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Blood, Vol. 94 No. 7 (October 1), 1999: pp. 2293-2300

Rapid Induction of CD40 on a Subset of Granulocyte Colony-Stimulating Factor-Mobilized CD34+ Blood Cells Identifies Myeloid Committed Progenitors and Permits Selection of Nonimmunogenic CD40minus Progenitor Cells

Damiano Rondelli, Roberto M. Lemoli, Marina Ratta, Miriam Fogli, Francesca Re, Antonio Curti, Mario Arpinati, and Sante Tura

From the Institute of Hematology and Medical Oncology "Seràgnoli," University of Bologna, Bologna, Italy.

CD40 antigen is a costimulatory molecule highly expressed on dendritic cells (DC) and activated B cells, which induces T-cell proliferation through the binding with CD40L receptor. In this study, we evaluated CD40 expression on normal CD34+ blood cells and functionally characterized CD34+CD40+ and CD34+CD40- cell subsets. CD40, CD80, and CD86 antigens were constitutively expressed on 3.2% ± 4.5%, 0%, and 1.8% ± 1.2% CD34+ blood cells, respectively. However, after 24 hours in liquid culture with medium alone, or with tumor-necrosis-factor-alpha (TNF-alpha ), or with allogeneic mononuclear cells 10.8% ± 3.8%, 75.3% ± 15.0% and 53.7% ± 17.0% CD34+ blood cells, respectively, became CD40+. After incubation for 24 hours with TNF-alpha CD34+CD40+ blood cells expressed only myeloid markers and contained less than 5% CD86+ and CD80+ cells. Also, a 24-hour priming with TNF-alpha or ligation of CD40 significantly increased the CD34+ blood cells alloantigen presenting function. Finally, purified CD34+CD40+ blood cells stimulated an alloreactive T-cell response in MLC, were enriched in granulocytic, monocytic, and dendritic precursors, and generated high numbers of DC in 11-14 d liquid cultures with GM-CSF, SCF, TNF-alpha and FLT-3L. In contrast, CD34+CD40- cells were poorly immunogenic, contained committed granulocytic and erythroid precursors and early progenitors, and differentiated poorly toward the DC lineage. In conclusion, a short incubation with TNF-alpha allows the selection of CD40+ blood progenitors, which may be a useful source of DC precursors for antitumor vaccine studies, and also a CD34+CD40- blood cell fraction that could be exploited in innovative strategies of allogeneic transplantation across HLA barriers.


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