A Balance between Positive and Negative Signals in Cytotoxic Lymphocytes Regulates the Polarization of Lipid Rafts during the Development of Cell-mediated Killing

doi:10.1084/jem.191.2.347

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© The Rockefeller University Press, 0022-1007/2000/1/347/ $5.00
The Journal of Experimental Medicine, Volume 191, Number 2, January 17, 2000 347-354

Original Article

A Balance between Positive and Negative Signals in Cytotoxic Lymphocytes Regulates the Polarization of Lipid Rafts during the Development of Cell-mediated Killing

Zhenkun Lou^a, Dragan Jevremovic^b, Daniel D. Billadeau^b, and Paul J. Leibson^b
^a Department of Pharmacology, Mayo Graduate and Medical Schools, Mayo Clinic, Rochester, Minnesota 55905
^b Department of Immunology, Mayo Graduate and Medical Schools, Mayo Clinic, Rochester, Minnesota 55905

Correspondence to: Paul J. Leibson, Dept. of Immunology, Mayo Clinic, 200 First St. SW, Rochester, MN 55905. Tel:507-284-4563 Fax:507-284-1637 E-mail:leibson.paul{at}mayo.edu.

Plasma membrane microdomains containing sphingolipids and cholesterol(lipid rafts) are enriched in signaling molecules. The cross-linkingof certain types of cell surface receptors initiates the redistributionof these lipid rafts, resulting in the formation of signalingcomplexes. However, little is known about the regulation ofthe initial raft redistribution and whether negative regulatorysignaling pathways target this phase of cellular activation.We used natural killer (NK) cells as a model to investigatethe regulation of raft redistribution, as both positive andnegative signals have been implicated in the development oftheir cellular function. Here we show that after NK cells formconjugates with sensitive tumor cells, rafts become polarizedto the site of target recognition. This redistribution of lipidrafts requires the activation of both Src and Syk family proteintyrosine kinases. In contrast, engagement of major histocompatibilitycomplex (MHC)-recognizing killer cell inhibitory receptors (KIRs)on NK cells by resistant, MHC-bearing tumor targets blocks raftredistribution. This inhibition is dependent on the catalyticactivity of KIR-associated SHP-1, a Src homology 2 (SH2) domaincontaining tyrosine phosphatase. These results suggest thatthe influence of integrated positive and negative signals onraft redistribution critically influences the development ofcell-mediated cytotoxicity.

Key Words: natural killer cell, signal transduction, cytotoxicity, immunologic,tyrosine kinase, tyrosine phosphatase

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