In vivo distribution of receptor for ecotropic murine leukemia virus and binding of envelope protein of Friend Murine leukemia virus

被引:0
|
作者
S. Yamaguchi
M. Hasegawa
T. Suzuki
H. Ikeda
S. Aizawa
K. Hirokawa
M. Kitagawa
机构
[1] Department of Pathology and Immunology,
[2] Aging and Developmental Sciences,undefined
[3] Tokyo Medical and Dental University,undefined
[4] Graduate School,undefined
[5] Tokyo,undefined
[6] Japan,undefined
[7] Radiation Hazards Research Group,undefined
[8] National Institute of Radiological Sciences,undefined
[9] Chiba,undefined
[10] Japan,undefined
[11] Laboratory of Immunogenetics,undefined
[12] National Institute of Animal Health,undefined
[13] Tsukuba,undefined
[14] Ibaraki,undefined
[15] Japan,undefined
[16] Laboratory of Infectious Diseases,undefined
[17] National Institute of Animal Health,undefined
[18] Tsukuba,undefined
[19] Ibaraki,undefined
[20] Japan,undefined
来源
Archives of Virology | 2003年 / 148卷
关键词
mRNA Expression; Green Fluorescence Protein; Binding Assay; Interference Effect; Envelope Protein;
D O I
暂无
中图分类号
学科分类号
摘要
 Ecotropic infection by Murine leukemia virus (MuLV) infection is initiated by the interaction between the receptor-binding domain of the viral surface glycoprotein (SU) and the cell-surface receptor, mCAT-1. To study the in vivo localization of viral binding site in mice, green fluorescence protein (GFP)-tagged Friend SU (F-SU/GFP) was incubated with tissue sections. Lymphohematopoietic organs and a part of the glandular tissues of C3H as well as C57BL/6 mice revealed positive signals for F-SU/GFP binding on the cell surface. In contrast, C4W mice, which is a partial congenic mouse strain carrying the Fv-4r gene on a BALB/c genetic background, exhibited negative signals in most of the organs except for a very weak binding in the pancreas. The expression of mCAT-1 mRNA determined by reverse transcriptase (RT)-polymerase chain reaction (PCR) revealed a similar distribution in C3H, C57BL/6 and C4W mice. Most of the organs including lymphohematopoietic organs and glandular organs revealed significant expression of mRNA for mCAT-1 gene, while the liver, heart and muscle did not. The results from binding assay were consistent with the fact that Friend MuLV-induced pathogenesis was usually associated with lymphohematopoietic systems, although mRNA expression for mCAT-1 was rather ubiquitous. The discrepancy between F-SU/GFP binding and mRNA expression for mCAT-1 in lymphohematopoietic organs of C4W mice would support the receptor interference effect by the Fv-4r gene causing the resistance of C4W mouse to Friend MuLV infection.
引用
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页码:1175 / 1184
页数:9
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