Pancreatic Cancer Clinical Trial
Official title:
Changes in Biomarkers From Blood Over Time in Patients With Pancreatic Adenocarcinoma
Pancreatic adenocarcinoma (PDAC) is the fourth leading cause of cancer mortality in the United States. The high mortality for these tumors is primarily attributed to the late stage in which most patients are diagnosed, leading to a dismal 5-year survival of 6% for all stages of PDAC. Surgical resection offers the best chance for survival, but most patients only present with symptoms after the tumor has metastasized, and as a result are not operative candidates. This creates a need to both identify patients at an earlier stage while their cancer is still resectable, and predict the aggressiveness of the disease in order to better target treatment. In addition, even patients who receive curative surgery are at a high risk of developing recurrence of disease. Thus, there is also a need to detect recurrence early so appropriate treatment can be provided. As several adjuvant chemotherapeutic regimens are now available, it will be important to identify as soon as possible that the cancer has become refractory to a given therapy. This will allow one to progress to second or third line therapy more quickly while the tumor burden is smaller. This purpose of this study is to identify biomarkers in the blood of patients with PDAC and determine how they can change over time in relation to treatment to assess for any correlation with patient outcomes, response to treatment, recurrence of disease and overall survival. This study will be limited to patients who present to the Johns Hopkins Hospital between January 1, 2015 and December 31, 2018 with PDAC. Blood will be drawn from all consenting patients at the time of initial diagnosis and after treatment. Patients will undergo treatment for their cancer based on personal preference, standard guidelines and discussion with medical, radiation, and surgical oncologists. Patients who undergo surgical resection will also have an additional blood sample collected after resection, and patients who undergo chemotherapy and/or radiation will have an additional blood sample draw at the end of this treatment. A patient could have blood collected at multiple intervals, i.e. a pre-treatment sample, sample post-neoadjuvant chemotherapy/radiation, sample post-surgery, and sample post-adjuvant chemotherapy/radiation. In patients, who have undergone curative resection of PDAC blood samples will be collected till they develop clinical recurrence of disease. For the first 2 years following surgery samples will be collected every 3-4 months. Beyond that the investigators will collect samples every 6 months for the next two years. For all patients found to be alive and disease free beyond 4 years after surgery samples will be collected once every year. These patients will be followed to determine disease-free and overall survival. With this study, the investigators aim to assess the potential utility of blood biomarkers over time for pancreatic tumors which will help both with early detection of disease and also recurrence of disease after surgery. Biomarkers identified would have the potential to create a new method for early diagnosis of patients with PDAC, predict overall survival, response to treatment, or risk of metastatic spread, and predict recurrence of disease, all of which has the potential to drastically improve outcomes for this deadly disease.
This is a single-institutional, prospective study at the Johns Hopkins Hospital which will be
conducted from January 1, 2015 to December 31, 2018. All patients who present to the Johns
Hopkins Hospital with a pancreatic adenocarcinoma (PDAC) for evaluation of treatment by
chemotherapy, radiation therapy, and/or surgery will be approached to participate in this
study, but only those who consent to the study will be included. All patients who consent to
participate in this trial will have blood drawn (approximately 50 ml or 3-4 tablespoons) at
the time of diagnosis but before any treatment had been administered. Further blood will be
drawn after any treatment. For example, those patients that undergo surgical resection will
also have blood drawn after resection prior to discharge. Those patients that undergo
treatment with chemotherapy, radiation therapy, and or biologic/vaccine therapy will have
blood drawn once after this treatment is completed. If a patient undergoes chemotherapy and
then surgical resection, he or she will have blood drawn after chemotherapy but before
surgical resection, and then again after surgical resection, all in addition to the
pre-treatment blood sample (see schema included in IRB). For the first 2 years following
surgery samples will be collected every 3-4 months. Beyond that the investigators will
collect samples every 6 months for the next two years. For all patients found to be alive and
disease free beyond 4 years after surgery samples will be collected once every year. This
blood will be stored in the investigators' research facility and as such will be labeled with
a de-identified code. If a patient refuses further blood draws at any time during the study
or is loss to follow-up, the samples that have been collected will still be utilized.
The blood will be processed on the day of collection, within 6 hours of being drawn. Twenty
(20) ml of blood, collected in two purple topped tubes, will be used for isolation of
circulating tumor cells (CTCs) through the Isolation by Size of Epithelial Tumor Cells assay
(ISET), which separates tumor cells by size onto a membrane which can be used for further
experiments. These 20 ml of blood will be mixed with ISET buffer per standard protocol and
filtered through the ISET machine onto membranes. These membranes will be stored at -20
degrees C under a de-identified number, and remain at these conditions for several years with
full preservation of the cells. Further experiments will be done on these membranes, which
include immunofluorescent staining, laser capture microscopy, and genetic analysis. The
remaining 30 ml of blood, collected in red and purple topped tubes, will be processed by a
standard protocol within 6 hours of collection. Blood will be double spun to remove white
blood cells, and plasma and will be frozen. Driver gene mutations characterized in the
resected tumors will be monitored by digital droplet Polymerase Chain Reaction (ddPCR),
including the Kirsten rat sarcoma viral oncogene homolog (k-ras), p53, p16/cdkn2a and the
Deleted in Pancreatic Cancer-4 gene (DPC4/SMAD4) to identify the presence of ctDNA and
whether levels are rising.
