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Published online February 5, 2007
doi:10.1083/jcb.200612025
The Journal of Cell Biology, Vol. 176, No. 4, 435-444
The Rockefeller University Press, 0021-9525 $30.00
© 2007 Cullen et al.
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Article

 Human and murine granzyme B exhibit divergent substrate preferences

Sean P. Cullen, Colin Adrain, Alexander U. Lüthi, Patrick J. Duriez, and Seamus J. Martin

Molecular Cell Biology Laboratory, Department of Genetics, The Smurfit Institute, Trinity College, Dublin 2, Ireland

Correspondence to Seamus J. Martin: martinsj{at}tcd.ie

The cytotoxic lymphocyte protease granzyme B (GzmB) can promote apoptosis through direct processing and activation of members of the caspase family. GzmB can also cleave the BH3-only protein, BID, to promote caspase-independent mitochondrial permeabilization. Although human and mouse forms of GzmB exhibit extensive homology, these proteases diverge at residues predicted to influence substrate binding. We show that human and mouse GzmB exhibit radical differences in their ability to cleave BID, as well as several other key substrates, such as ICAD and caspase-8. Moreover, pharmacological inhibition of caspases clonogenically rescued human and mouse target cells from apoptosis initiated by mouse GzmB, but failed to do so in response to human GzmB. These data demonstrate that human and murine GzmB are distinct enzymes with different substrate preferences. Our observations also illustrate how subtle differences in enzyme structure can radically affect substrate selection.

Abbreviations used in this paper: CTL, cytotoxic T lymphocyte; GzmB, granzyme B; NK, natural killer; PI, propidium iodide; SLO, streptolysin O.


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