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Article type: Research Article
Authors: Blanco, B. | Ferrández, M.D. | Correa, R. | Del Rio, M. | Guaza, C. | Hernanz, A. | De la Fuente, M.;
Affiliations: Department of Animal Physiology, Faculty of Biology, Complutense University, Madrid, Spain | Cajal Institute, CSIC, Madrid, Spain | Biochemistry Service, Hospital La Paz, Madrid, Spain
Note: [] Address correspondence to: Mónica De la Fuente, Departamento de Fisiología Animal, Facultad de Ciencias Biológicas, Universidad Complutense de Madrid, 28040 Madrid, Spain.
Abstract: The administration of the thiol compounds, N‐acetylcysteine (NAC) and in particular thioproline (thiazolidine‐4‐carboxylic acid) at 0.1% w/w concentration in the diet, improves lymphocyte functions in old female Swiss mice, as has been shown in our previous studies. In the present work, adult mice from two different strains, namely BALB/c (an inbred strain) and OF1‐Swiss (noninbred strain), were fed a diet supplemented with the above dose of each thiol compound jointly for five weeks. At 28 weeks of age, peritoneal cell suspensions were obtained and different steps of the phagocytic process, the most representative activity of macrophages, as well as interleukin‐1\beta (IL‐1\beta) production, were studied. Thus, adherence to substrate, mobility directed to a chemoattractant gradient (chemotaxis), ingestion of inert particles and superoxide anion production were analysed. The results show that diet supplementation with NAC plus thioproline increased all macrophage functions studied with the exception of superoxide anion production, which was decreased. These effects were more evident in macrophages from Swiss mice, whereas in BALB/c mice the stimulation of phagocytosis and IL‐1\beta production was lower and no differences were seen after treatment in adherence and superoxide anion production. These data suggest that immune function can be improved in adult mice by administration of the above thiol compounds, especially in the noninbred strain of OF1‐Swiss mice.
Keywords: Thioproline, N‐acetylcysteine, macrophages, phagocytic function, interleukin‐1[TeX:] \beta
Journal: Biofactors, vol. 10, no. 2-3, pp. 179-185, 1999
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