PLUTO: A Prospective Phase II Study of Perioperative TORIPALIMAB Plus LENVATINIB in Patients With Renal Cell Carcinoma Undergoing Nephrectomy

Jinling Hospital, China1 个研究点分布在 1 个国家目标入组 17 人2022年12月20日

概览

简要总结

The PLUTO-trial is a single-center, open-label, phase II trial investigating Toripalimab plus Lenvatinib in patients with multi-stage clear-cell renal cell carcinoma. In this trial, patients will be enrolled in one of three cohorts according to the stage of their clear-cell renal-cell carcinoma: localized, locally advanced and metastatic RCC. Patients in all cohorts will receive four to five cycles of preoperative Toripalimab (240mg Q3W IV) plus Lenvatinib (20mg QD PO) and will undergo nephrectomy within four weeks after the last cycle. Patients in cohort 1 who are considered to be at high risk according to pathology results of surgery specimen, and all the patients in cohort 2 are supposed to receive postoperative doses of Toripalimab (240mg Q3W IV) for at most 17 doses. Patients in cohort 3 are supposed to continue Toripalimab plus Lenvatinib after surgery.

The primary clinical endpoint of the study is immune-related pathological response to tumorigenesis, defined as the extent of tumor cell reduction in the tumor bed. Simon's two-stage design is used in this study. An initial cohort of 12 patients per cohort will be recruited, followed by an interim analysis. Recruitment to each cohort will be closed if a qualifying immune-related pathological response is not observed in any patient at an interim analysis. If qualifying immune-related pathological response is observed in at least one patient, additional 9 patients will be recruited in the cohort to 21 patients. Considering potential 10% dropout rate in the trial, an anticipation of 69 patients will be recruited for this study.

详细描述

The objective of this single-center clinical trial was to evaluate the objective response rate and safety of Toripalimab combined with tyrosine kinase inhibitors TKI (Lenvatinib) in neoadjuvant treatment of（T2a-T4NanyM0 or TanyN1M0） clear cell renal cell carcinoma.Toripalimab is a new antibody that may help activate the immune system by blocking the function of the inhibitory molecule PD-1. This is a single-institution, single-arm Phase 2 clinical trial. Patients will be treated with Toripalimab in combination with tyrosine kinase inhibitors TKI (Lenvatinib) and patients will undergo partial or radical nephrectomy after neoadjuvant therapy.

注册库

clinicaltrials.gov

开始日期

2022年12月20日

结束日期

2026年1月10日

最后更新

上个月

研究类型

Interventional

研究设计

Sequential

性别

All

研究者

发起方

Jinling Hospital, China

责任方

Principal Investigator

主要研究者

Le Qu

Associate chief urologist

Jinling Hospital, China

入排标准

入选标准

•Have fully understood and voluntarily signed the informed consent Form (ICF);
•Age: 18-80 years old (at the time of signing the informed consent); Both male and female; ECOG PS score: 0-1;
•RCC with clear cell component confirmed by histology or cytopathology, including locally advanced RCC with clear cell component;
•ECOG 0-1 points
•T1b-T2bN0M0, T3a-4N0M0, TanyN1M0 or M1RCC diagnosed by imaging at initial diagnosis:
•Cohort 1: T1b-T2bN0M0 RCC;
•Cohort 2: T3a-4N0M0 or TanyN1M0 RCC;
•Cohort 3: M1 RCC undergoing cytoreductive nephrectomy.
•Radical nephrectomy or partial nephrectomy or renal tumor enucleation was decided after the clinician made the treatment plan and communicated with the patient;
•Willingness and ability to comply with planned visits, therapeutic laboratory testing, and other procedures.

