Novel software developed helps predict markers called minor histocompatibility antigens to develop immune-based therapies for leukemia.
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‘Using the new software aids in predicting tumor markers and develops immune-based therapies for leukemia. ’
The researchers report at the 59th Annual American Society for Hematology Annual Meeting in Atlanta, that they were able to validate their approach for predicting markers -called minor histocompatibility antigens in a group of patients with blood cancers. The preliminary findings are an early step in the overall plan to use the software's predictions to develop immune-based therapies for leukemia.
"If you could identify and activate the immune cells that only target leukemia cells, and not normal, healthy cells, that would be a big win," said UNC Lineberger's Benjamin Vincent, MD, assistant professor in the UNC School of Medicine Division of Hematology/Oncology.
New Cancer-Causing Pathway Identified That Causes Leukemia
The DNA of immature blood cells, mainly white cells, becomes damaged in some way. This abnormality causes the blood cells to grow and divide continuously.
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Cancer is known as a genetic disease in which errors in DNA help to drive abnormal cell growth. When mutations or other genetic changes occur, sometimes the cell's machinery will read and translate those errors into abnormal proteins unique to cancer cells. This is one source of possible targets for the immune response in leukemia patients.
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The researchers hypothesized they could sequence cancer cells' versus normal cells' DNA and RNA to identify these targets, a process that required the development of custom bioinformatics software in the Vincent lab.
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In addition, they predicted more than 100 new antigen targets. Looking ahead, researchers want to use their software to develop several types of treatments that target these predicted antigens.
In one proposal, their goal is to improve stem cell transplants, which is the best chance of cure for many patients with high-risk blood cancer.
Vincent said they could potentially use their predictions to engineer donor immune cells to specifically target the cancer cell antigens while preventing graft-versus-host disease, in which the immune cells attack healthy tissues.
"We have developed a novel computational approach to predicting leukemia-specific antigens," Vincent said.
"The biggest takeaway is that we can now develop personalized cell therapies that target these antigens that we hypothesize will increase leukemia cures without causing graft versus host disease."
Source-Eurekalert
