Treatment of Sickle Cell Anemia Mouse Model with iPS Cells Generated from Autologous Skin

Jacob H. Hanna; Marius Wernig; Styliani Markoulaki; Chiao‐Wang Sun; Alexander Meissner; John P. Cassady; Caroline Beard; Tobias Brambrink; Li‐Chen Wu; Tim M. Townes; Rudolf Jaenisch

doi:10.1126/science.1152092

Treatment of Sickle Cell Anemia Mouse Model with iPS Cells Generated from Autologous Skin

Jacob H. Hanna(University of Alabama at Birmingham), Marius Wernig(University of Alabama at Birmingham), Styliani Markoulaki(University of Alabama at Birmingham), Chiao‐Wang Sun(University of Alabama at Birmingham), Alexander Meissner(University of Alabama at Birmingham), John P. Cassady(University of Alabama at Birmingham), Caroline Beard(University of Alabama at Birmingham), Tobias Brambrink(University of Alabama at Birmingham), Li‐Chen Wu(University of Alabama at Birmingham), Tim M. Townes(University of Alabama at Birmingham), Rudolf Jaenisch(University of Alabama at Birmingham)

Science

December 6, 2007

10.1126/science.1152092

Cited by 1,492

Abstract

It has recently been demonstrated that mouse and human fibroblasts can be reprogrammed into an embryonic stem cell-like state by introducing combinations of four transcription factors. However, the therapeutic potential of such induced pluripotent stem (iPS) cells remained undefined. By using a humanized sickle cell anemia mouse model, we show that mice can be rescued after transplantation with hematopoietic progenitors obtained in vitro from autologous iPS cells. This was achieved after correction of the human sickle hemoglobin allele by gene-specific targeting. Our results provide proof of principle for using transcription factor-induced reprogramming combined with gene and cell therapy for disease treatment in mice. The problems associated with using retroviruses and oncogenes for reprogramming need to be resolved before iPS cells can be considered for human therapy.

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