Literature DB >> 12759415

Mature but not immature Fas ligand (CD95L)-transduced human monocyte-derived dendritic cells are protected from Fas-mediated apoptosis and can be used as killer APC.

Sabine Hoves1, Stefan W Krause, Dagmar Halbritter, Huang-Ge Zhang, John D Mountz, Jürgen Schölmerich, Martin Fleck.   

Abstract

Several in vitro and animal studies have been performed to modulate the interaction of APCs and T cells by Fas (CD95/Apo-1) signaling to delete activated T cells in an Ag-specific manner. However, due to the difficulties in vector generation and low transduction frequencies, similar studies with primary human APC are still lacking. To evaluate whether Fas ligand (FasL/CD95L) expressing killer APC could be generated from primary human APC, monocyte-derived dendritic cells (DC) were transduced using the inducible Cre/Loxp adenovirus vector system. Combined transduction of DC by AdLoxpFasL and AxCANCre, but not single transduction with these vectors, resulted in dose- and time-dependent expression of FasL in >70% of mature DC (mDC), whereas <20% of immature DC (iDC) expressed FasL. In addition, transduction by AdLoxpFasL and AxCANCre induced apoptosis in >80% of iDC, whereas FasL-expressing mDC were protected from FasL/Fas (CD95/Apo-1)-mediated apoptosis despite coexpression of Fas. FasL-expressing mDC eliminated Fas(+) Jurkat T cells as well as activated primary T cells by apoptosis, whereas nonactivated primary T cells were not deleted. Induction of apoptosis in Fas(+) target cells required expression of FasL in DC and cell-to-cell contact between effector and target cell, and was not dependent on soluble FasL. Induction of apoptosis in Fas(+) target cells required expression of FasL in DC, cell-to-cell contact between effector and target cell, and was not dependent on soluble FasL. The present results demonstrate that FasL-expressing killer APC can be generated from human monocyte-derived mDC using adenoviral gene transfer. Our results support the strategy to use killer APCs as immunomodulatory cells for the treatment of autoimmune disease and allograft rejection.

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Year:  2003        PMID: 12759415     DOI: 10.4049/jimmunol.170.11.5406

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  11 in total

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3.  Alloantigen specific deletion of primary human T cells by Fas ligand (CD95L)-transduced monocyte-derived killer-dendritic cells.

Authors:  Christian Schütz; Sabine Hoves; Dagmar Halbritter; Huang-Ge Zhang; John D Mountz; Martin Fleck
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Review 5.  Killer artificial antigen-presenting cells: the synthetic embodiment of a 'guided missile'.

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Authors:  Zhongyu Liu; Xin Xu; Hui-Chen Hsu; Albert Tousson; Ping-Ar Yang; Qi Wu; Cunren Liu; Shaohua Yu; Huang-Ge Zhang; John D Mountz
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7.  Killer artificial antigen-presenting cells: a novel strategy to delete specific T cells.

Authors:  Christian Schütz; Martin Fleck; Andreas Mackensen; Alessia Zoso; Dagmar Halbritter; Jonathan P Schneck; Mathias Oelke
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Review 8.  Current state of type 1 diabetes immunotherapy: incremental advances, huge leaps, or more of the same?

Authors:  Brett Phillips; Massimo Trucco; Nick Giannoukakis
Journal:  Clin Dev Immunol       Date:  2011-07-18

9.  Killer artificial antigen presenting cells (KaAPC) for efficient in vitro depletion of human antigen-specific T cells.

Authors:  Christian Schütz; Martin Fleck; Jonathan P Schneck; Mathias Oelke
Journal:  J Vis Exp       Date:  2014-08-11       Impact factor: 1.355

10.  Urea-mediated cross-presentation of soluble Epstein-Barr virus BZLF1 protein.

Authors:  Sascha Barabas; Regina Gary; Tanja Bauer; Juha Lindner; Petra Lindner; Birgit Weinberger; Wolfgang Jilg; Hans Wolf; Ludwig Deml
Journal:  PLoS Pathog       Date:  2008-11-07       Impact factor: 6.823

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