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成骨蛋白-1调节神经细胞中L1和神经细胞黏附分子的基因表达。

Osteogenic protein-1 regulates L1 and neural cell adhesion molecule gene expression in neural cells.

作者信息

Perides G, Hu G, Rueger D C, Charness M E

机构信息

Department of Pathology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Biol Chem. 1993 Nov 25;268(33):25197-205.

PMID:8227084
Abstract

Osteogenic protein-1 (OP-1) is a member of the TGF-beta superfamily that is expressed in the nervous system. We recently showed that human recombinant osteogenic protein-1 (hOP-1) strongly promotes the aggregation of dividing neuroblastoma x glioma hybrid NG108-15 cells, in part by inducing the major isoforms of the neural cell adhesion molecule (N-CAM) (Perides, G., Safran, R. M., Rueger, D. C., and Charness, M. E. (1992) Proc. Natl. Acad. Sci. U. S. A. 89, 10326-10330). Here we show that hOP-1 induces L1 expression approximately 6-fold in NG108-15 cells without changing the levels of N-cadherin, neurofilament 200, Thy-1, tau, and G alpha s. OP-1 induction of L1 and N-CAM was unassociated with changes in cell proliferation and was not reproduced by cellular differentiation. The increased adhesiveness of hOP-1-treated NG108-15 cells could be inhibited in part by Fab fragments of an anti-L1 polyclonal antiserum. L1 and N-CAM expression first increased 12-18 h after hOP-1 treatment, reached a maximum after 2-3 days, persisted for up to 5 days, and returned to control levels 3 days after hOP-1 withdrawal. The increases in L1 and N-CAM protein levels were preceded or accompanied by large increases in the abundance of L1 and all detectable N-CAM mRNAs. Actinomycin D prevented the induction by hOP-1 of L1 and N-CAM mRNAs, suggesting that hOP-1 regulates immunoglobulin CAM gene transcription. OP-1 is the first described growth factor that regulates both N-CAM and L1 gene expression.

摘要

成骨蛋白-1(OP-1)是转化生长因子-β超家族的成员,在神经系统中表达。我们最近发现,人重组成骨蛋白-1(hOP-1)强烈促进分裂的神经母细胞瘤x胶质瘤杂交细胞NG108-15的聚集,部分原因是诱导神经细胞粘附分子(N-CAM)的主要亚型(Perides,G.,Safran,R.M.,Rueger,D.C.,和Charness,M.E.(1992年)美国国家科学院院刊89,10326-10330)。在这里,我们表明hOP-1在NG108-15细胞中诱导L1表达增加约6倍,而不改变N-钙粘蛋白、神经丝200、Thy-1、tau和Gαs的水平。OP-1对L1和N-CAM的诱导与细胞增殖的变化无关,也不能通过细胞分化再现。hOP-1处理的NG108-15细胞增加的粘附性可被抗L1多克隆抗血清的Fab片段部分抑制。L1和N-CAM的表达在hOP-1处理后12-18小时首次增加,2-3天后达到最大值,持续长达5天,并在hOP-1撤除后3天恢复到对照水平。L1和N-CAM蛋白水平的增加之前或伴随着L1和所有可检测到的N-CAM mRNA丰度的大幅增加。放线菌素D可阻止hOP-1对L1和N-CAM mRNA的诱导,表明hOP-1调节免疫球蛋白细胞粘附分子基因的转录。OP-1是第一个被描述的调节N-CAM和L1基因表达的生长因子。

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