Modulation of microRNA expression in human T-cell development: targeting of NOTCH3 by miR-150

Ontogenesis of T cells in the thymus is a complex process whose molecular control is poorly understood. The present study investigated microRNAs involved in human thymocyte differentiation by comparing the microRNA expression profiles of thymocytes at the double-positive, single-positive CD4+ and si...

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Veröffentlicht in:Blood 2011-06, Vol.117 (26), p.7053-7062
Hauptverfasser: Ghisi, Margherita, Corradin, Alberto, Basso, Katia, Frasson, Chiara, Serafin, Valentina, Mukherjee, Subhamoy, Mussolin, Lara, Ruggero, Katia, Bonanno, Laura, Guffanti, Alessandro, De Bellis, Gianluca, Gerosa, Gino, Stellin, Giovanni, D'Agostino, Donna M., Basso, Giuseppe, Bronte, Vincenzo, Indraccolo, Stefano, Amadori, Alberto, Zanovello, Paola
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Sprache:eng
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Zusammenfassung:Ontogenesis of T cells in the thymus is a complex process whose molecular control is poorly understood. The present study investigated microRNAs involved in human thymocyte differentiation by comparing the microRNA expression profiles of thymocytes at the double-positive, single-positive CD4+ and single-positive CD8+ maturation stages. Microarray analysis showed that each thymocyte population displays a distinct microRNA expression profile that reflects their developmental relationships. Moreover, analysis of small-RNA libraries generated from human unsorted and double-positive thymocytes and from mature peripheral CD4+ and CD8+ T lymphocytes, together with the microarray data, indicated a trend toward up-regulation of microRNA expression during T-cell maturation after the double-positive stage and revealed a group of microRNAs regulated during normal T-cell development, including miR-150, which is strongly up-regulated as maturation progresses. We showed that miR-150 targets NOTCH3, a member of the Notch receptor family that plays important roles both in T-cell differentiation and leukemogenesis. Forced expression of miR-150 reduces NOTCH3 levels in T-cell lines and has adverse effects on their proliferation and survival. Overall, these findings suggest that control of the Notch pathway through miR-150 may have an important impact on T-cell development and physiology.
ISSN:0006-4971
1528-0020
DOI:10.1182/blood-2010-12-326629