Pancreatic Cancer Clinical Trial
Official title:
Phase II Study of Sirolimus in Patients With Chemo-resistant, Recurrent or Metastatic Pancreatic Cancer
Pancreatic cancer is a highly malignant tumor of the digestive system.In China, the annual
mortality/morbidity of pancreatic cancer is as high as 0.88:1, and the morbidity and
mortality are still on the rise. The 5-year survival rate of pancreatic cancer patients in
the United States is only 8%, among which more than 50% of patients have distant metastasis
at the time of diagnosis, and the 5-year survival rate of advanced patients with distant
metastasis is as low as 3%, with extremely poor prognosis. Currently there is no standard
treatment for the first - and second-line treatment resistant and postoperative recurrent
patients to further prolong their survival.
mammilian target of rapamycin (mTOR) is a very important serine/threonine protein kinase
involved in the regulation of energy metabolism, cell growth, angiogenesis and other cellular
biological processes.Rapamycin (sirolimus) is a selective inhibitor of mTOR kinase, which can
inhibit the activation and proliferation of T lymphocytes to inhibit the immune
response.Currently, mTOR inhibitors are also widely used in tumor treatment. Several studies
have been performed to evaluate the efficacy of sirolimus in some solid tumors, and
encouraging results are obtained. However, the existing studies on mTOR inhibitors and
pancreatic cancer treatment are mostly phase I trials, with little evaluation of the
efficacy. Therefore, the phase II clinical trial of rapamycin in the treatment of pancreatic
cancer is very necessary.
In preclinical studies, investigators found that rapamycin can effectively inhibit the
angiogenesis of liver Cancer led by tumor-associated macrophages (TAM), thereby inhibiting
the progression of liver Cancer.In vitro experiments on pancreatic cancer showed that
rapamycin can directly inhibit the proliferation of pancreatic cancer cells.After the
treatment with rapamycin in the homologous xenograft tumor model of mice, it was found that
the tumor growth of mice was significantly inhibited. Further analysis suggested that
rapamycin not only directly inhibits tumor proliferation, but also reverses the immune
suppressive microenvironment of pancreatic cancer and promotes the T-cell-mediated anti-tumor
immune response.Preclinical findings suggest that rapamycin may benefit survival in
pancreatic cancer patients, which makes us very interested in the efficacy of rapamycin in
patients with advanced pancreatic cancer.Therefore, investigators designed this trial to
evaluate the clinical efficacy of rapamycin in patients with second-line resistance and
recurrence who lacked a standard treatment regimen.
1. Research purpose This clinical trial was designed to evaluate the anti-tumor effect of
sirolimus in patients with advanced or postoperative recurrent pancreatic cancer with
second-line standard therapy resistance.
2. Grouping and sample size calculation A single-arm study was designed. Based on clinical
experience and literature, the expected median survival period of patients with advanced
pancreatic cancer after second-line resistance or postoperative recurrence was about 3
months, and the median survival period of such patients was expected to be extended to 6
months after the treatment with sirolimus. The significance level of statistical test
was set at 0.05 and the power of test was set as 80%, the time of enrollment was set to
June 2021, and the time of follow-up was set to June 2023. The follow up loss rate was
predicted as 5%, and the number of cases needed to be enrolled was calculated as 36.
3. Clinical trial procedure For the cases to be included, the patient's medical history,
symptoms, signs and other conditions should be examined in advance, informed consent
should be obtained and signed, and the patient's age, height, weight, medical history,
symptoms, signs, pathological results, tumor node metastasis (TNM) stage and other
contents should be recorded.According to the test requirements, the study was designed
to be limited to 5 years, and the day of oral administration of sirolimus will be set as
the first day, tumor markers will be follow up every 3 weeks.Each 3-month review
includes symptoms, signs, adverse events, blood routine examination, liver and kidney
function, abdominal enhanced CT, liver enhanced MRI+ diffusion, and chest
high-resolution CT.
Overall survival (OS) was taken as the primary endpoint and then recorded to the
secondary endpoint. All results were recorded in the case report form, clinical efficacy
and safety were evaluated, and adverse events were observed.If the patient cannot come
to the hospital for reexamination, follow up will be conducted by telephone, email, etc.
4. Adverse events record and report Information on non-serious adverse events that occur
during treatment should be recorded on the clinical trial report form (CRF), and all
serious adverse events will be recorded in the CRF report form.Few patients in this
study may have serious liver and kidney function injury, may have allergy reaction,
secondary hypertension, hypercholesterolemia, serious infection and so on. In view of
the above possible situations, investigators will fully evaluate the liver and kidney
function before treatment, and give protective drugs for organ function; And the
corresponding adjuvant drugs such as blood pressure drugs, lipid-regulating drugs to
prevent sirolimus side effects;The symptoms and indicators of infection were closely
monitored. Once adverse events happen, report will be sent to the general manager and
the head of the hospital immediately, and also to the ethics committee of adverse events
within the specified time, and make unified analysis after the study.
5. Data management and statistical analysis Data recording and auditing: The observation
data will be recorded by the attending physician in the case report form, and the data
records shall be timely, complete, accurate and authentic.The form will be filled out in
black (or blue and black), any changes will be made by the relevant personnel, and then
signed and dated. The changes will not cover the original record. If possible, copy the
relevant test paper and paste it on the attached page after CRF.
Data entry: Establish data entry program and database for statistical analysis.
6. Informed consent The subject must obtain written informed consent before performing the
study procedures to inform the patient of the specific content related to the study. The
specific procedures for obtaining informed consent include: the patient's disease
characteristics, treatment plan and related risks shall be informed in detail by the
competent doctor, and the patient or legal guardian with civil capacity shall sign the
informed consent after fully knowing and understanding the relevant process and risks of
this study.
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