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क्लिनिकल ट्रायल NCT04947319 के लिए प्रतिरोधी प्राथमिक केंद्रीय तंत्रिका तंत्र लिंफोमा, प्राथमिक सीएनएस लिम्फोमा वर्तमान में सक्रिय, भर्ती नहीं है। सभी विवरणों के लिए क्लिनिकल ट्रायल रडार कार्ड दृश्य और AI खोज उपकरण देखें, या यहाँ कुछ भी पूछें।
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कार्ड दृश्य
खोज पर वापस जाएँ

Study of Tirabrutinib (ONO-4059) in Patients With Primary Central Nervous System Lymphoma (PROSPECT Study) चरण II 119

सक्रिय, भर्ती नहीं
चिकित्सा परीक्षण का विवरण मुख्य रूप से अंग्रेजी में उपलब्ध है। हालाँकि, ट्रायल रडार AI मदद कर सकता है! बस 'अध्ययन समझाएं' पर क्लिक करें और अपनी चुनी हुई भाषा में परीक्षण की जानकारी देखें और चर्चा करें।
क्लिनिकल ट्रायल NCT04947319 का मुख्य उद्देश्य उपचार का अध्ययन करना है। यह चिकित्सकीय अध्ययन प्रतिरोधी प्राथमिक केंद्रीय तंत्रिका तंत्र लिंफोमा, प्राथमिक सीएनएस लिम्फोमा से जुड़ा हुआ है और यह एक चरण II हस्तक्रियात्मक परीक्षण है। परीक्षण वर्तमान में सक्रिय, भर्ती नहीं चल रहा है। इसकी शुरुआत 29 दिसंबर 2021 को हुई थी, और इसमें कुल 119 प्रतिभागियों के नामांकन की योजना है। ओनो फार्मास्युटिकल इस परीक्षण का नेतृत्व कर रहे हैं और इसके 31 मार्च 2027 तक पूरा होने की उम्मीद है। ClinicalTrials.gov वेबसाइट पर यह जानकारी 24 अक्तूबर 2025 को अंतिम बार अपडेट की गई थी
संक्षिप्त सारांश
This study will evaluate the efficacy, safety, and pharmacokinetics of tirabrutinib monotherapy in patients with relapsed or refractory PCNSL (Part A), and tirabrutinib in combination with one of two different high dose methotrexate based regimens (methotrexate/ temozolomide/rituximab or rituximab/methotrexate/procarbazine/ vincristine) as first line therapy in patients with newly diagnosed, treatment naïve PCNSL (Pa...और दिखाएँ
आधिकारिक शीर्षक

An Open-label Phase II Study to Investigate the Efficacy, Safety, and Pharmacokinetics of Tirabrutinib in Patients With Primary Central Nervous System Lymphoma (PCNSL)

