The antimetastatic effect of a single low dose of cyclophosphamide involves modulation of galectin-1 and Bcl-2 expression

被引:0
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作者
Gabriel A. Rabinovich
Natalia Rubinstein
Pablo Matar
Viviana Rozados
Silvia Gervasoni
Graciela O. Scharovsky
机构
[1] Laboratorio de Inmunogenética,
[2] Hospital de Clínicas "José de San Martín",undefined
[3] Facultad de Medicina,undefined
[4] Universidad de Buenos Aires,undefined
[5] Buenos Aires,undefined
[6] Argentina,undefined
[7] Instituto de Genética Experimental,undefined
[8] Facultad de Ciencias Médicas,undefined
[9] Universidad Nacional de Rosario,undefined
[10] Santa Fe 3100,undefined
[11] (2000) Rosario,undefined
[12] Argentina,undefined
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关键词
Galectin-1 Bcl-2 Low-dose cyclophosphamide Lymphoma Metastasis;
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摘要
We have demonstrated that a single low dose of cyclophosphamide has an antimetastatic effect on lymphoma (L-TACB)-bearing rats by modulating the host immune response. Galectin-1, a member of the galectin family with specificity for β-galactosides, has potent immunomodulatory properties by regulating cell-matrix interactions and T-cell apoptosis. Since galectin-1 is expressed by highly metastatic tumors, in the present study we investigated the participation of this β-galactoside-binding protein in cyclophosphamide-induced immunomodulation. Inbred "e" rats were s.c. challenged with L-TACB. After 14 days, half of the animals received an i.p. injection of cyclophosphamide (10 mg/kg), and on day 21 tumors and spleens were excised. Cell extracts were prepared and galectin-1 expression was determined by Western blot analysis and correlated with Bcl-2 expression levels and the DNA fragmentation profile. Expression of galectin-1 was significantly decreased in tumors from cyclophosphamide-treated rats compared to non-treated rats. The same effect was observed regarding expression of Bcl-2 by tumors. In contrast, expression of Bcl-2 was significantly higher in spleens from treated animals than in non-treated rats. This effect correlated with a decreased intensity in the pattern of DNA fragmentation of spleen cells from cyclophosphamide-treated animals. Our results suggest that a single low dose of cyclophosphamide modulates the expression of galectin-1 and Bcl-2 by tumors, which could in turn influence the apoptotic threshold of spleen mononuclear cells. This mechanism could explain, at least in part, the antimetastatic effect evidenced in our tumor experimental model.
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页码:597 / 603
页数:6
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