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黑腹果蝇67A-D染色体区域的遗传分析。

Genetic analysis of chromosomal region 67A-D of Drosophila melanogaster.

作者信息

Leicht B G, Bonner J J

机构信息

Department of Biology, Indiana University, Bloomington 47405.

出版信息

Genetics. 1988 Jul;119(3):579-93. doi: 10.1093/genetics/119.3.579.

Abstract

In an effort to (1) characterize the 67 interval of chromosome 3 of Drosophila melanogaster genetically and (2) isolate mutations of the 67B1 small heat shock protein (hsp) gene cluster specifically, we undertook a mutational analysis of the 67A-D subinterval. Using a deficiency of the 67A2 to 67D11-13 region, Df(3L)AC1, we screened 8700 diepoxybutane-treated chromosomes and 7800 ethyl methanesulfonate-treated chromosomes for visible and lethal mutations throughout this interval and recovered 74 independent recessive lethal mutations, but no visible mutations. One of the lethal mutations, d29A6, was identified as an overlapping deficiency extending from 66F3 to 67B1. An additional 6000 diepoxybutane-treated chromosomes were screened for lethality over d29A6, yielding another four lethal mutations within the 67A2-B1 subinterval. These 78 lethal mutations, along with two others isolated in other laboratories, define 23 essential loci--6 within the 67A2-B1 subinterval and 17 within the 67A2 to D11-13 subinterval. Many of these loci appear to be required for imaginal development only, exhibiting late larval to pharate adult lethal phases. Examination of the 67A2-B1 lethal complementation groups for (1) earlier onset of lethality following a heat shock, (2) missing or altered small hsps on two-dimensional protein gels, and (3) restoration of viability by transformed wild-type copies of the small hsp genes indicates that none of these mutations affect the small hsps. On the basis of this analysis and the known homology of the genes, we conclude that the small hsps are functionally equivalent.

摘要

为了(1)从遗传学角度对黑腹果蝇3号染色体的67区间进行特征描述,以及(2)特异性分离67B1小热休克蛋白(hsp)基因簇的突变,我们对67A - D子区间进行了突变分析。利用67A2至67D11 - 13区域的缺失品系Df(3L)AC1,我们在整个该区间筛选了8700条经二环氧丁烷处理的染色体和7800条经甲磺酸乙酯处理的染色体,以寻找可见和致死突变,共获得74个独立的隐性致死突变,但未发现可见突变。其中一个致死突变d29A6被鉴定为一个重叠缺失,范围从66F3延伸至67B1。另外又对6000条经二环氧丁烷处理的染色体进行了针对d29A6的致死性筛选,在67A2 - B1子区间内又获得了另外四个致死突变。这78个致死突变,连同在其他实验室分离到的另外两个突变,定义了23个必需基因座——6个在67A2 - B1子区间内,17个在67A2至D11 - 13子区间内。这些基因座中的许多似乎仅在成虫发育中是必需的,表现出从幼虫后期到成虫前期的致死阶段。对67A2 - B1致死互补群进行如下检测:(1)热休克后致死性的更早出现,(2)二维蛋白质凝胶上小热休克蛋白的缺失或改变,以及(3)小热休克蛋白基因的野生型转化拷贝对活力的恢复情况,结果表明这些突变均未影响小热休克蛋白。基于这一分析以及基因的已知同源性,我们得出结论,小热休克蛋白在功能上是等效的。

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