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2B4 (CD244, SLAMF4) and CS1 (CD319, SLAMF7) in systemic lupus erythematosus and cancer

机译:2B4(CD244,SLAMF4)和CS1(CD319,SLAMF7)在Systemic Lupus红斑狼疮和癌症

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摘要

Signaling Lymphocyte Activation Molecule (SLAM) family receptors are expressed on different types of hematopoietic cells and play important role in immune regulation in health and disease. 2B4 (CD244, SLAMF4) and CS1 (CD319, CRACC, SLAMF7) were originally identified as NK cell receptors regulating NK cell cytolytic activity. 2B4 is expressed on all NK cells, a subpopulation of T cells, monocytes and basophils. Unlike other activating and inhibitory receptors, 2B4 (CD244) interaction with its ligand CD48 has been shown to mediate both activating and inhibitory functions. Defective signaling via 2B4 due to mutations in signaling adaptor SAP contributes to X-linked lymphoproliferative Disease (XLP). Expression of 2B4 and CS1 are altered in systemic lupus erythematosus (SLE). CS1 is overexpressed in multiple myeloma (MM) and anti-CS1 mab (Elotuzumab/Empliciti) has been approved by FDA as a breakthrough drug for treatment for MM patients. CAR -T cells or CAR -NK cells containing full length CS1 or the signaling domain of 2B4 with TCR-zeta have shown promising results to treat cancer and autoimmune diseases.
机译:信号传导淋巴细胞活化分子(SLAM)家庭受体在不同类型的造血细胞上表达,并在健康和疾病中的免疫调节中起着重要作用。最初将2B4(CD244,Slamf4)和CS1(CD319,CRACC,SLAMF7)鉴定为调节NK细胞细胞溶解活性的NK细胞受体。在所有NK细胞上表达2B4,T细胞,单核细胞和嗜碱性粒细胞的亚群。与其他活化和抑制剂受体不同,已显示与其配体CD48的2B4(CD244)相互作用,用于介导活化和抑制功能。由于信号衔接子SAP中的突变导致的通过2b4有缺陷的信号传导,有助于X链淋巴升降疾病(XLP)。 2B4和CS1的表达在全身性狼疮红斑(SLE)中改变。 CS1在多种骨髓瘤(mm)中过表达,并且通过FDA批准了抗CS1 mAb(Elotuzumab / Emplicti)作为MM患者治疗的突破性药物。含有全长CS1的CAR-T细胞或CARNK细胞或具有TCR-ZETA的2B4的信号结构域已经显示出对治疗癌症和自身免疫疾病的有希望的结果。

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