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A new era of cancer immunotherapy has begun. Chimeric antigen receptor T (CAR-T) cells, which have been genetically engineered to recognize the CD-19 antigen of B cells, have been successfully treated in various clinical trials for relapsed and refractory B cell malignancies. However, this treatment has several disadvantages. Side effects such as cytokine toxicity, tumor lysis syndrome, effects on healthy tissues, B cell hypoplasia, and genotoxicity can be fatal.
To avoid these drawbacks, CAR technology is being applied to other immune cells, such as natural killer (NK) cells. Unlike T cells, NK cells can be more easily fine-tuned to prevent treatment-related toxicity and immune-mediated adverse events. NK cells have great clinical significance because they contribute to graft-vs-leukemia / graft-vs-tumor effect but are not responsible for graft-vs-host disease. NK cells can be generated from various sources, such as cord blood, bone marrow, human embryonic stem cells, and induced pluripotent stem cells.
Primary NK cells engineered to express CAR have potential advantages over CAR-T cells.
Therefore, NK cell lines are attractive for CAR cell therapy.
As the leading cell therapeutics biotech that provides cell therapy related services, Creative Biolabs masters the most advanced CAR technology. With state-of-art CAR development platforms and advanced technologies, Creative Biolabs is capable of offering a broad range of CAR-NK early development services, including CAR engineered T cell biomarker identification and selection, design, construction, and analysis.
Creative Biolabs has also developed a series of novel platforms for enhanced CAR-NK Therapy. Please visit:
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