Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor

David S. Hong; Kathleen N. Moore; Johanna C. Bendell; Daniel D. Karp; Judy S. Wang; Susanna V. Ulahannan; Suzanne Jones; Wenjuan Wu; Gregory P. Donoho; Yan Ding; Andrew Capen; Xuejing Wang; Aimee Bence Lin; Manish R. Patel

doi:10.1158/1078-0432.CCR-20-3242

Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor

David S. Hong, Kathleen N. Moore, Johanna C. Bendell, Daniel D. Karp, Judy S. Wang, Susanna V. Ulahannan, Suzanne Jones, Wenjuan Wu, Gregory P. Donoho, Yan Ding, Andrew Capen, Xuejing Wang, Aimee Bence Lin, Manish R. Patel

Investigational Cancer Therapeutics

Research output: Contribution to journal › Article › peer-review

21 Scopus citations

Abstract

Purpose: Prexasertib, a checkpoint kinase 1 inhibitor (CHK1), exhibited modest monotherapy antitumor activity in previous studies. Preclinical data were generated to support the clinical combination of prexasertib +samotolisib, a PI3K/mTOR inhibitor. Patients and Methods: Prexasertib + samotolisib was first evaluated in triple-negative breast cancer (TNBC) cells, MDA-MB-231 orthotopic xenograft tumors, and TNBC patient- derived xenograft (PDX) mouse models. In the phase Ib trial, following dose escalation, the initial expansion arm (E1, solid tumors) explored prexasertib 105 mg/m2 intravenously every 14 days + samotolisib 200 mg orally twice daily. Subsequent expansion arms evaluated samotolisib 150 mgtwice daily in patients carrying PIK3CA mutations (E2, solid tumors) or with TNBC (E3). Safety and antitumor activity were assessed. Results: Prexasertib + samotolisib inhibited cell proliferation in TNBC lines and primary tumor growth in the MDA-MB-231 model. Prexasertib + samotolisib exhibited synergistic or additive effects in 30 of 38PDXsingle-mouse ("n=1") models, and provided rationale for clinical evaluation. In the phase Ib study, 53 patients were enrolled (escalation, n= 13; E1, n=9; E2, n= 15; and E3, n= 16). No dose-limiting toxicities (DLT) were observed during escalation; however, DLT-equivalent toxicities were observed in E1, leading to samotolisib dose reduction (150 mg twice daily) in E2/E3. Common treatment-related adverse events were leukopenia/neutropenia (94.3%), thrombocytopenia (62.3%), and nausea (52.8%). During escalation, 2 patients achieved partial response for an overall response rate (ORR) of 15.4%, and ORRs were 13.3% for E2 (PIK3CA) and 25% for E3 (TNBC). Conclusions: Prexasertib+samotolisib showed antitumor activity in preclinical models and preliminary efficacy in heavily pretreated patients. The clinical combination was associated with toxicity, suggesting supportive measures may be required. However, these data may inform future trials using other CHK1 and PI3K pathway inhibitors.

Original language	English (US)
Pages (from-to)	1864-1874
Number of pages	11
Journal	Clinical Cancer Research
Volume	27
Issue number	7
DOIs	https://doi.org/10.1158/1078-0432.CCR-20-3242
State	Published - Apr 2021

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/1078-0432.CCR-20-3242

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Hong, D. S., Moore, K. N., Bendell, J. C., Karp, D. D., Wang, J. S., Ulahannan, S. V., Jones, S., Wu, W., Donoho, G. P., Ding, Y., Capen, A., Wang, X., Lin, A. B., & Patel, M. R. (2021). Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor. Clinical Cancer Research, 27(7), 1864-1874. https://doi.org/10.1158/1078-0432.CCR-20-3242

Hong, DS, Moore, KN, Bendell, JC, Karp, DD, Wang, JS, Ulahannan, SV, Jones, S, Wu, W, Donoho, GP, Ding, Y, Capen, A, Wang, X, Lin, AB & Patel, MR 2021, 'Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor', Clinical Cancer Research, vol. 27, no. 7, pp. 1864-1874. https://doi.org/10.1158/1078-0432.CCR-20-3242

