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Rapamycin Induces a Caspase-Independent Cell Death in Human Monocytes

Authors :
Maurilio Ponzoni
Federico Bertuzzi
Ezio Bonifacio
Paola Maffi
Alessia Mercalli
Antonio Secchi
Valeria Sordi
F. De Taddeo
L. Bellio
P. Servida
Massimo Bernardi
G. Gatti
Lorenzo Piemonti
Mercalli, A
Sordi, V
Ponzoni, Maurilio
Maffi, P
De Taddeo, F
Gatti, G
Servida, P
Bernardi, M
Bellio, L
Bertuzzi, F
Secchi, Antonio
Bonifacio, E
Piemonti, Lorenzo
Source :
American Journal of Transplantation. 6:1331-1341
Publication Year :
2006
Publisher :
Elsevier BV, 2006.

Abstract

The immunosuppressive activity of rapamycin (RAPA) and its efficacy as an anti-rejection agent in organ transplantation have been ascribed principally to its anti-proliferative effects on T cells, while the activity on monocytes is partially unknown. In vitro, RAPA reduced monocyte survival by inducing a caspase-independent cell death. RAPA-induced monocyte cell death (RAPA-CD) was impeded by activation of granulocyte macrophage-colony stimulating factor family receptors or toll-like receptor 4, and by exposure to inflammatory cytokines. In vivo, in patients who received RAPA monotherapy as part of pre-conditioning for islet transplantation, RAPA affected survival of myeloid lineage cells. In the peripheral blood, CD33(+) and CD14(+) cells decreased, whereas lymphocytes appeared unaffected. In the bone marrow, myeloid precursors such as CD15(+) and CD15(+)/CD16(+) were selectively and significantly decreased, but no major cytotoxic effects were observed. The RAPA-CD suggests a dependence of monocytes on mammalian target of RAPA pathways for nutrient usage, and this feature implies that RAPA could be selectively useful as a treatment to reduce monocytes or myeloid cells in conditions where these cells negatively affect patient, suggesting a potential anti-inflammatory action of this drug.

Details

ISSN :
16006135
Volume :
6
Database :
OpenAIRE
Journal :
American Journal of Transplantation
Accession number :
edsair.doi.dedup.....b69e8ea1fafd0c97446f70b900649950