Matching energy of unicyclic and bicyclic graphs with a given diameter

Gutman and Wagner proposed the concept of matching energy (ME) and pointed out that the chemical applications of ME go back to the 1970s. Let G be a simple graph of order n and be the roots of its matching polynomial. The ME of G is defined to be the sum of the absolute values of . In this article, we characterize the graphs with minimal ME among all unicyclic and bicyclic graphs with a given diameter d. © 2014 Wiley Periodicals, Inc. Complexity 21: 224–238, 2015     

Targeting tribbles homolog 3 (TRIB3) protein against type 2 diabetes for the identification of potential inhibitors by in silico screening

Tribbles homolog 3 (TRIB3) protein is inhibiting the insulin signaling by directly binding to the Akt/PKB leading to insulin resistance in the pancreas causing type 2 diabetes mellitus. Hence, TRIB3 protein is considered as a possible drug target for the new lead identification against type 2 diabetes. In the present study, the homology model of TRIB3 protein was generated to explore its biochemical function and molecular interactions in the new lead identification. The energy minimization of TRIB3 protein was carried out and evaluated by validation protocols for structure reliability. The druggable binding site of TRIB3 protein was identified for the virtual screening and molecular docking studies. The Asinex-fragments library of 22634 small molecules was docked at TRIB3 active site using the Glide module to identify new chemical entities. A total of 9 molecules were identified as final hits from virtual screening and their potency was ranked using Glide score, Glide energies, and residues interactions. The 6 prioritized lead molecules were further optimized using AutoDock, Prime MM/GBSA, and percentage of human oral absorption for the identification of potential leads. The molecules L2, L5, and L6 are identified as lead inhibitors and are showing consistent interactions with key residues Glu194 and Lys196 of TRIB3 protein. The identified potential leads were analyzed by ADME properties for their drug likeness and HergIC50 values are predicted for the prevention of preclinical failures. The present work sheds light on the identification of the best lead molecules against TRIB3 protein and offers a route to design as novel potential drug candidates for T2DM.     

Steering spatially separated dual sites on nano-TiO2 through SMSI and lattice matching for robust photocatalytic hydrogen evolution

Spatial isolation of different functional sites at the nanoscale in multifunctional catalysts for steering reaction sequence and paths remains a major challenge. Herein, we reported the spatial separation of dual-site Au and RuO₂ on the nanosurface of TiO₂ (Au/TiO₂/RuO₂) through the strong metal-support interaction (SMSI) and the lattice matching (LM) for robust photocatalytic hydrogen evolution. The SMSI between Au and TiO₂ induced the encapsulation of Au nanoparticles by an impermeable TiO_x overlayer, which can function as a physical separation barrier to the permeation of the second precursor. The LM between RuO₂ and rutile-TiO₂ can increase the stability of RuO₂/TiO₂ interface and thus prevent the aggregation of dual-site Au and RuO₂ in the calcination process of removing TiO_x overlayer of Au. The photocatalytic hydrogen production is used as a model reaction to evaluate the performance of spatially separated dual-site Au/TiO₂/RuO₂ catalysts. The rate of hydrogen production of the Au/TiO₂/RuO₂ is as high as 84 μmol h⁻¹ g⁻¹ under solar light irradiation without sacrificial agents, which is 2.5 times higher than the reference Au/TiO₂ and non-separated Au/RuO₂/TiO₂ samples. Systematic characterizations verify that the spatially separated dual-site Au and RuO₂ on the nanosurface of TiO₂ can effectively separate the photo-generated carriers and lower the height of the Schottky barrier, respectively, under UV and visible light irradiation. This study provides new inspiration for the precise construction of different sites in multifunctional catalysts.     

