Pancreatic Cancer Clinical Trial
Official title:
A Phase III Study of Chemotherapy With or Without Algenpantucel-L (HyperAcute®-Pancreas) Immunotherapy in Subjects With Borderline Resectable or Locally Advanced Unresectable Pancreatic Cancer
Unfortunately, despite the best clinical efforts and breakthroughs in biotechnology, most
patients diagnosed with pancreatic cancer continue to die from the rapid progression of their
disease. One primary reason for this is that the disease is typically without symptoms until
significant local and/or distant spread has occurred and is often beyond the chance for cure
at the time of the diagnosis. The lack of any treatment to substantially increase long term
survival rates is reflected by the poor outcomes associated with this disease, specifically
time to disease progression and overall survival.
However, another important part of the body is now being looked at as a target for therapy
against this disease - the immune system. Scientists have clearly shown that pancreatic tumor
cells produce a number of defective proteins, or express normal proteins in highly
uncharacteristic ways, as part of this cancer. In some cancers, these abnormalities can cause
an immune response to the cancer cells much in the way one responds to infected tissue. In
progressive cancers however, the immune system fails to effectively identify or respond to
these abnormalities and the cancer cells are not attacked or destroyed for reasons not yet
fully understood. This clinical trial proposes a new way to stimulate the immune system to
recognize pancreatic cancer cells and to stimulate an immune response that destroys or blocks
the growth of the cancer.
This new method of treatment helps the immune system of pancreatic cancer patients to
"identify" the cancerous tissue so that it can be eliminated from the body. As an example,
most people are aware that patients with certain diseases may require an organ transplant to
replace a damaged kidney or heart. After receiving their transplant, these patients receive
special drugs because they are at great danger of having an immune response that destroys or
"rejects" the transplanted organ. This "rejection" occurs when their immune system responds
to differences between the cells of the transplanted organ and their own immune system by
attacking the foreign tissue in the same way as it would attack infected tissue. When the
differences between foreign tissues and the patient's body are even larger, as with the
differences between organs from different species, the rejection is very rapid, highly
destructive, and the immunity it generates is longlasting. This is called hyperacute
rejection and the medicine used to immunize patients in this protocol tries to harness this
response to teach a patient's immune system to fight their pancreatic cancer just as the body
would learn to reject a transplanted organ from an animal.
To do this, Algenpantucel-L immunotherapy contains human pancreatic cancer cells that contain
a mouse gene that marks the cancer cells as foreign to patient's immune systems. The immune
system therefore attacks these cancer cells just as they would attack any truly foreign
tissue, destroying as much as it can. Additionally, the immune system is stimulated to
identify differences (aside from the mouse gene) between these cancer cells and normal human
tissue as foreign. This "education" of the immune system helps treat the patient because
pancreatic cancer cells already present in a treated patient are believed to show some of the
same differences from normal tissue as the modified pancreatic cancer cells in the product.
Due to these similarities, the immune system, once "educated" by the Algenpantucel-L
immunotherapy, identifies the patient's cancer as foreign and attacks.
The chemotherapy combination to be used in this study has been shown to improve survival in
advanced pancreatic cancer and is being combined with an experimental pancreatic cancer
immunotherapy that stimulates the immune system to recognize and attack the cancer. One goal
of this study is to determine whether chemotherapy and immunotherapies can work cooperatively
to increase anti-tumor effects to levels beyond what would be seen with either treatment
alone.
In this experimental study, all patients are given a strong combination of anti-tumor
chemotherapies while some patients are also given injections of an immunotherapy drug
consisting of two types of pancreatic cancer cells that we have modified to make them more
easily recognized and attacked by the immune system. We propose to test this new treatment
protocol in patients with locally advanced pancreatic cancer to demonstrate that treatment
with the immunotherapy increases the time until the tumor progresses or increases overall
survival when given in combination with the current standard of care therapy for this
disease.
This protocol attempts to treat pancreatic cancer therapy using a naturally occurring barrier to xenotransplantation in humans to increase the efficacy of immunizing patients against their pancreatic cancer. In this protocol, the transfer of the murine α(1,3) galactosyltransferase [α(1,3)GT] gene to immunotherapy component cells results in the cell surface expression of α(1,3)galactosyl-epitopes (αgal) epitopes on membrane glycoproteins and glycolipids. These epitopes are the major target of the hyperacute rejection response. This response occurs when organs are transplanted from lower animal donor species into primates and results in rapid destruction of transplanted tissue and an augmented response against transplant antigens, including antigens not related to the αgal epitopes. Human hosts have pre-existing anti-α-gal antibodies that are thought to result from chronic immunological stimulation due to exposure to α-gal epitopes that are naturally expressed on normal gut flora and these antibodies may comprise up to 1% of serum immunoglobulin G (IgG). Opsonization and lysis of the immunotherapy component cells mediated by this antibody is believed to increase the efficiency of antigen processing by targeting vaccine components to antigen presenting cells via the Fcγ receptor. ;
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