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TAT-mediated transduction of MafA protein in utero results in enhanced pancreatic insulin expression and changes in islet morphology.

PLoS One.. 2011-08;  6(8):e22364
Vargas N, ?lvarez-Cubela S, Giraldo JA, Nieto M, Fort NM, Cechin S, GarcÍa E, Espino-Grosso P, Fraker CA, Ricordi C, Inverardi L, Pastori RL, DomÍnguez-Bendala J. Department of Surgery, University of Miami Leonard M. Miller School of Medicine, Miami, Florida, United States of America
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摘要

Alongside Pdx1 and Beta2/NeuroD, the transcription factor MafA has been shown to be instrumental in the maintenance of the beta cell phenotype. Indeed, a combination of MafA, Pdx1 and Ngn3 (an upstream regulator of Beta2/NeuroD) was recently reported to lead to the effective reprogramming of acinar cells into insulin-producing beta cells. These experiments set the stage for the development of new strategies to address the impairment of glycemic control in diabetic patients. However, the clinical applicability of reprogramming in this context is deemed to be poor due to the need to use viral vehicles for the delivery of the above factors. Here we describe a recombinant transducible version of the MafA protein (T... More

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