Prospective registration

EpCAM-targeted chimeric antigen receptor modified autologous T cells for clinical research of advanced gastric cancer

EpCAM-targeted chimeric antigen receptor modified autologous T cells for clinical research of advanced gastric cancer

Tang Fang 

Lu Zhengmao 

168 Changhai Road, Yangpu District, Shanghai

168 Changhai Road, Yangpu District, Shanghai

Shanghai Changhai Hospital

Shanghai Changhai Hospital

Yes

Shanghai Changhai Hospital Ethics Committee

Luo Tianhang

168 Changhai Road, Yangpu District, Shanghai

Shanghai Changhai Hospital

168 Changhai Road, Yangpu District, Shanghai

Research Foundation

advanced gastric cancer

Interventional study

0

Single arm 

Main purpose: 1.Carry out IMC001 intravenous drip treatment for patients with advanced gastric cancer, observe and evaluate the safety and tolerability of patients. Secondary purpose: 1.Treat patients with advanced gastric cancer with IMC001, and determine the maximum tolerated dose according to dose-limiting toxicity and clinical response, including possible side effects, and provide a plan and dosage regimen for clinical phase I-II treatment; 2.Assess the correlation between the pharmacodynamic (PD) biomarkers of IMC001 and clinical efficacy; the expansion and persistence of IMC001 in vivo and the correlation between the pharmacodynamic (PD) biomarkers and adverse events; 3.To evaluate the preliminary anti-tumor efficacy of IMC001 in patients with advanced gastric cancer. According to the Curative Effect Evaluation Standard for Solid Tumors (RECIST) Version V.1.1 and the Evaluation Standard for Immunotherapy Curative Effect for Solid Tumors (iRECIST), objective response rate (ORR), duration of response (DOR), disease control rate (DCR) and progression-free survival are adopted Phase (PFS) describes the preliminary anti-tumor activity; 4.Incidence of treatment-related adverse events.

1.Aged 18 to 70 years (including boundary value), both male and female;
2.Patients with locally advanced gastric cancer and metastatic gastric cancer who have failed second-line or above treatments in the past have no other feasible effective treatments, and the expected survival period of the subjects is >=12 weeks;
(1)Treatment failure is defined as: the occurrence of intolerable toxicity or disease progression during treatment or tumor recurrence or metastasis after the end of treatment;
(2)One or more chemotherapeutics with each line of treatment for >=1 cycle or longer; early adjuvant/neo-adjuvant therapy is allowed, if tumor recurrence develops during or <=24 weeks after completion of adjuvant/neo-adjuvant therapy And metastasis, the previous adjuvant/neo-adjuvant therapy is considered systemic chemotherapy;
(3)Allow pre-treatment to be targeted drugs, immunosuppressive agents or radiotherapy;
(4)Allow the initial treatment to be chemotherapy combined with targeted drugs.
3.According to the RECISTv 1.1 standard, the subject has at least 1 target lesion that can be evaluated stably;
4.The EpCAM histological staining of the biopsy tumor tissue sample is positive;
5.ECOG physical strength status score 0~1;
6.The subject has sufficient organ and bone marrow function. Laboratory screening must meet the following criteria (refer to NCI CTC AE 5.0). All laboratory test results should be within the following stable range and there is no continuous supportive treatment;
(1)Blood test: white blood cell WBC>=1.5x10^9/L; platelet count PLT>=60x10^9/L; hemoglobin content Hb>=8.0g/dL; lymphocyte LYM>=0.4x10^9/L;
(2)Blood biochemistry: serum creatinine<=1.5xULN, if serum creatinine>1.5xULN, creatinine clearance rate must be >50mL/min (calculated according to Cockcroft-Gault formula); serum total bilirubin<=1.5xULN, alanine Aminotransferase (ALT)<=2xULN; Aspartate aminotransferase (AST)<=2xULN (ALT<=5xULN in patients with liver metastasis or liver cancer, AST<=5xULN);
(3)Amylase and lipase <= 1.5 x ULN;
(4)Routine urine examination: urine protein <2+.
7.Left ventricular ejection fraction (LVEF)> 45% in cardiac color Doppler ultrasound examination within one month;
8.Fertility status: female patients of childbearing age or male patients whose sexual partners are females of childbearing age are willing to take effective contraceptive measures from the signing of the informed consent form to 6 months after the last cell infusion; females of childbearing age include premenopausal women and Women within 2 years after menopause. Subjects must agree to follow contraceptive instructions during treatment;
9.The subject must sign and date a written informed consent form;
10.The subject must be willing and able to comply with the predetermined treatment plan, laboratory examination, follow-up and other research requirements.

