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T细胞基因疗法根除乳腺癌传播

T Cell Gene Therapy to Eradicate Disseminated Breast Cancers
作者:Junghans, R. P. 作者单位:Army Medical Research and Materiel Command (Provisional), Fort Detrick, MD. 加工时间:2014-10-20 信息来源:科技报告(AD) 索取原文[52 页]
关键词:(生物学);乳腺癌;细胞临床医学;结肠癌
摘 要:There is no cure for metastatic breast cancer, which kills 40,000 American women (and 500 men) each year: all presently available treatments are palliative. Gene therapy techniques are used to introduce chimeric immunoglobulin-T cell receptors (IgTCR) into autologous patient T cells to create designer T cells that redirect the T cell immune system in a new type of immuno-gene therapy against breast cancer. Designer T cells have been created against the carcinoembryonic antigen (CEA) that is prominently present on many metastatic breast tumors (30-60). This exceeds the fraction that are Her2/neu overexpressing (20-25), making CEA an even better immune target for attacking breast cancer. Building on a prior study of CEA designer T cells in breast and colon cancer, 2nd generation designer T cells were created by incorporating into the IgTCR a CD28 co-stimulation cassette that was shown to oppose activation-induced cell death (AICD) of the T cells after tumor contact. This advanced generation modification leads to improved designer T cell survival and improved anti-tumor potency in preclinical models. Although the 2nd generation designer T cells produce interleukin 2 (IL2) growth factor on contact with tumor, interleukin 2 (IL2) supplementation is anticipated still to be required for optimal clinical therapeutic effect. However, the CBER/FDA has mandated a Phase I.
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