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Publication : Reprogramming of a melanoma genome by nuclear transplantation.

First Author  Hochedlinger K Year  2004
Journal  Genes Dev Volume  18
Issue  15 Pages  1875-85
PubMed ID  15289459 Mgi Jnum  J:91662
Mgi Id  MGI:3050163 Doi  10.1101/gad.1213504
Citation  Hochedlinger K, et al. (2004) Reprogramming of a melanoma genome by nuclear transplantation. Genes Dev 18(15):1875-85
abstractText  We have used nuclear transplantation to test whether the reprogramming activity of oocytes can reestablish developmental pluripotency of malignant cancer cells. We show here that the nuclei of leukemia, lymphoma, and breast cancer cells could support normal preimplantation development to the blastocyst stage but failed to produce embryonic stem (ES) cells. However, a blastocyst cloned from a RAS-inducible melanoma nucleus gave rise to ES cells with the potential to differentiate into multiple cell types in vivo including melanocytes, lymphocytes, and fibroblasts. Chimeras produced from these ES cells developed cancer with higher penetrance, shorter latency, and an expanded tumor spectrum when compared with the donor mouse model. These results demonstrate that the secondary changes of a melanoma nucleus are compatible with a broad developmental potential but predispose mice to melanomas and other malignant tumors on reactivation of RAS. Our findings serve as a paradigm for studying the tumorigenic effect of a given cancer genome in the context of a whole animal.
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