Abstract S6-04: The PI3K inhibitor, taselisib, has enhanced potency in PIK3CA mutant models through a unique mechanism of action

Friedman, LS; Edgar, KA; Song, Kyung Soon; Schmidt, Stephen; Kirkpatrick, DS; Phu, Lilian; Nannini, M; Hong, Rebecca; Chen, Fang-You; Crocker, Lisa; Young, Alyson L.; Sampath, Deepak

doi:10.1158/1538-7445.sabcs16-s6-04

Cited by 7 publications

(10 citation statements)

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“…Taselisib has increased potency against the mutant version of the PI3K alpha isoform, as demonstrated in chemical assays as well as in cancer cell lines (6). A higher therapeutic window due to greater selectivity for PIK3CA mutant isoforms has been shown in extensive laboratory studies (21) and is also suggested by the fact that partial responses were only observed in patients with PIK3CA-mutant tumors. The other indirect evidence for an enhanced therapeutic window is that at the chosen recommended dose, patients were able to stay on the study agent for prolonged periods of time.…”

Section: Discussionmentioning

confidence: 82%

Phase I Dose-Escalation Study of Taselisib, an Oral PI3K Inhibitor, in Patients with Advanced Solid Tumors

et al. 2017

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Taselisib is a potent and selective tumor growth inhibitor through PI3K pathway suppression. Thirty-four patients with locally advanced or metastatic solid tumors were treated (phase I study, modified 3+3 dose escalation; 5 cohorts; 3-16 mg taselisib once daily capsule). Taselisib pharmacokinetics were dose-proportional; mean half-life was 40 hours. Frequent dose-dependent, treatment-related adverse events included diarrhea, hyperglycemia, decreased appetite, nausea, rash, stomatitis, and vomiting. At 12 and 16 mg dose levels, dose limiting toxicities (DLT) were observed, with an accumulation of higher-grade adverse events after the cycle 1 DLT assessment window. Pharmacodynamic findings showed pathway inhibition at ≥3 mg in patient tumor samples, consistent with preclinical PIK3CA-mutant tumor xenograft models. Confirmed response rate was 36% for PIK3CA-mutant tumor patients with measurable disease (5/14: 4 breast cancer, [3 patients at 12 mg]; 1 NSCLC) where responses started at 3 mg, and 0% in patients with tumors without known PIK3CA hotspot mutations (0/15).

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Section: Discussionmentioning

confidence: 82%

Phase I Dose-Escalation Study of Taselisib, an Oral PI3K Inhibitor, in Patients with Advanced Solid Tumors

et al. 2017

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“…Early clinical trials of the isoform-selective inhibitors, alpelisib and taselisib, in breast cancer have produced results consistent with a previous meta-analysis of clinical trials of PI3K pathway inhibitors in patients with diverse cancers, revealing that patients with H1047R mutations had higher response rates than those with other PIK3CA mutations, or no mutations in this gene (Janku et al, 2013; Mayer et al, 2017). The p110β-sparing inhibitor, taselisib, (Table S1) was reported to induce degradation of mutant p110α (Friedman et al, 2017). It is conceivable that distinct activating mutations in p110α might confer differential susceptibilities drug-induced degradation; if this proves to be the case, perhaps drug-induced turnover of the p110α H1047R mutant underlies the increased taselisib sensitivity of tumors expressing this particular p110α oncoprotein.…”

Section: Therapeutic Targeting Of the Pi3k Pathway In Cancermentioning

confidence: 99%

The PI3K Pathway in Human Disease

Fruman

Chiu

Hopkins

et al. 2017

Cell

1,883

1,658

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Phosphoinositide 3-kinase (PI3K) activity is stimulated by diverse oncogenes and growth factor receptors, and elevated PI3K signaling is considered a hallmark of cancer. Many PI3K pathway-targeted therapies have been tested in oncology trials, resulting in regulatory approval of one isoform-selective inhibitor (idelalisib) for treatment of certain blood cancers, and a variety of other agents at different stages of development. In parallel to PI3K research by cancer biologists, investigations in other fields have uncovered exciting and often unpredicted roles for PI3K catalytic and regulatory subunits in normal cell function and in disease. Many of these functions impinge upon oncology by influencing the efficacy and toxicity of PI3K-targeted therapies. Here we provide a perspective on the roles of class I PI3Ks in the regulation of cellular metabolism and in immune system functions, two topics closely intertwined with cancer biology. We also discuss recent progress developing PI3K-targeted therapies for treatment of cancer and other diseases.

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“…Tumor PIK3CA H1047R in cancer cells in culture and patient-derived xenografts (PDX) without significant change in WT p110α (62). It spares p110β but also inhibits p110γ and p110δ.…”

Section: Pi3k Pi3kmentioning

confidence: 99%

Challenges for the Clinical Development of PI3K Inhibitors: Strategies to Improve Their Impact in Solid Tumors

2019

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The PI3K pathway is mutated and aberrantly activated in many cancers and plays a central role in tumor cell proliferation and survival, making it a rational therapeutic target. Until recently, however, results from clinical trials with PI3K inhibitors in solid tumors have been largely disappointing. Here, we describe several factors that have limited the success of these agents, including the weak driver oncogenic activity of mutant PI3K, suboptimal patient selection in trials, drug-related toxicities, feedback upregulation of compensatory mechanisms when PI3K is blocked, increased insulin production upon PI3Kα inhibition, lack of mutant-specifi c inhibitors, and a relative scarcity of studies using combinations with PI3K antagonists. We also suggest strategies to improve the impact of these agents in solid tumors. Despite these challenges, we are optimistic that isoformspecifi c PI3K inhibitors, particularly in combination with other agents, may be valuable in treating appropriately selected patients with PI3K-dependent tumors. signifi cance: Despite the modest clinical activity of PI3K inhibitors in solid tumors, there is an increasing understanding of the factors that may have limited their success. Strategies to ameliorate drug-related toxicities, use of rational combinations with PI3K antagonists, development of mutantselective PI3K inhibitors, and better patient selection should improve the success of these targeted agents against solid tumors.Research.on July 10, 2020.

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Abstract S6-04: The PI3K inhibitor, taselisib, has enhanced potency in PIK3CA mutant models through a unique mechanism of action

Cited by 7 publications

References 0 publications

Phase I Dose-Escalation Study of Taselisib, an Oral PI3K Inhibitor, in Patients with Advanced Solid Tumors

Phase I Dose-Escalation Study of Taselisib, an Oral PI3K Inhibitor, in Patients with Advanced Solid Tumors

The PI3K Pathway in Human Disease

Challenges for the Clinical Development of PI3K Inhibitors: Strategies to Improve Their Impact in Solid Tumors

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