Subjects who meet any of the following conditions cannot be selected for this study;
1.Influencing women during pregnancy and lactation.
2.Known history of human immunodeficiency virus (HIV) infection; acute or chronic active hepatitis B (HBsAg positive); acute or chronic active hepatitis C (HCV antibody positive).Syphilis antibody positive; Epstein-Barr virus antibody positive; Cytomegalovirus (CMV) infection (IgM positive).
3.Severe infections in active phase or poor clinical control or severe infections within 4 weeks after the first blood collection.
4.At present, there is a heart disease requiring treatment or a poorly controlled hypertension (defined as systolic blood pressure ≥140 mmHg and/or diastolic blood pressure ＞90 mmHg after treatment with standardized antihypertensive drugs).
5.The presence of any of the following cardiac clinical symptoms or diseases:
a)Unstable angina pectoris;
b)Myocardial infarction occurred within 1 year;
c)The resting state ECG examination QTc>450ms (male) or QTc>470ms (female);
d)The resting state ECG examination found abnormalities of important clinical significance (such as abnormal heart rate, conduction, morphological characteristics, etc.) or complete left bundle branch block or third-degree heart block or second-degree heart block or PR Interval> 250ms;
e)There are factors that increase the risk of QTc prolongation and abnormal heart rate, such as heart failure, hypokalemia, congenital long QT syndrome, family history of long QT syndrome, or sudden death of unexplained reasons in immediate family members under 40, or prolonged periods Period concomitant medication.
6.Those who have experienced gastrointestinal perforation, abdominal abscess, or recent (within 3 months) intestinal obstruction or imaging, clinical symptoms accompanied by intestinal obstruction.
7.Abnormal coagulation function (INR>1.5×ULN), have bleeding tendency or are receiving thrombolysis or anticoagulation therapy (such as warfarin or heparin), patients need long-term antiplatelet therapy (aspirin dose> 300mg/day; clopidogrel) Gray dose> 75mg/day).
8.Subjects who need to use corticosteroids or other immunosuppressive drugs for systemic treatment during the treatment period.
9.The blood oxygen saturation before treatment ≤95% (accept the finger oxygen test method).
10.Received systemic steroids equivalent to >15 mg/day of prednisone within 2 weeks before apheresis, except for inhaled steroids.
11.Before the pretreatment of lymphocyte depletion, the subject has a new arrhythmia, including but not limited to arrhythmia that cannot be controlled with drugs, hypotension that requires pressurizing agents, bacteria, fungi, or viruses that require intravenous antibiotics infection. Subjects who use test antibiotics to prevent infection are up to the investigator to determine whether they can continue to participate in the test.
12.Patients who are currently suffering from or have a history of central nervous system diseases, such as seizures, cerebrovascular ischemia/hemorrhage, dementia, cerebellar disease, or any autoimmune diseases involving the central nervous system; central nervous system metastases with clinical symptoms Or meningeal metastasis, or there is other evidence that the patient's central nervous system metastasis or meningeal metastasis has not been controlled, and the investigator judged it is not suitable for inclusion.
13.Patients who have had other malignant tumors before or at the same time, with the following exceptions:
Fully treated basal cell or squamous cell carcinoma (enough wound healing is required before being included in the study);
Cervical cancer or breast cancer in situ, after curative treatment, there is no sign of recurrence at least 3 years before the study;
The primary malignant tumor has been completely removed and completely remitted for ≥5 years.
14.Have received other CAR-T treatments and TCR-T treatments in the past.
15.Received anti-PD-1/PD-L1 monoclonal antibody treatment within 4 weeks before apheresis.
16.Subjects who have received other gene therapy in the past.
17.Subjects with severe mental disorders.
18 Participated in other clinical studies in the past 1 month.
19.Subjects withdrew from the study due to various reasons and could not participate in the study again.

Open, single arm, does not involve random methods.

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