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胸腺树突状细胞是致癌病毒SL3-3的主要靶标。

Thymic dendritic cells are primary targets for the oncogenic virus SL3-3.

作者信息

Uittenbogaart C H, Law W, Leenen P J, Bristol G, van Ewijk W, Hays E F

机构信息

Departments of Pediatrics, UCLA School of Medicine, Los Angeles, California, USA.

出版信息

J Virol. 1998 Dec;72(12):10118-25. doi: 10.1128/JVI.72.12.10118-10125.1998.

Abstract

The murine retrovirus SL3-3 causes malignant transformation of thymocytes and thymic lymphoma in mice of the AKR and NFS strains when they are inoculated neonatally. The objective of the present study was to identify the primary target cells for the virus in the thymuses of these mice. Immunohistochemical studies of the thymus after neonatal inoculation of the SL3-3 virus showed that cells expressing the viral envelope glycoprotein (gp70(+) cells) were first seen at 2 weeks of age. These virus-expressing cells were found in the cortex and at the corticomedullary junction in both mouse strains. The gp70(+) cells had the morphology and immunophenotype of dendritic cells. They lacked macrophage-specific antigens. Cell separation studies showed that bright gp70(+) cells were detected in a fraction enriched for dendritic cells. At 3 weeks of age, macrophages also expressed gp70. At that time, both gp70(+) dendritic cells and macrophages were found at the corticomedullary junction and in foci in the thymic cortex. At no time during this 3-week period was the virus expressed in cortical and medullary epithelial cells or in thymic lymphoid cells. Infectious cell center assays indicated that cells expressing infectious virus were present in small numbers at 2 weeks after inoculation but increased at 5 weeks of age by several orders of magnitude, indicating virus spread to the thymic lymphoid cells. Thus, at 2 weeks after neonatal inoculation of SL3-3, thymic dendritic cells are the first cells to express the virus. At 3 weeks of age, macrophages also express the virus. In subsequent weeks, the virus spreads to the thymocytes. This pathway of virus expression in the thymus allows the inevitable provirus integration in a thymocyte that results in a clonal lymphoma.

摘要

鼠逆转录病毒SL3-3在新生时接种到AKR和NFS品系小鼠体内,可导致胸腺细胞恶性转化和胸腺淋巴瘤。本研究的目的是确定该病毒在这些小鼠胸腺中的主要靶细胞。对新生接种SL3-3病毒后的胸腺进行免疫组织化学研究表明,表达病毒包膜糖蛋白的细胞(gp70(+)细胞)在2周龄时首次出现。在两种小鼠品系的皮质和皮质髓质交界处均发现了这些表达病毒的细胞。gp70(+)细胞具有树突状细胞的形态和免疫表型。它们缺乏巨噬细胞特异性抗原。细胞分离研究表明,在富含树突状细胞的部分中检测到明亮的gp70(+)细胞。3周龄时,巨噬细胞也表达gp70。此时,gp70(+)树突状细胞和巨噬细胞均在皮质髓质交界处和胸腺皮质的病灶中被发现。在这3周期间,皮质和髓质上皮细胞或胸腺淋巴细胞中均未表达病毒。感染性细胞中心分析表明,接种后2周时存在少量表达感染性病毒的细胞,但在5周龄时增加了几个数量级,表明病毒已传播至胸腺淋巴细胞。因此,新生接种SL3-3后2周,胸腺树突状细胞是最早表达病毒的细胞。3周龄时,巨噬细胞也表达病毒。在随后的几周内,病毒传播至胸腺细胞。胸腺中这种病毒表达途径使得前病毒不可避免地整合到胸腺细胞中,从而导致克隆性淋巴瘤。

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Dendritic cells and the replication of HIV-1.树突状细胞与HIV-1的复制
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The thymic microenvironment.胸腺微环境。
Immunol Today. 1993 Sep;14(9):445-59. doi: 10.1016/0167-5699(93)90248-J.

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