MMP-7 inhibits CTL – tumor cell interaction

doi:10.1186/1475-2867-4-S1-S6

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Cancer Cell International

Volume 4
Suppl 1

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Gregor S
Alla V
Kuball J
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Galle PR
Strand D
Strand S

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This article is part of the supplement: Association for Immunotherapy of Cancer: Cancer Immunotherapy – 2nd Annual Meeting .

Oral presentation

MMP-7 inhibits CTL – tumor cell interaction

S Gregor¹ , V Alla¹, J Kuball², M Theobald², PR Galle¹, D Strand¹ and S Strand¹

¹I. Medizinische Klinik und Poliklinik

²III. Medizinische Klinik und Poliklinik, Johannes Gutenberg-Universität Mainz, Germany

author email corresponding author email

from Association for Immunotherapy of Cancer: Cancer Immunotherapy – 2^ndAnnual Meeting
Mainz, Germany. 6–7 May 2004

Cancer Cell International 2004, 4(Suppl 1):S6doi:10.1186/1475-2867-4-S1-S6

The electronic version of this abstract is the complete one and can be found online at: http://www.cancerci.com/content/4/S1/S6

Received:	28 April 2004
Published:	1 July 2004

Oral presentation

MMP-7, the smallest member of the MMP-family, is a zinc-dependent metalloproteinase and is overexpressed in colon cancer and many other human cancers. Along with its prometastatic function, a fundamental role for MMP-7 has also been established in early tumor development, but the mechanism by which MMP-7 contributes to this, is still unknown.

Tumor specific cytotoxic T cells (CTLs) play a critical role in the control of tumor growth. They can induce apoptosis by CD95 as well as perforin/granzyme mediated pathways. Loss of CD95 may contribute to apoptosis resistance and immune escape of tumor cells leading to successful tumor outgrowth.

In our project we analyzed MMP-7 for its influence on CD95 mediated apoptosis and the cytolytic effector functions of CTLs. Furthermore we investigated the influence of MMP-7 cleavage activity on the adhesion and deadhesion of peptide specific CTL's to tumor targets.

In a cleavage assay with recombinant CD95 protein, we could show that MMP-7, cleaved approximately 2–3 kDa from the extracellular N-terminal end of CD95. In coculture experiments with ⁵¹Cr-labeled HepG2-cells, we found a significant decrease of cytotoxic action of peptide specific CTLs in the presence of MMP-7. In addition MMP-7 leads to a higher adhesion of CTLs and inhibits their deadhesion from HepG2 cells. Considering that CTL's are serial killers, alteration in adhesion/deadhesion functions can be detrimental for tumor specific CTL killing.

Our results show, that MMP-7 can contribute to the apoptosis resistance of tumor cells by different mechanisms. These activities may explain the contribution of MMP-7 to early tumor growth.

This article is part of the supplement: Association for Immunotherapy of Cancer: Cancer Immunotherapy – 2nd Annual Meeting .

MMP-7 inhibits CTL – tumor cell interaction

Oral presentation

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