Selective inhibition of Ras, phosphoinositide 3 kinase, and Akt isoforms increases the radiosensitivity of human carcinoma cell lines.

Selective inhibition of Ras, phosphoinositide 3 kinase, and Akt isoforms increases the radiosensitivity of human carcinoma cell lines.

Ras activation promotes the survival of tumor cells after DNA damage. To reverse this survival advantage, Ras signaling has been targeted for inhibition. Other contributors to Ras-mediated DNA damage survival have been identified using pharmacologic inhibition of signaling, but this approach is limi...

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Hlavní autoři: Kim, I, Bae, S, Fernandes, A, Wu, J, Muschel, R, Mckenna, W, Birnbaum, M, Bernhard, E
Médium: Journal article
Jazyk:English
Vydáno: 2005

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