Authors
Hyman, DSmyth, L
Donoghue, M
Westin, S
Bedard, P
Dean, Emma J
Bando, H
El-Khoueiry, A
Pérez-Fidalgo, J
Mita, A
Schellens, J
Chang, M
Reichel, J
Bouvier, N
Selcuklu, S
Soumerai, T
Torrisi, J
Erinjeri, J
Ambrose, H
Barrett, J
Dougherty, B
Foxley, A
Lindemann, J
McEwen, R
Pass, M
Schiavon, G
Berger, M
Chandarlapaty, S
Solit, D
Banerji, U
Baselga, J
Taylor, B
Affiliation
Memorial Sloan Kettering Cancer CenterIssue Date
2017-05-10
Metadata
Show full item recordAbstract
Purpose AKT1 E17K mutations are oncogenic and occur in many cancers at a low prevalence. We performed a multihistology basket study of AZD5363, an ATP-competitive pan-AKT kinase inhibitor, to determine the preliminary activity of AKT inhibition in AKT-mutant cancers. Patients and Methods Fifty-eight patients with advanced solid tumors were treated. The primary end point was safety; secondary end points were progression-free survival (PFS) and response according to Response Evaluation Criteria in Solid Tumors (RECIST). Tumor biopsies and plasma cell-free DNA (cfDNA) were collected in the majority of patients to identify predictive biomarkers of response. Results In patients with AKT1 E17K-mutant tumors (n = 52) and a median of five lines of prior therapy, the median PFS was 5.5 months (95% CI, 2.9 to 6.9 months), 6.6 months (95% CI, 1.5 to 8.3 months), and 4.2 months (95% CI, 2.1 to 12.8 months) in patients with estrogen receptor-positive breast, gynecologic, and other solid tumors, respectively. In an exploratory biomarker analysis, imbalance of the AKT1 E17K-mutant allele, most frequently caused by copy-neutral loss-of-heterozygosity targeting the wild-type allele, was associated with longer PFS (hazard ratio [HR], 0.41; P = .04), as was the presence of coincident PI3K pathway hotspot mutations (HR, 0.21; P = .045). Persistent declines in AKT1 E17K in cfDNA were associated with improved PFS (HR, 0.18; P = .004) and response ( P = .025). Responses were not restricted to patients with detectable AKT1 E17K in pretreatment cfDNA. The most common grade ≥ 3 adverse events were hyperglycemia (24%), diarrhea (17%), and rash (15.5%). Conclusion This study provides the first clinical data that AKT1 E17K is a therapeutic target in human cancer. The genomic context of the AKT1 E17K mutation further conditioned response to AZD5363.Citation
AKT inhibition in solid tumors with AKT1 mutations. 2017 J Clin OncolJournal
Journal of Clinical OncologyDOI
10.1200/JCO.2017.73.0143PubMed ID
28489509Type
ArticleLanguage
enISSN
1527-7755ae974a485f413a2113503eed53cd6c53
10.1200/JCO.2017.73.0143
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