LMP1 and EBNA2 constitute a minimal set of EBV genes for transformation of human B cells

LMP1 和 EBNA2 构成了用于转化人类 B 细胞的最小 EBV 基因集

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作者：Jingwei Zhang, Thomas Sommermann, Xun Li, Lutz Gieselmann, Kathrin de la Rosa, Maria Stecklum, Florian Klein, Christine Kocks, Klaus Rajewsky

期刊：	Frontiers in Immunology	影响因子：	5.700
时间：	2023	起止号：	2023 Dec 19:14:1331730.
doi：	10.3389/fimmu.2023.1331730	种属：	Human
研究方向：	细胞生物学	细胞类型：	B细胞

Conclusion

Our results identify a minimal set of EBV proteins sufficient for B cell transformation.

Methods

Here, we addressed this question by transducing human peripheral B cells from EBV-negative donors with retrovirus expressing the latent EBV genes encoding Latent Membrane Protein (LMP) 1 and 2A and Epstein-Barr Nuclear Antigen (EBNA) 2.

Results

LMP1 together with EBNA2, but not LMP1 alone or in combination with LMP2A was able to transform human primary B cells. LMP1/EBNA2-immortalized cell lines shared surface markers with EBV-transformed lymphoblastoid cell lines (LCLs). They showed sustained growth for more than 60 days, albeit at a lower growth rate than EBV-transformed LCLs. LMP1/EBNA2-immortalized cell lines generated tumors when transplanted subcutaneously into severely immunodeficient NOG mice.

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