A Phase 1/2 Study of Safety and Tolerability of MT-125 With Chemoradiation in Patients With Newly Diagnosed MGMT Methylated Glioblastoma (NOVA-GBM)
A Phase 1/2 Dose Escalation and Randomized Expansion Study of Safety, Tolerability, and Pharmacokinetics of MT-125 Monotherapy With Chemoradiation in Patients With Newly Diagnosed MGMT Methylated Glioblastoma
調査の概要
詳細な説明
MT-125 is a potent, selective, and central nervous system (CNS) permeable dual small molecule inhibitor of the non-muscle myosin II (NMII) paralogs, IIA and IIB. MT-125 is being developed by Myosin Therapeutics Inc. as a potential treatment for glioblastoma (GBM). NMIIs are molecular motor ATPases that act directly on actin to regulate the cytoskeleton's control of cellular processes such as movement, division, signaling and mitochondrial biology. As a result, simultaneous inhibition of NMIIA and IIB with MT-125 interferes with tumor cell proliferation, invasion and metastasis, while also generating reactive oxygen species (ROS) in tumor cells. The latter is due to the role of NMII in mitochondrial quality control and underlies the synergistic survival benefit observed in preclinical studies when MT-125 and radiation therapy (RT) are combined. Additionally, NMIIA is upregulated in several types of cancer, including GBM, speaking to its importance in cancer physiology and making these tumor cells highly sensitive to its inhibition. The focus of this clinical study is GBM.
Patients with GBM have a poor prognosis, and there have been no new Food and Drug Administration (FDA) approved drugs for these patients since 2008, when bevacizumab was approved. The current well-known standard of care for newly diagnosed GBM is maximal safe surgical resection followed by concurrent RT with temozolomide (TMZ). O6-methylguanine- DNA methyltransferase (MGMT) promoter methylation status is the most predictive biomarker for TMZ responsiveness, where patients with unmethylated MGMT do not respond to TMZ.
MT-125 significantly prolongs survival as a monotherapy in animal models and is synergistic with both RT and with FDA-approved oncogenic kinase inhibitors to further enhance survival. The Sponsor is currently evaluating MT-125 as a monotherapy in a first-in-human (FIH) trial (STAR-GBM) with standard of care RT in newly diagnosed isocitrate dehydrogenase (IDH) wildtype / MGMT unmethylated GBM. Due to the poor response of MGMT unmethylated tumors to TMZ, the chemotherapeutic is excluded in the STAR-GBM trial. Here we will evaluate MT-125 as a monotherapy in a Phase 1/2 trial (NOVA-GBM) in newly diagnosed IDH wildtype / MGMT methylated GBM with standard of care RT and TMZ, following the standard chemoradiation treatment regimen.
In the pivotal 28-day nonclinical safety studies of MT-125, no dose-limiting toxicities (DLT) or adverse effects (AE) were noted in any of the parameters evaluated (clinical observations, functional endpoints, clinical pathology, macroscopic and histologic tissue assessments) at doses up to the NOAELs, 20 mg/kg/day and 30 mg/kg/day in dogs and rats, respectively, which yielded systemic MT-125 exposures 10- to 16-fold greater than efficacious exposures in pharmacodynamic in vivo models. As the NOAELs in both studies were below the STD10 (rats) and HNSTD (dogs), the calculated safety margins are conservative.
The goal of this Phase 1/2, MT-125 dose escalation and expansion study is to evaluate the safety and tolerability of MT-125 administered 5 consecutive days per week with 2 days off for the 6 weeks of outpatient RT plus TMZ. Participants with newly diagnosed GBM with histologically or molecularly confirmed IDH wildtype and MGMT methylation will be eligible to enroll. The DLT observation window will be 6 weeks following first treatment administration, and a Bayesian Optimal Interval (BOIN) trial design will be used to efficiently evaluate up to four dose levels. Secondary endpoints for this Phase 1/2 study will include determining the maximum tolerated dose (MTD), which will contribute to the selection of the recommended phase 2 dose (RP2D) and evaluating the systemic pharmacokinetics (PK) of MT-125.
Once the MTD is determined, additional participants will be enrolled into a randomized, parallel dose expansion cohort, consisting of up to 2 potential doses of MT-125. The dose levels for the expansion cohort will be selected as the MTD and the dose below the MTD. Overall response rate (ORR) in those participants with measurable disease, progression-free survival (PFS6) in all participants, and Overall Survival (OS) in all participants are included as exploratory endpoints
If no MTD is identified within the initially defined dose range and all tested doses are deemed well-tolerated based on the observed DLTs, the study may be paused temporarily to allow consideration of dose levels beyond those originally planned.
