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一种新的生物物理减压模型,用于估计减压过程中和减压后关节弯曲的风险。

A new biophysical decompression model for estimating the risk of articular bends during and after decompression.

机构信息

Faculté de Médecine Nord, Université de la Méditerranée, UMR-MD2, P2COE, Institut de Neuroscience J Roche, 13916 Marseille Cedex 20, France.

出版信息

J Theor Biol. 2011 Aug 21;283(1):168-79. doi: 10.1016/j.jtbi.2011.05.002. Epub 2011 May 19.

Abstract

The biophysical models that intend to predict the risk of decompression sickness after a change of pressure are not numerous. Few approaches focus in particular on joints as target tissues, with the aim to describe properly the mechanisms inducing pain. Nevertheless, for this type of decompression incidents, called articular bends, no model proved to fit the empirical results for a broad range of exposures and decompression procedures. We present here an original biophysical decompression model for describing the occurrence of articular bends. A target joint is broken down into two parts that exchange inert gases with the blood by perfusion and with each other by diffusion over distances of a few millimetres. This diffusion pathway allows the slow amplification of microbubbles growing during and after decompression, consistent with the possible delayed occurrence of bends. The diffusion coefficients introduced into this model are larger than those introduced into most modern decompression models. Their value remains physical (#10(-9)m(2)/s). Inert gas exchanges and the formation, amplification and resorption of microbubbles during and after decompression were simulated. We used a critical gas volume criterion for predicting the occurrence of bends. A risk database extracted from COMEX experience and other published studies were used for the correlation of model parameters not known a priori. We considered a large range of exposure, and the commonly used inert gases nitrogen and helium. This correlation phase identified the worst biophysical conformations most likely to lead to the formation, in tissues such as tendons, of a large number of microbubbles recruited from pre-existing gas nuclei during decompression. The risk of bends occurrence was found to be linked to the total separated gas volume generated during and after decompression. A clamping phenomenon occurs soon after the start of decompression, greatly slowing the gas exchanges controlled especially by the oxygen window. This model, which reproduces many empirical findings, may be considered both descriptive and predictive.

摘要

旨在预测压力变化后减压病风险的生物物理模型并不多。少数方法特别关注关节作为靶组织,目的是正确描述引起疼痛的机制。然而,对于这种类型的减压事件,称为关节弯曲,没有一种模型被证明适用于广泛的暴露和减压程序的经验结果。我们在这里提出了一种原始的生物物理减压模型,用于描述关节弯曲的发生。一个靶关节被分解为两个部分,它们通过灌注与血液交换惰性气体,通过扩散在几毫米的距离内相互交换。这种扩散途径允许在减压过程中和减压后生长的微泡缓慢放大,这与弯曲可能的延迟发生一致。引入到该模型中的扩散系数大于引入到大多数现代减压模型中的扩散系数。它们的值仍然是物理的(#10(-9)m(2)/s)。在减压过程中和减压后,惰性气体交换以及微泡的形成、放大和吸收被模拟。我们使用临界气体体积标准来预测弯曲的发生。从 COMEX 经验和其他已发表的研究中提取的风险数据库用于关联事先未知的模型参数。我们考虑了广泛的暴露范围和常用的惰性气体氮气和氦气。这个相关阶段确定了最有可能导致在减压过程中从预先存在的气体核中招募大量微泡的组织(如肌腱)中形成大量微泡的最差生物物理构象。发现弯曲发生的风险与减压过程中和减压后产生的总分离气体体积有关。在减压开始后不久就会出现夹紧现象,大大减缓了主要由氧气窗口控制的气体交换。这种模型可以再现许多经验发现,既可以看作是描述性的,也可以看作是预测性的。

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