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《庄子》非“处置”类二价双向动作动词及其相关句式的考察
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作者 殷国光 华建光 《南开语言学刊》 2007年第2期51-66,155,共17页
本文采用配价语法理论,以词项为单位,对《庄子》非"处置"类二价双向动作动词进行了全面的考察,分析描写其语义特征、配价结构、基本句式、派生句式、配位规则,探讨它们之间的相互关系。
关键词 庄子 动词 配价 句式 非“处置”
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Simulation-based simplification of target-mediated drug disposition model of denosumab
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作者 Yu Fu Ye Yao +3 位作者 Peiming Ma Xuan Zhou Wei Lu Tianyan Zhou 《Journal of Chinese Pharmaceutical Sciences》 CAS CSCD 2018年第11期767-776,共10页
Target-mediated drug disposition (TMDD)model is one of the main modeling theories for studying nonlinear pharmacokinetics (PK)ofmonoclonal antibodies.However,there are too many parameters in full TMDD model to be esti... Target-mediated drug disposition (TMDD)model is one of the main modeling theories for studying nonlinear pharmacokinetics (PK)ofmonoclonal antibodies.However,there are too many parameters in full TMDD model to be estimated based on limited clinical data,leading to instability of the final model.In the present study,we analyzed the predictive ability and applicability of a simplified quasi-steady state (QSS)model with the assumption that the total target concentration was a constant parameter during treatment with monoelonal antibody in clinical data modeling.Based on the parameters of a published TMDD model of denosumab,simulations were performed at population and individual levels.Then,a simplified TMDD model,QSS model, was used to examine the effects of hypotheses,in which the total receptor concentration was constant or variable on model fit and stability of parameter estimation.Both simulations at the population level and model fit results of simulated individual data showed that at the therapeutic doses,the total receptor concentration had little influence on changes in drug concentration,and the model with constant total receptor concentration had the same predictive power.The validated hypothesis could be applied to clinical trial design and selection of the optimal PK model in the development of monoclonal antibodies. 展开更多
关键词 Target-mediated drug disposition model Monoclonal antibody Nonlinear pharmacokinetics DENOSUMAB SIMULATION
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