Study Results
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Basic Information
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RECRUITING
PHASE2
770 participants
INTERVENTIONAL
2020-08-15
2028-07-01
Brief Summary
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Detailed Description
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Conditions
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Study Design
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NON_RANDOMIZED
PARALLEL
TREATMENT
NONE
Study Groups
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Almonertinib-EGFR mutation
Administration: 110 mg oral qd, to disease progression or intolerable adverse effects.
Almonertinib 110 MG
Patients with advanced rare tumors who failed to standardized treatment carrying EGFR mutations will be administrated with Almonertinib.
Dacomitinib-EGFR mutation
Administration: 45 mg oral qd, to disease progression or intolerable adverse effects.
Dacomitinib 45 MG
Patients with advanced rare tumors who failed to standardized treatment carrying EGFR mutations will be administrated with Dacomitinib.
Alectinib-ALK fusion
Administration: 600 mg oral qd, to disease progression or intolerable adverse effects.
Alectinib 150 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion will be administrated with Alectinib.
Crizotinib-ALK fusion
Administration: 250 mg oral bid, to disease progression or intolerable adverse effects.
Crizotinib 250 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion, ROS-1 fusion, C-MET amplification, C-MET mutation will be administrated with Crizotinib.
Vemurafenib-BRAF mutation
Administration: 960 mg oral bid, to disease progression or intolerable adverse effects.
Vemurafenib 240 MG
Patients with advanced rare tumors who failed to standardized treatment carrying BRAF mutation will be administrated with Vemurafenib.
Niraparib-BRCA mutation or HRD
Administration: 200/300 mg oral qd, to disease progression or intolerable adverse effects.
Niraparib 200/300 MG
Patients with advanced rare tumors who failed to standardized treatment carrying BRCA1/2 mutation will be administrated with Olaparib.
Pyrotinib-HER-2 overexpression/amplification
Administration: 400 mg oral qd, to disease progression or intolerable adverse effects.
Pyrotinib 160/80 MG
Patients with advanced rare tumors who failed to standardized treatment carrying HER-2 mutation or HER-2 over expression/amplification will be administrated with Pyrotinib.
Imatinib-CKIT mutation
Administration: 400 mg oral qd, to disease progression or intolerable adverse effects.
Imatinib 400 MG
Patients with advanced rare tumors who failed to standardized treatment carrying CKIT mutation will be administrated with Imatinib.
Palbociclib-CDKN2A mutation
Administration: 125 mg oral qd for 21 days q28d, to disease progression or intolerable adverse effects.
Palbociclib 125mg
Patients with advanced rare tumors who failed to standardized treatment carrying CDKN2A mutation will be administrated with palbociclib.
Crizotinib-ROS-1 fusion
Administration: 250 mg oral bid, to disease progression or intolerable adverse effects.
Crizotinib 250 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion, ROS-1 fusion, C-MET amplification, C-MET mutation will be administrated with Crizotinib.
Crizotinib-C-MET amplification
Administration: 250 mg oral bid, to disease progression or intolerable adverse effects.
Crizotinib 250 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion, ROS-1 fusion, C-MET amplification, C-MET mutation will be administrated with Crizotinib.
Crizotinib-C-MET mutation
Administration: 250 mg oral bid, to disease progression or intolerable adverse effects.
Crizotinib 250 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion, ROS-1 fusion, C-MET amplification, C-MET mutation will be administrated with Crizotinib.
Pyrotinib-HER-2 mutation
Administration: 400 mg oral qd, to disease progression or intolerable adverse effects.
Pyrotinib 160/80 MG
Patients with advanced rare tumors who failed to standardized treatment carrying HER-2 mutation or HER-2 over expression/amplification will be administrated with Pyrotinib.
Sintilimab-PD-1
Administration: 200mg q21d, to disease progression or intolerable adverse effects.
Sintilimab 100MG
Patients with advanced rare tumors who failed to standardized treatment carrying no targeted alterations will be administrated with Sintilimab.
