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Title
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Nuclear translocation of granzyme B in target cell apoptosis
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MJ Pinkoski1,2, JA Heibein1, M Barry1 & RC Bleackley1
1Department of Biochemistry, University of Alberta, Edmonton, Alberta, Canada, T6G 2H7
2Division of Cellular Immunology, La Jolla Institute for Allergy and Immunology, 10355 Science Center Drive, San Diego, California, CA, USA
Correspondence to: RC Bleackley, Department of Biochemistry, University of Alberta, Edmonton, Alberta, Canada, T6G 2H7. Tel: (780) 492-3968; Fax: (780) 492-0886; E-mail: chris.bleackley@ualberta.ca
Edited by C Thiele
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Abstract
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Granzyme B is the prototypic member of a family of serine proteases localized to the cytolytic granules of cytotoxic lymphocytes. Together with another granule protein, perforin, granzyme B is capable of inducing all aspects of apoptotic death in target cells. A number of granzyme B substrates have been identified and it has been demonstrated that granzyme B is responsible, directly or indirectly, for the morphological nuclear changes observed in target cell apoptosis, including DNA fragmentation. In an earlier study, we showed that granzyme B binds to a nuclear protein in a manner dependent on its enzymatic activity. Here, we demonstrate that granzyme B is translocated rapidly to the nucleus in cells that have been induced to undergo apoptosis by a granzyme-dependent process, and that translocation is dependent on caspase activity. Appearance of granzyme B in the nucleus of target cells precedes the detection of DNA fragmentation. Although not directly responsible for DNA fragmentation, these data suggest a nuclear role for granzyme B in target cell apoptosis. c-Abl nuclear functions. Cell Death and Differentiation (2000) 7, 17 – 24.
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apoptosis; caspases; granzyme B; nuclear translocation
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Received 16 September 1999; Revised 28 September 1999; Accepted 4 October 1999
©
Macmillan Publishers Ltd 2000
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