स्वास्थ्य स्थितियां
प्रतिरोधी प्राथमिक केंद्रीय तंत्रिका तंत्र लिंफोमाप्राथमिक सीएनएस लिम्फोमा
अन्य अध्ययन आईडी
  • ONO-4059-09
NCT नंबर
NCT04947319
अध्ययन प्रारंभ तिथि (वास्तविक)
2021-12-29
अंतिम अद्यतन प्रकाशित
2025-10-24
अध्ययन की समाप्ति तिथि (अनुमानित)
2027-03-31
नामांकन (अनुमानित)
119
अध्ययन प्रकार
हस्तक्रियात्मक
चरण
चरण II
स्थिति
सक्रिय, भर्ती नहीं
प्रमुख शब्द
Bruton's Tyrosine Kinase Inhibitor, BTKi, tirabrutinib, ONO-4059, PROSPECT
प्राथमिक उद्देश्य
उपचार
डिज़ाइन आवंटन
गैर-यादृच्छिक
हस्तक्षेप मॉडल
समानांतर
अंधकरण
कोई नहीं (खुला लेबल)
समूह/हस्तक्षेप
प्रतिभागी समूह/शाखाहस्तक्षेप/उपचार
प्रयोगात्मकTirabrutinib monotherapy in patients with relapsed or refractory PCNSL (Part A)
Patients with relapsed or refractory PCNSL who meet eligibility criteria will be enrolled to receive tirabrutinib monotherapy.
Tirabrutinib
Part A: Tirabrutinib 480 mg, taken orally, once a day on an empty stomach. Tirabrutinib treatment may be continued until disease progression or clinically unacceptable toxicity is observed.
प्रयोगात्मकTirabrutinib + MTR in patients with newly diagnosed, treatment naïve PCNSL (Part B, Arm 1)
Patients with newly diagnosed treatment naïve PCNSL who meet eligibility criteria will be enrolled to receive tirabrutinib + methotrexate/temozolomide/rituximab (MTR)
Tirabrutinib
Part B, Arm 1 - Tirabrutinib 320 mg or 480 mg, taken orally, once a day on an empty stomach in combination with an MTR induction regimen. Tirabrutinib with MTR treatment will be continued for 4 induction cycles (28-day/cycle), or until disease progression or clinically unacceptable toxicity is observed. For patients not receiving consolidation treatment following induction, tirabrutinib 480 mg will be continued unti...और दिखाएँ
प्रयोगात्मकTirabrutinib + R-MPV in patients with newly diagnosed, treatment naïve PCNSL (Part B, Arm 2)
Patients with newly diagnosed treatment naïve PCNSL who meet eligibility criteria will be enrolled to receive tirabrutinib + rituximab/methotrexate/procarbazine/vincristine (R-MPV)
Tirabrutinib
Part B, Arm 2 - Tirabrutinib 320 mg or 480 mg, taken orally, once a day on an empty stomach in combination with an R-MPV induction regimen. Tirabrutinib with R-MPV treatment will be continued for 4 induction cycles (28-day/cycle), or until disease progression or clinically unacceptable toxicity is observed. For patients not receiving consolidation treatment following induction, tirabrutinib 480 mg will be continued ...और दिखाएँ
प्राथमिक परिणाम माप
परिणाम मापमाप विवरणसमय सीमा
Overall response rate (ORR) (Part A)
Overall response rate is defined as the proportion of patients with a best overall response of Complete response (CR), Complete response - unconfirmed (CRu), or (=partial response (PR) as determined by an independent review committee according to the International PCNSL Collaborative Group (IPCG) criteria.
1 year
Tirabrutinib dose estimate (Part B)
Estimate of tirabrutinib dose in combination with each backbone induction regimen (MTR and R-MPV) based upon treatment related AEs, SAEs, and toxicities observed during the initial cycle of induction therapy in the dose-ranging phase
1 month
Incidence and severity of adverse events (AEs) and serious adverse events (SAEs) during induction (Part B)
Adverse events at each visit with the NCI CTCAE v5.0 used as a guide for the grading of severity.
4 months
Complete response rate (CRR) (Part B)
Complete response rate is defined as the proportion of patients with a best overall response of CR or CRu as determined by an independent review committee according to the IPCG criteria.
4 months
द्वितीयक परिणाम माप
परिणाम मापमाप विवरणसमय सीमा
Duration of response (DOR) (Part A and B)
Duration of response is defined as the time between the date of first response (CR, CRu, or PR) and the date of the first PD according to the IPCG criteria, or date of death due to any cause, whichever occurs first.
2 years
Time to response (TTR) (Part A and B)
Time to response is defined as the time between the date of first administration of tirabrutinib and the date of first response (CR, CRu, or PR) as determined by IRC according to the IPCG criteria.
1 year
Best overall response (BOR) (Part A and B)
Best overall response based on independent review committee (IRC) response determination is defined as the best response and is derived programmatically based upon the visit responses determined by IRC from the date of administration of tirabrutinib to the date of PD as determined by IRC or the date of initiation of subsequent anticancer therapy for PCNSL, whichever occurs first.
1 year
Change in corticosteroid dose (Part A)
Descriptive statistics will be calculated for the actual corticosteroid dose and the change from baseline at each assessment point.
2 years
Incidence and severity of AEs and SAEs (Part A and B)
Adverse events at each visit with the NCI CTCAE v5.0 used as a guide for the grading of severity.
2 years
Laboratory abnormality profile of tirabrutinib as measured by incidence and severity of clinical laboratory abnormalities (Part A and B)
Results of laboratory tests
2 years
ECG parameters by 12 lead ECG (Part A and B)
Heart rate, RR and QT intervals, QTc (QTcF, QTcB), PR interval, and QRS width.
2 years
PK parameters (Cmax) of tirabrutinib in the plasma (Part A and B)
29 days
PK parameters (Tmax) of tirabrutinib in the plasma (Part A and B)
29 days
PK parameters (AUC) of tirabrutinib in the plasma (Part A and B)
29 days
भागीदारी सहायक
पात्रता मानदंड

