Nikolaev Viktor P
Department of Barophysiology and Dive Medicine, Institute of Biomedical Problems, Moscow, Russia.
Aviat Space Environ Med. 2004 Jul;75(7):603-10.
Decompression sickness (DCS) is caused by gas bubbles formed from pre-existing and new microscopic gas nuclei in blood and tissues. Assuming a random pattern of bubbling processes in living tissues, we developed a probabilistic model of DCS. We hypothesized that symptoms of DCS in an individual exposed to decompression appear when the total volume of bubbles in a unit volume of any tissue, w(t), exceeds the critical specific volume of a free gas phase, wcr. Therefore, one may consider the expectation of w(t)/wcr as a measure of the dynamic risk of gas bubble lesion of a given tissue segment.
Using the standard approach to estimation of various risks and the sum rule of probabilities of joint events, we defined the cumulative probability of DCS onset by the equation Pcum(t) = 1 - exp[Fcum(t)], where Fcum(t) = sigmaVnQnMnc(t), Qn = 1/wncr, where Vn is the volume of a tissue n. The function Mnc(t) coincides with the function Mn(t), defining a time history of the expectation of wn(t) until it achieves its maximum and then becomes a constant. Evaluating Pcum(t) for particular altitude decompressions, we identified the additive cumulative risk function of development of any DCS symptoms, Fcum-tot(t), with the function defining the cumulative risk of any bubble lesion of the "worst" virtual tissue (WVT) of Type A. On the other hand, we identified the additive cumulative risk function of development of intolerable DCS symptoms, Fcum-int(t), with the function defining the cumulative risk of acute bubble lesion of the WVT of Type phi.
We found parameters of the curves Pcum-tot(t) and Pcum-int(t) that fit the known empirical curves for the cumulative probability of DCS onset. For men performing mild exercise at 30 kPa after preoxygenation, our estimated parameters for curves Pcum-tot(t) indicate that the WVTs of Type A have nitrogen washout half-times of 260 and 290 min for preoxygenation times of 75 and 135 min, respectively. On the other hand, the parameters of curves Pcum-int(t) show that the WVTs of Type phi in men performing mild exercise at 20-40 kPa after preoxygenation during 0-6 h are virtual tissues with nitrogen washout half-times of 400 to 615 min.
Our model provides a new approach to predicting DCS risk for various decompression profiles. By demonstrating the dependence of DCS risk on body tissue parameters, the model explains why resistance to DCS in mammals increases with a lower body mass and greater specific blood flow in tissues.
减压病(DCS)由血液和组织中预先存在的以及新形成的微观气体核形成的气泡所致。假设活体组织中气泡形成过程呈随机模式,我们开发了一种减压病概率模型。我们假设,暴露于减压环境的个体出现减压病症状是因为任何组织单位体积内气泡的总体积w(t)超过了游离气相的临界比容wcr。因此,可以将w(t)/wcr的期望值视为给定组织段气泡损伤动态风险的一种度量。
使用估计各种风险的标准方法以及联合事件概率的求和规则,我们通过方程Pcum(t) = 1 - exp[Fcum(t)]定义减压病发病的累积概率,其中Fcum(t) = sigmaVnQnMnc(t),Qn = 1/wncr,其中Vn是组织n的体积。函数Mnc(t)与函数Mn(t)一致,Mn(t)定义了wn(t)期望值的时间历程,直至其达到最大值然后变为常数。通过评估特定高度减压时的Pcum(t),我们确定了任何减压病症状发展的累加累积风险函数Fcum - tot(t),以及定义A型“最差”虚拟组织(WVT)任何气泡损伤累积风险的函数。另一方面,我们确定了难以忍受的减压病症状发展的累加累积风险函数Fcum - int(t),以及定义φ型WVT急性气泡损伤累积风险的函数。
我们找到了Pcum - tot(t)和Pcum - int(t)曲线的参数,这些参数与减压病发病累积概率的已知经验曲线相符。对于预充氧后在30 kPa进行轻度运动的男性,我们对Pcum - tot(t)曲线估计的参数表明,对于预充氧时间分别为75分钟和135分钟的情况,A型WVT的氮洗脱半衰期分别为260分钟和290分钟。另一方面,Pcum - int(t)曲线的参数表明,在预充氧0 - 6小时后于20 - 40 kPa进行轻度运动的男性中,φ型WVT是氮洗脱半衰期为400至615分钟的虚拟组织。
我们的模型为预测各种减压方案的减压病风险提供了一种新方法。通过证明减压病风险对身体组织参数的依赖性,该模型解释了为什么哺乳动物对减压病的抵抗力会随着体重降低和组织中特定血流量增加而增强。
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