Phase I study of continuous MKC-1 in patients with advanced or metastatic solid malignancies using the modified Time-to-Event Continual Reassessment Method (TITE-CRM) dose escalation design

Summary Background MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with addition...

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Published in	Investigational new drugs Vol. 30; no. 3; pp. 1039 - 1045
Main Authors	Tevaarwerk, Amye, Wilding, George, Eickhoff, Jens, Chappell, Rick, Sidor, Carolyn, Arnott, Jamie, Bailey, Howard, Schelman, William, Liu, Glenn
Format	Journal Article
Language	English
Published	Boston Springer US 01.06.2012 Springer Nature B.V
Subjects	Adult Aged Algorithms Antineoplastic Agents - administration & dosage Antineoplastic Agents - adverse effects Antineoplastic Agents - pharmacokinetics Binding sites Cancer Cancer therapies Cell cycle Clinical trials Diarrhea Dose-Response Relationship, Drug Drug dosages Drug therapy Enrollments Female Humans Indoles - administration & dosage Indoles - adverse effects Indoles - pharmacokinetics Male Medicine Medicine & Public Health Metastasis Middle Aged Nausea Neoplasm Metastasis Neoplasms - drug therapy Neoplasms - metabolism Neoplasms - pathology Oncology Patients Pharmacokinetics Pharmacology Pharmacology/Toxicology Phase I Studies Radiation therapy Studies Toxicity Tumors Vomiting United States > US MKC-1 TITE-CRM Novel dose escalation designs Solid malignancy
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ISSN	0167-6997 1573-0646 1573-0646
DOI	10.1007/s10637-010-9629-6

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Abstract	Summary Background MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with additional effects against the mTor/AKT pathway. The primary objectives were to determine the maximum tolerated dose (MTD) and response of continuous MKC-1. Secondary objectives included characterizing the dose limiting toxicities (DLTs) and pharmacokinetics (PK). Methods Patients with solid malignancies were eligible, if they had measurable disease, ECOG PS ≤1, and adequate organ function. Exclusions included brain metastases and inability to receive oral drug. MKC-1 was dosed twice daily, continuously in 28-day cycles. Other medications were eliminated if there were possible drug interactions. Doses were assigned using a TITE-CRM algorithm following enrollment of the first 3 pts. Disease response was assessed every 8 weeks. Results Between 5/08–9/09, 24 patients enrolled (15 M/9 F, median 58 years, range 44–77). Patients 1–3 received 120 mg/d of MKC-1; patients 4–24 were dosed per the TITE-CRM algorithm: 150 mg [ n = 1], 180 [2], 200 [1], 230 [1], 260 [5], 290 [6], 320 [5]. The median time on drug was 8 weeks (range 4–28). The only DLT occurred at 320 mg (grade 3 fatigue). Stable disease occurred at 150 mg/d (28 weeks; RCC) and 320 mg/d (16 weeks; breast, parotid). Escalation halted at 320 mg/d. Day 28 pharmacokinetics indicated absorption and active metabolites. Conclusion Continuous MKC-1 was well-tolerated; there were no RECIST responses, although clinical benefit occurred in 3/24 pts. Dose escalation stopped at 320 mg/d, and this is the MTD as defined by the CRM dose escalation algorithm; this cumulative dose/cycle exceeds that determined from intermittent dosing studies. A TITE-CRM allowed for rapid dose escalation and was able to account for late toxicities with continuous dosing via a modified algorithm.
