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Deterministic model of dermal wound invasion incorporating receptor-mediated signal transduction and spatial gradient sensing

机译:结合受体介导的信号转导和空间梯度传感的皮肤创面侵袭性确定性模型

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摘要

During dermal wound healing, platelet-derived growth factor (PDGF) serves as both a chemoattractant and mitogen for fibroblasts, potently stimulating their invasion of the fibrin clot over a period of several days. A mathematical model of this process is presented, which accurately accounts for the sensitivity of PDGF gradient sensing through PDGF receptor/phosphoinositide 3-kinase-mediated signal transduction. Analysis of the model suggests that PDGF receptor-mediated endocytosis and degradation of PDGF allows a constant PDGF concentration pro. le to be maintained at the leading front of the fibroblast density pro. le as it propagates, at a constant rate, into the clot. Thus, the constant PDGF gradient can span the optimal concentration range for asymmetric phosphoinositide 3-kinase signaling and fibroblast chemotaxis, with near-maximal invasion rates elicited over a relatively broad range of PDGF secretion rates. A somewhat surprising finding was that extremely sharp PDGF gradients do not necessarily stimulate faster progression through the clot, because maintaining such a gradient through PDGF consumption is a potentially rate-limiting process.
机译:在真皮伤口愈合过程中,血小板衍生的生长因子(PDGF)既是成纤维细胞的趋化剂,又是有丝分裂原,可在几天内有效刺激其侵袭纤维蛋白凝块。提出了此过程的数学模型,该模型准确地说明了通过PDGF受体/磷酸肌醇3-激酶介导的信号转导作用的PDGF梯度传感的敏感性。对模型的分析表明,PDGF受体介导的内吞作用和PDGF的降解可保持恒定的PDGF浓度。保持在成纤维细胞密度亲的最前沿。当它以恒定的速度传播到血块中时。因此,恒定的PDGF梯度可以跨越不对称磷酸肌醇3-激酶信号传导和成纤维细胞趋化性的最佳浓度范围,在相对较宽的PDGF分泌率范围内引起接近最大的浸润率。一个令人惊讶的发现是,极其陡峭的PDGF梯度不一定会刺激血凝块更快地发展,因为通过PDGF消耗维持这种梯度是一个潜在的限速过程。

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