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The Desmosomal Cadherin Desmoglein-2 Experiences Mechanical Tension as Demonstrated by a FRET-Based Tension Biosensor Expressed in Living Cells

机译:Desmosomal钙黏着蛋白Desmoglein-2经历了机械张力这是由在活细胞中表达的基于FRET的张力生物传感器所证实的。

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摘要

Cell-cell junctions are critical structures in a number of tissues for mechanically coupling cells together, cell-to-cell signaling, and establishing a barrier. In many tissues, desmosomes are an important component of cell-cell junctions. Loss or impairment of desmosomes presents with clinical phenotypes in the heart and skin as cardiac arrhythmias and skin blistering, respectively. Because heart and skin are tissues that are subject to large mechanical stresses, we hypothesized that desmosomes, similar to adherens junctions, would also experience significant tensile loading. To directly measure mechanical forces across desmosomes, we developed and validated a desmoglein-2 (DSG-2) force sensor, using the existing TSmod Förster resonance energy transfer (FRET) force biosensor. When expressed in human cardiomyocytes, the force sensor reported high tensile loading of DSG-2 during contraction. Additionally, when expressed in Madin-Darby canine kidney (MDCK) epithelial or epidermal (A431) monolayers, the sensor also reported tensile loading. Finally, we observed higher DSG-2 forces in 3D MDCK acini when compared to 2D monolayers. Taken together, our results show that desmosomes experience low levels of mechanical tension in resting cells, with significantly higher forces during active loading.
机译:细胞间连接是许多组织中的关键结构,用于将细胞机械耦合在一起,细胞间信号传导并建立屏障。在许多组织中,桥粒是细胞间连接的重要组成部分。桥粒体的丢失或损伤表现为心脏和皮肤的临床表型,分别为心律不齐和皮肤起泡。因为心脏和皮肤是承受较大机械应力的组织,所以我们假设与粘附连接类似的桥粒也会承受很大的拉伸载荷。为了直接测量跨桥粒的机械力,我们使用现有的TSmodFörster共振能量转移(FRET)力生物传感器开发并验证了desmoglein-2(DSG-2)力传感器。当在人心肌细胞中表达时,力传感器报告收缩期间DSG-2的高拉伸负荷。此外,当在Madin-Darby犬肾(MDCK)上皮或表皮(A431)单层中表达时,该传感器还报告了拉伸载荷。最后,与2D单层相比,我们在3D MDCK腺泡中观察到更高的DSG-2力。两者合计,我们的结果表明,桥粒在静息细胞中的机械张力较低,在主动加载过程中的力明显较高。

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