A molding and using method for a bulk drug gastrointestinal absorption prediction BSPK model

A technology of gastrointestinal absorption and modeling method, which is applied in the fields of new drug design and pharmacokinetic research and development, and can solve problems such as application limitation, model ignoring drug absorption, and ignoring the influence of diffusion layer thickness.

Inactive Publication Date: 2011-05-04
SHANGHAI YUNYI HEALTHCARE MANAGEMENT
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  • Abstract
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AI Technical Summary

Problems solved by technology

[0005] The technical problem to be solved in the present invention is to overcome the following defects of the existing mathematical model of absorption: some macroscopic material balance methods are limited in application because they do not consider the process of drug dissolution; The influence of the thickness of the diffusion layer; some models ignore the absorption of drugs in the large intestine; some software is expensive, and its application is often limited due to data source problems in the early stage of drug screening and optimization; provide a method for the gastric The modeling method of the BSPK (full name: physiological structure-based pharmacokinetic model) model for intestinal absorption prediction. This model is based on the dissolution, sedimentation and absorption of drugs in multiple compartments of the gastrointestinal tract. A series of functions are established. Factors and variables such as logP, logD, pKa, solubility, dissolution rate, density, particle size, particle shape, particle size distribution, sedimentation rate, sedimentation particle size, sedimentation time, permeability, and human gastrointestinal physiological conditions are considered , suitable for the absorption prediction of acidic, basic, neutral and amphoteric drugs in different parts of the gastrointestinal tract

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  • A molding and using method for a bulk drug gastrointestinal absorption prediction BSPK model
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  • A molding and using method for a bulk drug gastrointestinal absorption prediction BSPK model

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Embodiment 1

[0061] This embodiment is used to illustrate a basic implementation method of the present invention, that is, after inputting the given values ​​of each parameter in the differential solver to obtain the predicted absorption percentage, compare it with the experimental absorption percentage to obtain the speed predicted by the model.

[0062] One, the object of the present invention is achieved through the following steps.

[0063] 1. Divide the gastrointestinal tract into several reasonable absorption sites based on the physiological structure.

[0064] In this example, the gastrointestinal tract is divided into three parts: stomach, small intestine and large intestine. Liquid and solid drugs pass through the three chambers, each with a different volume, flow rate, and residence time. It is assumed that the drugs in each chamber reach a steady state.

[0065] 2. Establish dissolution and absorption prediction functions for different absorption sites, each function has a giv...

Embodiment 2

[0102] The concrete application of the present invention not only comprises obtaining predicted value by known parameter value in embodiment 1, also can be applied to key parameter analysis, parameter suitable value prediction, absorption percentage prediction under special circumstances (as the influence of particle diameter and particle shape and the impact of settlement) etc., this embodiment is used to illustrate the analysis of key parameters.

[0103] Among the input parameters, some parameters have a significant impact on absorption and are called key parameters; some have no significant impact on absorption and are called non-key parameters. Through software prediction, key parameters affecting absorption can be analyzed, which is conducive to optimizing key parameters in order to improve drug absorption.

[0104] Specifically, the determination method of key parameters affecting absorption is as follows: other parameters are fixed, and two parameters are optional (sho...

Embodiment 3

[0108] The present invention can not only be used for absorption prediction, but also can infer appropriate parameters according to the ideal absorption value, which is beneficial to achieve ideal absorption in later in vivo tests by changing the salt form or dosage form of the drug in the early drug screening process.

[0109] Specifically, the ideal absorption percentage value is set, other parameters are fixed, the only variable is selected, different values ​​are input, and the predicted value is obtained through software calculation. Compared with the ideal absorption value, if the predicted value is close to the ideal absorption value, that is, the predicted value is within 1 / 2 to 2 times of the actual measured value, then the corresponding value is the appropriate value of the parameter.

[0110] The particle size, solubility, dose, permeability, log P, pKa of the active compound all have an effect on the percent absorption. The model can infer appropriate parameters ba...

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Abstract

The invention discloses a molding and using method for a bulk drug gastrointestinal absorption prediction BSPK model, which establishes a series of functions based on the bulk drug dissolution, settlement and absorption in multiple gastrointestinal compartments, and which takes into account many factors and variables as follows: drug logP, logD, pKa, solubility, dissolution rate, density, partical diameter, particle forms, particle diameter distribution, settlement rate, settlement particle diameter, settlement time, permeability and human gastrointestinal physiological conditions, etc. The method is applicable to acidic, alkalic, neutral and acidic-alkalic drug absorption prediction in different gastrointestinal parts. The invention, which is used in active compound gastrointestinal absorption prediction, not only raises the early stage drug screening accuracy, but also reduces the workload of preformulation researches. In this way, medicine clinical application process is accelerated with great scientific research value and application prospect.

Description

technical field [0001] The present invention relates to the fields of new drug design and pharmacokinetic research and development, in particular to the establishment of a pharmacokinetic model for predicting the dissolution and absorption behavior of active ingredients (crude drugs) in the gastrointestinal tract using a computer-aided differential solver modeling method. Background technique [0002] Pharmacokinetics is the study of fundamental or molecular-level interactions between drugs and the body, which lead to corresponding subsequent physiological responses. More than most drugs, their physiological effects are time- and concentration-dependent. Factors affecting the activity of drugs at the lesion site include drug absorption, distribution, metabolism, and excretion. In the process of drug research and development, some in vitro screening of potential compounds with activity is limited by the physicochemical and pharmacokinetic properties of the drug itself, but ...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): G06F19/00A61K49/00
Inventor 施斌洪鸣凰李原强
Owner SHANGHAI YUNYI HEALTHCARE MANAGEMENT
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