AbstractList	Summary Background MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with additional effects against the mTor/AKT pathway. The primary objectives were to determine the maximum tolerated dose (MTD) and response of continuous MKC-1. Secondary objectives included characterizing the dose limiting toxicities (DLTs) and pharmacokinetics (PK). Methods Patients with solid malignancies were eligible, if they had measurable disease, ECOG PS ≤1, and adequate organ function. Exclusions included brain metastases and inability to receive oral drug. MKC-1 was dosed twice daily, continuously in 28-day cycles. Other medications were eliminated if there were possible drug interactions. Doses were assigned using a TITE-CRM algorithm following enrollment of the first 3 pts. Disease response was assessed every 8 weeks. Results Between 5/08–9/09, 24 patients enrolled (15 M/9 F, median 58 years, range 44–77). Patients 1–3 received 120 mg/d of MKC-1; patients 4–24 were dosed per the TITE-CRM algorithm: 150 mg [ n = 1], 180 [2], 200 [1], 230 [1], 260 [5], 290 [6], 320 [5]. The median time on drug was 8 weeks (range 4–28). The only DLT occurred at 320 mg (grade 3 fatigue). Stable disease occurred at 150 mg/d (28 weeks; RCC) and 320 mg/d (16 weeks; breast, parotid). Escalation halted at 320 mg/d. Day 28 pharmacokinetics indicated absorption and active metabolites. Conclusion Continuous MKC-1 was well-tolerated; there were no RECIST responses, although clinical benefit occurred in 3/24 pts. Dose escalation stopped at 320 mg/d, and this is the MTD as defined by the CRM dose escalation algorithm; this cumulative dose/cycle exceeds that determined from intermittent dosing studies. A TITE-CRM allowed for rapid dose escalation and was able to account for late toxicities with continuous dosing via a modified algorithm. MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with additional effects against the mTor/AKT pathway. The primary objectives were to determine the maximum tolerated dose (MTD) and response of continuous MKC-1. Secondary objectives included characterizing the dose limiting toxicities (DLTs) and pharmacokinetics (PK). Patients with solid malignancies were eligible, if they had measurable disease, ECOG PS ≤1, and adequate organ function. Exclusions included brain metastases and inability to receive oral drug. MKC-1 was dosed twice daily, continuously in 28-day cycles. Other medications were eliminated if there were possible drug interactions. Doses were assigned using a TITE-CRM algorithm following enrollment of the first 3 pts. Disease response was assessed every 8 weeks. Between 5/08-9/09, 24 patients enrolled (15 M/9 F, median 58 years, range 44-77). Patients 1-3 received 120 mg/d of MKC-1; patients 4-24 were dosed per the TITE-CRM algorithm: 150 mg [n = 1], 180 [2], 200 [1], 230 [1], 260 [5], 290 [6], 320 [5]. The median time on drug was 8 weeks (range 4-28). The only DLT occurred at 320 mg (grade 3 fatigue). Stable disease occurred at 150 mg/d (28 weeks; RCC) and 320 mg/d (16 weeks; breast, parotid). Escalation halted at 320 mg/d. Day 28 pharmacokinetics indicated absorption and active metabolites. Continuous MKC-1 was well-tolerated; there were no RECIST responses, although clinical benefit occurred in 3/24 pts. Dose escalation stopped at 320 mg/d, and this is the MTD as defined by the CRM dose escalation algorithm; this cumulative dose/cycle exceeds that determined from intermittent dosing studies. A TITE-CRM allowed for rapid dose escalation and was able to account for late toxicities with continuous dosing via a modified algorithm. MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with additional effects against the mTor/AKT pathway. The primary objectives were to determine the maximum tolerated dose (MTD) and response of continuous MKC-1. Secondary objectives included characterizing the dose