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Safety and tolerability of AZD5363 in Japanese patients with advanced solid tumors

58

Citations

9

References

2016

Year

Abstract

Intermittent dosing of AZD5363 was more tolerable than continuous dosing. 480 mg bid intermittent 4/3 dosing for AZD5363 monotherapy was selected for further investigation. Preliminary evidence of antitumor activity was observed. Akt1 (E17K) is a potent driver mutation that may predict clinical response to AZD5363.

References

YearCitations

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