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味觉减退的长期新冠队列中唾液味觉素和磷蛋白减少。

Reduced Salivary Gustin and Statherin in Long-COVID Cohort with Impaired Bitter Taste.

作者信息

Chowdary Harika, Riley Naomi, Patel Parul, Gossweiler Ana G, Running Cordelia A, Srinivasan Mythily

机构信息

Oral Pathology, Medicine and Radiology, Indiana University School of Dentistry, Indianapolis, IN 46202, USA.

Oral Health Research Institute, Indiana University School of Dentistry, Indianapolis, IN 46203, USA.

出版信息

J Clin Med. 2024 Nov 13;13(22):6816. doi: 10.3390/jcm13226816.

Abstract

: Taste dysfunction is a frequent symptom of acute coronavirus disease (COVID)-19 caused by the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2). While the majority of those affected reported recovery over time, emerging data suggest that 20-25% of individuals experience persistent taste dysfunction, constituting a common symptom of long COVID. Gustation is mediated by continuously renewing taste bud cells. A balance between the counteracting processes of cell generation and cell death maintains the homeostatic turnover. Sonic hedgehog (SHH) is a morphogenic protein that promotes taste cell proliferation and differentiation. Enzymatic proteins such as gustin modulate the environment around the taste receptors and influence taste perception. Hence, we hypothesized that increased taste cell turnover and reduced taste-related salivary proteins contribute to the taste dysfunction in long COVID. : Unstimulated whole saliva (UWS) was collected from individuals with long COVID experiencing taste dysfunction after obtaining informed consent. The normal control included archived saliva samples catalogued prior to 2019. Taste perception was objectively determined by the waterless empirical taste test. The SHH, gustin, and inflammatory cytokines in UWS were determined with ELISA. The expressions of epithelial and taste-cell-specific markers in cellular saliva were assessed by immunoflurorescence. : Impaired bitter taste was the most common dysfunction in the long-COVID cohort. Salivary gustin was significantly lower in those with long COVID and correlated with lower bitter taste score. Cellular saliva showed keratin-10- and small-proline-rich protein-positive epithelial cells as well as SHH-, occluding- and KCNQ1-positive taste cells. : Salivary gustin could be a marker for impaired bitter taste in long COVID.

摘要

味觉功能障碍是由严重急性呼吸综合征冠状病毒2(SARS-CoV-2)引起的急性冠状病毒病(COVID-19)的常见症状。虽然大多数受影响者报告随着时间推移味觉功能有所恢复,但新出现的数据表明,20%-25%的个体存在持续性味觉功能障碍,这是长期新冠的常见症状。味觉是由不断更新的味蕾细胞介导的。细胞生成和细胞死亡这两种相互抵消的过程之间的平衡维持着内稳态更新。音猬因子(SHH)是一种形态发生蛋白,可促进味觉细胞的增殖和分化。诸如味觉素等酶蛋白可调节味觉受体周围的环境并影响味觉感知。因此,我们推测味觉细胞更新增加和味觉相关唾液蛋白减少导致了长期新冠患者的味觉功能障碍。

在获得知情同意后,从患有味觉功能障碍的长期新冠患者中收集未刺激的全唾液(UWS)。正常对照组包括2019年之前编目的存档唾液样本。通过无水经验味觉测试客观地测定味觉感知。用酶联免疫吸附测定法(ELISA)测定UWS中的SHH、味觉素和炎性细胞因子。通过免疫荧光评估细胞唾液中上皮细胞和味觉细胞特异性标志物的表达。

苦味味觉受损是长期新冠患者队列中最常见的功能障碍。长期新冠患者的唾液味觉素显著降低,且与较低的苦味评分相关。细胞唾液显示角蛋白-10和富含小脯氨酸蛋白阳性的上皮细胞以及SHH、闭合蛋白和钾通道蛋白Q1阳性的味觉细胞。

唾液味觉素可能是长期新冠患者苦味味觉受损的标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b6a/11594764/bd31931ea0af/jcm-13-06816-g001.jpg

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