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A Controlled Clinical Study on D-TACE Combined with Molecular Targeted Drugs and Immune Checkpoint Inhibitors with or Withouts Hepatic Artery Infusion Therapy for Large Hepatocellular Carcinoma

A Controlled Clinical Study on D-TACE Combined with Molecular Targeted Drugs and Immune Checkpoint Inhibitors with or Without Continuous Hepatic Artery Perfusion Therapy for Large Hepatocellular Carcinoma

Shiguang Chen 

Zhuting Fang, Shiguang Chen 

No. 420 Fuma Road, Fuzhou 350014, China

No. 420 Fuma Road, 350014 Fuzhou, China

Fujian Cancer Hospital

Fujian Cancer Hospital

Yes

Ethics Committee for Scientific Research and New Technologies of Fujian Cancer Hospital

Meimei Chen

Office of the Ethics Committee, 2nd Floor, Building 3, Former Labor Service Company, Fujian Cancer Hospital

Fujian Cancer Hospital

No. 420 Fuma Road, 350014 Fuzhou, China

None

Hepatocellular Carcinoma

Interventional study

N/A

Parallel 

To evaluate the safety and efficacy of D-TACE combined with continuous hepatic artery infusion and systemic therapy versus D-TACE combined with systemic therapy in subjects with large hepatocellular carcinoma (main lesion ≥10 cm).

1. Previously histologically/cytologically confirmed components including fibrolamellar hepatocellular carcinoma, sarcomatoid hepatocellular carcinoma, cholangiocarcinoma, etc.; 2. A history of malignant tumors other than hepatocellular carcinoma, unless the following criteria are met: The patient has received possible curative treatment and there is no evidence of the disease within 5 years; Skin basal cell carcinoma, skin squamous cell carcinoma, superficial bladder cancer, cervical carcinoma in situ and other carcinomas in situ that have been successfully resected; 3. Diffuse tumor lesions; 4. A history of hepatic encephalopathy, hepatorenal syndrome, or a history of liver transplantation; 5. Pleural effusion, ascites, or pericardial effusion that requires drainage due to clinical symptoms; 6. Central nervous system metastasis; 7. Suffering from diseases that affect the absorption, distribution, metabolism, or clearance of the study drug (such as severe vomiting, chronic diarrhea, intestinal obstruction, malabsorption, etc.); 8. Previous or concurrent medications/treatments: Previous treatment with targeted therapies against signaling pathways such as anti - VEGF and/or VEGFR, RAF, MEK (e.g., sorafenib, lenvatinib, regorafenib) or immunomodulators such as anti - PD - 1, anti - PD - L1, anti - CTLA - 4; Previous hepatic arterial infusion chemotherapy; Safety: 9. Active bleeding or abnormal coagulation function, with a bleeding tendency or currently receiving thrombolytic, anticoagulant, or anti - platelet therapy; 10. Other significant clinical and laboratory abnormalities that the investigator believes affect the safety evaluation, such as uncontrolled diabetes, chronic kidney disease, grade II or higher peripheral neuropathy (CTCAE V5.0), abnormal thyroid function, etc.; 11. Active infections requiring treatment; 12. Active hepatitis B (HBsAg positive and abnormal liver function): If the HBV - DNA is ≥10⁴ copies/ml within 14 days before treatment, antiviral treatment should be carried out first until it drops below 10⁴ copies/ml before entering the study, and antiviral treatment should be continued while monitoring liver function and serum HBV - DNA levels; 13. Active hepatitis C (HCV - RNA ≥10³ copies/ml and abnormal liver function [ALT or AST > 3×ULN accompanied by TBIL > 2×ULN or clinical jaundice]); 14. Not recovered from surgery, such as having unhealed incisions or severe postoperative complications; 15. Pregnant or lactating women, and male or female patients of child - bearing potential who are unwilling or unable to take effective contraceptive measures.

Researchers use computers to generate random numbers for randomization

None

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Six months after the publication of the research, contact the research leader via email to obtain reasonable information.

Data acquisition Method: Paper CRF, collected by electronic EDC system, extracted from HIS system. Content: demographic information (age, gender, etc.), clinical characteristics (diagnosis, treatment history), observation indicators (test results, imaging data), follow-up information. Time: At the time of enrollment, samples were collected at 1, 3, and 6 months after treatment, and every 3 months thereafter until disease progression or death occurred. Personnel: Trained research assistants are responsible for data collection. data management Storage: Electronic databases are encrypted and stored on hospital servers or in the cloud, with restricted authorized access. Backup: Automatically backup to storage devices every week. Audit: A dedicated person conducts logical checks (completeness, accuracy) and conducts regular spot checks on data. Quality control: Develop SOP, clean up duplicate data, verify and handle outliers. Security and confidentiality: anonymize sensitive information, comply with ethical regulations, and limit data access.