Adenocarcinoma Clinical Trial
Official title:
Perioperative Stromal Depletion Strategies in Pancreatic Ductal Adenocarcinoma
We will be conducting a Phase II study investigating PEGPH20 in combination with gemcitabine
and nab-paclitaxel in patients with borderline resectable pancreatic ductal adenocarcinoma
(PDAC) at the Helen Diller Family Comprehensive Cancer Center at University of California,
San Francisco (UCSF). There are multiple definitions of borderline resectable PDAC including
the MD Anderson definition and the criteria developed during the Consensus Conference
sponsored by the American Hepato-Pancreato-Biliary Association, Society of Surgical Oncology,
and Society for Surgery of the Alimentary Tract. Borderline resectable PDAC cases will be
identified per the definition developed in the currently running inter-group pilot trial for
borderline resectable pancreatic cancer (NCT01821612). Per this trial, borderline resectable
PDAC is defined as "presence of any one or more of the following on CT:
- An interface between the primary tumor and the superior mesenteric vein or portal vein
(SMV-PV) measuring ≥ 180° of the circumference of the vessel wall
- Short-segment occlusion of the SMV-PV with normal vein above and below the level of
obstruction that is amenable to resection and venous reconstruction
- Short segment interface (of any degree) between tumor and hepatic artery with normal
artery proximal and distal to the interface that is amenable to resection and
reconstruction.
- An interface between the tumor, and Superior mesenteric artery (SMA) measuring < 180º of
the circumference of the vessel wall.
This trial will be conducted in two parts. In Part I, pre-treatment endoscopic ultrasound
(EUS)-guided core biopsies of the pancreatic tumor, CA 19-9 levels and functional MRIs
including Dynamic contrast-enhanced (DCE)-MRI and Diffusion-weighted magnetic resonance
imaging (DWI-MRI) will be obtained for the first fifteen patients enrolled. After a 1-week
run-in period with PEGPH20 on days 1 and 4, patients will have repeat EUS-guided core
biopsies, functional MRI, CA 19-9 level and baseline CT chest, abdomen and pelvis.
Subsequently, patients will be started on treatment with PEGPH20, gemcitabine and
nab-paclitaxel given weekly for 3 weeks, every 28 days. To evaluate the disease response to
treatment, CA 19-9 levels will be checked monthly and restaging CT chest, abdomen and pelvis
will be obtained every 8 weeks. If there is disease progression at any point in the study,
patients will be taken off of study and alternative treatments will be offered. At the
completion of 4 cycles of therapy, restaging CT scans will be obtained to determine
resectability. If the patients are found to have resectable disease, an additional functional
MRI will be obtained to evaluate the PDAC stroma. If the patients are able to have successful
surgeries, tissue analyses will be performed on the resected pancreatic tumor. These patients
will then proceed to get 2 cycles of adjuvant chemotherapy with gemcitabine and
nab-paclitaxel. If the patients are deemed to be surgical candidates but are found to have
unresectable disease in the operating room, an intraoperative core biopsy of the pancreatic
tumor will be obtained for tissue analyses. At the time of initiation of therapy with
PEGPH20, patients will be started on prophylactic dose of enoxaparin 1 mg/kg subcutaneous
daily. This will be continued throughout the study participation.
In Part II, an additional 21 patients will be enrolled, and will begin neoadjuvant therapy
with PEGPH20, gemcitabine and nab-paclitaxel without the 1 week run-in of PEGPH20-only or the
pre- and post-run-in EUS-guided biopsies.
For Specific Aim 1, we will be monitoring the post-operative complication of clinically
relevant pancreatic fistula within one week of surgery per the standard clinical guidelines
as noted above. Common clinical presentations of pancreatic fistula include abdominal pain,
leukocytosis and fever (temperature >100.4 degrees). Diagnostic work-up of pancreatic fistula
will be with CT abdomen with contrast, which has a sensitivity of 63% and specificity of 83%
for detecting pancreatic fistula. The pancreatic fistulas will be categorized into grades A,
B or C as previously reported. Our study will be investigating only clinically relevant
pancreatic fistulas, i.e. grades B or C. Depending on the grade of pancreatic fistula,
patients will be treated as indicated with conservative treatment options including bowel
rest, antibiotics, somatostatin analogues and percutaneous drainage or surgical
re-exploration. We will also track other relevant post-operative complications such as
delayed wound healing, development of wound dehiscence or wound infection.
