Enhancement of endothelialization by topographical features is mediated by PTP1B-dependent endothelial adherens junctions remodeling
Enhancement of endothelialization by topographical features is mediated by PTP1B-dependent endothelial adherens junctions remodeling
RationaleFailure of small synthetic vascular grafts is largely due to late endothelialization and has been an ongoing challenge in the treatment of cardiovascular diseases. ObjectivePrevious strategies developed to promote graft endothelialization include surface topographical modulation and biochemical modifications. However, these have been met with limited success. Importantly, although the integrity of Endothelial Cell (EC) monolayer is crucial for endothelialization, the crosstalk between surface topography and cell-cell connectivity is still not well understood. Here we explored a combined strategy that utilizes both topographical features and pharmacological perturbations. Methods and resultWe characterized EC behaviors in response to micron-scale grating topography in conjunction with pharmacological perturbations of endothelial adherens junctions (EAJ) regulators. We studied the EA.hy 926 cell-cell junctions and monolayer integrity using the junctional markers upon the inhibitory effect of EAJ regulator on both planar and grating topographies substrates.We identified a protein tyrosine phosphatase, PTP1B, as a potent regulator of EAJ stability. Next, we studied the physiologically relevant behaviors of EC using primary human coronary arterial endothelial cells (HCAEC). Our results showed that PTP1B inhibition synergized with grating topographies to modulate EAJ rearrangement, thereby controlling global EC monolayer sheet orientation, connectivity and collective cell migration to promote endothelialization.Our results showed that PTP1B inhibition synergized with grating topographies to modulate EAJ rearrangement, thereby controlling global EC monolayer sheet orientation, connectivity and collective cell migration and proliferation. ConclusionThe synergistic effect of PTP1B inhibition and grating topographies could be useful for the promotion of endothelialization by enhancing EC migration and proliferation.
Gorji Azita、Toh Pearlyn Jia Ying、Toyama Yusuke、Kanchanawong Pakorn、Toh Yi-Chin
Mechanobiology Institute National University of SingaporeMechanobiology Institute National University of SingaporeMechanobiology Institute National University of Singapore||Department of Biological Sciences, National University of SingaporeMechanobiology Institute National University of Singapore||Department of Biomedical Engineering, National University of SingaporeDepartment of Biomedical Engineering, National University of Singapore||Institute for Health Innovation and Technology, National University of Singapore||The N.1 Institute for Health, National University of Singapore||NUS Tissue Engineering Programme, National University of Singapore
基础医学生物科学研究方法、生物科学研究技术生理学
Endothelial cellsEndothelial integritytopography sensingProtein Tyrosine PhosphatasePTP1BVE-cadherin
Gorji Azita,Toh Pearlyn Jia Ying,Toyama Yusuke,Kanchanawong Pakorn,Toh Yi-Chin.Enhancement of endothelialization by topographical features is mediated by PTP1B-dependent endothelial adherens junctions remodeling[EB/OL].(2025-03-28)[2025-05-05].https://www.biorxiv.org/content/10.1101/766816.点此复制
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