研究の種類
入学 (推定)
段階
- フェーズ2
- フェーズ 1
連絡先と場所
研究場所
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Arizona
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Phoenix、Arizona、アメリカ、85054
- Mayo Clinic Hospital
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コンタクト:
- Clinical Trials Referral Office
- 電話番号:855-776-0015
- メール:mayocliniccancerstudies@mayo.edu
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主任研究者:
- Shannon F Fortin-Ensign, MD, PhD
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Florida
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Jacksonville、Florida、アメリカ、32224
- Mayo Clinic Hospital
-
コンタクト:
- Clinical Trials Referral Office
- 電話番号:855-776-0015
- メール:mayocliniccancerstudies@mayo.edu
-
主任研究者:
- Wendy J Sherman, MD
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Minnesota
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Rochester、Minnesota、アメリカ、55905
- Mayo Clinic Hospital
-
コンタクト:
- Clinical Trials Referral Office
- 電話番号:855-776-0015
- メール:mayocliniccancerstudies@mayo.edu
-
主任研究者:
- Ugur Sener, MD
-
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参加基準
適格基準
就学可能な年齢
- 大人
- 高齢者
健康ボランティアの受け入れ
説明
Inclusion Criteria:
- Age ≥18 years at the time of signing the informed consent form (ICF).
- New Diagnosed with histologically or molecularly confirmed IDH wildtype and MGMT methylated GBM.
- Eastern Cooperative Oncology Group (ECOG) Performance Status (PS) 0, 1 or 2..
The following laboratory values obtained ≤15 days prior to registration:
- Hemoglobin ≥9.0 g/dL
- Absolute neutrophil count (ANC) ≥1500/mm3
- Platelet count ≥100,000/mm3
- Total bilirubin ≤1.5 x upper limit of normal (ULN)
- Alanine aminotransferase (ALT) and aspartate transaminase (AST) ≤3 x ULN (or ≤5 x ULN for participants with liver involvement)
- Prothrombin time (PT)/ International normalized ratio (INR)/ Activated partial thromboplastin time (aPTT) ≤1.5 x ULN OR if participant is receiving anticoagulant therapy and INR or aPTT is within target range of therapy
- Serum eGFR ≥60 ml/min
- QTc 470 ms on triplicate 12 lead ECG ≤29 days prior to registration. NOTE: QTc intervals will be corrected using Fridericia's formula (Fridericia 1920)
- Echocardiographic Assessment: Left Ventricular Ejection Fraction (LVEF) ≥ 55%.
Negative serum pregnancy test done ≤7 days prior to first dose of MT-125 administration, for persons of childbearing potential only.
a. If >7 days between last test and first dose of study treatment, the serum pregnancy test will be repeated.
- Has provided written informed consent.
- Ability to complete questionnaire(s) by themselves or with assistance.
- Willing to return to enrolling institution for follow-up (during the Active Monitoring Phase of the study).
- On a stable dose of steroids for at least 2 weeks prior to enrollment
Exclusion Criteria:
Any of the following because this study involves an investigational agent, the genotoxic, mutagenic, and teratogenic effects of which on the developing fetus and newborn are unknown:
- Pregnant persons
- Nursing persons
- Persons of childbearing potential and persons able to father a child who are unwilling to employ adequate contraception (see Appendix 2 for highly effective forms of contraception)
- Co-morbid systemic illnesses or other severe concurrent disease which, in the judgment of the investigator, would make the participant inappropriate for entry into this study or interfere significantly with the proper assessment of safety and toxicity of the prescribed regimens.
- Receiving any other investigational agent.
- Any concomitant disease, condition, or treatment that could interfere with the conduct of the study, or that would, in the opinion of the Investigator or Sponsor, pose an unacceptable risk to the participant in the study or interfere with the interpretation of study data.
- Other active malignancy requiring therapy such as RT, chemotherapy, or immunotherapy. Participants on hormonal therapy for treated breast or prostate cancer are permitted if they meet other eligibility criteria. NOTE: Participants with malignancies under active surveillance are still eligible.
研究計画
研究はどのように設計されていますか?
