Melanoma Clinical Trial
Official title:
A Study of Ipilimumab Plus Cytokine-induced Killer Immunotherapy for Stage II Melanoma Patients
For investigators' current experimental clinical trial, patients are given 4 injections of ipilimumab, given 3 weeks apart x 4 injections with or without cytokine-induced killer therapy. Investigators propose to test this dual therapy in patients with melanoma who have known stage I, metastatic melanoma. Investigators hypothesize that this form of combinatorial immunotherapy will result in tumor stabilization or shrinkage, significant prolongation of progression-free, disease-free or overall survival compared to the use of ipilimumab alone
despite the best clinical efforts and breakthroughs in biotechnology, most patients
diagnosed with advanced stage melanoma continue to die from their disease. Reasons for this
include: 1) patients are often diagnosed at a time when their melanoma has already spread to
other sites such as the chest cavity, bone, liver, and brain limiting the options for
surgical excision and 2) the cancer cells are resistant or become resistant to chemotherapy
drugs used to treat the patient. Resistance to one type of chemotherapy agent often rapidly
leads to resistance against many other chemotherapy drugs. These reasons are the major
causes of cancer progression that are usually discussed when considering treatment options
for patients with disease that continues to grow and spread. However, another important part
of the body should be considered-- the immune system. Scientists have clearly shown that
melanoma cells produce a number of abnormal proteins or abnormal amounts of certain proteins
found in normal melanoma cells. Normally one would expect a patient to develop an immune
response against these abnormal proteins found in their cancer and attack them much the way
the investigators would fight off an infection from a foreign bacteria or virus. However,
for reasons that scientists do not fully understand, the immune system fails to respond
adequately to these abnormal proteins and does not destroy the melanoma cells. This human
clinical trial proposes a new way to make the immune system recognize the cancer cells and
encourages it to attack and destroy them.
In this project, the investigators have put a mouse gene into human melanoma cancer cells,
so that those cells produce these abnormal sugar patterns and stimulate the immune system to
attack the melanoma. This strategy works well to kill other human cancer cells in the
laboratory, but it needs to be tried in melanoma patients to see if it will be effective and
to determine if such a treatment causes any side effects. Investigators propose to test this
new treatment in patients with melanoma to see if it can stop, slow or destroy tumors in
these patients. Patients will be injected with an anti-tumor immunotherapy consisting of
three types of dead human melanoma cancer cells that have been genetically altered to
express the mouse gene responsible for making this abnormal sugar-protein on the cells.
In this Phase II Study, patients with early stage melanoma will undergo a series of
intradermal injections with cytokine-induced killer therapy. These cell lines have been
transduced with a recombinant. In addition to the cik therapy, some patients will also
receive ipilimumab as an important component of this immunization strategy that will attempt
to enhance and activate the host immune system to destroy growing tumor cells. Endpoints of
the study include safety assessments, and clinical, tumor and immunological responses.
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Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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