Abstract
BackgroundStudies elucidated that Th17 cells are important contributors to the pathogenesis of many immune-mediated diseases, and IL-17A is present in pathologic intervertebral disc (IVD) tissues. However, the mechanisms, how these cells traffic into the degenerate discs are not clear.Materials and MethodsThe samples collected from 53 patients had been divided into 3 groups: Group P (annulus fibrosus was intact), Group E (annulus fibrosus was reptured) and normal control. Immunohistochemistry was used to detect the expression of CCL20, CCR6, IL-17A, TNF–α and CD4 in IVD tissues. Moreover, nucleus pulposus (NP) cells had been cultured in the presence and absence of Th17 associated cytokines. The supernatants were detected for CCL20 concentrations by ELISA, and the NP cells for the expression of CCL20 mRNA. Additionally, peripheral blood (PB) samples had undergone detection for the expression of CCR6 mRNA and the proportion of IL-17-producing cells, including the surface expression of CCR6.ResultsImmunohistochemistry revealed that CCL20 and TNF-α were expressed in degenerated NP cells. Double-labeled immunofluorescence elaborated, IL-17-producing cells (CD4+IL-17A+ and CD4+CCR6+) appeared in the Group E samples, but no traces or expression in Group P and normal control. IL-17A and TNF-α, alone or combined, could enhance CCL20 secretion in a dose-dependent manner, which was obtained through RT-PCR results. There was a notable difference of CCR6 mRNA expression between patients and normal controls. In comparison to controls, flow cytometry data indicated that the proportion of IL-17-producing cells and the CCR6 expression in PB were significantly increased.ConclusionOur results provide a potential explanation for involvement of the CCL20-CCR6 system in the trafficking of IL-17-producing cells to degenerated IVD tissues. Additionally, our results explain the contribution of Th17 associated cytokines to the development of degenerated discs via the up-regulation of CCL20 secretion from NP cells, which forms a positive chemotactic feedback loop.
Highlights
Disc herniation is currently well established as an immunemediated inflammatory process
Immunohistochemistry revealed that CCL20 and TNF-a were expressed in degenerated nucleus pulposus (NP) cells
IL-17A and TNF-a, alone or combined, could enhance CCL20 secretion in a dose-dependent manner, which was obtained through RT-PCR results
Summary
Disc herniation is currently well established as an immunemediated inflammatory process. Numerous studies in human and mice have suggested that Th17 cells play a leading role in the pathogenesis of many different immune-mediated diseases, including rheumatoid arthritis [10,11], psoriasis [12,13], asthma [14,15] and inflammatory bowel disease [16,17]. The cells from those lesions, including synoviocytes, keratinocytes, bronchial epithelial cells and colon epithelial cells, can produce abundant amounts of CCL20, a specific ligand for CCR6. The mechanisms, how these cells traffic into the degenerate discs are not clear
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