limiting toxicities (DLTs) and pharmacokinetics (PK).BACKGROUNDMKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with additional effects against the mTor/AKT pathway. The primary objectives were to determine the maximum tolerated dose (MTD) and response of continuous MKC-1. Secondary objectives included characterizing the dose limiting toxicities (DLTs) and pharmacokinetics (PK).Patients with solid malignancies were eligible, if they had measurable disease, ECOG PS ≤1, and adequate organ function. Exclusions included brain metastases and inability to receive oral drug. MKC-1 was dosed twice daily, continuously in 28-day cycles. Other medications were eliminated if there were possible drug interactions. Doses were assigned using a TITE-CRM algorithm following enrollment of the first 3 pts. Disease response was assessed every 8 weeks.METHODSPatients with solid malignancies were eligible, if they had measurable disease, ECOG PS ≤1, and adequate organ function. Exclusions included brain metastases and inability to receive oral drug. MKC-1 was dosed twice daily, continuously in 28-day cycles. Other medications were eliminated if there were possible drug interactions. Doses were assigned using a TITE-CRM algorithm following enrollment of the first 3 pts. Disease response was assessed every 8 weeks.Between 5/08-9/09, 24 patients enrolled (15 M/9 F, median 58 years, range 44-77). Patients 1-3 received 120 mg/d of MKC-1; patients 4-24 were dosed per the TITE-CRM algorithm: 150 mg [n = 1], 180 [2], 200 [1], 230 [1], 260 [5], 290 [6], 320 [5]. The median time on drug was 8 weeks (range 4-28). The only DLT occurred at 320 mg (grade 3 fatigue). Stable disease occurred at 150 mg/d (28 weeks; RCC) and 320 mg/d (16 weeks; breast, parotid). Escalation halted at 320 mg/d. Day 28 pharmacokinetics indicated absorption and active metabolites.RESULTSBetween 5/08-9/09, 24 patients enrolled (15 M/9 F, median 58 years, range 44-77). Patients 1-3 received 120 mg/d of MKC-1; patients 4-24 were dosed per the TITE-CRM algorithm: 150 mg [n = 1], 180 [2], 200 [1], 230 [1], 260 [5], 290 [6], 320 [5]. The median time on drug was 8 weeks (range 4-28). The only DLT occurred at 320 mg (grade 3 fatigue). Stable disease occurred at 150 mg/d (28 weeks; RCC) and 320 mg/d (16 weeks; breast, parotid). Escalation halted at 320 mg/d. Day 28 pharmacokinetics indicated absorption and active metabolites.Continuous MKC-1 was well-tolerated; there were no RECIST responses, although clinical benefit occurred in 3/24 pts. Dose escalation stopped at 320 mg/d, and this is the MTD as defined by the CRM dose escalation algorithm; this cumulative dose/cycle exceeds that determined from intermittent dosing studies. A TITE-CRM allowed for rapid dose escalation and was able to account for late toxicities with continuous dosing via a modified algorithm.CONCLUSIONContinuous MKC-1 was well-tolerated; there were no RECIST responses, although clinical benefit occurred in 3/24 pts. Dose escalation stopped at 320 mg/d, and this is the MTD as defined by the CRM dose escalation algorithm; this cumulative dose/cycle exceeds that determined from intermittent dosing studies. A TITE-CRM allowed for rapid dose escalation and was able to account for late toxicities with continuous dosing via a modified algorithm. MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using intermittent dosing schedule, however additional preclinical data suggested continuous dosing could be efficacious with additional effects against the mTor/AKT pathway. The primary objectives were to determine the maximum tolerated dose (MTD) and response of continuous MKC-1. Secondary objectives included characterizing the dose limiting toxicities (DLT) and pharmacokinetics (PK). Methods Patients with solid malignancies were eligible, if they had measurable disease, ECOG PS ≤1, and adequate organ function. Exclusions included brain metastases and inability to receive oral drug. MKC-1 was dosed twice daily, continuously in 28-day cycles. Other medications were eliminated if there were possible drug interactions. Doses were assigned using a TITE-CRM algorithm following enrollment of the first 3 pts. Disease response was assessed every 8 weeks. Results Between 5/08-9/09, 24 patients enrolled (15 M/9 F, median 58 years, range 44-77). Patients 1-3 received 120 mg/d of MKC-1; patients 4-24 were dosed per the TITE-CRM algorithm: 150 mg [n=1], 180 [2], 200 [1], 230 [1], 260 [5], 290 [6], 320 [5]. The median time on drug was 8 weeks (range 4-28). The only DLT occurred at 320 mg (grade 3 fatigue). Stable disease occurred at 150 mg/d (28 weeks; RCC) and 320 mg/d (16 weeks; breast, parotid). Escalation halted at 320 mg/d. Day 28 pharmacokinetics indicated absorption and active metabolites. Conclusion Continuous MKC-1 was well-tolerated; there were no RECIST responses, although clinical benefit occurred in 3/24 pts. Dose escalation stopped at 320 mg/d, and this is the MTD as defined by the CRM dose escalation algorithm; this cumulative dose/cycle exceeds that determined from intermittent dosing studies. A TITE-CRM allowed for rapid dose escalation and was able to account for late toxicities with continuous dosing via a modified algorithm. [PUBLICATION ABSTRACT]
Author	Tevaarwerk, Amye Sidor, Carolyn Wilding, George Bailey, Howard Liu, Glenn Eickhoff, Jens Chappell, Rick Arnott, Jamie Schelman, William
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CitedBy_id	crossref_primary_10_1186_s12874_020_01012_z crossref_primary_10_1016_j_ygyno_2012_08_040 crossref_primary_10_1186_s12885_021_08440_0 crossref_primary_10_1016_j_molonc_2014_07_025 crossref_primary_10_1080_10543406_2017_1289952 crossref_primary_10_1038_nrclinonc_2013_35 crossref_primary_10_1186_1745_6215_13_145 crossref_primary_10_1158_1078_0432_CCR_15_2365 crossref_primary_10_1007_s10637_011_9708_3 crossref_primary_10_1016_j_ctrv_2025_102906 crossref_primary_10_1200_JCO_2013_54_6051 crossref_primary_10_3389_fped_2016_00025
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References_xml	– volume: 25 start-page: 83 year: 1999 end-page: 101 ident: CR12 article-title: Clinical pharmacology of anticancer agents in relation to formulations and administration routes publication-title: Cancer Treat Rev doi: 10.1053/ctrv.1998.0107 – volume: 22 start-page: 3366 year: 2004 end-page: 74 ident: CR3 article-title: Phase I and pharmacokinetic study of the novel oral cell-cycle inhibitor Ro 31-7453 in patients with advanced solid tumors publication-title: J Clin Oncol doi: 10.1200/JCO.2004.12.007 – volume: 52 start-page: 673 year: 1996 end-page: 84 ident: CR6 article-title: Continual reassessment method: a likelihood approach publication-title: Biometrics doi: 10.2307/2532905 – volume: 27 start-page: e19005 issue: suppl year: 2009 ident: CR1 article-title: Phase I/II study of MKC-1 and pemetrexed (PEM) as second-line therapy in patients (pts) with advanced non-small cell lung cancer (NSCLC) publication-title: J Clin Oncol – volume: 27 start-page: 5577 issue: suppl year: 2009 ident: CR4 article-title: Phase II study of MKC-1 in patients with metastatic or resistant epithelial ovarian cancer or advanced endometrial cancer publication-title: J Clin Oncol – volume: 56 start-page: 1177 year: 2000 end-page: 82 ident: CR8 article-title: Sequential designs for phase I clinical trials with late-onset toxicities publication-title: Biometrics doi: 10.1111/j.0006-341X.2000.01177.x – ident: CR11 – volume: 24 start-page: 4426 year: 2006 end-page: 33 ident: CR7 article-title: Designing dose-escalation trials with late-onset toxicities using the time-to-event continual reassessment method publication-title: J Clin Oncol doi: 10.1200/JCO.2005.04.3844 – volume: 92 start-page: 205 year: 