Skewed differentiation of bone marrow CD34+ cells of tumor bearers from dendritic toward monocytic cells, and the redirection of differentiation toward dendritic cells by 1α, 25-dihydroxyvitamin D3

1999 
Abstract Tumor presence is detrimental to the development of antigen-presenting dendritic cells. Since dendritic cells can arise from CD34 + precursor cells, the present study assessed the capacity of bone marrow CD34 + cells from tumor bearers to develop into dendritic cells when cultured in the absence of either tumor cells or their products. Culturing bone marrow CD34 + cells from mice bearing Lewis lung carcinomas yielded a lower number of dendritic cells than arose from CD34 + cells of normal mice. This reduced yield of dendritic cells was associated with a shift to development of monocytic cells and a reduced antigen presenting capability by the cultures. When the CD34 + cell cultures from tumor bearers were supplemented with the differentiation-inducing hormone 1α,25-dihydroxyvitamin D 3 , there was the restoration of dendritic cell development and antigen presenting ability. These results show that CD34 + cells from tumor bearers remain defective in their development into dendritic cells even when cultured outside the tumor environment, but development of dendritic cells can be restored with 1α,25-dihydroxyvitamin D 3 .
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