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首页> 外文期刊>Journal of proteome research >Quantitative Mass Spectrometry Measurements Reveal Stoichiometry of Principal Postsynaptic Density Proteins
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Quantitative Mass Spectrometry Measurements Reveal Stoichiometry of Principal Postsynaptic Density Proteins

机译:定量质谱测量揭示了主要突触后密度蛋白的化学计量

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Quantitative studies are presented of postsynaptic density (PSD) fractions from rat cerebral cortex with the ultimate goal of defining the average copy numbers of proteins in the PSD complex. Highly specific and selective isotope dilution mass spectrometry assays were developed using isotopically labeled polypeptide concatemer internal standards. Interpretation of PSD protein stoichiometry was achieved as a molar ratio with respect to PSD-95 (SAP-90, DLG4), and subsequently, copy numbers were estimated using a consensus literature value for PSD-95. Average copy numbers for several proteins at the PSD were estimated for the first time, including those for AIDA-1, BRAGs, and densin. Major findings include evidence for the high copy number of AIDA-1 in the PSD (144 +/- 30)-equivalent to that of the total GKAP family of proteins (150 +/- 27)-suggesting that AIDA-I is an element of the PSD scaffold. The average copy numbers for NMDA receptor sub-units were estimated to be 66 +/- 18, 27 +/- 9, and 45 +/- 15, respectively, for GluN1, GluN2A, and GluN2B, yielding a total of 34 10 NMDA channels. Estimated average copy numbers for AMPA channels and their auxiliary sub-units TARPs were 68 +/- 36 and 144 +/- 38, respectively, with a stoichiometry of similar to 1:2 supporting the assertion that most AMPA receptors anchor to the PSD via TARP sub-units. This robust, quantitative analysis of PSD proteins improves upon and extends the list of major PSD components with assigned average copy numbers in the ongoing effort to unravel the complex molecular architecture of the PSD.
机译:定量研究提出了来自大鼠大脑皮层的突触后密度(PSD)分数,其最终目的是确定PSD复合物中蛋白质的平均拷贝数。使用同位素标记的多肽串联体内部标准物开发了高度特异性和选择性的同位素稀释质谱分析法。以相对于PSD-95的摩尔比(SAP-90,DLG4)实现PSD蛋白化学计量的解释,随后,使用PSD-95的共识文献值估算拷贝数。首次估计了PSD处几种蛋白质的平均拷贝数,包括AIDA-1,BRAG和Densin的平均拷贝数。主要发现包括PSD中AIDA-1的高拷贝数(144 +/- 30)的证据-相当于总GKAP蛋白质家族(150 +/- 27)的拷贝数-暗示AIDA-1是一个元素的PSD支架。估计GluN1,GluN2A和GluN2B的NMDA受体亚单位的平均拷贝数分别为66 +/- 18、27 +/- 9和45 +/- 15,总共产生34 10 NMDA渠道。 AMPA通道及其辅助亚单位TARP的估计平均拷贝数分别为68 +/- 36和144 +/- 38,化学计量比类似于1:2,支持大多数AMPA受体通过锚定到PSD的主张。 TARP子单元。对PSD蛋白质的这种强大的定量分析改进并扩展了具有指定平均拷贝数的主要PSD成分列表,从而不断探索PSD的复杂分子结构。

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