首页> 美国卫生研究院文献>Immunology >CD44 isoforms containing exons V6 and V7 are differentially expressed on mitogenically stimulated normal and Epstein-Barr virus-transformed human B cells.
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CD44 isoforms containing exons V6 and V7 are differentially expressed on mitogenically stimulated normal and Epstein-Barr virus-transformed human B cells.

机译:含有外显子V6和V7的CD44亚型在有丝分裂刺激的正常人和爱泼斯坦-巴尔病毒转化的人B细胞上差异表达。

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摘要

CD44, a cell adhesion molecule, exists in multiple isoforms that are generated by RNA alternative splicing. CD44 isoforms containing exon V6 (CD44 V6) have been associated with tumorigenesis and metastasis. We investigated the association between human B-cell activation and CD44 V6 isoform expression by analysing its expression in resting and mitogenically stimulated B cells. Results showed that resting B cells expressed the CD44 H (no variable exon) isoform alone. Activation of B cells [phorbol myristate acetate (PMA), surface immunoglobulin cross-linking alone or in the presence of interleukin-2 (IL-2)] induced CD44E (variable exon V8-10), R2 (VIO) and CD44 isoforms containing exons V6 and/or V7 (CD44 V6/V7). Epstein-Barr virus (EBV) infection of B cells, an alternative method of B-cell activation, induced the expression of CD44 E and R2 but not CD44 V6/V7. These results indicate that CD44 V6/V7 expression depends on the mode of activation. CD44 isoform expression was also investigated in a panel of EBV-negative and EBV-positive Burkitt's lymphoma (BL) B-cell lines. EBV-negative BL cells did not express CD44. In contrast, EBV-positive BL cells expressed CD44 H, R2 and E but not CD44 V6/V7 isoforms, suggesting an association between EBV infection and CD44 isoform induction. To determine directly the role of EBV in CD44 isoform induction, an EBV-negative BL cell line, BL30 (negative for all isoforms of CD44), BL30 infected in vitro with the EBNA-2-defective P3HR1 (BL30/P3HR1), and the wild-type B95-8 strain of EBV (BL30/B95-8) were examined. The parental BL30 cells infected with the wild-type EBV strain, but not with the P3HR-1 strain, expressed CD44 H, R2 and E isoforms, as seen in EBV-immortalized B cells. These studies suggest that (1) alternative splicing of CD44 isoforms is differentially regulated depending on the mode and state of cell activation, and that (2) the CD44 V6/V7 isoforms may represent B-cell activation antigens that are induced by mitogenic stimulation but not following EBV infection.
机译:CD44是一种细胞粘附分子,以多种RNA异构体剪接形式存在。含有外显子V6(CD44 V6)的CD44亚型与肿瘤发生和转移有关。我们通过分析静息和有丝分裂刺激的B细胞中的表达来研究人B细胞活化与CD44 V6亚型表达之间的关联。结果显示,静止的B细胞仅表达CD44 H(无外显子)亚型。 B细胞的激活[佛波醇肉豆蔻酸乙酸酯(PMA),表面免疫球蛋白单独交联或在白介素2(IL-2)存在下]诱导CD44E(可变外显子V8-10),R2(VIO)和CD44亚型外显子V6和/或V7(CD44 V6 / V7)。 B细胞的另一种感染方法是B细胞的爱泼斯坦巴尔病毒(EBV)感染,诱导CD44 E和R2的表达,而不诱导CD44 V6 / V7的表达。这些结果表明CD44 V6 / V7表达取决于激活方式。还在一组EBV阴性和EBV阳性的伯基特淋巴瘤(BL)B细胞系中研究了CD44亚型的表达。 EBV阴性BL细胞不表达CD44。相反,EBV阳性BL细胞表达CD44 H,R2和E,但不表达CD44 V6 / V7亚型,提示EBV感染与CD44亚型诱导之间存在关联。为了直接确定EBV在CD44亚型诱导中的作用,需要使用EBNA-2缺陷型P3HR1(BL30 / P3HR1)体外感染的EBV阴性BL细胞系BL30(对于CD44的所有亚型均为阴性),BL30。检查了野生型EBV B95-8株(BL30 / B95-8)。如在EBV永生化B细胞中所见,用野生型EBV株感染但未感染P3HR-1株的亲本BL30细胞表达CD44 H,R2和E同工型。这些研究表明(1)CD44亚型的可变剪接取决于细胞激活的方式和状态,并且(2)CD44 V6 / V7亚型可能代表有丝分裂刺激诱导的B细胞激活抗原,但不跟随EBV感染。

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