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Merck

Mu-calpain activation in beta-lapachone-mediated apoptosis.

Cancer biology & therapy (2003-05-17)
Colleen Tagliarino, John J Pink, Kathryn E Reinicke, Sara M Simmers, Shelly M Wuerzberger-Davis, David A Boothman
ABSTRACT

Beta-lapachone (beta-Lap) triggers apoptosis in a number of human breast and prostate cancer cell lines through a unique apoptotic pathway that is dependent upon NQO1, a two-electron reductase. Recently, our laboratory showed that beta-lap-exposed MCF-7 cells exhibited an early increase in intracellular cytosolic Ca(2+) from endoplasmic reticulum stores, and that BAPTA-AM (an intracellular Ca(2+) chelator) blocked these early increases and partially inhibited all aspects of beta-lap-induced apoptosis. We now show that exposure of NQO1-expressing breast cancer cells to beta-lap stimulates a unique proteolytic apoptotic pathway involving mu-calpain activation. No apparent activation of m-calpain was noted. Upon activation, mu-calpain translocated to the nucleus concomitant with specific nuclear proteolytic events. Apoptotic responses in beta-lap-exposed NQO1-expressing cells were significantly delayed and survival enhanced by exogenous over-expression of calpastatin, a natural inhibitor of mu- and m-calpains. Furthermore, purified mu-calpain cleaved PARP to a unique fragment (approximately 60 kDa), not previously reported for calpains. We provide evidence that beta-lap-induced, mu-calpain-stimulated apoptosis does not involve any known apoptotic caspases; the activated fragments of caspases were not observed after beta-lap exposures, nor were there any changes in the pro-enzyme forms as measured by Western blot analyses. The ability of beta-lap to trigger an apparently novel, p53-independent, calpain-mediated apoptotic cell death further support the development of this drug for improved breast cancer therapy.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
Anti-Caspase 9 Antibody, clone 96-2-22, clone 96-2-22, Upstate®, from mouse
Sigma-Aldrich
Anti-Calpain Antibody, small subunit of µ- or m-Calpains (Calpain I or II), clone P1, ascites fluid, clone P1, Chemicon®