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Serum and Urine Biomarker Elevation Indicating the Onset of Deep Tissue Injury as Examined on a Rat Model

机译:血清和尿液生物标志物升高指示在大鼠模型上检查的深部组织损伤的发作

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摘要

Deep tissue injury (DTI) is a serious pressure ulcer (PU) which initiates in deep tissue, mainly muscle, and progresses rapidly to a full-thickness wound [1, 2]. Therefore, an early indication should help in increasing awareness and providing prompt intervention to prevent it from progressing to an open wound, which is susceptible to infection and typically needs prolonged and aggressive care. However, the diagnosis of DTI is currently still vague at best[2] with only subjective tools. This situation calls for tools for objectively sensing the tissue changes while the skin is still intact, to allow development of evidence-based protocols for early diagnosis and treatment. Since DTI initiates from deep muscle layer around a bony prominence, a tool that sensitive to muscle damage may have the potential to objectively sense the onset of a DTI in clinical application. A number of molecular biomarkers have been reported in the literature as suitable for indicating muscle damage. Some of the most promising biomarkers are myoglobin and heart-type fatty acid binding protein (H-FABP). Myoglobin and H-FABP are two relatively small muscle proteins that show a very fast release time after skeletal muscle damageecrosis when no myocardial infarction or damage is present; therefore, they may be used to identify skeletal muscle injury in DTI formation. The objective of this study was to initially test whether myoglobin and H-FABP in serum and urine respond quickly to pressure induced deep tissue injury on a rat model. It is expected that knowledge gained from this study may lead to a promising new methodology to sense the visually invisible DTI.
机译:深层组织损伤(DTI)是一种严重的压疮(PU),其始于深部组织(主要是肌肉),并迅速发展为全层伤口[1、2]。因此,早期适应症应有助于提高认识并提供及时干预,以防止其发展成易感染的开放性伤口,通常需要长期和积极的护理。然而,仅凭主观工具,DTI的诊断目前仍充其量[2]。这种情况需要在皮肤仍然完好无损时客观地感知组织变化的工具,以允许开发基于证据的方案以进行早期诊断和治疗。由于DTI从围绕骨突出的深部肌肉层开始,因此对肌肉损伤敏感的工具在临床应用中可能具有客观感知DTI发作的潜力。文献中已经报道了许多分子生物标志物,它们适于指示肌肉损伤。一些最有希望的生物标志物是肌红蛋白和心脏型脂肪酸结合蛋白(H-FABP)。肌红蛋白和H-FABP是两种相对较小的肌肉蛋白,当不存在心肌梗塞或损伤时,在骨骼肌损伤/坏死后显示出非常快的释放时间。因此,它们可用于识别DTI形成中的骨骼肌损伤。这项研究的目的是最初测试大鼠模型中血清和尿液中的肌红蛋白和H-FABP是否对压力引起的深部组织损伤快速反应。期望从这项研究中获得的知识可能会导致一种有前途的新方法来感知视觉上不可见的DTI。

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  • 会议地点 Naples FL(US);Naples FL(US)
  • 作者单位

    Departments of Physical Therapy HumanrnMovement Sciences, Feinberg School ofrnMedicine, Northwestern University, Chicago, IL,rnUSA Orthopaedic Surgery,rnFeinberg School of Medicine,rnNorthwestern University,rnChicago, IL, USA;

    Departments of Physical Therapy HumanrnMovement Sciences, Feinberg School ofrnMedicine, Northwestern University, Chicago, IL,rnUSA rn(2) Sensory Motor Performance Program,rnRehabilitation Institute of Chicago, Chicago, IL,rnUSA;

    Departments of Physical Therapy HumanrnMovement Sciences, Feinberg School ofrnMedicine, Northwestern University, Chicago, IL,rnSA;

    Departments of Physical Therapy HumanrnMovement Sciences, Feinberg School ofrnMedicine, Northwestern University, Chicago, IL,rnSA;

    Life Diagnostics, Inc., West Chester, PA, USA;

    et al;

  • 会议组织
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 人体工程学;
  • 关键词

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