Your search keyword '"Yu-hong Li"' showing total 4 results

1. Influence of age and sex on pharmacodynamics of propofol in neurosurgical patients: model development1

Author

Yu-hong Li, Jian-guo Xu, and Fu-sheng Wu

Subjects

Pharmacology, business.industry, Sex factors, Pharmacodynamics, Anesthesia, Medicine, Pharmacology (medical), Model development, General Medicine, business, Age and sex, Propofol, medicine.drug

Abstract

Influence of age and sex on pharmacodynamics of propofol in neurosurgical patients: model development

Published

2006

2. Population pharmacokinetics of propofol in Chinese patients

Author

Yu-Hong, Li, Jian-Zhong, Rui, Yong-Gang, Zhou, Li-Qin, Wang, Su-E, Fu, Jian-Jun, Yang, Fu-Kun, Liu, Shu-Ya, Hu, Quan, Wen, and Jian-Guo, Xu

Subjects

Adult, Male, China, Metabolic Clearance Rate, Body Weight, Age Factors, Middle Aged, Asian People, Nonlinear Dynamics, Humans, Female, Propofol, Anesthetics, Intravenous, Aged

Abstract

To analyze population pharmacokinetics of propofol in Chinese surgical patients using a nonlinear mixed-effect model (NONMEM) program and to quantitate the effects of covariance of gender, age, and body weight.The population pharmacokinetics of propofol was investigated in 76 selective surgical patients (37 males and 39 females aged 19-77 a, weighing 39-86 kg). A total of 1439 blood samples were analyzed using NONMEM (NONMEM Project Group, University of California, San Francisco, CA). Interindividual variability was estimated for clearances and distribution volumes. The effects of age, body weight, and gender were investigated.The pharmacokinetics of propofol in Chinese patients was best described by a three-compartment pharmacokinetic model. Body weight was found to be a significant factor for the elimination clearance, the two inter-compartmental clearances, and the volume of the central compartment. The volumes of the shallow peripheral compartment and deep peripheral compartment remain constant for all individuals. The estimates of these parameters for a 60-kg adult were 1.56 L/min, 0.737 L/min, 0.360 L/min, 12.1 L, 43 L, and 213 L, respectively. For old patients, the elimination clearance and volume of the central compartment decreased.The pharmacokinetics of propofol in Chinese patients can be well described by a standard three-compartment pharmacokinetic model. Inclusion of age and body weight as covariances significantly improved the model. Adjusting pharmacokinetics to the individual patients should improve the precision of target-controlled infusion system.

Published

2003

3. Good Manufacturing Practices production and analysis of a DNA vaccine against dental caries.

Author

Ya-ping YANG, Yu-hong LI, Ai-hua ZHANG, Lan BI, and Ming-wen FAN

Subjects

DNA vaccines, DENTAL caries vaccines, DRUG efficacy, ENDOTOXINS, IMMUNIZATION, LABORATORY rats

Abstract

AbstractAim:To prepare a clinical-grade anti-caries DNA vaccine pGJA-P/VAX and explore its immune effect and protective efficacy against a cariogenic bacterial challenge.Methods:A large-scale industrial production process was developed under Good Manufacturing Practices (GMP) by combining and optimizing common unit operations such as alkaline lysis, precipitation, endotoxin removal and column chromatography. Quality controls of the purified bulk and final lyophilized vaccine were conducted according to authoritative guidelines. Mice and gnotobiotic rats were intranasally immunized with clinical-grade pGJA-P/VAX with chitosan. Antibody levels of serum IgG and salivary SIgA were assessed by an enzyme-linked immunosorbent assay (ELISA), and caries activity was evaluated by the Keyes method. pGJA-P/VAX and pVAX1 prepared by a laboratory-scale commercial kit were used as controls.Results:The production process proved to be scalable and reproducible. Impurities including host protein, residual RNA, genomic DNA and endotoxin in the purified plasmid were all under the limits of set specifications. Intranasal vaccination with clinical-grade pGJA-P/VAX induced higher serum IgG and salivary SIgA in both mice and gnotobiotic rats. While in the experimental caries model, the enamel (E), dentinal slight (Ds), and dentinal moderate (Dm) caries lesions were reduced by 21.1%, 33.0%, and 40.9%, respectively.Conclusion:The production process under GMP was efficient in preparing clinical-grade pGJA-P/VAX with high purity and intended effectiveness, thus facilitating future clinical trials for the anti-caries DNA vaccine. [ABSTRACT FROM AUTHOR]

Published

2009

4. Enhanced efficacy of CTLA-4 fusion anti-caries DNA vaccines in gnotobiotic hamsters.

Author

Feng Zhang, Yu-hong Li, Ming-wen Fan, Rong Jia, Qing-an Xu, Ji-hua Guo, Fei Yu, and Qi-wei Tian

Subjects

DNA vaccines, PREVENTIVE medicine, HAMSTERS, DENDRITIC cells, STREPTOCOCCUS mutans, ANTIGENS

Abstract

Aim: To evaluate the comparative immunogenicity and protective efficacy of the cytotoxic T-lymphocyte-associated antigen 4 (CTLA-4) fusion anti-caries DNA vaccines pGJA-P/VAX1, pGJA-P, and non-fusion anti-caries DNA construct pGLUA-P in hamsters. In addition, the ability of CTLA-4 to target pGJA-P/VAX1-encoding antigen to dendritic cells was tested in vitro. Methods: All DNA constructs contain genes encoding the A-P regions of a cell surface protein (PAc) and the glucan binding (GLU) domain of glucosyltransferases (GTFs) of cariogenic organism Streptococcus mutans. Human dendritic cells were mixed with the CTLA-4-Ig-GLU-A-P protein expressed by pGJA-P/VAX1-transfected cells and analyzed by flow cytometry. Gnotobiotic hamsters were immunized with anti-caries DNA vaccines by intramuscular injection or intranasal administration. Antibody responses to a representative antigen PAc were assayed by ELISA, and caries protection was evaluated by Keyes caries scores. Results: A flow cytometric analysis demonstrated that CTLA-4-Ig-GLU-A-P protein was capable of binding to human dendritic cells. pGJA-P/VAX1 and pGJA-P induced significantly higher specific salivary and serum anti-PAc antibody responses than pGLUA-P. Significantly fewer caries lesions were also observed in hamsters immunized with pGJA-P/VAX1 and pGJA-P. There was no significant difference in the anti-PAc antibody level or caries scores between pGJA-P/VAX1 and pGJA-P-immunized groups. Conclusion: Antigen encoded by CTLA-4 fusion anti-caries DNA vaccine pGJA-P/VAX1 could specifically bind to human dendritic cells through the interaction of CTLA-4 and B7 molecules. Fusing antigen to CTLA-4 has been proven to greatly enhance the immunogenicity and protective efficacy of anti-caries DNA vaccines. [ABSTRACT FROM AUTHOR]

Published

2007