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Abstract
Annual Review of Immunology
Vol. 20: 323-370 (Volume publication date April 2002)
(doi:10.1146/annurev.immunol.20.100201.131730)
LYMPHOCYTE-MEDIATED CYTOTOXICITY

John H. Russell1 and Timothy J. Ley2
1Department of Molecular Biology and Pharmacology, Washington University School of Medicine, St. Louis, Missouri 63110; e-mail:
2Departments of Medicine and Genetics, Siteman Cancer Center, Washington University School of Medicine, St. Louis, Missouri 63110; e-mail:

Abstract Virtually all of the measurable cell-mediated cytotoxicity delivered by cytotoxic T lymphocytes and natural killer cells comes from either the granule exocytosis pathway or the Fas pathway. The granule exocytosis pathway utilizes perforin to traffic the granzymes to appropriate locations in target cells, where they cleave critical substrates that initiate DNA fragmentation and apoptosis; granzymes A and B induce death via alternate, nonoverlapping pathways. The Fas/FasL system is responsible for activation-induced cell death but also plays an important role in lymphocyte-mediated killing under certain circumstances. The interplay between these two cytotoxic systems provides opportunities for therapeutic interventions to control autoimmune diseases and graft vs. host disease, but oversuppression of these pathways may also lead to increased viral susceptibility and/or decreased tumor cell killing.

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Authors:
John H. Russell
Timothy J. Ley
Keywords:
granule exocytosis
Fas
apoptosis
perforin
granzymes

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