Chimeric Antigen Receptor T Cells Targeting claudin18.2 in Solid Tumors.

Conditions

Advanced Solid Tumor

Keywords

Advanced solid tumor, claudin18.2, CAR-T cell therapy

Brief summary

An open label, single/multiple dose exploratory clinical study to evaluate the safety, efficacy, and pharmacokinetics of autologous humanized anti-claudin18.2 chimeric antigen receptor T cell in advanced solid tumor.

Detailed description

This study is an open, single/multiple infusion, dose escalation/dose regimen finding study to assess the safety and pharmacokinetics of CAR-CLDN18.2 T cell therapy, and to obtain the preliminary efficacy results in subjects who have been diagnosed with advanced solid tumor with positive claudin 18.2 expression and failed to standard systemic treatment.

Li J, Liu L, Tao M, Han Z, Ma M, Jiang L, Liu C, Liu D, Zhang P, Zhang M, Xue R, Gong J, Zhang X, Shen L, Qi C.

2025-11-29

10.1038/s41416-025-03289-7

Decoding the response and resistant features to the Claudin18.2-specific CAR-T cell CT041 in gastric cancer: A multi-omics exploratory biomarker analysis of the phase 1 clinical trial.

Haoxin Peng, Yang Chen, Dan Liu, Chang Liu, X. Zhang et al. (8 authors)

Journal of Clinical Oncology2025-05-281 citations

10.1200/jco.2025.43.16_suppl.4015

Peripheral blood neutrophils contribute to Claudin18.2-specific CAR-T cell treatment resistance in advanced gastric cancer.

Li J, Tao M, Liu L, Liu C, Ma M, Liu D, Zhang P, Zhang M, Xue R, Gong J, Zhang C, Zhang X, Shen L, Qi C.

2025-04-171 citations

10.1038/s41416-025-03015-3

Exploring the therapeutic efficacy difference in claudin18.2-targeted cell therapy revealed by single-cell sequencing

Mingyang Ma, Chang Liu, Lei Jiang, Dan Liu, Panpan Zhang et al. (15 authors)

iScience2025-01-074 citations

10.1016/j.isci.2025.111768

Claudin18.2-specific CAR T cells in gastrointestinal cancers: phase 1 trial final results.

Qi C, Liu C, Gong J, Liu D, Wang X, Zhang P, Qin Y, Ge S, Zhang M, Peng Z, Zhou J, Lu Z, Lu M, Cao Y, Yuan J, Wang Y, Wang Z, Xue R, Peng X, Wang Y, Yuan D, Li J, Zhang X, Shen L.

2024-06-03112 citations

10.1038/s41591-024-03037-z

Claudin18.2-targeted chimeric antigen receptor T cell-therapy for patients with gastrointestinal cancers: Final results of CT041-CG4006 phase 1 trial.

Changsong Qi, Chang Liu, Jifang Gong, Jian Li, Dan Liu et al. (20 authors)

Journal of Clinical Oncology2024-06-019 citations

10.1200/jco.2024.42.16_suppl.2501

Abstract 6316: Exploring the resistant mechanism of CAR T cell therapy targeting CLDN18.2 by single-cell sequencing

Mingyang Ma, Changsong Qi, Chang Liu, Lei Jiang, Min Tao et al. (14 authors)

Cancer Research2024-03-22

10.1158/1538-7445.am2024-6316

CT041 CAR T cell therapy for Claudin18.2-positive metastatic pancreatic cancer.

Qi C, Xie T, Zhou J, Wang X, Gong J, Zhang X, Li J, Yuan J, Liu C, Shen L.

2023-09-0949 citations

10.1186/s13045-023-01491-9

Abstract 6482: CLDN18.2 expression is associated with clinicopathological features and prognosis of Chinese patients with digestive system cancers: a retrospective analysis

Chong XiaoYi, Changsong Qi, Jifang Gong, Miao Zhang, Mingyang Ma et al. (15 authors)

Cancer Research2023-04-041 citations

10.1158/1538-7445.am2023-6482

Multicenter phase Ib trial in the U.S. of salvage CT041 CLDN18.2-specific chimeric antigen receptor T-cell therapy for patients with advanced gastric and pancreatic adenocarcinoma.

