Abstract

Natural killer cell function results from the balance of expression of inhibitory and activating receptors at the plasma membrane. This unit of the program will define membrane traffic pathways involved in post-translational control of NK cell receptor expression in order to determine how regulation of these pathways can influence NK cell function. There has only been limited analysis of endocytic pathways of NK receptors and no NK receptors have been analyzed for their biosynthetic pathways. The studies in this unit redress these deficits of information with the goals of comparing endocytic and biosynthetic regulation of activating and inhibitory KIRs, as well as defining chaperone pathways that influence KIR folding and stability. In addition, membrane traffic pathways regulating NK cell-target cell interactions at the synapse will be defined.
The specific aims are as follows.
Aim 1 is to characterize the endocytic behavior of inhibitory (KIR2DL1) and activating (KIR2DS1) NK receptors to test the hypothesis that surface activity of each class of receptor is regulated by different responses to ligand. The role of CDS signaling in KIR endocytosis will also be assessed.
Aim 2 is to test the hypothesis that polymorphism of the KIR3DL1 locus can influence receptor expression at the NK cell plasma membrane by affecting membrane traffic behavior in the biosynthetic pathway and to compare the biosynthetic pathways of inhibitory and activating KIR. These studies will establish the chaperone pathways that influence levels of KIR receptor expression and that are susceptible to polymorphic variation of the receptors, as well as to stress effects during infection.
Aim 3 is to test the hypothesis that clathrin-mediated membrane traffic at the NK cell-target synapse is required for functional killer-target interactions. The involvement of clathrin in ligand trans-endocytosis by NK cells and in cytotoxicity of target cells will be analyzed using techniques that inhibit clathrin expression. Definition of receptor trafficking pathways by the studies proposed for this unit of the program makes it possible to understand how receptor polymorphisms and the signaling pathways of NK receptors could influence the relative receptor expression levels that are critical for determining individual NK cell activity. This information is needed to appreciate the functional interplay of NK cell populations operating during HIV infection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI064520-04
Application #
7600396
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2008-03-01
Project End
2010-02-28
Budget Start
2008-03-01
Budget End
2009-02-28
Support Year
4
Fiscal Year
2008
Total Cost
$256,740
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Batista, Mariana D; Tincati, Camilla; Milush, Jeffrey M et al. (2013) CD57 expression and cytokine production by T cells in lesional and unaffected skin from patients with psoriasis. PLoS One 8:e52144
Milush, Jeffrey M; López-Vergès, Sandra; York, Vanessa A et al. (2013) CD56negCD16? NK cells are activated mature NK cells with impaired effector function during HIV-1 infection. Retrovirology 10:158
Co, Elizabeth C; Gormley, Matthew; Kapidzic, Mirhan et al. (2013) Maternal decidual macrophages inhibit NK cell killing of invasive cytotrophoblasts during human pregnancy. Biol Reprod 88:155
Batista, Mariana D; Ho, Emily L; Kuebler, Peter J et al. (2013) Skewed distribution of natural killer cells in psoriasis skin lesions. Exp Dermatol 22:64-6
Ndhlovu, Lishomwa C; Lopez-Vergès, Sandra; Barbour, Jason D et al. (2012) Tim-3 marks human natural killer cell maturation and suppresses cell-mediated cytotoxicity. Blood 119:3734-43
Taner, Sabrina B; Pando, Marcelo J; Roberts, Allison et al. (2011) Interactions of NK cell receptor KIR3DL1*004 with chaperones and conformation-specific antibody reveal a functional folded state as well as predominant intracellular retention. J Immunol 186:62-72
Long, Brian R; Erickson, Ann E; Chapman, Joan M et al. (2010) Increased number and function of natural killer cells in human immunodeficiency virus 1-positive subjects co-infected with herpes simplex virus 2. Immunology 129:186-96
Sun, Joseph C; Beilke, Joshua N; Lanier, Lewis L (2010) Immune memory redefined: characterizing the longevity of natural killer cells. Immunol Rev 236:83-94
Lopez-Vergès, Sandra; Milush, Jeffrey M; Pandey, Suchitra et al. (2010) CD57 defines a functionally distinct population of mature NK cells in the human CD56dimCD16+ NK-cell subset. Blood 116:3865-74
Milush, Jeffrey M; Long, Brian R; Snyder-Cappione, Jennifer E et al. (2009) Functionally distinct subsets of human NK cells and monocyte/DC-like cells identified by coexpression of CD56, CD7, and CD4. Blood 114:4823-31

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