अध्ययन के लिए पात्र आयु
वयस्क, वृद्ध वयस्क
अध्ययन के लिए न्यूनतम आयु
18 Years
अध्ययन के लिए पात्र लिंग
सभी
  1. Written informed consent by the patient prior to screening
  2. Patients aged ≥ 18 years on the day of consenting to the study
  3. Pathologic diagnosis of PCNSL
  4. Relapse or refractory PCNSL with at least one prior high dose methotrexate (HD-MTX) based therapy for PCNSL
  5. Measurable brain lesion with a minimum diameter > 1.0 cm in gadolinium enhanced magnetic resonance imaging (MRI) performed within 14 days before starting tirabrutinib treatment
  6. Eastern Cooperative Oncology Group performance score (ECOG PS) of 0, 1 or 2
  7. Life expectancy of at least 3 months
  8. Adequate bone marrow, renal, and hepatic function

Inclusion Criteria (Part B)

  1. Written informed consent by the patient prior to screening
  2. Patients aged ≥ 18 years on the day of consenting to the study
  3. Pathologic diagnosis of PCNSL within the past 3 months
  4. No prior anti-tumor treatments for PCNSL
  5. Patients who, in the opinion of the Investigator, are suitable to receive treatment with a high dose methotrexate containing regimen
  6. Measurable brain lesion with a minimum diameter > 1.0 cm in gadolinium enhanced MRI performed within 14 days before starting study treatment
  7. ECOG PS of 0, 1 or 2
  8. Life expectancy of at least 6 months
  9. Adequate bone marrow, renal, and hepatic function

  1. Intraocular PCNSL with no brain lesion

  2. Patient who is intolerant of contrast enhanced MRI due to allergic reactions to contrast agents

  3. Patient with non-B cell PCNSL

  4. Patient with systemic presence of lymphoma

  5. Prior chemotherapy within 21 days, nitrosourea within 42 days, an antibody drug with anticancer activity (e.g., rituximab) within 28 days, prior radiotherapy within 14 days, prior major invasive surgery within 28 days, or allogeneic stem cell transplant within 6 months before starting tirabrutinib treatment

  6. Prior BTK inhibitor treatment

  7. Prior investigational drugs (including treatment in clinical research, unapproved combination products, and new dosage forms) within 28 days or 5 half-lives, whichever is shorter, before starting tirabrutinib treatment

  8. Concomitant systemic corticosteroid on an ongoing basis within 14 days before starting tirabrutinib treatment, with the exception of the following:

    • Equivalent of up to 10 mg/day of prednisone for a disease other than PCNSL
    • Equivalent of up to 50 mg/day of prednisone (equal to 8 mg/day of dexamethasone) for patients with lesions of the brain or spinal cord or both

  9. Patient who has received a CYP3A4 inducer or P-gp inducer within 14 days before starting tirabrutinib treatment

  10. Concomitant warfarin, any other warfarin derivative anticoagulant, vitamin K antagonists, novel oral anticoagulants, or antiplatelet therapy on an ongoing basis within 7 days before starting tirabrutinib treatment

  11. Active malignancy, other than PCNSL requiring systemic therapy

  12. Poorly controlled comorbidity, severe heart, severe lung disease, clinically significant liver diseases that could affect protocol compliance or safety or efficacy assessments

  13. Patient with bleeding diathesis

  14. Patients with a history of moderate or severe hepatic impairment

  15. QTcF > 480 milliseconds or requirement for ongoing treatment with concomitant medications that prolong the QT interval

  16. Active infection, including a HIV, cytomegalovirus infection or SARS-CoV-2, or has had, within 28 days before starting tirabrutinib treatment, an infection (other than nail trichophytosis) that requires hospitalization or an intravenous antibiotic

  17. Prior history of hypersensitivity or anaphylaxis to tirabrutinib

  18. Prior history of Stevens Johnson Syndrome or Toxic Epidermal Necrolysis

  19. Medical history of organ allografts

  20. Tests positive for HIV-1 antibody and HIV-2 antibody, human T-lymphotropic virus 1 antibody, hepatitis B (HB) antigen, or hepatitis C virus (HCV) antibody. Tests positive for HBs antibody or hepatitis B virus core protein antibody and has a result of at least detectable in a hepatitis B virus deoxyribonucleic acid assay despite testing negative for HBs antigen.