Combination ARM-Niraparib & Sintilimab
Niraparib (200mg oral qd) combined with Sintilimab (200mg iv q21d) after acquired resistance to Niraparib.
Niraparib 200/300 MG
Patients with advanced rare tumors who failed to standardized treatment carrying BRCA1/2 mutation will be administrated with Olaparib.
Sintilimab 100MG
Patients with advanced rare tumors who failed to standardized treatment carrying no targeted alterations will be administrated with Sintilimab.
Combination ARM-Vemurafenib & Atezolizumab
Vemurafenib (960 mg oral bid) \& Atezolizumab (1200mg iv q21d) after acquired resistance to Vemurafenib.
Vemurafenib 240 MG
Patients with advanced rare tumors who failed to standardized treatment carrying BRAF mutation will be administrated with Vemurafenib.
Atezolizumab 1680 MG
Patients with BRAF mutation treated with vemurafenib, after acquired resistance, will combine vemurafenib with atezolizumab.
Combination ARM-Palbociclib & Atezolizumab
Palbociclib (125 mg oral qd for 21 days q28d) combined with Atezolizumab (1680mg iv q28d) after acquired resistance to Palbociclib.
Palbociclib 125mg
Patients with advanced rare tumors who failed to standardized treatment carrying CDKN2A mutation will be administrated with palbociclib.
Atezolizumab 1680 MG
Patients with BRAF mutation treated with vemurafenib, after acquired resistance, will combine vemurafenib with atezolizumab.
Interventions
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Almonertinib 110 MG
Patients with advanced rare tumors who failed to standardized treatment carrying EGFR mutations will be administrated with Almonertinib.
Dacomitinib 45 MG
Patients with advanced rare tumors who failed to standardized treatment carrying EGFR mutations will be administrated with Dacomitinib.
Alectinib 150 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion will be administrated with Alectinib.
Crizotinib 250 MG
Patients with advanced rare tumors who failed to standardized treatment carrying ALK fusion, ROS-1 fusion, C-MET amplification, C-MET mutation will be administrated with Crizotinib.
Pyrotinib 160/80 MG
Patients with advanced rare tumors who failed to standardized treatment carrying HER-2 mutation or HER-2 over expression/amplification will be administrated with Pyrotinib.
Imatinib 400 MG
Patients with advanced rare tumors who failed to standardized treatment carrying CKIT mutation will be administrated with Imatinib.
Niraparib 200/300 MG
Patients with advanced rare tumors who failed to standardized treatment carrying BRCA1/2 mutation will be administrated with Olaparib.
Palbociclib 125mg
Patients with advanced rare tumors who failed to standardized treatment carrying CDKN2A mutation will be administrated with palbociclib.
Vemurafenib 240 MG
Patients with advanced rare tumors who failed to standardized treatment carrying BRAF mutation will be administrated with Vemurafenib.
Sintilimab 100MG
Patients with advanced rare tumors who failed to standardized treatment carrying no targeted alterations will be administrated with Sintilimab.
Atezolizumab 1680 MG
Patients with BRAF mutation treated with vemurafenib, after acquired resistance, will combine vemurafenib with atezolizumab.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
2. Patients with advanced or metastatic rare solid tumor confirmed by histological confirmed;
3. ECOG score is 0 or 1; ECOG score needs to be evaluated 7 days before the first treatment;
4. Expected survival ≥12 weeks;
5. According to Response Evaluation Criteria in Solid Tumor (RECIST 1.1), there is at least one imaging measurable lesions, which has obvious disease progress before radiotherapy or after radiotherapy;
6. Within the scope of CMPA approved drug indications, the disease has progressed after the standard treatment recommended by NCCN or CSCO guidelines (if there is standard treatment, the recommended level is IA-IIA), or there is no standard effective treatment plan, or it is no longer suitable for standard anti-tumor treatment, or the patients refuse the standard treatment plan;
7. Fresh biopsy tissue samples (obtained within 12 weeks before the first use of the drug, 4 pieces of coarse needle biopsy must be provided, and no other anti-tumor treatment, systemic anti infection treatment, vaccination, et al.) and peripheral blood samples must be provided for molecular typing;
8. Must have a primary or metastatic paraffin specimen (without radiotherapy) other than bone metastatic lesions before enrollment (within 2 years, 15-20 sheets, 4-6μm thick white slices, of which 5 need to be glued and baked ). If requirements are not met, investigator are allowed the decision to enroll subjects according to the specific situation.
