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口腔抗病毒防御:唾液和饮料样低渗动态调节口腔上皮细胞中抗病毒人 MxA 的无膜生物分子凝聚物的形成。

Oral Antiviral Defense: Saliva- and Beverage-like Hypotonicity Dynamically Regulate Formation of Membraneless Biomolecular Condensates of Antiviral Human MxA in Oral Epithelial Cells.

机构信息

Department of Cell Biology and Anatomy, New York Medical College, Valhalla, NY 10595, USA.

Department of Medicine, New York Medical College, Valhalla, NY 10595, USA.

出版信息

Cells. 2024 Mar 28;13(7):590. doi: 10.3390/cells13070590.

Abstract

The oral mucosa represents a defensive barrier between the external environment and the rest of the body. Oral mucosal cells are constantly bathed in hypotonic saliva (normally one-third tonicity compared to plasma) and are repeatedly exposed to environmental stresses of tonicity, temperature, and pH by the drinks we imbibe (e.g., hypotonic: water, tea, and coffee; hypertonic: assorted fruit juices, and red wines). In the mouth, the broad-spectrum antiviral mediator MxA (a dynamin-family large GTPase) is constitutively expressed in healthy periodontal tissues and induced by Type III interferons (e.g., IFN-λ1/IL-29). Endogenously induced human MxA and exogenously expressed human GFP-MxA formed membraneless biomolecular condensates in the cytoplasm of oral carcinoma cells (OECM1 cell line). These condensates likely represent storage granules in equilibrium with antivirally active dispersed MxA. Remarkably, cytoplasmic MxA condensates were exquisitely sensitive sensors of hypotonicity-the condensates in oral epithelium disassembled within 1-2 min of exposure of cells to saliva-like one-third hypotonicity, and spontaneously reassembled in the next 4-7 min. Water, tea, and coffee enhanced this disassembly. Fluorescence changes in OECM1 cells preloaded with calcein-AM (a reporter of cytosolic "macromolecular crowding") confirmed that this process involved macromolecular uncrowding and subsequent recrowding secondary to changes in cell volume. However, hypertonicity had little effect on MxA condensates. The spontaneous reassembly of GFP-MxA condensates in oral epithelial cells, even under continuous saliva-like hypotonicity, was slowed by the protein-phosphatase-inhibitor cyclosporin A (CsA) and by the K-channel-blocker tetraethylammonium chloride (TEA); this is suggestive of the involvement of the volume-sensitive WNK kinase-protein phosphatase (PTP)-K-Cl cotransporter (KCC) pathway in the regulated volume decrease (RVD) during condensate reassembly in oral cells. The present study identifies a novel subcellular consequence of hypotonic stress in oral epithelial cells, in terms of the rapid and dynamic changes in the structure of one class of phase-separated biomolecular condensates in the cytoplasm-the antiviral MxA condensates. More generally, the data raise the possibility that hypotonicity-driven stresses likely affect other intracellular functions involving liquid-liquid phase separation (LLPS) in cells of the oral mucosa.

摘要

口腔黏膜是机体与外界环境之间的一道防御屏障。口腔黏膜细胞不断受到低渗唾液(正常情况下比血浆低三分之一渗透压)的浸泡,并且反复受到我们饮用的饮料的渗透压、温度和 pH 值等环境应激的影响(例如,低渗:水、茶和咖啡;高渗:各种果汁和红酒)。在口腔中,广谱抗病毒介质 MxA(一种动力蛋白家族的大 GTP 酶)在健康的牙周组织中持续表达,并被 III 型干扰素诱导(例如,IFN-λ1/IL-29)。内源性诱导的人 MxA 和外源性表达的人 GFP-MxA 在口腔癌细胞(OECM1 细胞系)的细胞质中形成无膜生物分子凝聚物。这些凝聚物可能代表与具有抗病毒活性的弥散 MxA 处于平衡状态的储存颗粒。值得注意的是,细胞质 MxA 凝聚物对低渗性非常敏感——凝聚物在暴露于类似唾液的三分之一低渗性后 1-2 分钟内在口腔上皮细胞中解体,并在接下来的 4-7 分钟内自发重新组装。水、茶和咖啡增强了这种解聚作用。用 calcein-AM(细胞质“大分子拥挤”的报告者)预加载的 OECM1 细胞中的荧光变化证实,这个过程涉及大分子解拥挤,随后由于细胞体积的变化而重新拥挤。然而,高渗性对 MxA 凝聚物几乎没有影响。即使在持续类似唾液的低渗性下,GFP-MxA 凝聚物在口腔上皮细胞中的自发重新组装也被蛋白磷酸酶抑制剂环孢菌素 A(CsA)和钾通道阻断剂四乙铵氯化物(TEA)所减缓;这提示参与体积敏感的 WNK 激酶-蛋白磷酸酶(PTP)-K-Cl 共转运体(KCC)途径在口腔细胞中凝聚物重新组装过程中的体积调节性减少(RVD)。本研究确定了口腔上皮细胞中低渗应激的一种新的亚细胞后果,即细胞质中一类相分离生物分子凝聚物(抗病毒 MxA 凝聚物)的快速和动态结构变化。更普遍地说,这些数据提出了一种可能性,即低渗性应激可能会影响口腔黏膜细胞中涉及液-液相分离(LLPS)的其他细胞内功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4e12/11011872/d51a083c5f5c/cells-13-00590-g001.jpg

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