デザインの詳細
- 主な目的:処理
- 割り当て:非ランダム化
- 介入モデル:並列代入
- マスキング:なし(オープンラベル)
武器と介入
参加者グループ / アーム |
介入・治療 |
|---|---|
|
実験的:MT-125 at 25 mg
Up to 6 participants will receive 25 mg of MT-125 for 5 days then off for 2 days for a total of 6 weeks in combination of RT plus TMZ
|
これは、Ind 170975に基づく治験中の新薬です。
|
|
実験的:MT-125 at 50 mg
Up to 6 participants will receive 50 mg of MT-125 for 5 days then off for 2 days for a total of 6 weeks in combination of RT plus TMZ
|
これは、Ind 170975に基づく治験中の新薬です。
|
|
実験的:MT-125 at 83.5 mg
Up to 6 participants will receive 83.5 mg of MT-125 for 5 days then off for 2 days for a total of 6 weeks in combination of RT plus TMZ
|
これは、Ind 170975に基づく治験中の新薬です。
|
|
実験的:MT-125 at 100 mg
Up to 6 participants will receive 100 mg of MT-125 for 5 days then off for 2 days for a total of 6 weeks in combination of RT plus TMZ
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これは、Ind 170975に基づく治験中の新薬です。
|
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実験的:MT-125 at MTD and one dose lower than MTD
Participants will be randomized to receive either MTD or one dose lower than MTD for 5 days, then off 2 days for a total of 6 weeks in combination with RT plus TMZ
|
これは、Ind 170975に基づく治験中の新薬です。
|
この研究は何を測定していますか?
主要な結果の測定
結果測定 |
メジャーの説明 |
時間枠 |
|---|---|---|
|
Dose Limiting Toxicity Measurement
時間枠:Day 1 through 6 weeks of treatment
|
The dose escalation portion of this study will follow a BOIN design with cohorts containing a min of 3 DLT evaluable participants.
If the observed DLT rate at the current dose is ≤0.236, then the decision will be to escalate the dose to the next higher dose level; if the observed DLT rate at the current dose is >0.359, then the decision will be to deescalate the dose to the next lower dose level; otherwise, the decision will be to stay at the current dose level.
|
Day 1 through 6 weeks of treatment
|
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Incidence and Severity of AEs
時間枠:Day 1 through 6 weeks of treatment
|
Incidence and Severity, attribution, grade and type of AE will be assessed based on the NCI CTCAE v5.
|
Day 1 through 6 weeks of treatment
|
二次結果の測定
結果測定 |
メジャーの説明 |
時間枠 |
|---|---|---|
|
最大耐量
時間枠:1日目から40日目
|
MT-125の最大耐量(MTD)を決定します
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1日目から40日目
|
|
PKパラメーター-T1/2
時間枠:勉強日に完了。 1日目、2日目、5日目、19日目、33日目、40日目
|
薬物の血漿濃度が50%減少するのに必要な時間
|
勉強日に完了。 1日目、2日目、5日目、19日目、33日目、40日目
|
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フェーズ2の用量を決定します
時間枠:1日目から6週間の治療
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MT-125の推奨されるフェーズ2用量(RP2D)を決定する
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1日目から6週間の治療
|
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PK Parameters- Cmax
時間枠:Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
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The time it takes for a drug to reach a maximum concentration after administration.
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Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
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PK Parameters-AUC 0-24hr
時間枠:Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
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Area under the plasma concentration-time curve over the last 24 hour dosing interval.
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Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
|
|
PK Parameters - CL
時間枠:Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
|
CL will quantify the body's efficiency in eliminating MT-125
|
Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
|
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PK Parameters - Vss
時間枠:Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
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The steady state volume of distribution that describes how MT-125 distributes throughout the body once it has reached a state of equilibrium.
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Completed on study days; Day 1, Day 2, Day 5, Day 19, Day 33 and Day 40
|
その他の成果指標
結果測定 |
メジャーの説明 |
時間枠 |
|---|---|---|
|
ORRなどの臨床的有効性測定に関する予備的データを取得するため
時間枠:治療完了後平均1年を経過した時点での第1日目
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測定可能な疾患を有する患者における全奏効率
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治療完了後平均1年を経過した時点での第1日目
|
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臨床的有効性に関する予備的データを得るための探索的分析
時間枠:治療完了後最大1年間
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MRI画像に基づく6ヶ月間の無増悪生存期間(PFS6)
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治療完了後最大1年間
|
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臨床的有効性に関する予備データを得るために
時間枠:治療完了後平均1年経過した時点におけるDay 1。
|
全生存期間(OS)
|
治療完了後平均1年経過した時点におけるDay 1。
|
協力者と研究者
スポンサー
協力者
出版物と役立つリンク
一般刊行物
- Yuan Y, Hess KR, Hilsenbeck SG, Gilbert MR. Bayesian Optimal Interval Design: A Simple and Well-Performing Design for Phase I Oncology Trials. Clin Cancer Res. 2016 Sep 1;22(17):4291-301. doi: 10.1158/1078-0432.CCR-16-0592. Epub 2016 Jul 12.
- Stupp R, Mason WP, van den Bent MJ, Weller M, Fisher B, Taphoorn MJ, Belanger K, Brandes AA, Marosi C, Bogdahn U, Curschmann J, Janzer RC, Ludwin SK, Gorlia T, Allgeier A, Lacombe D, Cairncross JG, Eisenhauer E, Mirimanoff RO; European Organisation for Research and Treatment of Cancer Brain Tumor and Radiotherapy Groups; National Cancer Institute of Canada Clinical Trials Group. Radiotherapy plus concomitant and adjuvant temozolomide for glioblastoma. N Engl J Med. 2005 Mar 10;352(10):987-96. doi: 10.1056/NEJMoa043330.
