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Realistic Temporal Variations of Shear Stress Modulate MMP-2 and MCP-1 Expression in Arteriovenous Vascular Access

机译:切应力的现实时间变化调节动静脉血管通路中的MMP-2和MCP-1表达。

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Venous neointimal hyperplasia (VNH) lesions are prone to localized development within the vascular access junction (VAJ) and efferent vein of arteriovenous (AV) fistulae and grafts. The creation of VAJ dramatically alters the local venous hemodynamics with high pulsatile flow velocities enter the vein resulting in blood-flow separation, recirculation and flow reversal. This study conducted a computational hemodynamic investigation of an idealized AV graft and realistic AV fistula which demonstrated a complex hemodynamic environment within the VAJ, producing elevated wall shear stress (WSS) magnitudes and significant spatial and temporal WSS gradients in the VAJ. These hemodynamic patterns and non-physiological WSSs are postulated to initiate VNH development at the transcriptional level. Human umbilical vein endothelial cells (HUVEC) were exposed to elevated temporal WSS waveforms obtained from the aforementioned computational analysis, using a cone-and-plate bioreactor. Using real-time RT-PCR, early induction of MMP-2 and delayed transcriptional upregulation of MCP-1 was observed following EC exposure to VAJ high wall shear forces. These results indicate that MMP-2 and MCP-1 may be induced by high WSS present in the VAJ, suggesting a link between elevated WSS magnitudes and temporal gradients, extracellular matrix decomposition, smooth muscle cell migration and proliferation, and the subsequent VNH development in AV VAJs.
机译:静脉内膜增生(VNH)病变易于在血管通路(VAJ)和动静脉(AV)瘘管和移植物的传出静脉内局部发展。 VAJ的产生极大地改变了局部静脉血流动力学,其中高脉动血流速度进入静脉,导致血流分离,再循环和血流逆转。这项研究对理想的AV移植物和真实的AV瘘进行了计算血液动力学研究,结果表明VAJ内存在复杂的血液动力学环境,从而在VAJ中产生了升高的壁切应力(WSS)幅度以及明显的时空WSS梯度。假定这些血液动力学模式和非生理性WSS在转录水平上启动了VNH的发育。使用锥板生物反应器,将人脐静脉内皮细胞(HUVEC)暴露于从上述计算分析获得的升高的瞬时WSS波形。使用实时RT-PCR,在EC暴露于VAJ高壁剪切力后,观察到MMP-2的早期诱导和MCP-1的转录上调延迟。这些结果表明,VAJ中存在的高WSS可能诱导MMP-2和MCP-1,这表明WSS强度和时间梯度升高,细胞外基质分解,平滑肌细胞迁移和增殖以及随后的VNH发育之间存在联系。 AV VAJ。

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