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Cellular-scale transport in deformed skeletal muscle following spinal cord injury

机译:脊髓损伤后骨骼肌变形中的细胞尺度转运

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摘要

Deep tissue injury (DTI) is a severe pressure ulcer initiating in weight-bearing skeletal muscles. Being common in spinal cord injury (SCI) patients, DTI is associated with mechanical cell damage and ischaemia. Muscle microanatomy in SCI patients is characterised by reduced myofibre sizes and smaller, fewer capillaries. We hypothesise that these changes influence mass transport in SCI muscles, making DTI more probable. Using multiphysics models of microscopic cross-sections through normal and SCI muscles, we studied effects of the following factors on transport of glucose and myoglobin (potential biomarker for early DTI detection): (i) abnormal SCI muscle microanatomy, (ii) large tissue deformations and (iii) ischaemia. We found that the build-up of concentrations of glucose and myoglobin is slower for SCI muscles, which could be explained by the pathological SCI microanatomy. These findings overall suggest that microanatomical changes in muscles post-SCI play an important role in the vulnerability of the SCI patients to DTI.
机译:深层组织损伤(DTI)是在负重骨骼肌中引发的严重压疮。 DTI在脊髓损伤(SCI)患者中很常见,与机械性细胞损伤和缺血有关。 SCI患者的肌肉显微解剖学特征是肌纤维大小减小,毛细血管更少,数量更少。我们假设这些变化会影响SCI肌肉的质量运输,从而使DTI更有可能。使用通过正常和SCI肌肉的微观横截面的多物理场模型,我们研究了以下因素对葡萄糖和肌红蛋白(早期DTI检测的潜在生物标志物)转运的影响:(i)SCI肌肉显微解剖异常,(ii)大组织变形(iii)缺血。我们发现,SCI肌肉的葡萄糖和肌红蛋白浓度升高较慢,这可以通过病理性SCI显微解剖来解释。这些发现总体上表明,SCI后肌肉的微观解剖学变化在SCI患者对DTI的脆弱性中起重要作用。

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