Persistent Expression Of The Full Genome Of Hepatitis C Virus In B Cells Induces Spontaneous Development Of B-Cell Lymphomas In Vivo

Kohara Kyoko,Kasama Yuri,Sekiguchi Satoshi,Saito Makoto, Tanaka Kohsuke, Satoh Masaaki, Kuwahara Kazuhiko,Sakaguchi Nobuo,Takeya Motohiro,Hiasa Yoichi,Kohara Michinori,Tsukiyamakohara Kyoko, キョウコ コハラ,ユリ カサマ,サトシ セキグチ,マコト サイトウ, コウスケ タナカ, マサアキ サトウ,カズヒコ クワハラ,ノブオ サカグチ,モトヒロ タケヤ, ヨウイチ ヒアサ,ミチノリ コハラ, 恭子 小原, 由里 笠間, 敏 関口,誠 齊藤,康介 田中,正明 佐藤, 一彦 桑原, 薫雄 阪口,元裕 竹屋,陽一 日浅, 道法 小原

BLOOD(2010)

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摘要
Extrahepatic manifestations of hepatitis C virus (HCV) infection occur in 40%-70% of HCV-infected patients. B-cell non-Hodgkin lymphoma is a typical extrahepatic manifestation frequently associated with HCV infection. The mechanism by which HCV infection of B cells leads to lymphoma remains unclear. Here we established HCV transgenic mice that express the full HCV genome in B cells (RzCD19Cre mice) and observed a 25.0% incidence of diffuse large B-cell non-Hodgkin lymphomas (22.2% in males and 29.6% in females) within 600 days after birth. Expression levels of aspartate aminotransferase and alanine aminotransferase, as well as 32 different cytokines, chemokines and growth factors, were examined. The incidence of B-cell lymphoma was significantly correlated with only the level of soluble interleukin-2 receptor alpha subunit (sIL-2R alpha) in RzCD19Cre mouse serum. All RzCD19Cre mice with substantially elevated serum sIL-2R alpha levels (> 1000 pg/mL) developed B-cell lymphomas. Moreover, compared with tissues from control animals, the B-cell lymphoma tissues of RzCD19Cre mice expressed significantly higher levels of IL-2R alpha. We show that the expression of HCV in B cells promotes non-Hodgkin-type diffuse B-cell lymphoma, and therefore, the RzCD19Cre mouse is a powerful model to study the mechanisms related to the development of HCV-associated B-cell lymphoma. (Blood. 2010;116(23):4926-4933)
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immunohistochemistry
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