Soluble Fibrin Inhibits Lymphocyte Adherence and Cytotoxicity Against Tumor Cells: Implications for Cancer Metastasis and Immunotherapy

Author:

Biggerstaff John P.1,Weidow Brandy2,Dexheimer Judith2,Warnes Gary3,Vidosh Jacqueline2,Patel Shonak2,Newman Michael4,Patel Pretesh2

Affiliation:

1. Biological Imaging Unit, University of Tennessee, Knoxville, Tennessee,

2. Biological Imaging Unit, University of Tennessee, Knoxville, Tennessee

3. Flow Cytometry and Imaging Core Facilities, Institute of Cell and Molecular Science, Queen Mary University of London, London, UK

4. University of Tennessee Statistics Consulting Center, University of Tennessee, Knoxville, Tennessee

Abstract

Circulating soluble fibrin (sFn) is elevated in many cancer patients. It is a marker for ongoing disseminated intravascular coagulation and may have prognostic significance. We have demonstrated that sFn inhibited monocyte adherence and cytotoxicity by a mechanism involving blockade of monocyte αMβ2 and tumor cell CD54. It was, therefore, hypothesized that sFn also inhibits lymphocyte and interleukin-2—activated lymphocyte (LAK) adherence and cytotoxicity against tumor cells. This study sought to identify the lymphocyte subset responsible for adherence and killing of A375 melanoma cells and whether sFn inhibited these parameters. Lymphocyte and LAK cell adherence and cytotoxicity, which was adherence dependent, were inhibited by preincubation with purified or plasma-derived sFn. The lymphocyte and LAK cell activities were primarily a result of CD8+ MHC (major histocompatibility complex) unrestricted cytotoxic T cells. These results suggest that elevated levels of circulating sFn may be immunosuppressive and may reduce the efficacy of adoptive immunotherapies.

Publisher

SAGE Publications

Subject

Hematology,General Medicine

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