Cutting edge: Rapid and efficient in vivo cytotoxicity by cytotoxic T cells is independent of granzymes A and B

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Date

2009

Authors

Regner, Matthias
Pavlinovic, Lisa
Koskinen, Aulikki
Young, Nicolie
Trapani, Joseph A
Mullbacher, Arno

Journal Title

Journal ISSN

Volume Title

Publisher

American Association of Immunologists

Abstract

Cytotoxic T (Tc) cells lyse target cells via exocytosis of granules containing perforin (perf) and granzymes (gzm). In vitro, gzm delivery into the target cell cytosol results in apoptosis, and in the absence of gzm A and B the induction of apoptosis is severely impaired. However, using in vivo Tc cell killing assays, we find that virus-immune, gzm A x B-deficient (gzmAxB -/-) mice are competent to eliminate adoptively transferred target cells pulsed with an immunodominant Tc cell determinant as rapidly and completely as their wild-type counterparts. Specific target cell elimination occurred with similar kinetics in both spleen and lymph nodes. Thus, neither gzmA nor gzmB are required for rapid and efficient in vivo cytotoxicity by Tc cells.

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Keywords

Keywords: granzyme A; granzyme B; granzyme; Gzmb protein, mouse; adoptive transfer; animal experiment; animal tissue; apoptosis; article; controlled study; cytosol; cytotoxic T lymphocyte; cytotoxicity; female; immune adherence; in vitro study; in vivo study; lymph

Citation

URI

http://hdl.handle.net/1885/37599

Collections

ANU Research Publications

Source

Journal of Immunology

Type

Journal article

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DOI

10.4049/jimmunol.0900466

Restricted until

2037-12-31

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