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首页> 外文期刊>BMC Molecular Biology >The calcium channel beta2(CACNB2)subunit repertoire in teleosts.
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The calcium channel beta2(CACNB2)subunit repertoire in teleosts.

机译:硬骨鱼中的钙通道β2(CACNB2)亚基。

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摘要

Background Cardiomyocyte contraction is initiated by influx of extracellular calcium through voltage- gated calcium channels.These oligomeric channels utilize auxiliary beta subunits to chaperone the pore-formingαsubunit to the plasma membrane,and to modulate channel electrophysiology.Several beta subunit family members are detected by RT-PCR in the embryonic heart.Null mutations in mouse beta2,but not in the other three beta family members,are embryonic lethal at E10.5 due to defects in cardiac contractility. However,a drawback of the mouse model is that embryonic heart rhythm is difficult to study in live embryos due to their intra-uterine development.Moreover,phenotypes may be obscured by secondary effects of hypoxia.As a first step towards developing a model for contributions ofβsubunits to the onset of embryonic heart rhythm,we characterized the structure and expression of beta2 subunits in zebrafish and other teleosts. Results Cloning of two zebrafish beta2 subunit genes(beta2.1 and beta2.2)indicated they are membrane- associated guanylate kinase(MAGUK)-family genes.Zebrafish beta2 genes show high conservation with mammals within the SH3 and guanylate kinase domains that comprise the"core"of MAGUK proteins,but beta2.2 is much more divergent in sequence than beta2.1. Alternative splicing occurs at the N-terminus and within the internal HOOK domain.In bothβ2 genes,alternative short ATG-containing first exons are separated by some of the largest introns in the genome,suggesting that individual transcript variants could be subject to independent cis-regulatory control.In the Tetraodon nigrovidis and Fugurubripes genomes,we identified single beta2 subunit gene loci.Comparative analysis of the teleost and human beta2 loci indicates that the short 5'exon sequences are highly conserved. A subset of 5'exons appear to be unique to teleost genomes,while others are shared with mammals.Alternative splicing is temporally and spatially regulated in embryo and adult. Moreover,a different subset of splicedβ2 transcript variants is detected in the embryonic heart compared to the adult. Conclusions These studies refine our understanding of beta2 subunit diversity arising from alternative splicing,and provide the groundwork for functional analysis of beta2 subunit diversity in the embryonic heart.
机译:背景心肌细胞的收缩是通过电压门控钙通道通过细胞外钙的流入而引发的。这些寡聚通道利用辅助β亚基来陪伴质膜的成孔α亚基,并调节通道的电生理。RT检测到了多个β亚基家族成员。 -PCR在胚胎心脏中。由于心脏收缩力的缺陷,小鼠beta2中的空突变(在其他三个beta家族成员中没有)在E10.5处具有胚胎致死性。然而,小鼠模型的缺点是由于活体胚胎的子宫内发育,很难在活胚胎中研究胚胎心律。此外,低氧的继发性效应可能会掩盖表型。作为建立供体模型的第一步β亚基与胚胎心律的发作有关,我们表征了斑马鱼和其他硬骨鱼中β2亚基的结构和表达。结果克隆了两个斑马鱼的beta2亚基基因(beta2.1和beta2.2),表明它们是膜相关的鸟苷酸激酶(MAGUK)家族基因。斑马鱼的beta2基因对SH3和鸟苷酸激酶结构域内的哺乳动物具有高度的保守性。 MAGUK蛋白的“核心”,但beta2.2的序列差异比beta2.1大得多。选择性剪接发生在N末端和内部HOOK结构域内。在两个β2基因中,含有短ATG的第一短外显子被基因组中一些最大的内含子隔开,这表明各个转录物变体可能受到独立的顺式作用。调节控制。在四齿龙和古古里普里斯基因组中,我们鉴定出单个beta2亚基基因位点。硬骨鱼和人beta2位点的比较分析表明,短的5'外显子序列是高度保守的。 5'外显子的一个子集似乎是硬骨鱼基因组所独有的,而其他的则与哺乳动物共有。选择性剪接在胚胎和成体中在时间和空间上受到调节。而且,与成人相比,在胚胎心脏中检测到剪接的β2转录物变体的不同子集。结论这些研究完善了我们对替代剪接产生的β2亚基多样性的理解,并为胚胎心脏中β2亚基多样性的功能分析提供了基础。

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