9. If there is pleural or peritoneal effusion, the specimens must be taken for pathological cytological examination of which 300 ml samples must be provided;
8. Major surgical operations or incomplete healing of injury within 28 days prior to study treatment's first administration and chest radiotherapy of \> 30 Gy within 6 months.
9. History of receiving other investigational drugs within 14 days or 5 half-lives (whichever is longer) prior to the first administration.
10. History of receiving live vaccine within 30 days prior to the first administration. Seasonal influenza vaccines that do not contain live viruses are allowed.
11. History of hypersensitivity to the active ingredients or non-active excipients of the study drug, hypersensitivity to drugs with chemical structure similar to the study drug or hypersensitivity to similar drugs of the study drug.
12. Current active infection requiring systemic treatment (antibiotics); or any of the following:
1. HIV positive or known history of acquired immunodeficiency syndrome;
2. Hepatitis B virus (HBV) or hepatitis C virus (HCV) infection is defined as HBsAg positive and the number of HBV DNA copies exceeds the upper limit of normal value, or HCV AB positive;
3. Active tuberculosis (with exposure history or positive tuberculosis test; with clinical and / or imaging manifestations);
4. Positive antibody of Treponema Pallidum.
13. Current evidenced uncontrollable systemic diseases (such as severe mental, neurological, epilepsy or dementia, unstable or uncompensated respiratory, cardiovascular, liver or kidney diseases, uncontrolled hypertension \[i.e., still greater than or equal to CTCAE Grade 3 hypertension after drug treatment\]).
14. History of myocardial infarction, coronary artery / peripheral artery bypass or cerebrovascular accident within 3 months.
15. Diagnosed with a second type of malignant tumor within 5 years before the first diagnosis of a rare solid tumor (excluding completely resected basal cell carcinoma, bladder carcinoma in situ, cervical carcinoma in situ).
16. History of receiving of any organ transplantation, including allogeneic stem cell transplantation. Transplantation without immunosuppression (corneal transplantation, hair transplantation) is excluded.
17. Cardiovascular disease or symptom includes any of the following:
1. History of Congestive Heart Failure requiring treatment and of New York Heart Association class III / IV CHF (see Appendix 3) ;
2. Current ventricular arrhythmia requiring antiarrhythmic drugs treatment, or uncontrollable or unstable arrhythmia;
3. Severe conduction disorder (such as grade II or III AV block);
4. Angina requiring treatment;
5. QT interval (QTC) of 12 lead ECG is ≥ 450 ms in male and ≥ 470 MS in female;
6. History of congenital long QT syndrome, congenital short QT syndrome, torsade de pointe or pre-excitation syndrome;
7. History of LVEF decline to below 50% determined by echocardiography or MUGA scan;
8. History of myocardial infarction in the past 6 months.
18. Inadequate bone marrow reserve or organ function evidenced by the following laboratory results:
1. Absolute value of neutrophils \< 1.5 × 109 / L;
2. Platelet count \< 100 × 109 / L (transfusion dependent patients should be excluded from this study);
3. Hemoglobin \< 90g / L;
4. ALT is \> 2.5 x Upper Limit of Normal (ULN) If there is no clear liver metastases, ALT \> 5 x ULN if there is liver metastases;
5. Aspartate aminotransferase (AST) \> 2.5 x ULN If there is no definite liver metastases. AST \> 5x ULN if there is liver metastases;
6. Total bilirubin \> 1.5 x ULN if there is no liver metastases; Total bilirubin \> 3 x ULN if there is definite Gilbert syndrome (Unconjugated Hyperbilirubinemia) or liver metastases;
7. Creatinine \> 1.5 x ULN with Creatinine clearance \< 50 ml / min (measured value, or calculated value by Cockcroft Gault formula); Only when Creatinine \> 1.5 x ULN, Creatinine clearance needs to be checked for confirmation;
8. If bone metastasis is present and investigator concluded that liver function is adequate, the increase of ALP alone will not be excluded;
9. Coagulation function: INR, PT, APTT\> 1.5 times ULN (whether the patients using or not using anticoagulant drugs can be enrolled is determined by the investigator).
