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计算预测和鉴定小鼠 Prkaca 基因普遍表达的新剪接变异体。

Computational prediction and characterisation of ubiquitously expressed new splice variant of Prkaca gene in mouse.

机构信息

Faculty of Life Sciences, Department of Biochemistry, A.M. University, Aligarh 202 002, Uttar Pradesh, India.

出版信息

Cell Biol Int. 2013 Jul;37(7):687-93. doi: 10.1002/cbin.10080. Epub 2013 Mar 26.

DOI:10.1002/cbin.10080
PMID:23456795
Abstract

Prkaca gene of mouse encodes for a cAMP dependent protein kinase catalytic alpha subunit. PKA occurs naturally as a 4-membered structure having two regulatory (R) and two catalytic (C) subunits each encoded by separate gene. Alternatively spliced two transcript variants are known for the Prkaca gene, which encode for two isoforms of PKA C-subunits, namely Cα1 and Cα2. These isoforms arise as a result of alternative splicing of the first coding exon with the internal exons. We have identified a new transcript variant using combinatorial approach of bioinformatics and molecular biology techniques involving RT-PCR, semi-nested PCR and sequencing. The new transcript variant encoding Cα3 isoform has N-terminus that differs from Cα1 and Cα2 isoforms. Cα3 isoform also arise as a result of alternative splicing of first coding exon with the internal exon. Newly identified transcript is expressed ubiquitously in different tissues examined.

摘要

小鼠的 Prkaca 基因编码一个依赖 cAMP 的蛋白激酶催化α亚基。PKA 自然存在于由两个调节 (R) 和两个催化 (C) 亚基组成的四聚体结构中,每个亚基分别由单独的基因编码。Prkaca 基因有两种选择性剪接的转录变体,它们编码两种 PKA C 亚基同工型,即 Cα1 和 Cα2。这些同工型是由于第一个编码外显子与内部外显子的选择性剪接而产生的。我们使用涉及 RT-PCR、半巢式 PCR 和测序的生物信息学和分子生物学技术的组合方法鉴定了一种新的转录变体。编码 Cα3 同工型的新转录变体的 N 端与 Cα1 和 Cα2 同工型不同。Cα3 同工型也是由于第一个编码外显子与内部外显子的选择性剪接而产生的。新鉴定的转录本在不同检查的组织中普遍表达。

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