首页> 美国卫生研究院文献>Advances in Virology >Epstein-Barr Virus- (EBV-) Immortalized Lymphoblastoid Cell Lines (LCLs) Express High Level of CD23 but Low CD27 to Support Their Growth
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Epstein-Barr Virus- (EBV-) Immortalized Lymphoblastoid Cell Lines (LCLs) Express High Level of CD23 but Low CD27 to Support Their Growth

机译:EB病毒永生化的淋巴母细胞样细胞系(LCL)表达高水平的CD23但低CD27来支持其生长

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摘要

Epstein-Barr virus (EBV) is one of the common human herpesvirus types in the world. EBV is known to infect more than 95% of adults in the world. The virus mainly infects B lymphocytes and could immortalize and transform the cells into EBV-bearing lymphoblastoid cell lines (LCLs). Limited studies have been focused on characterizing the surface marker expression of the immortalized LCLs. This study demonstrates the generation of 15 LCLs from sixteen rheumatoid arthritis (RA) patients and a healthy volunteer using B95-8 marmoset-derived EBV. The success rate of LCL generation was 88.23%. All CD19+ LCLs expressed CD23 (16.94-58.9%) and CD27 (15.74-80.89%) on cell surface. Our data demonstrated two distinct categories of LCLs (fast- and slow-growing) (p<0.05) based on their doubling time. The slow-growing LCLs showed lower CD23 level (35.28%) compared to fast-growing LCLs (42.39%). In contrast, the slow-growing LCLs showed higher percentage in both CD27 alone and CD23+CD27+ in combination. Overall, these findings may suggest the correlations of cellular CD23 and CD27 expression with the proliferation rate of the generated LCLs. Increase expression of CD23 may play a role in EBV immortalization of B-cells and the growth and maintenance of the EBV-transformed LCLs while CD27 expression might have inhibitory effects on LCL proliferation. Further investigations are warranted to these speculations.
机译:爱泼斯坦-巴尔病毒(EBV)是世界上常见的人类疱疹病毒类型之一。众所周知,EBV感染了全世界95%以上的成年人。该病毒主要感染B淋巴细胞,并且可以永生并转化为带有EBV的淋巴母细胞样细胞系(LCL)。有限的研究集中于表征永生化的LCL的表面标志物表达。这项研究表明,使用B95-8 mo猴衍生的EBV,可从16名类风湿性关节炎(RA)患者和一名健康志愿者中产生15条LCL。拼箱拼箱的成功率为88.23%。所有CD19 + LCL在细胞表面表达CD23(16.94-58.9%)和CD27(15.74-80.89%)。我们的数据基于其倍增时间展示了LCL的两个不同类别(快速增长和缓慢增长)(p <0.05)。与快速增长的LCL(42.39%)相比,缓慢增长的LCL显示较低的CD23水平(35.28%)。相反,缓慢增长的LCL在单独的CD27和组合的CD23 + CD27 +中均显示较高的百分比。总体而言,这些发现可能表明细胞CD23和CD27表达与所产生LCL的增殖速率之间的相关性。 CD23的表达增加可能在B细胞的EBV永生化以及EBV转化LCL的生长和维持中起作用,而CD27的表达可能对LCL增殖具有抑制作用。这些推测值得进一步调查。

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