Researchers at the University of North Carolina have developed a new immunotherapy approach that selectively destroys acute myeloid leukemia (AML) cells while sparing healthy blood tissue, addressing a critical challenge in treating this aggressive blood cancer. The findings were published in the journal Blood and represent a potential advancement in cancer therapy.
Immunologist Gianpietro Dotti and hematologist Paul Armistead led the research teams, which engineered immune cells capable of distinguishing between cancerous and normal cells. Current therapies often struggle with this distinction, leading to toxic side effects and limited effectiveness. The new method could expand treatment options for patients with AML, a disease with a five-year survival rate of only about 30%.
The study details how the modified immune cells attack leukemia cells while leaving healthy blood cells unharmed. This precision could reduce the severe side effects associated with conventional treatments like chemotherapy and stem cell transplants. Further research may pave the way for even more advanced and potentially side-effect-free cancer therapies.
The development comes as companies like Calidi Biotherapeutics Inc. (NYSE American: CLDI) focus on similar innovative cancer treatments. The field of immunotherapy is rapidly evolving, with researchers exploring ways to harness the body’s immune system to fight cancer more effectively.
This breakthrough is particularly significant for AML patients who have limited treatment options, especially those who relapse after initial therapy. The UNC approach could lead to more targeted and less toxic treatments, improving quality of life for patients. However, the research is still in early stages, and further studies are needed to confirm its efficacy and safety in humans.
The potential implications extend beyond AML. If successful, similar engineering strategies could be applied to other cancers where separating malignant cells from healthy tissue is challenging. The UNC team’s work underscores the promise of personalized medicine and immune-based therapies in oncology.
For more information, refer to the full study in Blood and updates from the University of North Carolina.
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