Gregory P. Botta, Carlos Becerra, Zhaohui Jin, Dae Won Kim, Dan Zhao et al. (11 authors)

Journal of Clinical Oncology2022-06-0129 citations

10.1200/jco.2022.40.16_suppl.2538

Claudin18.2-specific CAR T cells in gastrointestinal cancers: phase 1 trial interim results.

Qi C, Gong J, Li J, Liu D, Qin Y, Ge S, Zhang M, Peng Z, Zhou J, Cao Y, Zhang X, Lu Z, Lu M, Yuan J, Wang Z, Wang Y, Peng X, Gao H, Liu Z, Wang H, Yuan D, Xiao J, Ma H, Wang W, Li Z, Shen L.

2022-05-09419 citations

10.1038/s41591-022-01800-8

Interventions

DRUGCAR-CLDN18.2 T-Cells

Preconditioning with fludarabine, cyclophosphamide, based chemotherapy regimen at sub-clinical doses • Chimeric Antigen Receptor T Cells Targeting Claudin18.2

DRUGPD-1 Monoclonal Antibody

Chimeric Antigen Receptor T Cells Targeting Claudin18.2 with PD-1

DRUGChemotherapy

First-line systemic therapy according to physician's choice

Study design

Allocation

NON_RANDOMIZED

Intervention model

SINGLE_GROUP

Primary purpose

TREATMENT

Masking

NONE

Eligibility

Sex/Gender

ALL

Age

18 Years to 75 Years

Healthy volunteers

No

Inclusion criteria

1. Aged 18 to 75 years, male or female; 2. Subjects with pathologically confirmed solid tumors (ie, advanced gastric cancer, esophagogastricgastroesophageal junction cancer, and pancreatic cancer) and have been failed to at least first-one prior line of systemic treatment; 3. Tumor tissue samplessample was positive for claudin 18.2 positive through for claudin18.2 IHC staining;assay(≥2+, and ≥40%); 4. Estimated life expectancy \> 12 weeks; 5. According to the RECIST 1.1, there is at least one measurable or unmeasurable tumor lesionslesion； 6. ECOG physical status score 0 \ 1, within 24 hours prior to apheresis, and at baseline (prior to pre-treatment); 7. Sufficient venous access for mononuclear cell collection (abbreviation: apheresis) 8. Subjects should have adequate organ functions before screening and pre-treatment (at baseline). 9. Female subjects of childbearing age must undergo a serum pregnancy test at screening and prior to preconditioning and the results must be negative, and are willing to use a very effective and reliable method of contraception within 1 year after the last study treatment. The methods that can be used are: bilateral tubal ligation / bilateral salpingectomy or bilateral tubal occlusion; or approved oral, injection or hormone-imparting contraceptive methods; or barrier contraceptive method: containing spermicidal foam / Gel/film/cream/suppository condom or occlusive cap (diaphragm or cervix/cap); 10. Men who have actively sexual intercourse with women with child-bearing potential, must agree to use barrier-based contraception if they have no vasectomy, for example, a condom containing a spermicidal foam/gel/film/paste/suppository, or use a contraceptive method for their spouse (see article 9 of the inclusion criteria). Moreover, all men are absolutely forbidden to donate sperm within 1 year after receiving the last study treatment infusion； 11. Subject participates in this clinical trial and sign Informed Consent Form voluntarily.