  21. Patient is unable to swallow tablets; has malabsorption, malabsorption syndrome, or a comorbidity that affects gastric function; has undergone complete resection of the stomach or small intestine; has ulcerative colitis or symptomatic inflammatory bowel disease; or has partial or complete intestinal obstruction.

  22. Women who are pregnant or lactating

  23. Patient is found incapable of giving consent due to dementia or another such condition

  24. Patient is found to be otherwise ineligible for the study by the Investigator or sub-Investigator.

Exclusion Criteria (Part B)

  1. Intraocular PCNSL with no brain lesion

  2. Patients for whom the selected backbone regimen medications (i.e, methotrexate/temozolomide/rituximab for MTR and rituximab/methotrexate/procarbazine/vincristine for R-MPV) are contraindicated

  3. Patients with a history of intolerable toxicity, hypersensitivity, anaphylaxis to the selected backbone regimen medications

  4. Patient who is intolerant of contrast enhanced MRI due to allergic reactions to contrast agents

  5. Patient with non-B cell PCNSL

  6. Patient with systemic presence of lymphoma

  7. Prior chemotherapy within 21 days, nitrosourea within 42 days, an antibody drug with anticancer activity (e.g., rituximab) within 28 days, prior radiotherapy within 14 days, prior major invasive surgery within 28 days, or allogeneic stem cell transplant within 6 months before starting tirabrutinib treatment

  8. Prior BTK inhibitor treatment

  9. Prior investigational drugs (including treatment in clinical research, unapproved combination products, and new dosage forms) within 28 days or 5 half-lives, whichever is shorter, before starting tirabrutinib treatment

  10. Concomitant systemic corticosteroid on an ongoing basis within 14 days before starting tirabrutinib treatment, with the exception of the following:

    • Equivalent of up to 10 mg/day of prednisone for a disease other than PCNSL
    • Equivalent of up to 50 mg/day of prednisone (equal to 8 mg/day of dexamethasone) for patients with lesions of the brain or spinal cord or both

  11. Patient who has received a CYP3A4 inducer or P-gp inducer within 14 days before starting tirabrutinib treatment

  12. Concomitant warfarin, any other warfarin derivative anticoagulant, vitamin K antagonists, novel oral anticoagulants, or antiplatelet therapy on an ongoing basis within 7 days before starting tirabrutinib treatment

  13. Active malignancy, other than PCNSL requiring systemic therapy

  14. Poorly controlled comorbidity, severe heart, severe lung disease, clinically significant liver diseases that could affect protocol compliance or safety or efficacy assessments

  15. Patient with bleeding diathesis

  16. Patients with a history of moderate or severe hepatic impairment

  17. QTcF > 480 milliseconds or requirement for ongoing treatment with concomitant medications that prolong the QT interval

  18. Active infection, including a HIV, cytomegalovirus infection or SARS-CoV-2, or has had, within 28 days before starting tirabrutinib treatment, an infection (other than nail trichophytosis) that requires hospitalization or an intravenous antibiotic

  19. Prior history of hypersensitivity or anaphylaxis to tirabrutinib

  20. Prior history of Stevens Johnson Syndrome or Toxic Epidermal Necrolysis

  21. Medical history of organ allografts

  22. Tests positive for HIV-1 antibody and HIV-2 antibody, human T-lymphotropic virus 1 antibody, HBs antigen, or HCV antibody. Tests positive for HBs antibody or hepatitis B virus core protein antibody and has a result of at least detectable in a hepatitis B virus deoxyribonucleic acid assay despite testing negative for HBs antigen.

