光标记作用酸(mTFD-MPAB),其结构与S-mTFD-MPPB的区别仅在于手性和两个氢(丙基与烯丙基)。根据GABAAR同源模型之间的距离,预计S-mTFD-MPPB和R-mTFD-MPAB在γ + -位点以不同的方向结合γ2Ser-280和β3Met-227。这些结果为S-mTFD-MPPB对α1β3γ2GABAAR功能的抑制提供了解释,并首次证明了GABAAR跨膜结构域中的亚基间结合位点结合了负和正变构调节剂。

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