Exclusion criteria

1. Pregnant or lactating women; 2. HIV, Treponema pallidum or HCV serologically positive; 3. Any uncontrollable active infection, including but not limited to active tuberculosis, HBV infection (HBsAg positive, or HBcAb positive and HBV DNA positive); 4. Subjects have clinically significant thyroid dysfunction determined by investigator (serum thyroid hormone assays TT4, TT3, FT3, FT4, and serum thyroid stimulating hormone TSH) which is not suitable for entering into the study; 5. The side effects caused by the previous treatment of the subjects did not return to CTCAE ≤1; except hair loss and, hyperpigmentation or other tolerable events determined by investigator or laboratory abnormalities allowed by the protocol; 6. Subjects who are using steroidshave recieved ≥15 mg/day glucocorticoid systemically currently within 7 days prior to apheresis; those using inhaled steroids recently or currently are not excluded; 7. Previously allergic to immunotherapy and related drugs, history of severe allergiespreconditioning drug such as cyclophosphamide, fludarabine, or allergiestocilizumab or allergic to components of CT041CAR-CLDN18.2T injection, allergic to β-lactam antibiotics;the CT041 infusion; 8. Previously received any chimeric antigen receptor-modified T-cells(including CAR-T、TCR-T) . 9. Subjects have untreated or symptomatic brain metastases; 10. Subjects have central or extensivelywith centralcor diffused metastases in lung and .extensiveor diffused metastases in liver;liveror with rapid tumor progression since screening period evaluated by the investigator preconditioning (at baseline)； 11. The largest target tumor lesion\>4cm 12. Subjects with unstable or active ulcers and gastrointestinal bleeding currently; 13. Subjects with a history of organ transplantation or awaiting organ transplantation; 14. Subjects requiring anticoagulant therapy; 15. Subjects requiring continuous anti-platelet therapy; 16. Subjects who have undergone major surgery or significant trauma within 4 weeks prior to apheresis, or who are expected to undergo major surgery during the study; 17. There are no other serious diseases that may limit subjects' participation in this trial; 18. The investigator assessed that the subject was unable or unwilling to comply with the requirements of the study protocol; 19. Blood oxygen saturation ≤ 95% before pre-treatmentapheresis or preconditioning (accept finger oxygen detection method); 20. Prior to pretreatmentpreconditioning, subjects developed, including but not limited to, new arrhythmias that could not be controlled with drugs, hypotension requiring pressor agent, bacterial, fungal or viral infections that required intravenous antibiotics. Creatinine clearance rate \<40mL / min; The investigator judges that the subject is not suitable for continuing the trial. Subjects who use antibiotics to prevent infection can continue the trials if judged by the investigator; 21. The subject has a central nervous system disease sign or an abnormal neurological test result with clinical significance; 22. The subject is currently suffered from or have suffered from other incurable malignant tumors within previous 3 years, except in situ cervical cancer or skin basal cell cancer.

Design outcomes

Primary

Measure	Time frame	Description
Dose-limiting toxicity (DLT)	28 days of single infusion	Safety
Maximum tolerated dose (MTD)	28 days of single infusion	tolerability

Secondary

Measure	Time frame	Description
Antitumor efficacy-Progression-free survival (PFS)	1 year	The period from the day when the subject receives the infusion of cells to the first recorded tumor progression (whether treated or not) or death of any cause, which occurs first.
Antitumor efficacy-Duration of response (DOR)	1 year	The period from the first evaluation of CR or PR to the first evaluation of PD or death of any cause
Antitumor efficacy-Duration of disease control (DDC)	1 year	The period from the first evaluation of clinical benefit to the first evaluation of PD or any cause of death.
Pharmacokinetics (the number of cell copies and cell persistence duration in peripheral blood)	26 weeks	CAR-CLDN18.2 DNA in peripheral blood detected by q-PCR at each visit after infusion
Antitumor efficacy-Objective response rate (ORR)	1 year	The number of cases in which tumor size is reduced to PR or CR / the total number of evaluable cases (%). In the event of PR or CR, the subjects should confirm it no less than 4 weeks after the first evaluation
Antitumor efficacy-Disease control rate (DCR)	1 year	The number of cases in which response are achieved from the start of cell infusion/the total number of evaluable cases (%).
Long term survival follow up	15 years	The period from the first infusion to any cause of death
Antitumor efficacy-Overall survival (OS)	1 years	The period from the first infusion to any cause of death
Number of participants with treatment-related adverse events as assessed by CTCAE v5.0	1 year	Adverse events occurring through 26 weeks and 12 months post infusion of CAR-CLDN18.2 T-Cell infusion, such as abnormalities or changes in laboratory examinations, physical examinations, vital signs, etc.

Countries

China

Outcome results

None listed