Data will be collected, de-identified and analyzed as a single dataset at the Johns Hopkins
Hospital. Data will be obtained from patient electronic and paper clinical charts from the
John Hopkins Hospital starting on 1/1/2015, with only data in existence as of 1/1/2015
collected. More specifically, radiology, chemotherapy, operative and pathology reports,
discharge summaries, and clinic notes will be reviewed and data from these sources collected.
For patients lost to follow-up, the Social Security Death Index (but will not need to collect
social security numbers) will be searched for evidence of death. Collected patient data will
be entered into a dedicated database. Data will only be collected in order to correlate
outcomes and tumor characteristics with the biomarkers identified during this study.
Following data accrual and prior to analysis, all personal identifiers will be deleted and no
identifiable information will be present at the time of statistical analysis. The subject
data generated will not appear in the subject's medical record and will be used for research
purposes only. The data will be recorded in a password-protected, secure database within the
Principal Investigator's office and will be accessible only by the key personnel. After all
data for a particular subject is collected, the subject's identity will be deleted to assure
confidentiality.
The data that are collected in this study will not be used for the clinical management of any
patient on study.
Inclusion/Exclusion Criteria
The investigators will include all patients who present to the Johns Hopkins Hospital for
treatment with a diagnosis of a pancreatic adenocarcinoma. Subjects will only be included if
they are over the age of 18 year old and plan to undergo their treatment at the Johns Hopkins
Hospital. All patients with non-primary pancreas tumors, pancreatic neuroendocrine tumors, or
benign pancreatic masses will be excluded. Patients will be excluded if they have already
undergone treatment of any kind at another institution.
The investigators aim to include data from at least 200 patients over the three years of this
study. The primary outcome will be the identify biomarkers in the blood from patients with
pancreatic adenocarcinoma and the changes in these biomarkers over time in relation to
treatment. These biomarkers will include specific antibodies, circulating tumor cells (CTCs)
and circulating tumor DNA (ctDNA). Secondary outcomes will include the relationship of
pre-treatment biomarker levels or changes in biomarker levels to disease-free and overall
survival, risk of metastases, recurrence of disease and response to treatment. Patient,
tumor, and surgical characteristics will be collected for all patients included in this
study. Differences between characteristics will be statistically compared between patients.
In addition, these characteristics will be analyzed as possible predictors of survival using
univariate and multivariate analyses through the log-rank test and Cox-proportional hazard
models. These characteristics will include:
1. Patient and tumor clinical demographics including age, gender, race, primary tumor
location, location of metastases, tumor grade, and Carbohydrate Antigen 19-9 (CA19-9)
levels pre- and post-chemotherapy and pre- and post-resection.
2. Chemotherapy variables including type, number of cycles, response, and timing
(neoadjuvant and/or adjuvant).
3. Operative variables including type of resection, number of lymph nodes resected,
vascular proximity of tumor, histopathology, and post-operative mortality and
complications.
4. Long-term variables including presence and location of recurrence and status
(alive/dead).
5. Levels of specific biomarkers at the various time points of blood draws.
6. Numbers of circulating tumor cells at each time point in addition to genetic mutations
present in the cells.
For all patients, overall survival will be calculated as the time between the date of the
first pre-treatment blood draw to the date of the last known follow-up visit or death,
whichever comes first. For patients who undergo surgical resection the investigators will
calculate time to disease recurrence as measured from the day of surgery for pancreatic
resection to the date of documented disease recurrence or death, whichever comes first. Time
to disease recurrence and overall survival will be described with Kaplan-Meier curves and
will be compared by log-rank test. The 1- and 5-year overall survival rate will be estimated
with its 95% confidence interval. Statistical significance will be set for a p-value at or
below 0.05.
The primary risks to this patient will be associated with the blood collection, but are no
more than minimal given collection with be by venipuncture and no more than 50 ml will be
taken at a time. The general risks associated with venous blood draw include bruising or
minor bleeding at the site of venous puncture, which would be managed with the application of
pressure.
There will be no direct benefit to patients in this study, as results generated will not be
used for management of these patients. This study has the potential to benefit future
patients by identifying methods for early diagnosis of patients with pancreatic cancer and
predicting overall survival, response to treatment, or risk of metastatic spread, and
predicting recurrence of disease, all of which has the potential advantage of improving
outcomes for this deadly disease.
There will be no compensation given to subjects in this study. Costs in this study will be
related to the cost of blood draws during various scheduled clinic visits. These will be
minimal.
All patients who agree to participate in this study will be required to sign a consent form
for the collection, storage, and use of their blood.
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