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在哺乳动物细胞中表达的N-甲基-D-天冬氨酸受体的分子特征为离散受体分子内三种亚基类型的共存提供了证据。

Molecular characterization of N-methyl-D-aspartate receptors expressed in mammalian cells yields evidence for the coexistence of three subunit types within a discrete receptor molecule.

作者信息

Chazot P L, Coleman S K, Cik M, Stephenson F A

机构信息

Department of Pharmaceutical Chemistry, School of Pharmacy, London, United Kingdom.

出版信息

J Biol Chem. 1994 Sep 30;269(39):24403-9.

PMID:7929101
Abstract

The N-methyl-D-aspartate R1 (NMDA R1), NMDA R2A, and NMDA R2C subunits were expressed transiently in double or triple combinations in human embryonic kidney (HEK) 293 cells. The biochemical and pharmacological properties of the cloned receptors were compared with those of adult mouse forebrain and cerebellum. Under conditions established for maximal expression, cotransfection of the NMDA R1 and R2C subunits yielded a protein detected immunologically with a molecular size of 780,000-850,000 daltons. No cell death was observed in the transfected cells, and the KD for [3H]MK801 binding to the NMDA R1/R2C receptor was 346 +/- 158 nM. This was in contrast to a value of KD = 22 +/- 9 nM found for native cerebellar receptors. Co-transfection with NMDA R1/R2A/R2C subunits with a DNA ratio, 1:3:3, resulted in the expression of a protein with a size similar to the NMDA R1/R2C combination, but the affinity of [3H]MK801 was now 22 +/- 5 nM, and the percentage cell death post-transfection was 89 +/- 17%. Immunoprecipitation assays of detergent-solubilized transfected cells with NMDA R1 subunit-specific antibodies co-precipitated the NMDA R2A and NMDA R2C subunits in 1/2A and 1/2C transfections, respectively. Similarly, immunoprecipitations with either NMDA R1 or NMDA R2C subunit-specific antibodies co-precipitated the NMDA R2A subunit in the R1/2A/2C triple transfections. These results show that the three NMDA receptor subunit types can co-assemble following their co-expression in mammalian cells with a pharmacological profile that is similar to that found for adult cerebellar NMDA receptors.

摘要

N-甲基-D-天冬氨酸受体1(NMDA R1)、NMDA R2A和NMDA R2C亚基以双重或三重组合的形式在人胚肾(HEK)293细胞中瞬时表达。将克隆受体的生化和药理学特性与成年小鼠前脑和小脑的特性进行了比较。在建立的最大表达条件下,NMDA R1和R2C亚基的共转染产生了一种通过免疫检测到的蛋白质,其分子大小为780,000 - 850,000道尔顿。在转染细胞中未观察到细胞死亡,[3H]MK801与NMDA R1/R2C受体结合的解离常数(KD)为346±158 nM。这与天然小脑受体的KD值22±9 nM形成对比。以1:3:3的DNA比例将NMDA R1/R2A/R2C亚基共转染,导致表达一种大小与NMDA R1/R2C组合相似的蛋白质,但[3H]MK801的亲和力现在为22±5 nM,转染后细胞死亡百分比为89±17%。用NMDA R1亚基特异性抗体对经去污剂溶解的转染细胞进行免疫沉淀分析,在1/2A和1/2C转染中分别共沉淀出NMDA R2A和NMDA R2C亚基。同样,在R1/2A/2C三重转染中,用NMDA R1或NMDA R2C亚基特异性抗体进行免疫沉淀时,均共沉淀出NMDA R2A亚基。这些结果表明,三种NMDA受体亚基类型在哺乳动物细胞中共表达后可以共同组装,其药理学特征与成年小脑NMDA受体相似。

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