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胎儿和成年大鼠肌肉乙酰胆碱受体通道电导的结构决定因素。

Structural determinants of channel conductance in fetal and adult rat muscle acetylcholine receptors.

作者信息

Herlitze S, Villarroel A, Witzemann V, Koenen M, Sakmann B

机构信息

Abteilung Zellphysiologie, Max-Planck-Institut für medizinische Forschung, Heidelberg, Germany.

出版信息

J Physiol. 1996 May 1;492 ( Pt 3)(Pt 3):775-87. doi: 10.1113/jphysiol.1996.sp021345.

Abstract
  1. The structural basis of the developmentally regulated increase in endplate channel conductance in rat, where the gamma-subunit of the fetal muscle acetylcholine receptor (gamma-AChR) is replaced by the epsilon-subunit in the adult muscle receptor (epsilon-AChR), was investigated by analysing the structure of gamma- and epsilon-subunit genes and by expressing recombinant AChR channels of different molecular composition in Xenopus oocytes and measuring their single-channel conductance. 2. The gamma- and epsilon-subunit genes each have twelve exons. In both subunits, the four homologous segments, designated M1, M2, M3 and M4, which are thought to contribute to the formation of the pore, are encoded by four separate exons, E7, E8, E9 and E12. 3. Chimaeric epsilon(gamma)- or gamma(epsilon)-subunits were constructed from the parental epsilon- and gamma-subunits, respectively. Exchanging the four hydrophobic segments (M1-M4) of the gamma-subunit for those of the epsilon-subunit and vice versa completely reversed the difference in conductance between gamma-AChR and epsilon-AChR channels. 4. Effects of single- and multiple-point mutations in M1-M4 segments of gamma- and epsilon-subunits indicate that the major determinants of the difference in conductance between fetal and adult endplate channels are located in the M2 segment. The key differences are the exchange of alanine/threonine (gamma-subunit) for serine/isoleucine (epsilon-subunit) in M2, and the lysine (gamma-subunit) for glutamine (epsilon-subunit) exchanges in the regions flanking the M2 segment.
摘要
  1. 研究了大鼠终板通道电导发育调控性增加的结构基础。在大鼠中,胎儿肌肉乙酰胆碱受体(γ-AChR)的γ亚基在成体肌肉受体(ε-AChR)中被ε亚基取代。通过分析γ亚基和ε亚基基因的结构,以及在非洲爪蟾卵母细胞中表达不同分子组成的重组AChR通道并测量其单通道电导来进行研究。2. γ亚基和ε亚基基因各有12个外显子。在这两个亚基中,被认为有助于形成孔道的四个同源片段,即M1、M2、M3和M4,由四个单独的外显子E7、E8、E9和E12编码。3. 分别从亲代ε亚基和γ亚基构建了嵌合的ε(γ)-或γ(ε)-亚基。将γ亚基的四个疏水片段(M1-M4)与ε亚基的进行交换,反之亦然,完全逆转了γ-AChR和ε-AChR通道之间的电导差异。4. γ亚基和ε亚基M1-M4片段中单点和多点突变的影响表明,胎儿和成体终板通道电导差异的主要决定因素位于M2片段。关键差异在于M2中丙氨酸/苏氨酸(γ亚基)被丝氨酸/异亮氨酸(ε亚基)取代,以及M2片段侧翼区域赖氨酸(γ亚基)被谷氨酰胺(ε亚基)取代。
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fe8/1158899/30734ffc5457/jphysiol00295-0148-a.jpg

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