星形孢菌素通过多种激酶激活诱导U937细胞快速同型细胞间黏附。
Staurosporine induces rapid homotypic intercellular adhesion of U937 cells via multiple kinase activation.
作者信息
Cho Jae Youl, Katz David R, Chain Benjamin M
机构信息
Department of Immunology and Molecular Pathology, Windeyer Institute of Medical Sciences, University College London, 46 Cleveland Street, London W1T 4JF.
出版信息
Br J Pharmacol. 2003 Sep;140(2):269-76. doi: 10.1038/sj.bjp.0705436. Epub 2003 Aug 26.
Abstract
- Staurosporine is a broad-specificity kinase inhibitor, which has acted as lead compound for the development of some novel cytotoxic compounds for treatment of cancer. This study investigates the unexpected observation that staurosporine can also induce homotypic cellular aggregation. 2. In this study, staurosporine is shown to activate rapid homotypic aggregation of U937 cells, at concentrations below those required to induce cell death. This activity is a particular feature of staurosporine, and is not shared by a number of other kinase inhibitors. The proaggregating activity of staurosporine is inhibited by deoxyglucose, cytochalasin B and colchicine. Staurosporine-induced aggregation can be distinguished from that induced by the phorbol 12-myristate 13-acetate by faster kinetics and insensitivity to cycloheximide. Staurosporine induces translocation of conventional and novel, but not atypical isoforms of protein kinase C (PKC). Aggregation induced by staurosporine is inhibited by a number of inhibitors of PKC isoforms, and by inhibitors of protein tyrosine kinases. Staurosporine also induces rapid phosphorylation of ERK and p38, and inhibitors of both these enzymes block aggregation. 3. Staurosporine induces dysregulated activation of multiple kinase signaling pathways in U937 cells, and the combined activity of several of these pathways is essential for the induction of aggregation.
摘要
- 星形孢菌素是一种具有广泛特异性的激酶抑制剂,它曾作为开发一些用于治疗癌症的新型细胞毒性化合物的先导化合物。本研究调查了一个意外发现,即星形孢菌素也能诱导同型细胞聚集。2. 在本研究中,星形孢菌素在低于诱导细胞死亡所需浓度时,能激活U937细胞的快速同型聚集。这种活性是星形孢菌素的一个特殊特征,许多其他激酶抑制剂并不具备。脱氧葡萄糖、细胞松弛素B和秋水仙碱可抑制星形孢菌素的促聚集活性。星形孢菌素诱导的聚集与佛波酯12-肉豆蔻酸酯13-乙酸酯诱导的聚集在动力学上更快且对放线菌酮不敏感,从而得以区分。星形孢菌素诱导传统和新型蛋白激酶C(PKC)亚型的易位,但不诱导非典型亚型的易位。星形孢菌素诱导的聚集受到多种PKC亚型抑制剂以及蛋白酪氨酸激酶抑制剂的抑制。星形孢菌素还能诱导ERK和p38的快速磷酸化,这两种酶的抑制剂均可阻断聚集。3. 星形孢菌素在U937细胞中诱导多种激酶信号通路的失调激活,这些通路中几种的联合活性对于诱导聚集至关重要。
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