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Generation of a FasL-based Proapoptotic Fusion Protein Devoid of Systemic Toxicity Due to Cell-surface Antigen-restricted Activation

Overview
Journal J Biol Chem
Specialty Biochemistry
Date 2003 May 30
PMID 12773535
Citations 21
Authors
Dierk Samel
Dafne Muller
Jeannette Gerspach
Constance Assohou-Luty
Gabriele Sass
Gisa Tiegs
Klaus Pfizenmaier
Harald Wajant
Affiliations
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Abstract

We describe the construction of a FasL fusion protein devoid of systemic toxicity, inducing apoptosis only on cell-surface antigen-positive cells. The fusion protein consists carboxyl-terminally of the extracellular domain of FasL and amino-terminally of a fibroblast activation protein (FAP)-specific single chain antibody fragment (sc40-FasL). The latter allows immobilization-dependent conversion of the inactive soluble FasL fusion protein into an entity with membrane FasL-like activity. Thus, sc40-FasL efficiently induced apoptosis only in FAP-expressing cells. In accordance with a strict target-selective activity of sc40-FasL, the intravenous application of this reagent in mice revealed no signs of systemic toxicity and prevented growth of xenotransplanted FAP-positive (but not FAP-negative) tumor cells. The principle described here for the first time, in which cell-surface antigen-mediated activation of Fas permits local activation of Fas in vivo, opens novel avenues for the use of Fas signaling in cancer therapy.

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