The tissue analyses will include review of the immunohistochemical (IHC) stains for actin,
hyaluronic acid staining with binding protein probe, proliferation as measured by ki-67% and
Phospho-histone H3 (Ph-H3); cell apoptosis as evaluated by IHC stain for cleaved caspase 3
(CC3) and Tunel. If limited tissue sample is obtained via the core biopsies, the priority of
tissue analysis will be as follows: (1) fixed in formalin for H&E and IHC (Ph-H3; CC3/Tunel;
Hyaluronic Acid (HA) binding); (2) fixed in Optimal Cutting Temperature (OTC) such that IHC
with difficult antibodies can be done (to potentially obtain mRNA or DNA). The IHC studies
will be done at the UCSF Helen Diller Family Comprehensive Cancer Center Immunohistochemistry
and Molecular Pathology Core. The tissue analyses of the biopsy and surgical specimens will
be done by study pathologist.
The CT and magnetic resonance (MR) imaging analyses will be performed at the Abdominal
Imaging at UCSF. To decrease the impact that metal stents may have on the functional MRI
results, we will include only patients who have plastic stents in our study. In addition, to
reduce variability in results, the DCE-MRI and DWI-MRI will be obtained on the same MR
machine at a similar time of day as the baseline scan. The DCE-MRI images will be analyzed by
calculating Ktrans and DWI-MRI images will be analyzed by calculating apparent diffusion
coefficient (ADC) as described elsewhere. We will scan patients in a torso coil on a 3T
clinical MR scanner. Imaging will include MR diffusion with b-values of 0, 125, and 500 for
estimates of perfusion and tumor, and dynamic contrast-enhanced MR imaging (DCE-MRI) for
measurement of Ktrans, blood volume, and blood flow. The region of tumor will be determined
by MR imaging in reference to the baseline CT scans. The native T1 of the pancreas and liver
will be calculated from a series of four, 3D, spoiled gradient recalled echo (SPGR) sequences
with different flip angles. The conventional DCE-MRI will be acquired as a 3D, fast spoiled
gradient echo sequence, covering the targeted areas of the pancreas or liver, at a temporal
resolution of 5 sec over 6 minutes after the administration of 0.1 mmol/kg gadobenate
dimeglumine. DCE-MRI images will be post-processed using MIStar software (Apollo Medical
Imaging, Melbourne, Australia), which allows for motion correction to account for any shifts
in data. Datasets with artifacts will be eliminated before further post processing. After
contrast delivery, the new T1 is calculated and is presumed to change with the Gd
concentration such that [Gd] = (1/T1-1/T10)/R1 where R1 is assumed to be 4.5 sec-1 mmol/L-1
at 3T.
Run-in Period with PEGPH20
- Days 1, 4
PEGPH20 3 ug/kg Dexamethasone 8mg PO 1-2 hours pre-PEGPH20 and PO 8-to-12 hours post-PEGPH20
*Start enoxaparin 1 mg/kg subcutaneous daily on day 1 (to be continued throughout the trial)
- On day 8 of run-in period with PEGPH20, EUS-directed core biopsy, CA 19-9, functional MRI
and CT chest, abdomen (pancreatic protocol) and pelvis will be obtained.
Cycle 1 and onward
-Day 1, 8, 15
PEGPH20 3 ug/kg + Gemcitabine 1000mg/m2 + nab-Paclitaxel 125mg/m2 Dexamethasone 8mg PO 1-2
hours pre-PEGPH20 and PO 8-to-12 hours post-PEGPH20
- Gemcitabine and nab-paclitaxel will be administered 2-4 hours post-PEGPH20.
- Neoadjuvant therapy will be four 28-day cycles with CT chest, abdomen and pelvis scans
and CA 19-9 measurements every 8 weeks. Patients will be taken off of the study if there
is any evidence of disease progression.
- After four cycles of neoadjuvant therapy, patients will be evaluated for surgical
resection depending on the CT scan findings obtained on cycle 4, day 21.
- If they have resectable disease, they will have a functional MRI following the restaging
CT scan. If patients have successful resection, they will receive 2 additional cycles of
gemcitabine and nab-paclitaxel. If they are found to have unresectable disease in the
operating room, an intra-operative core biopsy will be obtained.
- If they have unresectable disease on the restaging scans following 4 cycles of therapy,
they will be taken off of the study.
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