Safety and pharmacokinetics of milademetan, a MDM2 inhibitor, in Japanese patients with solid tumors: A phase I study

Safety and pharmacokinetics of milademetan, a MDM2 inhibitor, in Japanese patients with solid tumors: A phase I study

Milademetan (DS‐3032, RAIN‐32) is an orally available mouse double minute 2 (MDM2) antagonist with potential antineoplastic activity owing to increase in p53 activity through interruption of the MDM2‐p53 interaction. This phase I, dose‐escalating study assessed the safety, tolerability, efficacy, an...

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Veröffentlicht in:Cancer science 2021-06, Vol.112 (6), p.2361-2370
Hauptverfasser: Takahashi, Shunji, Fujiwara, Yutaka, Nakano, Kenji, Shimizu, Toshio, Tomomatsu, Junichi, Koyama, Takafumi, Ogura, Mariko, Tachibana, Masaya, Kakurai, Yasuyuki, Yamashita, Tomonari, Sakajiri, Sakura, Yamamoto, Noboru
Format: Artikel
Sprache:eng
Schlagworte:
Adverse events
Anemia
Antitumor activity
Appetite loss
Blood cell count
Blood transfusions
Cancer therapies
Cell cycle
Cytokines
Dictionaries
Disease control
Dosage
DS‐3032
Laboratories
Lymphoma
Lymphomas
MDM2 protein
milademetan
Mutation
Nausea
Neutropenia
Oncology
Original
Patients
Pharmacokinetics
phase I clinical trial
Platelets
RAIN‐32
Response rates
Safety
Safety and security measures
Solid tumors
Thrombocytopenia
Tumor proteins
Tumors
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Zusammenfassung:Milademetan (DS‐3032, RAIN‐32) is an orally available mouse double minute 2 (MDM2) antagonist with potential antineoplastic activity owing to increase in p53 activity through interruption of the MDM2‐p53 interaction. This phase I, dose‐escalating study assessed the safety, tolerability, efficacy, and pharmacokinetics of milademetan in 18 Japanese patients with solid tumors who relapsed after or were refractory to standard therapy. Patients aged ≥ 20 years received oral milademetan once daily (60 mg, n = 3; 90 mg, n = 11; or 120 mg, n = 4) on days 1 to 21 in a 28‐day cycle. Dose‐limiting toxicities, safety, tolerability, maximum tolerated dose, pharmacokinetics, and recommended dose for phase II were determined. The most frequent treatment‐emergent adverse events included nausea (72.2%), decreased appetite (61.1%), platelet count decreased (61.1%), white blood cell count decreased (50.0%), fatigue (50.0%), and anemia (50.0%). Dose‐limiting toxicities (three events of platelet count decreased and one nausea) were observed in the 120‐mg cohort. The plasma concentrations of milademetan increased in a dose‐dependent manner. Stable disease was observed in seven out of 16 patients (43.8%). Milademetan was well tolerated and showed modest antitumor activity in Japanese patients with solid tumors. The recommended dose for phase II was considered to be 90 mg in the once‐daily 21/28‐day schedule. Future studies would be needed to further evaluate the potential safety, tolerability, and clinical activity of milademetan in patients with solid tumors and lymphomas. The trial was registered with Clinicaltrials.jp: JapicCTI‐142693. We are presenting the first report of a phase I study evaluating the safety, tolerability, efficacy, and pharmacokinetics of milademetan in Japanese patients with advanced solid tumors. The plasma concentrations of milademetan increased in a dose‐dependent manner. Milademetan was well tolerated and showed modest antitumor activity in Japanese patients with solid tumors.
ISSN:1347-9032
1349-7006
DOI:10.1111/cas.14875