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一种神经生长因子调节的信使核糖核酸编码一种新的中间丝蛋白。

A nerve growth factor-regulated messenger RNA encodes a new intermediate filament protein.

作者信息

Leonard D G, Gorham J D, Cole P, Greene L A, Ziff E B

机构信息

Department of Biochemistry, New York University Medical Center, New York 10016.

出版信息

J Cell Biol. 1988 Jan;106(1):181-93. doi: 10.1083/jcb.106.1.181.

Abstract

Differential screening of a cDNA library from the PC12 rat pheochromocytoma cell line previously revealed a clone, clone 73, whose corresponding mRNA is induced by nerve growth factor (NGF). Induction parallels NGF-stimulated PC12 differentiation from a chromaffinlike phenotype to a sympathetic neuronlike phenotype. We report that DNA sequence analysis reveals that clone 73 mRNA encodes an intermediate filament (IF) protein whose predicted amino acid sequence is distinct from the known sequences of other members of the IF protein family. The sequence has highest homology with desmin and vimentin and includes the highly conserved central alpha-helical rod domain with the characteristic heptad repeat of hydrophobic residues, but has lower homology in the amino-terminal head and carboxyl-terminal tail domains. The head domain contains a large number of serine residues which are potential phosphorylation sites. The expression of clone 73 in vivo in the nervous system of the adult rat was investigated by in situ hybridization of clone 73 probes to tissue sections. The mRNA is expressed at high levels in ganglia of the peripheral nervous system, including the superior cervical ganglion (sympathetic), ciliary ganglion (parasympathetic), and dorsal root ganglion (sensory). In the central nervous system, motor nuclei of cranial nerves III, IV, V, VI, VII, X, and XII as well as ventral horn motor neurons and a restricted set of other central nervous system nuclei express the clone 73 mRNA. Tissues apart from those of the nervous system did not in general express the mRNA, with only very low levels detected in adrenal gland. We discuss the implications of these results for the mechanism of NGF-induced PC12 cell differentiation, the pathways of neuronal development in vivo, and the possible function of the clone 73 IF protein and its relationship to other IF proteins.

摘要

对源自PC12大鼠嗜铬细胞瘤细胞系的cDNA文库进行差异筛选,先前已鉴定出一个克隆,即克隆73,其对应的mRNA可被神经生长因子(NGF)诱导。这种诱导与NGF刺激PC12细胞从嗜铬样表型分化为交感神经元样表型的过程平行。我们报告,DNA序列分析表明,克隆73 mRNA编码一种中间丝(IF)蛋白,其预测的氨基酸序列与IF蛋白家族其他成员的已知序列不同。该序列与结蛋白和波形蛋白具有最高的同源性,包括具有特征性疏水残基七肽重复序列的高度保守的中央α螺旋杆状结构域,但在氨基末端头部和羧基末端尾部结构域的同源性较低。头部结构域含有大量潜在磷酸化位点的丝氨酸残基。通过将克隆73探针与组织切片进行原位杂交,研究了克隆73在成年大鼠神经系统中的体内表达情况。该mRNA在周围神经系统的神经节中高水平表达,包括颈上神经节(交感神经)、睫状神经节(副交感神经)和背根神经节(感觉神经)。在中枢神经系统中,动眼神经、滑车神经、三叉神经、展神经、面神经、迷走神经和舌下神经的运动核以及脊髓前角运动神经元和一组其他受限制的中枢神经系统核表达克隆73 mRNA。除神经系统组织外,其他组织一般不表达该mRNA,仅在肾上腺中检测到极低水平的表达。我们讨论了这些结果对NGF诱导PC12细胞分化机制、体内神经元发育途径以及克隆73 IF蛋白可能的功能及其与其他IF蛋白关系的影响。

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