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基于接收机钟差的GPS完好性自主检测算法 被引量:14
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作者 许龙霞 李孝辉 《宇航学报》 EI CAS CSCD 北大核心 2011年第3期537-542,共6页
传统的基于最小二乘法和奇偶矢量的接收机自主完好性检测(Receiver Autonomous Integrity Monito-ring,RAIM)算法均是利用冗余观测量进行一致性检验实现的,其检测统计量均由伪距残差构造得到。本文采用接收机钟差作为RAIM算法的判据,基... 传统的基于最小二乘法和奇偶矢量的接收机自主完好性检测(Receiver Autonomous Integrity Monito-ring,RAIM)算法均是利用冗余观测量进行一致性检验实现的,其检测统计量均由伪距残差构造得到。本文采用接收机钟差作为RAIM算法的判据,基本思想是根据钟差历史解算值建立接收机钟差二次多项式模型,从而得到当前时刻的钟差预测值。同时解算当前时刻的钟差值,将这两者之差与钟差门限值进行比较来判断系统当前时刻是否存在故障。本文首先分析了伪距偏移量对接收机钟差的影响,然后给出确定钟差门限值的方法。结合用户解算位置和接收机钟差利用子集比较法实现了故障识别的功能。因本文给出的故障检测算法不是基于冗余观测量的,故该方法在四颗可见星下就可进行故障检测,与传统的RAIM算法相比降低了RAIM算法对可见星个数的要求,该点在实验部分进行了仿真验证。另外还对可用星多于四颗的基于接收机钟差的RAIM算法进行了故障检测和故障识别部分的仿真,验证了本文方法的可行性。 展开更多
关键词 接收机完好性自主检测 钟差门限值 故障检测 故障识别 子集比较法
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In Silico Investigation of Agonist Activity of a Structurally Diverse Set of Drugs to hPXR Using HM-BSM and HM-PNN
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作者 张一鸣 常美佳 +1 位作者 杨旭曙 韩晓 《Journal of Huazhong University of Science and Technology(Medical Sciences)》 SCIE CAS 2016年第3期463-468,共6页
The human pregnane X receptor(hPXR) plays a critical role in the metabolism, transport and clearance of xenobiotics in the liver and intestine. The hPXR can be activated by a structurally diverse of drugs to initiat... The human pregnane X receptor(hPXR) plays a critical role in the metabolism, transport and clearance of xenobiotics in the liver and intestine. The hPXR can be activated by a structurally diverse of drugs to initiate clinically relevant drug-drug interactions. In this article, in silico investigation was performed on a structurally diverse set of drugs to identify critical structural features greatly related to their agonist activity towards h PXR. Heuristic method(HM)-Best Subset Modeling(BSM) and HM-Polynomial Neural Networks(PNN) were utilized to develop the linear and non-linear quantitative structure-activity relationship models. The applicability domain(AD) of the models was assessed by Williams plot. Statistically reliable models with good predictive power and explain were achieved(for HM-BSM, r^2=0.881, q^2_(LOO)=0.797, q^2_(EXT)=0.674; for HM-PNN, r^2=0.882, q^2_(LOO)=0.856, q^2_(EXT)=0.655). The developed models indicated that molecular aromatic and electric property, molecular weight and complexity may govern agonist activity of a structurally diverse set of drugs to h PXR. 展开更多
关键词 human pregnane X receptor agonist activity heuristic method-Best subset Modeling heu ristic method-Polynomial Neural Networks structural features quantitative structure-activity relation ship
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