- Wen PY, Macdonald DR, Reardon DA, Cloughesy TF, Sorensen AG, Galanis E, Degroot J, Wick W, Gilbert MR, Lassman AB, Tsien C, Mikkelsen T, Wong ET, Chamberlain MC, Stupp R, Lamborn KR, Vogelbaum MA, van den Bent MJ, Chang SM. Updated response assessment criteria for high-grade gliomas: response assessment in neuro-oncology working group. J Clin Oncol. 2010 Apr 10;28(11):1963-72. doi: 10.1200/JCO.2009.26.3541. Epub 2010 Mar 15.
- Hegi ME, Diserens AC, Gorlia T, Hamou MF, de Tribolet N, Weller M, Kros JM, Hainfellner JA, Mason W, Mariani L, Bromberg JE, Hau P, Mirimanoff RO, Cairncross JG, Janzer RC, Stupp R. MGMT gene silencing and benefit from temozolomide in glioblastoma. N Engl J Med. 2005 Mar 10;352(10):997-1003. doi: 10.1056/NEJMoa043331.
- Hegi ME, Genbrugge E, Gorlia T, Stupp R, Gilbert MR, Chinot OL, Nabors LB, Jones G, Van Criekinge W, Straub J, Weller M. MGMT Promoter Methylation Cutoff with Safety Margin for Selecting Glioblastoma Patients into Trials Omitting Temozolomide: A Pooled Analysis of Four Clinical Trials. Clin Cancer Res. 2019 Mar 15;25(6):1809-1816. doi: 10.1158/1078-0432.CCR-18-3181. Epub 2018 Dec 4.
- Melhem JM, Detsky J, Lim-Fat MJ, Perry JR. Updates in IDH-Wildtype Glioblastoma. Neurotherapeutics. 2022 Oct;19(6):1705-1723. doi: 10.1007/s13311-022-01251-6. Epub 2022 May 31.
- Kenchappa RS, Radnai L, Young EJ, Zarco N, Lin L, Dovas A, Meyer CT, Haddock A, Hall A, Toth K, Canoll P, Nagaiah NKH, Rumbaugh G, Cameron MD, Kamenecka TM, Griffin PR, Miller CA, Rosenfeld SS. MT-125 inhibits non-muscle myosin IIA and IIB and prolongs survival in glioblastoma. Cell. 2025 Aug 21;188(17):4622-4639.e19. doi: 10.1016/j.cell.2025.05.019. Epub 2025 Jun 10.
- Liu S, Yuan Y. Bayesian optimal interval designs for phase I clinical trials. Journal of the Royal Statistical Society: Series C (Applied Statistics). 2015;64(3):507-23. . : . .
研究記録日
主要日程の研究
研究開始 (推定)
一次修了 (推定)
研究の完了 (推定)
試験登録日
最初に提出
QC基準を満たした最初の提出物
最初の投稿 (実際)
学習記録の更新
投稿された最後の更新 (実際)
QC基準を満たした最後の更新が送信されました
最終確認日
詳しくは
本研究に関する用語
キーワード
追加の関連 MeSH 用語
その他の研究ID番号
- MT-125-GBM-201
- 26C19 (その他の助成金/資金番号:Florida Cancer Innovation Fund)
個々の参加者データ (IPD) の計画
個々の参加者データ (IPD) を共有する予定はありますか?
医薬品およびデバイス情報、研究文書
米国FDA規制医薬品の研究
米国FDA規制機器製品の研究
この情報は、Web サイト clinicaltrials.gov から変更なしで直接取得したものです。研究の詳細を変更、削除、または更新するリクエストがある場合は、register@clinicaltrials.gov。 までご連絡ください。 clinicaltrials.gov に変更が加えられるとすぐに、ウェブサイトでも自動的に更新されます。
MT-125の臨床試験
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Myosin Therapeutics Inc.National Cancer Institute (NCI); Mayo Clinic募集
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Tanabe Pharma Corporation完了
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Mitsubishi Tanabe Pharma Corporation完了再発寛解型多発性硬化症クロアチア, ブルガリア, チェコ共和国, イタリア, ロシア連邦, スペイン, イギリス, ドイツ, リトアニア, ポーランド, ベルギー, ハンガリー, セルビア, フィンランド, ウクライナ, スイス, カナダ, 七面鳥
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Mitsubishi Tanabe Pharma Corporation完了
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University of NebraskaNortheast Nebraska Public Health Department完了
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Tanabe Pharma Corporation完了