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同源异型基因产物对细胞分化和增殖的控制。

The homeotic gene products in the control of cell differentiation and proliferation.

作者信息

Corte G, Airoldi I, Briata P, Corsetti M T, Daga A, Massa A, Sanseverino L, Lancia F

机构信息

Istituto di Chimica Biologica, dell'Università di Genova, Italy.

出版信息

Cancer Detect Prev. 1993;17(2):261-6.

PMID:8104694
Abstract

Embryo development is controlled by a successive series of genes that provide each cell in the growing embryo with precise position information. Knowledge of these genes is known most completely from Drosophila, where a simple initial pattern generated by maternal effect genes is gradually segmented by the sequential transient expression of three successive series of genes: the gap genes, the pair-rule genes, and the segment polarity genes. Superimposing their action on the preexisting segments, these homeotic genes cause unique and often very distinctive patterns of differentiation for different segments. In humans, about 40 homeotic genes have been identified and are grouped into four clusters on chromosomes 2, 7, 12, and 17, whose organization reflects their spatial and temporal expression. Several homeotic genes have been found expressed not only in embryonic tissues, but also in adult tissues, most notably in the hematopoietic lineage, and also in tumors, especially leukemia, teratocarcinoma, and neuroblastoma, wherein their expression pattern is modified in a complex manner by retinoic acid. The target genes of the transcription factors encoded by the homeotic genes are largely unknown, but recent reports indicate that they may regulate the expression of adhesion molecules on the membrane and the production of components of the extracellular matrix. Abnormal expression of these genes can therefore affect not only cell proliferation, but also the spread of cells to aberrant locations.

摘要

胚胎发育由一系列连续的基因控制,这些基因赋予发育中的胚胎中的每个细胞精确的位置信息。对这些基因的了解在果蝇中最为全面,在果蝇中,由母体效应基因产生的简单初始模式通过三个连续系列基因(间隙基因、成对规则基因和体节极性基因)的顺序短暂表达逐渐被分割。这些同源异型基因将它们的作用叠加在预先存在的体节上,导致不同体节出现独特且通常非常明显的分化模式。在人类中,已鉴定出约40个同源异型基因,并将它们分为4个簇,分别位于2号、7号、12号和17号染色体上,它们的组织方式反映了它们的时空表达。已发现几个同源异型基因不仅在胚胎组织中表达,也在成体组织中表达,最显著的是在造血谱系中,在肿瘤中也有表达,尤其是白血病、畸胎瘤和神经母细胞瘤,在这些肿瘤中,它们的表达模式会被视黄酸以复杂的方式修饰。同源异型基因编码的转录因子的靶基因大多未知,但最近的报告表明,它们可能调节膜上黏附分子的表达以及细胞外基质成分的产生。因此,这些基因的异常表达不仅会影响细胞增殖,还会影响细胞向异常位置的扩散。

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