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Released By CCRM
September 1, 2019
Conventional cancer treatments (e.g. surgery, chemotherapy/radiation) do not specifically target cancer cells and, as a result, can cause extensive off-target damage, and complications for patients. In the last several years, ground-breaking research and advancements in genetic engineering have led to the development of a novel treatment strategy, known as immune therapy, that is rapidly emerging as an alternative to conventional cancer treatments. By re-deploying the body’s own immune cells to target and kill cancer cells, immune therapy provides a more targeted method to treat cancer. The most advanced development in cellular immunotherapy for cancer has been bioengineered T-cells, modified to express a special surface receptor called a chimeric antigen receptor (CAR). CARs target unique receptors on specific cancer cells, allowing CAR-Ts to selectively recognize, bind, and kill cancer cells in vivo by initiating the body’s natural immune response. CAR-Ts have made the most impact in the treatment of leukemias and lymphomas. To date, this has led to the approval of two commercial CAR-T cell therapies targeting these indications: Yescarta® (Kite Pharma) and Kymriah® (Novartis). Both therapies are approved for the treatment of B-cell lymphoma, and work by targeting the CD19 surface antigen. CD19-targeted CAR-Ts have demonstrated great efficacy in the lab and in the clinic. The CD19 receptor is found on all B-cells and is not specific to cancerous cells. However, patients can survive without B-cells, and therefore the lack of specificity has not hampered the use of CAR-Ts in the treatment of B-cell lymphoma. The next challenge is to find ways to use CAR-Ts for indications with more complex targets, where specificity is crucial. Improved targeting of CAR-Ts is important because the receptors on most types of cancer cells are also expressed on many healthy cell types, making the identification of a cancer-cell-specific target challenging. Current efforts in the field are focused on developing more sophisticated approaches to define cancer cell targets. For example, some approaches are using multiple antigen targeting strategies, while others are combining CAR-Ts with other drugs or biologics, such as checkpoint inhibitors. Many groups developing the next generation of CAR-Ts are focused on engineering new safety mechanisms to prevent the immune system from kicking into overdrive in response to the introduction of CAR-Ts. Commonly referred to as a cytokine storm, the severe and potentially life-threatening immune response experienced by some patients treated with CAR-Ts is one of the biggest safety concerns associated with this treatment. Current research aims to engineer tools that will allow for more fine-turned control over modified T-cells in vivo. For instance, bioengineered cells that can be controlled with suicide switches, are one approach to this challenge. Effective use of these novel enhancements will aim to address some of the clinical challenges associated with these therapies and allow the power of CAR-T to be harnessed to treat a wider array of cancers more safely and effectively. Despite success in the clinic, the adoption of CAR-Ts will face many hurdles due to a high price tag. For example, Kymriah was initially priced at USD$475,000 for a single-dose. Cost Drivers for CAR-T Therapies
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