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Haploinsufficiency of PTEN augments the chemotactic response of lymphocytes, alters gene expression, and results in autoimmunity Fox, Joanne

Abstract

The ability of the cell to respond to physiological cues and integrate signals from outside sources is important for normal cellular function. The generation of second messengers is a central mechanism by which the cell activates signal transduction cascades that mediate cellular responses. Phosphatidylinositol lipid species (PIP) act as important second messengers in the membrane. Phosphatidylinositol-3-kinase (PI3K) and PTEN are responsible for regulating levels of PIP species and thus, are implicated in the control of many important cellular processes. Regulation of cellular activation is particularly important in the immune system where abnormal activation of lymphocytes can lead to developmental defects, impaired ability to defend against infection, and disease. In support of this, we and others have demonstrated that mice lacking a single allele of Pten develop an autoimmune disease that worsens with age. We observed increased lymph node size, splenomegaly, and elevated levels of serum immunoglobulins in Pten +/- mice. No evidence of major developmental defects were found in Pten +/- lymphocytes, however increased responsiveness of both B and T cells was detected. In the immune system, migration to specialized microenvironments ensures the proper development, differentiation, survival, elimination and activation of lymphocytes. The complex network of celhcell interactions that occurs during an immune response is also controlled by migratory events. Thus, we examined the role of Pten in the control of lymphocyte migration. We found that Pten +/- lymphocytes had an augmented chemotactic response to stromal cell derived factor-1 (SDF-1). We also demonstrated increased phosphorylation of protein kinase B (PKB) in response to SDF-1. Stimulation of lymphocytes with SDF-1 led to changes in gene expression. The expression of a subset of genes was altered in Pten +/- T cells. These observations provide evidence of a regulatory role for PTEN in lymphocytes and implicate PTEN in the dysregulation of the immune system that occurs during autoimmunity.

Item Metadata

Title
Haploinsufficiency of PTEN augments the chemotactic response of lymphocytes, alters gene expression, and results in autoimmunity
Creator
Fox, Joanne
Publisher
University of British Columbia
Date Issued
2002
Description
The ability of the cell to respond to physiological cues and integrate signals from outside sources is important for normal cellular function. The generation of second messengers is a central mechanism by which the cell activates signal transduction cascades that mediate cellular responses. Phosphatidylinositol lipid species (PIP) act as important second messengers in the membrane. Phosphatidylinositol-3-kinase (PI3K) and PTEN are responsible for regulating levels of PIP species and thus, are implicated in the control of many important cellular processes. Regulation of cellular activation is particularly important in the immune system where abnormal activation of lymphocytes can lead to developmental defects, impaired ability to defend against infection, and disease. In support of this, we and others have demonstrated that mice lacking a single allele of Pten develop an autoimmune disease that worsens with age. We observed increased lymph node size, splenomegaly, and elevated levels of serum immunoglobulins in Pten +/- mice. No evidence of major developmental defects were found in Pten +/- lymphocytes, however increased responsiveness of both B and T cells was detected. In the immune system, migration to specialized microenvironments ensures the proper development, differentiation, survival, elimination and activation of lymphocytes. The complex network of celhcell interactions that occurs during an immune response is also controlled by migratory events. Thus, we examined the role of Pten in the control of lymphocyte migration. We found that Pten +/- lymphocytes had an augmented chemotactic response to stromal cell derived factor-1 (SDF-1). We also demonstrated increased phosphorylation of protein kinase B (PKB) in response to SDF-1. Stimulation of lymphocytes with SDF-1 led to changes in gene expression. The expression of a subset of genes was altered in Pten +/- T cells. These observations provide evidence of a regulatory role for PTEN in lymphocytes and implicate PTEN in the dysregulation of the immune system that occurs during autoimmunity.
Extent
11633569 bytes
Genre
Thesis/Dissertation
Type
Text
File Format
application/pdf
Language
eng
Date Available
2009-11-13
Provider
Vancouver : University of British Columbia Library
Rights
For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use.
DOI
10.14288/1.0099735
URI
http://hdl.handle.net/2429/14910
Degree
Doctor of Philosophy - PhD
Program
Genetics
Affiliation
Medicine, Faculty of; Medical Genetics, Department of
Degree Grantor
University of British Columbia
Graduation Date
2002-11
Campus
UBCV
Scholarly Level
Graduate
Aggregated Source Repository
DSpace

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For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use.