10. Myocardial enzyme CK and CKMB test values are not in the normal range;
11. The examination value of thyroid function is not within the normal range or it is not slightly abnormal but does not need treatment.
19. History of swallowing dysfunction, active gastrointestinal disease or other diseases that significantly affect the absorption, distribution, metabolism and excretion of oral drugs. The patients with history of subtotal gastrectomy. (Note: this standard is not applicable to the sub schemes with the investigational drug as injection).
20. Pregnant or lactating women.
21. Serious medical or mental illness that may affect program compliance and tolerance to treatment.
22. Those investigators believe that patients with other potential risks are not suitable for this study.
Exclusion Criteria
12. Toxic and side effects caused by previous treatment need to be restored to ≤ Grade 1 or returned to the baseline value (NCI-CTCAE version 5.0, except for hair loss);
13. Negative pregnancy test (only applicable for women with childbearing potential). No childbearing potential is defined as being postmenopausal for longer than one year or having undergone surgical sterilization or hysterectomy. All patients (male and female) agree to use an effective form of contraceptive measures and continue its use for the duration of treatment and within 8 weeks after the end of treatment;
14. Signed, written informed consent of volunteers that join the group shall follow the study treatment plan, follow-up plan and cooperate to observe the adverse events and efficacy.
1. History of PD-1 / PD-L1 drug treatment.
2. History of the targeted drug treatment of this study.
3. Allergies towards drug ingredients or excipients in this study.
4. History of interstitial lung disease or radiation pneumonitis of any type.
5. Central Nervous System (CNS) metastases with brain metastases-related symptoms, which is not stable in neurology, or need to increase steroid dosage to control CNS disease. (Note: Patients with controlled CNS metastasis are eligible to participate in this study. Before entering the study, subject must have completed radiotherapy or CNS tumor metastasis surgery for more than fourteen days, neurological function must be in a stable state with no new neurological defects found in the clinical examination and no new problems found in the CNS imaging examination. If necessity arises for subjects to use steroids for CNS metastases treatment, said steroid treatment dose must have reached stable treatment for ≥ 3 months at least two weeks before entering the study.
6. Current uncontrollable third cavity effusion, such as a large amount of pleural effusion or ascites.
18 Years
ALL
No
Sponsors
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Cancer Institute and Hospital, Chinese Academy of Medical Sciences
OTHER
Responsible Party
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Ning Li
Chief, Office of Clinical Trial Center, CancerIHCAMS
Principal Investigators
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Ning Li, Doctor
Role: STUDY_CHAIR
Cancer Institute and Hospital, Chinese Academy of Medical Sciences
Locations
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Cancer hospital Chinese Academy of Medical Sciences
Beijing, , China
Countries
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Central Contacts
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References
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Wang S, Huang HY, Wu D, Fang H, Ying J, Bai Y, Yu Y, Fang Y, Jiang N, Sun C, Yu A, Fan Q, Xing S, Ni Y, Zhang W, Wu C, Ji X, Wang H, Guo Y, Tang Q, Wang Y, Tang Y, Li N. Platform study of genotyping-guided precision medicine for rare solid tumours: a study protocol for a phase II, non-randomised, 18-month, open-label, multiarm, single-centre clinical trial testing the safety and efficacy of multiple Chinese-approved targeted drugs and PD-1 inhibitors in the treatment of metastatic rare tumours. BMJ Open. 2021 Jun 3;11(6):e044543. doi: 10.1136/bmjopen-2020-044543.
Other Identifiers
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NCC2380
Identifier Type: -
Identifier Source: org_study_id
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