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一种预测用于光动力治疗的他拉泊芬钠在心肌间质浓度的三室药代动力学模型:一种结合测量荧光和荧光室起源分析的方法

A Three-Compartment Pharmacokinetic Model to Predict the Interstitial Concentration of Talaporfin Sodium in the Myocardium for Photodynamic Therapy: A Method Combining Measured Fluorescence and Analysis of the Compartmental Origin of the Fluorescence.

作者信息

Uno Yuko, Ogawa Emiyu, Aiyoshi Eitaro, Arai Tsunenori

机构信息

School of Fundamental Science and Technology, Graduate School of Science and Technology, Keio University, 3-14-1, Hiyoshi, Kohoku-ku, Yokohama City, Kanagawa 223-8522, Japan.

School of Allied Health Science, Kitasato University, Kanagawa 252-0373, Japan.

出版信息

Bioengineering (Basel). 2018 Dec 21;6(1):1. doi: 10.3390/bioengineering6010001.

Abstract

To evaluate the effectiveness of photodynamic therapy occurring in the interstitial space of the myocardium, we estimated the interstitial concentration of talaporfin sodium in the canine myocardium by constructing a three-compartment pharmacokinetic model based on measured changes in talaporfin sodium plasma concentration and myocardial fluorescence. Differential rate equations of talaporfin sodium concentration in the plasma, interstitial space, and cell compartment were developed with individual compartment volume, concentration, and rate constants. Using measured volume ratios based on histological examinations, we defined that the myocardial fluorescence consisted of the linear addition of fluorescence generated from these three compartments. The rate constants were obtained by fitting to minimize the sum of the squared errors between the measured talaporfin sodium concentrations and the calculated concentrations divided by the number of data points using the conjugate gradient method in MATLAB. We confirmed that this fitting operation may be appropriate, because a coefficient of determination between the measured talaporfin sodium changes and the calculated concentrations using our equations was 0.99. Consequently, to estimate the interstitial concentration in the canine myocardium, we propose a three-compartment pharmacokinetic model construction methodology using measured changes in talaporfin sodium plasma concentration and changes in myocardial fluorescence.

摘要

为了评估发生在心肌间质空间的光动力疗法的有效性,我们通过基于所测量的替拉泊芬钠血浆浓度和心肌荧光变化构建三室药代动力学模型,来估算犬心肌中替拉泊芬钠的间质浓度。利用血浆、间质空间和细胞室中替拉泊芬钠浓度的微分速率方程,结合各个室的体积、浓度和速率常数进行分析。基于组织学检查所测得的体积比,我们确定心肌荧光是由这三个室产生的荧光线性叠加而成。速率常数通过拟合来获得,使用MATLAB中的共轭梯度法,使所测量的替拉泊芬钠浓度与计算浓度之间的误差平方和除以数据点数后最小化。我们证实这种拟合操作可能是合适的,因为使用我们的方程计算得出的替拉泊芬钠变化与测量浓度之间的决定系数为0.99。因此,为了估算犬心肌中的间质浓度,我们提出一种利用所测量的替拉泊芬钠血浆浓度变化和心肌荧光变化来构建三室药代动力学模型的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e01/6466385/88e2cdb47ebe/bioengineering-06-00001-g001.jpg

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