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果蝇黑腹果蝇致死(2)巨幼虫肿瘤抑制基因调控细胞命运的分子基础。

Molecular basis for the regulation of cell fate by the lethal (2) giant larvae tumour suppressor gene of Drosophila melanogaster.

作者信息

Mechler B M, Török I, Schmidt M, Opper M, Kuhn A, Merz R, Protin U

机构信息

Institute of Genetics, Johannes Gutenberg University, Mainz, Federal Republic of Germany.

出版信息

Ciba Found Symp. 1989;142:166-78; discussion 178-80. doi: 10.1002/9780470513750.ch11.

Abstract

Tumour suppressor genes act as recessive determinants of cancer. Their function is required for normal cell growth and differentiation during development. When both alleles of these developmental genes are inactivated, cell growth becomes unrestricted. In Drosophila, a series of genes have been identified which when mutated produce tissue-specific tumours. Of these the lethal(2)giant larvae (l(2)gl) gene is the best studied. Homozygous l(2)gl mutations cause the development of malignant tumours in the brain and the imaginal discs. Genomic DNA from the l(2)gl locus has been cloned, introduced back into l(2)gl mutant animals by P-element-mediated transformation and shown to restore normal development. The nucleotide sequence of the l(2)gl gene (13.1 kb) has been determined, as well as the sequences of the two classes of transcripts. These transcripts encode two polypeptides of 127 kDa and 78 kDa, respectively. Both proteins have been immunologically identified. Analyses of the spatial distribution of both l(2)gl transcripts and proteins revealed that during early embryogenesis the l(2)gl gene is uniformly expressed in all cells and tissues. In late embryos, the l(2)gl expression becomes gradually restricted to tissues presenting no morphological or neoplastic alteration in the mutant animals. Further mosaic experiments pointed out that the critical period for the establishment of tumorigenesis is limited to early embryogenesis at a time when the l(2)gl expression is most intense in all cells.

摘要

肿瘤抑制基因作为癌症的隐性决定因素。在发育过程中,它们的功能对于正常细胞生长和分化是必需的。当这些发育基因的两个等位基因都失活时,细胞生长就会不受限制。在果蝇中,已经鉴定出一系列基因,当它们发生突变时会产生组织特异性肿瘤。其中,致死(2)巨幼虫(l(2)gl)基因是研究得最深入的。纯合的l(2)gl突变会导致大脑和成虫盘出现恶性肿瘤。来自l(2)gl基因座的基因组DNA已被克隆,通过P因子介导的转化重新导入l(2)gl突变动物中,并显示可恢复正常发育。已经确定了l(2)gl基因(13.1 kb)的核苷酸序列以及两类转录本的序列。这些转录本分别编码127 kDa和78 kDa的两种多肽。两种蛋白质都已通过免疫学方法鉴定。对l(2)gl转录本和蛋白质的空间分布分析表明,在胚胎发育早期,l(2)gl基因在所有细胞和组织中均一表达。在晚期胚胎中,l(2)gl的表达逐渐局限于突变动物中未出现形态学或肿瘤性改变的组织。进一步的镶嵌实验指出,肿瘤发生确立的关键时期仅限于胚胎发育早期,此时l(2)gl在所有细胞中的表达最为强烈。

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