The expression of bitter taste receptor TAS2R38 in patients with chronic rhinosinusitis

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作者
Karolina Zborowska-Piskadło
Małgorzata Stachowiak
Natalia Rusetska
Elżbieta Sarnowska
Janusz Siedlecki
Karolina Dżaman
机构
[1] Miedzyleski Hospital,Department of Otolaryngology
[2] Maria Sklodowska-Curie Institute-Oncology Center,Department of Molecular and Translational Oncology
[3] Centre of Postgraduate Medical Education,Department of Otolaryngology
来源
Archivum Immunologiae et Therapiae Experimentalis | 2020年 / 68卷
关键词
TAS2R38; Chronic rhinosinusitis; Bitter taste receptor;
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摘要
Chronic rhinosinusitis (CRS) is a frequent disease with high social impact and multifactorial pathogenesis. Recently, the bitter taste receptor TAS2R38 has been described to play a role in upper airway innate mucosal defense. The aim was to determine the localization and expression of the TAS2R38 in the selected cell lines and tissue collected from patient suffered from CRS as well as to correlate the results with clinical data. Moreover, the purpose was the estimation of the TAS2R38 distribution changes during acute and CRS. Forty-two patients undergoing nasal surgery were enrolled in the study. The TAS2R38 expression was assessed in the collected tissues using immunohistochemistry and immunocytochemistry methods. The western blot analysis was performed on human cell lines HeLa, MCF7, MDA-MB-231 to assess the location of the TAS2R38 protein. Moreover, the HeLa cell line was used as a model of acute inflammation induces by lipopolysaccharide. Immunohistochemistry analysis displayed a statistically significant difference of TAS2R38 level in the patients with CRS compared to healthy control and was different in CRS with and without nasal polyps. The results showed the abundance of TAS2R38 receptor in the cell nucleus in patients with CRS and cell lines. The variance in TAS2R38 receptor expression in two CRS types suggests their different pathogenesis. The first time in literature, we confirmed the presence of plasma membrane TAS2R38 receptor in the cell nuclei in CRS as well as in cell lines, what strongly suggests the different than membrane TAS2R38 function.
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