A pharmacokinetically (PK) and pharmacodynamically (PD) driven phase I trial of the pan-AKT inhibitor AZD5363 with expansion cohorts in PIK3CA mutant breast and gynecological cancers.

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RESEARCH PRODUCT

A pharmacokinetically (PK) and pharmacodynamically (PD) driven phase I trial of the pan-AKT inhibitor AZD5363 with expansion cohorts in PIK3CA mutant breast and gynecological cancers.

Paul Elvin Andrew Foxley Shaista Salim Peter Lawrence Philippe L. Bedard Jan H.m. Schellens Helen Ambrose Barry R. Davies Gerald Batist Udai Banerji Shannon N. Westin Emma Dean Ed Casson Peter Kabos Benoit You Justin P.o. Lindemann Jose Alejandro Perez-fidalgo James W.t. Yates Paul Rugman

subject

Oncology Target lesion Cancer Research medicine.medical_specialty Akt inhibitor AZD5363 business.industry Nausea Pharmacology medicine.disease Rash Clinical trial Breast cancer Oncology Internal medicine Toxicity Medicine medicine.symptom business Adverse effect

description

Background: AZD5363 is a novel potent pan-AKT inhibitor (IC50of AKT1, AKT2 and AKT3 of 3, 7 and 7nM respectively) with preclinical activity across a range of models. Methods: The trial had an adaptive design that allowed changes in schedule based on toxicity, PK, and PD findings. AZD5363 was administered orally (PO) twice a day (BID). Three schedules were explored: continuous dosing (7/7), four days a week, (4/7) and two days a week (2/7). PD biomarkers including pAKT, pGSK3?, and pPRAS40 were measured by IHC in pre- and post-treatment tumor biopsies. Once a RP2D was established, two expansion cohorts of PIK3CA-mutant ER+ve breast (B) and gynecological (G) cancers were explored. Results: 47, 21 and 22 patients were treated on the 7/7, 4/7 and 2/7 schedules respectively, with a further 27 and 18 patients recruited to the B and G cohorts to date. The MTDs of 7/7, 4/7 and 2/7 were 320mg BID, 480mg BID and 640mg BID respectively. The dose limiting toxicities (DLTs) were rash and diarrhea for 7/7, and hyperglycemia for 2/7. No DLTs were identified for 4/7. The most common causally-related adverse events CTC Grade 3 were hyperglycemia (20%), diarrhea (10%), rash (10%), nausea (3%) and fatigue (1%). PK profiles at the RP2D of 480mg BID (4/7) showed a multi-dose Css,max of 1426ng/mL and AUCssof 7952ng.hr/mL, which were consistent with exposures that gave tumor regression in preclinical models. Pre- and post-treatment biopsies confirmed target engagement in tumor tissue, with an increase in pAKT and reductions in pGSK3? and pPRAS40. Based on toxicity, PK and PD profiles 480mg BID (4/7) was chosen as the R2PD for single agent AZD5363, with the option of using 640mg BID (2/7) as a pharmacologically active dose for future combination studies. Target lesion shrinkage was observed in 7/15 and 4/14 in the B and G cohorts respectively to date, and with RECIST responses in evaluable patients of 3/15 (20%) and 1/14 (7%). Conclusions: Based on toxicity, PK and PD data two intermittent schedules of AZD5363 have been identified for further exploration. Promising single agent activity has been seen in PIK3CA-mutant breast cancer providing support for ongoing combination studies. Clinical trial information: NCT01226316.

year	journal	country	edition	language
2015-05-20	Journal of Clinical Oncology

https://doi.org/10.1200/jco.2015.33.15_suppl.2500