Altered macrophage differentiation and immune dysfunction in tumor development

Antonio Sica(Istituti di Ricovero e Cura a Carattere Scientifico), Vincenzo Bronte
Journal of Clinical Investigation
May 1, 2007
Cited by 1,233Open Access
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Abstract

Tumors require a constant influx of myelomonocytic cells to support the angiogenesis and stroma remodeling needed for their growth. This is mediated by tumor-derived factors, which cause sustained myelopoiesis and the accumulation and functional differentiation of myelomonocytic cells, most of which are macrophages, at the tumor site. An important side effect of the accumulation and functional differentiation of these cells is that they can induce lymphocyte dysfunction. A complete understanding of the complex interplay between neoplastic and myelomonocytic cells might offer novel targets for therapeutic intervention aimed at depriving tumor cells of important growth support and enhancing the antitumor immune response.


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