Abstract

The goal of this project is to study how a novel class of cancer therapeutics impact lymphocyte function. These compounds are active-site inhibitors of the bserine/threonine kinase mTOR (mammalian target of rapamycin). The mTOR kinase is present in two complexes, termed mTORC1 and mTORC2, with distinct substrates and function. The natural compound rapamycin is a selective mTOR inhibitor that potently suppresses lymphocyte proliferation, and is used clinically for immunosuppression. However, rapamycin is an allosteric mTORC1 inhibitor that does not acutely inhibit mTORC2. Novel, active-site (ATP-competitive) mTOR inhibitors block all functions of both mTOR complexes and have more potent cytostatic and cytotoxic effects than rapamycin in cancer cell lines. Consequently, there are worldwide efforts to develop active-site mTOR inhibitors for cancer therapy. The immunoregulatory properties of active-site mTOR inhibitors, however, have not been reported. Defining the effects of these agents on lymphocyte activation will reveal their potential as novel immunosuppressants, while also addressing concerns about host defense and anti- tumor immunity in the cancer therapy setting. Our preliminary data suggest that active-site mTOR inhibitors are selectively toxic to leukemia cells compared to nontransformed lymphocytes. In this project we will use a carefully selected set of experimental approaches to address one specific aim: to compare the effects of rapamycin and active-site mTOR inhibitors on lymphocyte activation and differentiation. We will use both in vitro and in vivo systems, and study both T cells and B cells. Inhibitors will be studied over a concentration range to facilitate comparisons of potency. For T cells, we will use T cell receptor-transgenic systems to measure proliferation in response to cognate antigen. We will employ adoptive transfer approaches to assess T cell expansion in vivo. We will also measure cytokine-mediated survival and T helper differentiation. For B cells, we will measure proliferation and survival in response to different mitogens and cytokines. We will compare the differentiation of B cells into antibody-secreting cells and their ability to produce antibodies in immunized mice. We will correlate the functional responses of lymphocytes with signal transduction events, to determine the molecular basis for inhibitor effects.

Public Health Relevance

This project will study a newly discovered class of anti-cancer drugs and determine how they affect the immune response. This work will help us understand and predict potential side effects of these drugs on the immune system of cancer patients. In addition, we might find evidence that the drugs will be useful to treat immune-related diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Small Research Grants (R03)
Project #
5R03AI085462-02
Application #
8019056
Study Section
Transplantation, Tolerance, and Tumor Immunology (TTT)
Program Officer
Gondre-Lewis, Timothy A
Project Start
2010-02-15
Project End
2012-01-31
Budget Start
2011-02-01
Budget End
2012-01-31
Support Year
2
Fiscal Year
2011
Total Cost
$71,245
Indirect Cost

  Institution

Name
University of California Irvine
Department
Biochemistry
Type
Schools of Arts and Sciences
DUNS #
046705849
City
Irvine
State
CA
Country
United States
Zip Code
92697

  Publications

Limon, Jose J; So, Lomon; Jellbauer, Stefan et al. (2014) mTOR kinase inhibitors promote antibody class switching via mTORC2 inhibition. Proc Natl Acad Sci U S A 111:E5076-85
So, Lomon; Fruman, David A (2012) PI3K signalling in B- and T-lymphocytes: new developments and therapeutic advances. Biochem J 442:465-81
Beagle, Brandon; Fruman, David A (2011) A lipid kinase cousin cooperates to promote cancer. Cancer Cell 19:693-5
Limon, Jose J; Fruman, David A (2010) B cell receptor signaling: picky about PI3Ks. Sci Signal 3:pe25