  23. Patient is unable to swallow tablets; has malabsorption, malabsorption syndrome, or a comorbidity that affects gastric function; has undergone complete resection of the stomach or small intestine; has ulcerative colitis or symptomatic inflammatory bowel disease; or has partial or complete intestinal obstruction.

  24. Women who are pregnant or lactating

  25. Patient is found incapable of giving consent due to dementia or another such condition

  26. Patient is found to be otherwise ineligible for the study by the Investigator or sub-Investigator.

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कोई संपर्क डेटा नहीं।
39 1 देशों में अध्ययन स्थान

Alabama

University of Alabama at Birmingham School of Medicine, Birmingham, Alabama, 35233, United States

Arizona

Mayo Clinic- Phoenix, Phoenix, Arizona, 85054, United States

California

City of Hope Comprehensive Breast Cancer Center, Duarte, California, 91010, United States
University of California, Irvine, Irvine, California, 92868, United States
Stanford University, Palo Alto, California, 94304, United States

Colorado

University of Colorado Denver, Aurora, Colorado, 80045, United States

Connecticut

Yale Cancer Center, New Haven, Connecticut, 06510, United States

District of Columbia

Georgetown University, Lombardi Comprehensive Cancer Center, Washington D.C., District of Columbia, 20037, United States

Florida

Mayo Clinic- Jacksonville, Jacksonville, Florida, 32224, United States
University of Miami-Sylvester Cancer Center, Miami, Florida, 33136, United States
Orlando Health, Orlando, Florida, 32806, United States
Moffitt Cancer Center- Miami, Pembroke Pines, Florida, 33028, United States

Georgia

Piedmont Healthcare, Atlanta, Georgia, 30318, United States

Kentucky

University of Kentucky, Lexington, Kentucky, 40536, United States

Massachusetts

Massachusetts General Hospital, Boston, Massachusetts, 02114, United States
Beth Israel Deaconess Medical Center, Boston, Massachusetts, 02215, United States
Dana-Farber Cancer Institute - Brigham & Women's Hospital, Boston, Massachusetts, 02215, United States

Michigan

University Of Michigan, Ann Arbor, Michigan, 41809, United States
Henry Ford Hospital, Detroit, Michigan, 48202, United States

Missouri

The University of Kansas Cancer Center (KUCC) (Kansas City Cancer Center (KCCC)) - North, Kansas City, Missouri, 64154, United States

Nebraska

University of Nebraska Medical Center, Omaha, Nebraska, 68198, United States

New Jersey

Hackensack University Medical Center - John Theurer Cancer, Hackensack, New Jersey, 07601, United States

New York

Roswell Park Comprehensive Cancer Center (RPCCC) (Roswell Park Cancer Institute (RPCI)), Buffalo, New York, 14263, United States
Memorial Sloan Kettering, New York, New York, 10022, United States
Columbia University Irving Medical Center, New York, New York, 10032, United States

North Carolina

Levine Cancer Center, Charlotte, North Carolina, 28204, United States
Duke University School of Medicine, Durham, North Carolina, 27705, United States

Ohio

Cleveland Clinic, Cleveland, Ohio, 44106, United States

Oregon

Providence Health Cancer Center, Portland, Oregon, 97239, United States

Pennsylvania

Penn State Hershey Cancer Center, Hershey, Pennsylvania, 17033, United States
Abramson Cancer Center University of Pennsylvania, Philadelphia, Pennsylvania, 19104, United States
Hillman Cancer Center, University of Pittsburgh, Pittsburgh, Pennsylvania, 15232, United States

Rhode Island

Lifespan Rhode Island Hospital, Providence, Rhode Island, 02903, United States

Tennessee

Vanderbilt-Ingram Cancer Center, Nashville, Tennessee, 37232, United States

Texas

Houston Methodist Research Institute (HMRI), Houston, Texas, 77030, United States
MD Anderson Cancer Center, Houston, Texas, 77030, United States

Utah

The University of Utah - Huntsman Cancer Institute (HCI), Salt Lake City, Utah, 84112, United States

Vermont

The University of Vermont - Fletcher Allen Health Care, Burlington, Vermont, 05401, United States

Washington

Seattle Cancer Care Alliance, Seattle, Washington, 98109, United States