2000 end-page: 16 ident: CR10 article-title: New guidelines to evaluate the response to treatment in solid tumors. European Organization for Research and Treatment of Cancer, National Cancer Institute of the United States, National Cancer Institute of Canada publication-title: J Natl Cancer Inst doi: 10.1093/jnci/92.3.205 – ident: CR5 – volume: 14 start-page: 1149 year: 1995 end-page: 61 ident: CR13 article-title: Some practical improvements in the continual reassessment method for phase I studies publication-title: Stat Med doi: 10.1002/sim.4780141102 – volume: 10 start-page: 4374 year: 2004 end-page: 82 ident: CR2 article-title: A phase I clinical and pharmacokinetic study of Ro 31-7453 given as a 7- or 14-day oral twice daily schedule every 4 weeks in patients with solid tumors publication-title: Clin Cancer Res doi: 10.1158/1078-0432.CCR-04-0135 – volume: 25 start-page: 2027 year: 2006 end-page: 42 ident: CR9 article-title: A model-based approach in the estimation of the maximum tolerated dose in phase I cancer clinical trials publication-title: Stat Med doi: 10.1002/sim.2334 – volume: 24 start-page: 4426 year: 2006 ident: 9629_CR7 publication-title: J Clin Oncol doi: 10.1200/JCO.2005.04.3844 – volume: 25 start-page: 2027 year: 2006 ident: 9629_CR9 publication-title: Stat Med doi: 10.1002/sim.2334 – ident: 9629_CR5 doi: 10.1200/jco.2008.26.15_suppl.1046 – ident: 9629_CR11 – volume: 56 start-page: 1177 year: 2000 ident: 9629_CR8 publication-title: Biometrics doi: 10.1111/j.0006-341X.2000.01177.x – volume: 14 start-page: 1149 year: 1995 ident: 9629_CR13 publication-title: Stat Med doi: 10.1002/sim.4780141102 – volume: 22 start-page: 3366 year: 2004 ident: 9629_CR3 publication-title: J Clin Oncol doi: 10.1200/JCO.2004.12.007 – volume: 27 start-page: e19005 issue: suppl year: 2009 ident: 9629_CR1 publication-title: J Clin Oncol doi: 10.1200/jco.2009.27.15_suppl.e19005 – volume: 92 start-page: 205 year: 2000 ident: 9629_CR10 publication-title: J Natl Cancer Inst doi: 10.1093/jnci/92.3.205 – volume: 10 start-page: 4374 year: 2004 ident: 9629_CR2 publication-title: Clin Cancer Res doi: 10.1158/1078-0432.CCR-04-0135 – volume: 25 start-page: 83 year: 1999 ident: 9629_CR12 publication-title: Cancer Treat Rev doi: 10.1053/ctrv.1998.0107 – volume: 52 start-page: 673 year: 1996 ident: 9629_CR6 publication-title: Biometrics doi: 10.2307/2532905 – volume: 27 start-page: 5577 issue: suppl year: 2009 ident: 9629_CR4 publication-title: J Clin Oncol doi: 10.1200/jco.2009.27.15_suppl.5577
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Snippet	Summary Background MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor... MKC-1 is an oral cell-cycle inhibitor with broad antitumor activity in preclinical models. Clinical studies demonstrated modest antitumor activity using...
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SubjectTerms	Adult Aged Algorithms Antineoplastic Agents - administration & dosage Antineoplastic Agents - adverse effects Antineoplastic Agents - pharmacokinetics Binding sites Cancer Cancer therapies Cell cycle Clinical trials Diarrhea Dose-Response Relationship, Drug Drug dosages Drug therapy Enrollments Female Humans Indoles - administration & dosage Indoles - adverse effects Indoles - pharmacokinetics Male Medicine Medicine & Public Health Metastasis Middle Aged Nausea Neoplasm Metastasis Neoplasms - drug therapy Neoplasms - metabolism Neoplasms - pathology Oncology Patients Pharmacokinetics Pharmacology Pharmacology/Toxicology Phase I Studies Radiation therapy Studies Toxicity Tumors Vomiting
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Title	Phase I study of continuous MKC-1 in patients with advanced or metastatic solid malignancies using the modified Time-to-Event Continual Reassessment Method (TITE-CRM) dose escalation design
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