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Dive into the research topics where Catherine M. Sanders is active.

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Featured researches published by Catherine M. Sanders.


Experimental and Molecular Pathology | 2010

Toll-like receptor and chemokine receptor expression in HIV-infected T lymphocyte subsets

Catherine M. Sanders; Julius M. Cruse; Robert E. Lewis

In the present investigation, flow cytometric techniques were utilized to evaluate 100 cases of HIV and 20 normal controls for CXCR4, CCR5, and TLR4 expression in CD4-positive T cells, CD8-positive T cells, regulatory T cells, and Th17 cells, and fluorescence intensity values were determined. TLR4 was expressed by CD4+ T cells and CD8+ T cells in 97 cases, by regulatory T cells in 88 of 95 cases, and by Th17 cells in 93 of 95 cases, while it remained negative in all 20 normal controls. These data indicate that TLR4 upregulation is not limited to gram-negative bacterial infection nor is expression limited to myeloid cells. Upregulation of TLR4 in HIV patients may either be directly or indirectly related to the presence of the virus. CXCR4 was positively expressed by CD4+ T cells in 96 HIV cases, CD8+ T cells in 95, regulatory T cells in 89 of 95 cases evaluated, and Th17 cells in all 92 cases evaluated, while expression remained negative in the majority of normal controls. CCR5 was positively expressed by CD4+ and CD8+ T cells in all 100 HIV cases and by regulatory T cells in 89 of 95 cases evaluated, while expression was negative in most CD4+ and regulatory T cells of normal controls. Statistically significant differences were detected when TLR4 expression by CD4+ and CD8+ T cells was compared to stage of disease. TLR4 expression decreased as infection progressed from acute phase to AIDS. In addition, expression of TLR4 by all T cell subsets was slightly decreased in patients receiving HAART therapy. Results also reveal a positive correlation between CXCR4, CCR5, and TLR4 expression indicating that TLR4 expression and chemokine expression pathways are linked.


Experimental and Molecular Pathology | 2006

The immunophenotype of pre-TALL/LBL revisited

Robert E. Lewis; Julius M. Cruse; Catherine M. Sanders; Rachel N. Webb; Benjamin F. Tillman; Kevin Beason; John T. Lam; Jonathan Koehler


Experimental and Molecular Pathology | 2007

Aberrant expression of T-cell markers in acute myeloid leukemia.

Robert E. Lewis; Julius M. Cruse; Catherine M. Sanders; Rachel N. Webb; Jeanann L. Suggs


Experimental and Molecular Pathology | 2007

Contrasting antigenic maturation patterns in M0-M2 versus M3 acute myeloid leukemias

Robert E. Lewis; Julius M. Cruse; Rachel N. Webb; Catherine M. Sanders; Kevin Beason


The FASEB Journal | 2007

Aberrant expression of T-cell markers in acute myeloid leukemia

Robert E. Lewis; Julius M. Cruse; Catherine M. Sanders; Rachel N. Webb; Jeanann L. Suggs


The FASEB Journal | 2008

Induction of adaptive immunity by flagellin does not require TLR5 or robust innate immune activation

Catherine M. Sanders; Satoshi Uematsu; Shizuo Akira; Andrew T. Gewirtz


The FASEB Journal | 2008

Antibody identification by Luminex technology in renal allotransplant recipients

Robert A. Lewis; Julius M. Cruse; Catherine M. Sanders; Rachel N. Webb; Jeanann L. Suggs; Wendy Thomson


The FASEB Journal | 2008

TLR4 related to CXCR4 and CCR5 expression in HIV

Catherine M. Sanders; Julius M. Cruse; Robert E. Lewis


The FASEB Journal | 2007

Toll-like receptors, cytokines and HIV-1

Catherine M. Sanders; Julius M. Cruse; Robert E. Lewis; John W. Coker


The FASEB Journal | 2007

Zap-70 and CD38 as predictors of IgVH mutation in CLL

Julius M. Cruse; Robert E. Lewis; Catherine M. Sanders; Jeanann L. Suggs; Rachel N. Webb

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Julius M. Cruse

University of Mississippi Medical Center

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Robert E. Lewis

University of Mississippi Medical Center

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Rachel N. Webb

University of Mississippi Medical Center

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Jeanann L. Suggs

University of Mississippi Medical Center

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Kevin Beason

University of Mississippi Medical Center

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John T. Lam

University of Mississippi Medical Center

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Jonathan Koehler

University of Mississippi Medical Center

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Benjamin F. Tillman

University of Mississippi Medical Center

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