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保守锌指基因INSM1在胚胎期和成年期神经发生过程中的祖细胞和新生神经元中瞬时表达。

Transient expression of the conserved zinc finger gene INSM1 in progenitors and nascent neurons throughout embryonic and adult neurogenesis.

作者信息

Duggan Anne, Madathany Thomas, de Castro Sandra C P, Gerrelli Dianne, Guddati Kumar, García-Añoveros Jaime

机构信息

Department of Anesthesiology, Northwestern University Feinberg School of Medicine, Chicago, Illinois 60611, USA.

出版信息

J Comp Neurol. 2008 Apr 1;507(4):1497-520. doi: 10.1002/cne.21629.

Abstract

INSM1 is a zinc-finger protein expressed in the developing nervous system and pancreas as well as in medulloblastomas and neuroendocrine tumors. With in situ hybridization combined with immunohistochemistry, we detected INSM1 mRNA in all embryonic to adult neuroproliferative areas examined: embryonic neocortex, ganglionic eminence, midbrain, retina, hindbrain, and spinal cord; autonomic, dorsal root, trigeminal and spiral ganglia; olfactory and vomeronasal organ epithelia; postnatal cerebellum; and juvenile to adult subgranular zone of dentate gyrus, subventricular zone, and rostral migratory stream leading to olfactory bulb. In most of these neurogenic areas, subsets of neuronal progenitors and nascent, but not mature, neurons express INSM1. For example, in developing cerebellum, INSM1 is present in proliferating progenitors of the outer external granule layer (EGL) and in postmitotic cells of the inner EGL, but not in mature granule cell neurons. Also, lining the neural tube from spinal cord to neocortex in mouse as well as human embryos, cells undergoing mitosis apically do not express INSM1. By contrast, nonsurface progenitors located in the basal ventricular and/or subventricular zones express INSM1. Whereas apical progenitors are proliferative and generate one or two additional progenitors, basal progenitors are thought to divide terminally and symmetrically to produce two neurons. The nematode ortholog of INSM1, EGL-46, is expressed during terminal symmetric neurogenic divisions and regulates the termination of proliferation. We propose that, in mice and humans, INSM1 is likewise expressed transiently during terminal neurogenic divisions, from late progenitors to nascent neurons, and particularly during symmetric neuronogenic divisions.

摘要

INSM1是一种锌指蛋白,在发育中的神经系统和胰腺以及髓母细胞瘤和神经内分泌肿瘤中表达。通过原位杂交结合免疫组织化学,我们在所有检查的胚胎至成人神经增殖区域中检测到INSM1 mRNA:胚胎新皮质、神经节隆起、中脑、视网膜、后脑和脊髓;自主神经节、背根神经节、三叉神经节和螺旋神经节;嗅觉和犁鼻器上皮;出生后的小脑;以及幼年至成年齿状回颗粒下区、脑室下区和通向嗅球的吻侧迁移流。在这些神经源性区域中的大多数,神经元祖细胞和新生但未成熟的神经元亚群表达INSM1。例如,在发育中的小脑中,INSM1存在于外颗粒层(EGL)的增殖祖细胞和内颗粒层的有丝分裂后细胞中,但不存在于成熟的颗粒细胞神经元中。此外,在小鼠和人类胚胎中,从脊髓到新皮质的神经管内衬,顶端进行有丝分裂的细胞不表达INSM1。相比之下,位于基底脑室和/或脑室下区的非表面祖细胞表达INSM1。顶端祖细胞具有增殖能力,可产生一到两个额外的祖细胞,而基底祖细胞被认为进行终末对称分裂以产生两个神经元。INSM1的线虫直系同源物EGL - 46在终末对称神经源性分裂期间表达,并调节增殖的终止。我们提出,在小鼠和人类中,INSM1同样在终末神经源性分裂期间短暂表达,从晚期祖细胞到新生神经元,特别是在对称神经元生成分裂期间。

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