Cytotoxic Activity and Lymphocyte Subtypes in Mice Selected for Maximal and Minimal Inflammatory Response after Transplantation of B16F10 and S91 Melanoma Cells

Author:

Castoldi Lindsey1ORCID,Romagnoli Graziela Gorete23,de Assis Golim Marjorie4,Ribeiro Orlando Garcia5,Martinez Ibañez Olga Célia5,Maria Durvanei Augusto6,Pinto Domeneghini Andréa Vanessa7,Gameiro Maria Carolina2,Martins Priscila Raquel2,Mischan Martha Maria8,Kaneno Ramon2

Affiliation:

1. Health Sciences Institute, Federal University of Mato Grosso-UFMT, Sinop, Mato Grosso, Brazil

2. Department of Chemical and Biological Sciences, Institute of Bioscience of Botucatu, São Paulo State University-UNESP, Botucatu, São Paulo, Brazil

3. Department Health Science, Oeste Paulista University-UNOESTE, Jaú, São Paulo, Brazil

4. Hemocentro Division, School of Medicine of Botucatu, São Paulo State University-UNESP, Botucatu, São Paulo, Brazil

5. Laboratory of Immunogenetics, Institute Butantan, São Paulo, São Paulo, Brazil

6. Laboratory of Biochemistry and Biophysics, Institute Butantan, São Paulo, São Paulo, Brazil

7. Central Paulista University Center - UNICEP, São Carlos, São Paulo, Brazil

8. Department of Biostatistics, Institute of Bioscience of Botucatu, São Paulo State University-UNESP, Botucatu, São Paulo, Brazil

Abstract

AIRmax and AIRmin mice strains were selected according to the intensity of their acute inflammatory responsiveness. Previous studies have shown that AIR mice differ in their resistance to chemically induced skin tumors and in the development of melanoma metastases, in addition to differences in neutrophil and NK cells activity. In the present work, we aimed to evaluate whether the difference of susceptibility to murine melanoma is associated with NK cytotoxic activity against Yac.1 cells and lymphocyte subsets. Mice were subcutaneously inoculated with B16F10 or S91 melanoma cells. After 7, 14, or 30 days, the animals were euthanized to analyze the number of lymphocyte subsets, cytotoxic activity, and number of cytokine-producing spleen cells. AIRmax mice presented a higher number of CD4+/CD25+ cells than that of AIRmin mice following inoculation of B16F10 cells, whereas inoculation of S91 cells reduced CD4+/CD25+ and increased TCD8+ cell subsets in the AIRmax mice. AIRmax mice had a higher number of interleukin (IL)-10- and IL-12-producing cells and a lower number of interferon-γ–producing cells than those of AIRmin mice at 30 days. The cytotoxic activity of nonadherent spleen cells was similar in both the AIR strains. These results suggest that melanoma cells can induce different responses in AIR mice, possibly owing to alterations in regulatory mechanisms, such as the action of CD4+/CD25+ regulatory T cells and IL-10, in AIRmax mice.

Funder

Fundação de Amparo à Pesquisa do Estado de São Paulo

Publisher

Hindawi Limited

Subject

Immunology and Allergy

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