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Prepublished online as a Blood First Edition Paper on March 20, 2003; DOI 10.1182/blood-2002-10-3055.

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Submitted October 7, 2002
Accepted March 11, 2003

Sorting of soluble TNF-receptor for granule storage in hematopoietic cells as a principle for targeting of selected proteins to inflamed sites

Ying Gao, Hanna Rosen, Ellinor Johnsson, Jero Calafat, Hans Tapper, and Inge Olsson*

Department of Hematology, Laboratory Medicine, Lunds Universitet, Lund, Sweden
The Netherlands Cancer Institute, Amsterdam, The Netherlands
Department of Cell and Molecular Biology, Lunds Universitet, Lund, Sweden

* Corresponding author; email: inge.olsson{at}hematologi.lu.se.

Hematopoietic cells have secretory lysosomes that degranulate at the inflammatory site upon stimulation. We asked whether one could target exogenous proteins with a therapeutic potential to secretory lysosomes in hematopoietic cells. For this purpose, we expressed a soluble TNF receptor form (sTNFR1) in hematopoietic cell lines. In order to accomplish targeting to secretory lysosomes both ER-retention and constitutive secretion has to be prevented. ER-retention was facilitated by addition of a transmembrane (tm) sequence and constitutive secretion was overcome by incorporating a cytosolic sorting signal (Y) from CD63. This signal directed the resulting sTNFR1-tm-Y to secretory lysosomes. Confirmation of these results was provided from biosynthetic radiolabeling, subcellular fractionation, immunofluorescence microscopy and immunoelectron microscopy. The tm-Y fragment was cleaved by proteolysis resulting in generation of the membrane-free sTNFR1 in secretory lysosomes. Our results suggest a potential for using the storage organelles of hematopoietic cells as vehicles for targeting sites of inflammation with therapeutically active agents.


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