Variability in CRP, regulatory T cells and effector T cells over time in gynaecological cancer patients: a study of potential oscillatory behaviour and correlations
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Titre | Variability in CRP, regulatory T cells and effector T cells over time in gynaecological cancer patients: a study of potential oscillatory behaviour and correlations |
Type de publication | Journal Article |
Year of Publication | 2014 |
Auteurs | Madondo MT, Tuyaerts S, Turnbull BB, Vanderstraeten A, Kohrt H, Narasimhan B, Amant F, Quinn M, Plebanski M |
Journal | JOURNAL OF TRANSLATIONAL MEDICINE |
Volume | 12 |
Pagination | 179 |
Date Published | JUN 23 |
Type of Article | Article |
ISSN | 1479-5876 |
Mots-clés | CRP, Gynaecological malignancies, inflammation, Teff, Treg |
Résumé | Background: The inflammatory marker, C reactive protein has been proposed to also be a biomarker for adaptive immune responses in cancer patients with a possible application in time based chemotherapy. Fluxes in serum CRP levels were suggested to be indicative of a cyclical process in which, immune activation is followed by auto- regulating immune suppression. The applicability of CRP as a biomarker for regulatory or effector T cells was therefore investigated in a cohort of patients with gynaecological malignancies. Methods: Peripheral blood samples were obtained from a cohort of patients at 7 time points over a period of 12 days. Serum and mononuclear cells were isolated and CRP levels in serum were detected using ELISA while regulatory and effector T cell frequencies were assessed using flow cytometry. To test periodicity, periodogram analysis of data was employed while Pearson correlation and the Wilcoxon signed rank test were used to determine correlations. Results: The statistical analysis used showed no evidence of periodic oscillation in either serum CRP concentrations or T-eff and T-reg frequencies. Furthermore, there was no apparent correlation between serum CRP concentrations and the corresponding frequencies of T-regs or T-effs. Relative to healthy individuals, the disease state in the patients neither significantly affected the mean frequency of Tregs nor the mean coefficient of variation within the T-reg population over time. However, both T-eff mean frequency and mean coefficient of variation were significantly reduced in patients. Conclusion: Using our methods we were unable to detect CRP oscillations that could be used as a consistent serial biomarker for time based chemotherapy. |
DOI | 10.1186/1479-5876-12-179 |