METHODS FOR ENGINEERING HIGHLY ACTIVE T CELL FOR IMMUNOTHERAPHY
    22.
    发明申请
    METHODS FOR ENGINEERING HIGHLY ACTIVE T CELL FOR IMMUNOTHERAPHY 审中-公开
    用于工作用于免疫印迹的高活性T细胞的方法

    公开(公告)号:US20160120906A1

    公开(公告)日:2016-05-05

    申请号:US14894426

    申请日:2014-05-13

    Applicant: CELLECTIS

    Abstract: The present invention relates to methods for developing engineered T-cells for immunotherapy and more specifically to methods for modifying T-cells by inactivating at immune checkpoint genes, preferably at least two selected from different pathways, to increase T-cell immune activity. This method involves the use of specific rare cutting endonucleases, in particular TALE-nucleases (TAL effector endonuclease) and polynucleotides encoding such polypeptides, to precisely target a selection of key genes in T-cells, which are available from donors or from culture of primary cells. The invention opens the way to highly efficient adoptive immunotherapy strategies for treating cancer and viral infections.

    Abstract translation: 本发明涉及用于发展用于免疫治疗的工程化T细胞的方法,更具体地涉及通过在免疫检查点基因(优选至少两个选自不同途径)中灭活来增加T细胞免疫活性来修饰T细胞的方法。 该方法包括使用特定的稀有切割内切核酸酶,特别是TALE-核酸酶(TAL效应子内切核酸酶)和编码这种多肽的多核苷酸,以精确地靶向T细胞中的关键基因的选择,其可从供体或从原代培养获得 细胞。 本发明开辟了一种治疗癌症和病毒感染的高效过继免疫治疗策略。

    CD19 SPECIFIC CHIMERIC ANTIGEN RECEPTOR AND USES THEREOF

    公开(公告)号:US20210060079A1

    公开(公告)日:2021-03-04

    申请号:US17099608

    申请日:2020-11-16

    Applicant: Cellectis

    Abstract: The present invention relates to chimeric antigen receptors (CAR). CARs are able to redirect immune cell specificity and reactivity toward a selected target exploiting the ligand-binding domain properties. In particular, the present invention relates to a Chimeric Antigen Receptor in which extracellular ligand binding is a scFV derived from a CD19 monoclonal antibody, preferably 4G7. The present invention also relates to polynucleotides, vectors encoding said CAR and isolated cells expressing said CAR at their surface. The present invention also relates to methods for engineering immune cells expressing 4G7-CAR at their surface which confers a prolonged “activated” state on the transduced cell. The present invention is particularly useful for the treatment of B-cells lymphomas and leukemia.

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