首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Developmentally regulated expression of the novel cancer anti-apoptosis gene survivin in human and mouse differentiation.
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Developmentally regulated expression of the novel cancer anti-apoptosis gene survivin in human and mouse differentiation.

机译:新型抗癌凋亡基因survivin在人类和小鼠分化中的发育调控表达。

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摘要

Inhibitors of programmed cell death (apoptosis) may regulate tissue differentiation and aberrantly promote cell survival in neoplasia. A novel apoptosis inhibitor of the IAP gene family, designated survivin, was recently found in all of the most common human cancers but not in normal, terminally differentiated adult tissues. The expression of survivin in embryonic and fetal development was investigated. Immunohistochemistry and in situ hybridization studies demonstrated strong expression of survivin in several apoptosis-regulated fetal tissues, including the stem cell layer of stratified epithelia, endocrine pancreas, and thymic medulla, with a pattern that did not overlap with that of another apoptosis inhibitor, bcl-2. A sequence-specific antibody to survivin immunoblotted a single approximately 16.5-kd survivin band in human fetal lung, liver, heart, kidney, and gastrointestinal tract. In mouse embryo, prominent and nearly ubiquitous distribution of survivin was found at embryonic day (E)11.5, whereas at E15 to -21, survivin expression was restricted to the distal bronchiolar epithelium of the lung and neural-crest-derived cells, including dorsal root ganglion neurons, hypophysis, and the choroid plexus. These data suggest that expression of survivin in embryonic and fetal development may contribute to tissue homeostasis and differentiation independently of bcl-2. Aberrations of this developmental pathway may result in prominent re-expression of survivin in neoplasia and abnormally prolonged cell viability.
机译:程序性细胞死亡(凋亡)抑制剂可调节组织分化并异常促进瘤形成中的细胞存活。最近,在所有最常见的人类癌症中,但在正常的,终末分化的成人组织中,没有发现一种称为IAP基因家族的新型凋亡抑制剂,称为survivin。研究了survivin在胚胎和胎儿发育中的表达。免疫组织化学和原位杂交研究表明,survivin在几种受凋亡调节的胎儿组织中强烈表达,包括分层上皮的干细胞层,内分泌胰腺和胸腺髓质,其模式与另一种凋亡抑制剂bcl并不重叠。 -2。针对survivin的序列特异性抗体可在人胎儿肺,肝,心脏,肾脏和胃肠道中免疫印迹单个大约16.5 kd的survivin条带。在小鼠胚胎中,在胚胎第(E)11.5天发现了survivin的突出分布,几乎无处不在,而在E15到-21时,survivin的表达仅限于肺的细支气管上皮和神经-衍生的细胞,包括背侧根神经节神经元,垂体和脉络丛。这些数据表明survivin在胚胎和胎儿发育中的表达可能有助于组织稳态和独立于bcl-2的分化。此发育途径的异常可能导致survivin在赘生物中显着重新表达,并异常延长了细胞活力。

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