Phase I Safety, Pharmacokinetic, and Pharmacodynamic Study of SAR245408 (XL147), an Oral Pan-Class I PI3K Inhibitor, in Patients with Advanced Solid Tumors

Shapiro, Geoffrey I.; Rodón, Jordi; Bedell, Cynthia; Kwak, Eunice L.; Baselga, José; Braña, Irene; Pandya, Shuchi S.; Scheffold, Christian; Laird, A. Douglas; Nguyen, Linh T.; Xu, Yi; Égile, Coumaran; Edelman, Gerald M.

doi:10.1158/1078-0432.ccr-13-1777

Cited by 145 publications

(116 citation statements)

References 28 publications

(39 reference statements)

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“…In a single-agent phase I study, robust pharmacodynamic activity across diverse tumors was evident regardless of mutational status. For example, PI3K pathway inhibition was roughly comparable in a tongue squamous cell carcinoma harboring a PIK3CA E545K mutation with that seen in tumors lacking detectable PI3K pathway alterations (24). Moreover, in that study, a partial response was evident in a patient with non-small cell lung cancer, although no mutations affecting the PI3K pathway were detected in archival tumor tissue from the patient (24).…”

Section: Discussionmentioning

confidence: 70%

“…For example, PI3K pathway inhibition was roughly comparable in a tongue squamous cell carcinoma harboring a PIK3CA E545K mutation with that seen in tumors lacking detectable PI3K pathway alterations (24). Moreover, in that study, a partial response was evident in a patient with non-small cell lung cancer, although no mutations affecting the PI3K pathway were detected in archival tumor tissue from the patient (24). It is also not yet clear whether the presence of PIK3CA mutations or PTEN deficiency will be predictive of greater clinical responsiveness to PI3K pathway inhibitors in general, although an analysis based on combining the results of multiple early-stage trials suggested that PIK3CA H1047R mutations are associated with response (25).…”

Section: Discussionmentioning

confidence: 95%

“…The plasma concentrations associated with pharmacodynamic activity and antitumor efficacy in mice are comparable with plasma concentrations associated with PI3K pathway inhibition in a single-agent phase I clinical study (compare Supplementary Table S5 with clinical pharmacokinetics summarized in ref. 24). …”

Section: Discussionmentioning

confidence: 99%

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The Selective PI3K Inhibitor XL147 (SAR245408) Inhibits Tumor Growth and Survival and Potentiates the Activity of Chemotherapeutic Agents in Preclinical Tumor Models

Foster

Yamaguchi

Hsu

et al. 2015

Molecular Cancer Therapeutics

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Dysregulation of PI3K/PTEN pathway components, resulting in hyperactivated PI3K signaling, is frequently observed in various cancers and correlates with tumor growth and survival. Resistance to a variety of anticancer therapies, including receptor tyrosine kinase (RTK) inhibitors and chemotherapeutic agents, has been attributed to the absence or attenuation of downregulating signals along the PI3K/PTEN pathway. Thus, PI3K inhibitors have therapeutic potential as single agents and in combination with other therapies for a variety of cancer indications. XL147 (SAR245408) is a potent and highly selective inhibitor of class I PI3Ks (a, b, g, and d). Moreover, broad kinase selectivity profiling of >130 protein kinases revealed that XL147 is highly selective for class I PI3Ks over other kinases. In cellular assays, XL147 inhibits the formation of PIP 3 in the membrane, and inhibits phosphorylation of AKT, p70S6K, and S6 in multiple tumor cell lines with diverse genetic alterations affecting the PI3K pathway. In a panel of tumor cell lines, XL147 inhibits proliferation with a wide range of potencies, with evidence of an impact of genotype on sensitivity. In mouse xenograft models, oral administration of XL147 results in dose-dependent inhibition of phosphorylation of AKT, p70S6K, and S6 with a duration of action of at least 24 hours. Repeat-dose administration of XL147 results in significant tumor growth inhibition in multiple human xenograft models in nude mice. Administration of XL147 in combination with chemotherapeutic agents results in antitumor activity in xenograft models that is enhanced over that observed with the corresponding single agents.

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Section: Discussionmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 95%

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The Selective PI3K Inhibitor XL147 (SAR245408) Inhibits Tumor Growth and Survival and Potentiates the Activity of Chemotherapeutic Agents in Preclinical Tumor Models

Foster

Yamaguchi

Hsu

et al. 2015

Molecular Cancer Therapeutics

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“…As illustrated in Table 1, PD endpoints may include assessments of protein phosphorylation markers, measures of cellular proliferation/apoptosis, cell-cycle regulation biomarkers, and epigenetic changes (17)(18)(19)(20)(21)(22)(23)(24)(25)(26).…”

Section: Serial Tumor Biopsiesmentioning

confidence: 99%

Pharmacodynamic Biomarkers: Falling Short of the Mark?

Gainor

Longo

Chabner

2014

Clinical Cancer Research

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In recent years, the clinical development of targeted therapies has been advanced by a greater understanding of tumor biology and genomics. Nonetheless, drug development remains a slow and costly process. An additional challenge is that targeted therapies may benefit only a subset of patients treatedtypically those patients whose tumors are dependent on the target of interest. Thus, there is a growing need for the incorporation of both predictive and pharmacodynamic (PD) biomarkers in drug development. Predictive biomarkers are important to help guide patient selection, while PD biomarkers can provide information on the pharmacologic effects of a drug on its target. PD studies may provide insights into proof of mechanism (i.e., Does the agent hit its intended target?) and proof of concept (i.e., Does hitting the drug target result in the desired biologic effect?). PD studies may also provide information on the optimal biologic dosing or scheduling of a targeted agent. Herein, we review PD endpoints in the context of targeted drug development in non-small cell lung cancer, highlighting some of the key challenges encountered to date. In doing so, we discuss recent experiences with repeat tumor biopsies, surrogate tissue analysis, alternative clinical trial designs (e.g., window-of-opportunity trials), circulating biomarkers, and mechanism-based toxicity assessments. The application of such technologies and biomarkers in early clinical trials may facilitate rational drug development, while enhancing our understanding of why certain targeted therapies succeed or fail.

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“…63 This molecule has shown good pharmacokinetic properties in animals and humans and is currently in Phase II trials for metastatic estrogen receptor (ER)-positive breast cancer and non-small cell lung cancer. Another agent derived from the heterocyclic compound quinoxalin (benzopyrazine) is XL147, 64 which is being tested in combination with other therapies including chemotherapy and targeted agents such as erlotinib and trastuzumab.…”

Section: Genomic Alterations In the Pathwaymentioning

confidence: 99%

Rationale-based therapeutic combinations with PI3K inhibitors in cancer treatment

Castel

Toska

Zumsteg

et al. 2014

Molecular & Cellular Oncology

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Phase I Safety, Pharmacokinetic, and Pharmacodynamic Study of SAR245408 (XL147), an Oral Pan-Class I PI3K Inhibitor, in Patients with Advanced Solid Tumors

Cited by 145 publications

References 28 publications

The Selective PI3K Inhibitor XL147 (SAR245408) Inhibits Tumor Growth and Survival and Potentiates the Activity of Chemotherapeutic Agents in Preclinical Tumor Models

The Selective PI3K Inhibitor XL147 (SAR245408) Inhibits Tumor Growth and Survival and Potentiates the Activity of Chemotherapeutic Agents in Preclinical Tumor Models

Pharmacodynamic Biomarkers: Falling Short of the Mark?

Rationale-based therapeutic combinations with PI3K inhibitors in cancer treatment

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