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突出蛋白(果蝇弯曲基因座产物)的同步和异步肌肉同工型都含有功能性激酶结构域。

Both synchronous and asynchronous muscle isoforms of projectin (the Drosophila bent locus product) contain functional kinase domains.

作者信息

Ayme-Southgate A, Southgate R, Saide J, Benian G M, Pardue M L

机构信息

Department of Molecular Biology, Lehigh University, Bethlehem, Pennsylvania 18015.

出版信息

J Cell Biol. 1995 Feb;128(3):393-403. doi: 10.1083/jcb.128.3.393.

Abstract

In Drosophila, the large muscle protein, projectin, has very different localizations in synchronous and asynchronous muscles, suggesting that projectin has different functions in different muscle types. The multiple projectin isoforms are encoded by a single gene; however they differ significantly in size (as detected by gel mobility) and show differences in some peptide fragments, presumably indicating alternative splicing or termination. We now report additional sequence of the projectin gene, showing a kinase domain and flanking regions highly similar to equivalent regions of twitchin, including a possible autoinhibitory region. In spite of apparent differences in function, all isoforms of projectin have the kinase domain and all are capable of autophosphorylation in vitro. The projectin gene is in polytene region 102C/D where the bentD phenotype maps. The recessive lethality of bentD is associated with a breakpoint that removes sequence of the projectin kinase domain. We find that different alleles of the highly mutable recessive lethal complementation group, l(4)2, also have defects in different parts of the projectin sequence, both NH2-terminal and COOH-terminal to the bentD breakpoint. These alleles are therefore renamed as alleles of the bent locus. Adults heterozygous for projectin mutations show little, if any, effect of one defective gene copy, but homozygosity for any of the defects is lethal. The times of death can vary with allele. Some alleles kill the embryos, others are larval lethal. These molecular studies begin to explain why genetic studies suggested that l(4)2 was a complex (or pseudoallelic) locus.

摘要

在果蝇中,大型肌肉蛋白——肌联蛋白,在同步肌和非同步肌中有非常不同的定位,这表明肌联蛋白在不同类型的肌肉中具有不同的功能。多种肌联蛋白同工型由单个基因编码;然而,它们在大小上有显著差异(通过凝胶迁移检测),并且在一些肽片段上也存在差异,推测这表明存在可变剪接或终止。我们现在报告肌联蛋白基因的额外序列,显示出一个激酶结构域及其侧翼区域与肌动蛋白结合蛋白的等效区域高度相似,包括一个可能的自抑制区域。尽管功能上存在明显差异,但肌联蛋白的所有同工型都具有激酶结构域,并且都能够在体外进行自磷酸化。肌联蛋白基因位于多线染色体区域102C/D,弯曲D(bentD)表型定位于此。弯曲D的隐性致死性与一个去除肌联蛋白激酶结构域序列的断点相关。我们发现,高度可变的隐性致死互补群l(4)2的不同等位基因在肌联蛋白序列的不同部分也存在缺陷,这些部分位于弯曲D断点的氨基末端和羧基末端。因此,这些等位基因被重新命名为弯曲基因座的等位基因。肌联蛋白突变杂合的成虫几乎不受一个缺陷基因拷贝的影响,但任何一种缺陷的纯合性都是致死的。死亡时间可能因等位基因而异。一些等位基因会杀死胚胎,另一些则是幼虫致死。这些分子研究开始解释为什么遗传学研究表明l(4)2是一个复杂(或拟等位基因)基因座。

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