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在端脑神经元分化过程中,神经纤维瘤病1(NF1)基因产物神经纤维瘤蛋白与F-肌动蛋白或微管细胞骨架的差异定位。

Differential localization of the neurofibromatosis 1 (NF1) gene product, neurofibromin, with the F-actin or microtubule cytoskeleton during differentiation of telencephalic neurons.

作者信息

Li C, Cheng Y, Gutmann D A, Mangoura D

机构信息

Department of Pediatrics, The University of Chicago, Chicago, IL 60637, USA.

出版信息

Brain Res Dev Brain Res. 2001 Oct 24;130(2):231-48. doi: 10.1016/s0165-3806(01)00190-0.

Abstract

The protein product of the neurofibromatosis 1 gene, neurofibromin, is abundantly expressed in the cerebral cortex during development, but its physiological role remains unknown. To gain insights into the functions of neurofibromin in neurons, we examined patterns of expression and subcellular localization of neurofibromin during neuronal differentiation. Western blot analysis of telencephali homogenates throughout chick embryogenesis revealed that neurofibromin expression increased during embryonic development. Further analysis showed that telencephalic neurons were also enriched in neurofibromin in culture and that a biphasic gain in expression correlated well with both phases of differentiation in culture, first with a massive outgrowth of processes and gains in neurotransmitter phenotype differentiation, and then with synapse formation. Compared to proteins associated with distinct cytoskeleton systems, the pattern of neurofibromin expression correlated closely with that of the cortical cytoskeleton protein paxillin. Moreover, analysis of immunofluorescence staining of neurofibromin showed that in the presence of a protein crosslinker which preserves both soluble and filamentous cytoskeleton proteins after extraction with Triton X-100, neurofibromin colocalized with F-actin only during the first differentiation phase. This colocalization persisted when the actin cytoskeleton was collapsed with cytochalasin D treatment. In contrast, during the second phase of differentiation neurofibromin colocalized with microtubules, but not F-actin, and the staining pattern was disrupted with nocodazole, but not cytochalasin. A constant finding under all conditions was the presence of neurofibromin in the nucleus, which supports the idea that the bipartite nuclear targeting sequence between residues 2555 and 2572 of neurofibromin may be functional. In summary, we have shown that telencephalic neurons and astroblasts are enriched in neurofibromin and that the subcellular targeting of neurofibromin toward the actin or the microtubule cytoskeleton is developmentally regulated.

摘要

神经纤维瘤病1基因的蛋白质产物神经纤维瘤蛋白在发育过程中于大脑皮层大量表达,但其生理作用仍不清楚。为深入了解神经纤维瘤蛋白在神经元中的功能,我们研究了神经纤维瘤蛋白在神经元分化过程中的表达模式和亚细胞定位。对整个鸡胚胎发育过程中的端脑匀浆进行蛋白质印迹分析显示,神经纤维瘤蛋白的表达在胚胎发育过程中增加。进一步分析表明,端脑神经元在培养物中也富含神经纤维瘤蛋白,且表达的双相增加与培养物中的两个分化阶段密切相关,首先与突起的大量生长和神经递质表型分化相关,然后与突触形成相关。与与不同细胞骨架系统相关的蛋白质相比,神经纤维瘤蛋白的表达模式与皮质细胞骨架蛋白桩蛋白的表达模式密切相关。此外,对神经纤维瘤蛋白免疫荧光染色的分析表明,在用Triton X - 100提取后,在一种能保留可溶性和丝状细胞骨架蛋白的蛋白质交联剂存在的情况下,神经纤维瘤蛋白仅在第一个分化阶段与F - 肌动蛋白共定位。当用细胞松弛素D处理使肌动蛋白细胞骨架塌陷时,这种共定位持续存在。相反,在分化的第二阶段,神经纤维瘤蛋白与微管共定位,但不与F - 肌动蛋白共定位,并且染色模式在用诺考达唑处理时被破坏,但在用细胞松弛素处理时未被破坏。在所有条件下一个不变的发现是神经纤维瘤蛋白存在于细胞核中,这支持了神经纤维瘤蛋白第2555至2572位残基之间的双分核靶向序列可能具有功能的观点。总之,我们已经表明端脑神经元和成纤维细胞富含神经纤维瘤蛋白,并且神经纤维瘤蛋白向肌动蛋白或微管细胞骨架的亚细胞靶向是受发育调控的。

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