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MOLECULAR SWITCH-MEDIATED CONTROL OF ENGINEERED CELLS

机译:分子开关介导的工程细胞控制

摘要

The present disclosure relates to therapeutic methods and clinically useful molecular switches, for which activity or degradation of a switch-presenting polypeptide can be precisely induced via administration or withdrawal of an FDA-approved drug. Certain aspects of the disclosure relate to an engineered drug-inducible heterodimeric system including a first polypeptide presenting a CRBN polypeptide disrupted for or lacking a DDB1-interacting domain and a second polypeptide presenting a CRBN polypeptide substrate, where binding between the CRBN polypeptide and the CRBN polypeptide substrate are inducible via administration of an FDA-approved thalidomide analog immunomodulatory drug (IMiD). Another aspect of the disclosure relates to a chimeric antigen receptor (CAR) that presents a minimal fragment of the CRBN polypeptide substrate IKZF3 capable of triggering proteasomal degradation of CAR upon administration of an FDA-approved IMiD.
机译:本公开涉及治疗方法和临床上有用的分子开关,其可通过给予或撤回FDA批准的药物精确地诱导开关呈递多肽的活性或降解。 本公开的某些方面涉及一种工程化药物可诱导的异二聚体系,包括呈现用于破坏或缺乏DDB1相互作用结构域的CRBN多肽的第一多肽和呈现CRBN多肽基质的第二多肽,其中CRBN多肽与CRBN之间的结合 通过给予FDA批准的沙利度胺模拟免疫调节药物(IMID)诱导多肽底物。 本公开的另一方面涉及一种嵌合抗原受体(轿车),其呈现CRBN多肽底物IKZF3的最小片段,其能够在施用FDA批准的IMID时触发汽车的蛋白酶体降解。

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