@article{c6e3d008c41d4dcea2d6a9b0dbd188d3,

title = "Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor",

abstract = "Purpose: Prexasertib, a checkpoint kinase 1 inhibitor (CHK1), exhibited modest monotherapy antitumor activity in previous studies. Preclinical data were generated to support the clinical combination of prexasertib +samotolisib, a PI3K/mTOR inhibitor. Patients and Methods: Prexasertib + samotolisib was first evaluated in triple-negative breast cancer (TNBC) cells, MDA-MB-231 orthotopic xenograft tumors, and TNBC patient- derived xenograft (PDX) mouse models. In the phase Ib trial, following dose escalation, the initial expansion arm (E1, solid tumors) explored prexasertib 105 mg/m2 intravenously every 14 days + samotolisib 200 mg orally twice daily. Subsequent expansion arms evaluated samotolisib 150 mgtwice daily in patients carrying PIK3CA mutations (E2, solid tumors) or with TNBC (E3). Safety and antitumor activity were assessed. Results: Prexasertib + samotolisib inhibited cell proliferation in TNBC lines and primary tumor growth in the MDA-MB-231 model. Prexasertib + samotolisib exhibited synergistic or additive effects in 30 of 38PDXsingle-mouse ({"}n=1{"}) models, and provided rationale for clinical evaluation. In the phase Ib study, 53 patients were enrolled (escalation, n= 13; E1, n=9; E2, n= 15; and E3, n= 16). No dose-limiting toxicities (DLT) were observed during escalation; however, DLT-equivalent toxicities were observed in E1, leading to samotolisib dose reduction (150 mg twice daily) in E2/E3. Common treatment-related adverse events were leukopenia/neutropenia (94.3%), thrombocytopenia (62.3%), and nausea (52.8%). During escalation, 2 patients achieved partial response for an overall response rate (ORR) of 15.4%, and ORRs were 13.3% for E2 (PIK3CA) and 25% for E3 (TNBC). Conclusions: Prexasertib+samotolisib showed antitumor activity in preclinical models and preliminary efficacy in heavily pretreated patients. The clinical combination was associated with toxicity, suggesting supportive measures may be required. However, these data may inform future trials using other CHK1 and PI3K pathway inhibitors.",

author = "Hong, {David S.} and Moore, {Kathleen N.} and Bendell, {Johanna C.} and Karp, {Daniel D.} and Wang, {Judy S.} and Ulahannan, {Susanna V.} and Suzanne Jones and Wenjuan Wu and Donoho, {Gregory P.} and Yan Ding and Andrew Capen and Xuejing Wang and Lin, {Aimee Bence} and Patel, {Manish R.}",

note = "Publisher Copyright: {\textcopyright} 2021 American Association for Cancer Research.",

year = "2021",

month = apr,

doi = "10.1158/1078-0432.CCR-20-3242",

language = "English (US)",

volume = "27",

pages = "1864--1874",

journal = "Clinical Cancer Research",

issn = "1078-0432",

publisher = "American Association for Cancer Research Inc.",

number = "7",

}

TY - JOUR

T1 - Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor

AU - Hong, David S.

AU - Moore, Kathleen N.

AU - Bendell, Johanna C.

AU - Karp, Daniel D.

AU - Wang, Judy S.

AU - Ulahannan, Susanna V.

AU - Jones, Suzanne

AU - Wu, Wenjuan

AU - Donoho, Gregory P.

AU - Ding, Yan

AU - Capen, Andrew

AU - Wang, Xuejing

AU - Lin, Aimee Bence

AU - Patel, Manish R.