排除标准

•Signs of tumor metastasis involving the central nervous system;
•History of malignant tumors other than the study disease within the previous 5 years, with the exception of malignant tumors that can be expected to be cured with treatment (including but not limited to adequately treated thyroid cancer, carcinoma in situ of the cervix, basal or squamous cell skin cancer, or ductal carcinoma in situ of the breast treated with radical surgery);
•Prior to participating in the study, patients had received other systemic treatment drugs, including targeted drugs, immunotherapy drugs and their combination regimens, or local anti-tumor therapy, or received investigational drugs or device therapy;
•Underwent major surgery (judged by the investigator) within 4 weeks before the first trial dose, were recovering, or were unable to undergo baseline puncture;
•History of severe drug allergy, including but not limited to antibody drugs;
•patients with contraindications to immunotherapy restart, including but not limited to:
•Grade 2-4 immune myocarditis;
•Severe grade 4 proteinuria;
•Severe or life-threatening grade 4 immune hepatitis;
•Severe grade 3-4 immune pneumonitis;

研究组 & 干预措施

Toripalimab + Lenvatinib followed by nephrectomy

After 4-5 cycles of preoperative therapy, patients will undergo nephrectomy within 4 weeks. Patients with WHO/ISUP grading 4 RCC in cohort 1, and all patients of cohort 2 and 3 will receive postoperative dosing within 4 weeks for at most 17 doses. Subsequent follow-up will then be completed to assess adverse events and long-term outcomes. Cohort 1: Localized RCC (cT1b-T2bN0M0). Nephrectomy following preoperative therapy. For patients with WHO/ISUP grading 4 RCC in the resected tumor, postoperative dosing of Toripalimab beginning within 4 weeks after surgery for at most 17 doses. Cohort 2: Locally advanced RCC (cT3-4N0M0 or cTanyN1M0). Nephrectomy following preoperative therapy. Postoperative dosing of Toripalimab beginning within 4 weeks after surgery for at most 17 doses. Cohort 3: Metastatic RCC (cTanyNanyM1). Cytoreductive nephrectomy following preoperative therapy. Postoperative dosing of Toripalimab plus Lenvatinib beginning within 4 weeks after surgery for at most 17 doses.

干预措施: Toripalimab

Toripalimab + Lenvatinib followed by nephrectomy

After 4-5 cycles of preoperative therapy, patients will undergo nephrectomy within 4 weeks. Patients with WHO/ISUP grading 4 RCC in cohort 1, and all patients of cohort 2 and 3 will receive postoperative dosing within 4 weeks for at most 17 doses. Subsequent follow-up will then be completed to assess adverse events and long-term outcomes. Cohort 1: Localized RCC (cT1b-T2bN0M0). Nephrectomy following preoperative therapy. For patients with WHO/ISUP grading 4 RCC in the resected tumor, postoperative dosing of Toripalimab beginning within 4 weeks after surgery for at most 17 doses. Cohort 2: Locally advanced RCC (cT3-4N0M0 or cTanyN1M0). Nephrectomy following preoperative therapy. Postoperative dosing of Toripalimab beginning within 4 weeks after surgery for at most 17 doses. Cohort 3: Metastatic RCC (cTanyNanyM1). Cytoreductive nephrectomy following preoperative therapy. Postoperative dosing of Toripalimab plus Lenvatinib beginning within 4 weeks after surgery for at most 17 doses.

干预措施: Lenvatinib

结局指标

主要结局

Immune-related pathologic reponse rate (irPR）

时间窗: Date of surgery

IrPR is defined as the proportion of patients achieving a complete pathologic or major pathologic response. Complete or major pathological response are assessed according to the proportion of viable residual tumor in the initial tumor bed of HE sections from tumor tissue. Complete pathological response means no viable residue tumor in the initial tumor bed, and major pathological response with a ≤10% viable residue tumor in the initial tumor bed.

次要结局

Adverse events(From first dose to 28 days after last dose)
Imaging density changes of lesions(Baseline to date of surgery)
Surgical morbidity(From date of surgery up to 28 days after surgery)
Objective response rate (ORR)(Baseline to date of surgery)
Down-staging rate of primary tumor T staging(Baseline to date of surgery)
Rate of distant metastasis(Up to 2 years after surgery. Patients will be followed every 3 months the 1st year, and every 6 months the next year.)
Progression free survival (PFS)(Up to 2 years after surgery. Patients will be followed every 3 months the 1st year, and every 6 months the next year.)