Modulation of Apoptosis in Rat Thymocytes by Analogs of Staurosporine: Lack of Direct Association with Inhibition of Protein Kinase C

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Vol. 54, Issue 4, 663-670, October 1998

Modulation of Apoptosis in Rat Thymocytes by Analogs of Staurosporine: Lack of Direct Association with Inhibition of Protein Kinase C

Siobhan T. Harkin, Gerald M. Cohen, and Andreas Gescher

Medical Research Council Toxicology Unit, Centre for Mechanisms of Human Toxicity, University of Leicester, Leicester LE1 9HN, United Kingdom

Protein kinase C (PKC) is an important constituent of the signaling pathways involved in apoptosis. The PKC inhibitor staurosporineinduces apoptosis in many cell types. We characterized the roleof PKC in the induction of apoptosis in immature rat thymocytesby investigating the effects of staurosporine with those of fiveanalogs. Four of them, the indolocarbazoles CGP 41251 and UCN-01and the bisindolylmaleimides RO 31-8220 and GF 109203X, possesshigh PKC-inhibitory specificity and potency, whereas one, theUCN-01 stereoisomer UCN-02, is a weak PKC inhibitor. Apoptosiswas examined by flow cytometry, internucleosomal DNA cleavage,and formation of large DNA fragments. Staurosporine, UCN-01, andUCN-02 induced a concentration- and time-dependent increase inapoptosis, whereas neither CGP 41251, RO 31-8220, nor GF 109203Xinduced apoptosis. The mechanism of induction of apoptosis bystaurosporine, UCN-01, and UCN-02 was clearly different from themechanism that mediates induction of apoptosis by etoposide anddexamethasone, as judged by differential effects of modulatorsof apoptosis. Staurosporine, UCN-01, and UCN-02 at concentrationsof a hundredth to a thousandth of those at which they inducedapoptosis, and RO 31-8220 inhibited apoptosis elicited by thapsigarginbut not apoptosis caused by dexamethasone or etoposide. The resultssuggest that (i) UCN-01 and UCN-02 mimic staurosporine as inducersof thymocyte apoptosis; (ii) staurosporine, UCN-01 and UCN-02share a biphasic effect on apoptosis in rat thymocytes, beinginhibitory at low concentrations and stimulatory at high concentrations;and (iii) inhibition of PKC alone is insufficient for inductionof apoptosis in thymocytes.

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