PY - 2021/4

Y1 - 2021/4

N2 - Purpose: Prexasertib, a checkpoint kinase 1 inhibitor (CHK1), exhibited modest monotherapy antitumor activity in previous studies. Preclinical data were generated to support the clinical combination of prexasertib +samotolisib, a PI3K/mTOR inhibitor. Patients and Methods: Prexasertib + samotolisib was first evaluated in triple-negative breast cancer (TNBC) cells, MDA-MB-231 orthotopic xenograft tumors, and TNBC patient- derived xenograft (PDX) mouse models. In the phase Ib trial, following dose escalation, the initial expansion arm (E1, solid tumors) explored prexasertib 105 mg/m2 intravenously every 14 days + samotolisib 200 mg orally twice daily. Subsequent expansion arms evaluated samotolisib 150 mgtwice daily in patients carrying PIK3CA mutations (E2, solid tumors) or with TNBC (E3). Safety and antitumor activity were assessed. Results: Prexasertib + samotolisib inhibited cell proliferation in TNBC lines and primary tumor growth in the MDA-MB-231 model. Prexasertib + samotolisib exhibited synergistic or additive effects in 30 of 38PDXsingle-mouse ("n=1") models, and provided rationale for clinical evaluation. In the phase Ib study, 53 patients were enrolled (escalation, n= 13; E1, n=9; E2, n= 15; and E3, n= 16). No dose-limiting toxicities (DLT) were observed during escalation; however, DLT-equivalent toxicities were observed in E1, leading to samotolisib dose reduction (150 mg twice daily) in E2/E3. Common treatment-related adverse events were leukopenia/neutropenia (94.3%), thrombocytopenia (62.3%), and nausea (52.8%). During escalation, 2 patients achieved partial response for an overall response rate (ORR) of 15.4%, and ORRs were 13.3% for E2 (PIK3CA) and 25% for E3 (TNBC). Conclusions: Prexasertib+samotolisib showed antitumor activity in preclinical models and preliminary efficacy in heavily pretreated patients. The clinical combination was associated with toxicity, suggesting supportive measures may be required. However, these data may inform future trials using other CHK1 and PI3K pathway inhibitors.

AB - Purpose: Prexasertib, a checkpoint kinase 1 inhibitor (CHK1), exhibited modest monotherapy antitumor activity in previous studies. Preclinical data were generated to support the clinical combination of prexasertib +samotolisib, a PI3K/mTOR inhibitor. Patients and Methods: Prexasertib + samotolisib was first evaluated in triple-negative breast cancer (TNBC) cells, MDA-MB-231 orthotopic xenograft tumors, and TNBC patient- derived xenograft (PDX) mouse models. In the phase Ib trial, following dose escalation, the initial expansion arm (E1, solid tumors) explored prexasertib 105 mg/m2 intravenously every 14 days + samotolisib 200 mg orally twice daily. Subsequent expansion arms evaluated samotolisib 150 mgtwice daily in patients carrying PIK3CA mutations (E2, solid tumors) or with TNBC (E3). Safety and antitumor activity were assessed. Results: Prexasertib + samotolisib inhibited cell proliferation in TNBC lines and primary tumor growth in the MDA-MB-231 model. Prexasertib + samotolisib exhibited synergistic or additive effects in 30 of 38PDXsingle-mouse ("n=1") models, and provided rationale for clinical evaluation. In the phase Ib study, 53 patients were enrolled (escalation, n= 13; E1, n=9; E2, n= 15; and E3, n= 16). No dose-limiting toxicities (DLT) were observed during escalation; however, DLT-equivalent toxicities were observed in E1, leading to samotolisib dose reduction (150 mg twice daily) in E2/E3. Common treatment-related adverse events were leukopenia/neutropenia (94.3%), thrombocytopenia (62.3%), and nausea (52.8%). During escalation, 2 patients achieved partial response for an overall response rate (ORR) of 15.4%, and ORRs were 13.3% for E2 (PIK3CA) and 25% for E3 (TNBC). Conclusions: Prexasertib+samotolisib showed antitumor activity in preclinical models and preliminary efficacy in heavily pretreated patients. The clinical combination was associated with toxicity, suggesting supportive measures may be required. However, these data may inform future trials using other CHK1 and PI3K pathway inhibitors.

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U2 - 10.1158/1078-0432.CCR-20-3242

DO - 10.1158/1078-0432.CCR-20-3242

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AN - SCOPUS:85104889770

SN - 1078-0432

VL - 27

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JO - Clinical Cancer Research

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ER -

Preclinical evaluation and phase ib study of prexasertib, a chk1 inhibitor, and samotolisib (LY3023414), a dual PI3K/mTOR inhibitor

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