In silico virtual screening of potent inhibitor to hamper the interaction between HIV-1 integrase and LEDGF/p75 interaction using E-pharmacophore modeling,molecular docking,and dynamics simulations

The rapid increase of HIV-1 infection throughout the globe has a high demand for a superior drug with lesser side effects. LEDGF/p75, the human Lens Epithelium-Derived Growth Factor is identified as a promising cellular cofactor with integrase in facilitating the viral replication in an early stage by acting as a tethering factor in the pre-integration to the chromatin. Therefore, the present study was designed to identify a potent inhibitor by applying an E-pharmacophore based virtual screening, molecular docking, and dynamics simulation approaches. Finally, ZINC22077550 and ZINC32124441 were best identified potent molecules with the efficient binding affinity, strong hydrogen bonding, and acceptable pharmacological properties to hamper the interaction between integrase and LEDGF/p75. Further, the DFT and MDS studies were also analyzed, and shown a favorable energetic state and dynamic stability then reference compound. In conclusion, we suggest that these findings could be novel therapeutics in the future and may increase the lifespan of individuals suffering from viral infection.     

基于语义的软件服务故障自动诊断模型

模仿学习是机器人仿生机制研究的主要内容之一,即通过观察、理解、学习、模仿示教行为实现机器人的仿生特性。基于高斯过程分别表达采集离散示教信号所构成的示教轨迹和含有未知参数策略的模仿轨迹,构建模仿学习方法框架,将概率模型匹配引入到模仿学习中,以KL散度为代价函数比较两种轨迹的概率分布,运用梯度下降法寻求使KL散度最小的最优模仿控制策略,将策略应用于模仿机器人以完成与示教相同的模仿任务。以关节型机器人的机械臂摆动行为模仿为学习任务进行仿真,结果表明基于概率轨迹匹配的模仿学习方法能够实现机械臂摆动行为模仿,学习过程较传统方法简易且学习效果较好。     

基于机器视觉的车辆保险盒在线检测研究

摘要: 车辆保险盒作为汽车电控系统中的一个重要的元器件,其质量好坏直接影响汽车的性能,传统的车辆保险盒检测主要依靠人工检测,检测费时费力,针对该问题,提出一种基于视觉的车辆保险盒在线检测方法,分析了产品图像校正到标准模板图像的位置误差,采用SURF(Speeded Up Robust Feature)算法和平面单应性理论将待检产品图像变换到标准模板位置,利用颜色直方图匹配和模板匹配完成保险盒上元件的检测。实验结果证明,该方法检测效率高,稳定可靠,能够满足在线检测的要求,具有一定实用价值。     

基于非同步替代光谱定标的地表下垫面影响分析

对760nm附近的氧气吸收带,选用植被、枯萎植被、人工地物、沙地和雪地五种典型地表类型,基于模拟数据进行非同步替代光谱定标方法的误差分析,比较不同地表类型得到的光谱定标准确度,为高光谱成像仪的非同步替代光谱定标提供定标图像选择策略.结果表明:运用两种光谱匹配方法——光谱角度匹配和欧氏距离法得到的定标误差基本一致;730~800nm的地表反射率曲线标准差在0.05nm以内时,定标误差集中在±0.5nm范围内;人工地物类型中个别地物如橄榄绿光泽涂料和植被大面积覆盖的图像数据不适合用于非同步替代光谱定标.     

ω-芋螺毒素的定量构效关系与虚拟筛选

ω-芋螺毒素属于海洋生物活性多肽,由24-31个氨基酸残基组成.特异性作用于电压敏感的钙离子通道(VGCCs),能够直接开发成药物或作为先导化合物进行新药开发.本文应用新型氨基酸残基结构描述符cscales和遗传偏最小二乘算法,对ω-芋螺毒素进行定量构效关系(QSAR)研究,并设计、构建了容量为2244个化合物的N-型和P/Q-型VGCC拮抗剂虚拟组合多肽库,然后分别采用QSAR模型预测和相似性搜索方法对组合多肽库进行了虚拟筛选.研究结果表明,建立的N-型和P/Q-型VGCC拮抗剂QSAR模型均具有较好的预测能力,交叉验证相关系数(CV-r2)均大于0.89.主成分分析和聚类分析结果表明,虚拟组合多肽库中化合物具有较好的结构多样性和差异性.通过虚拟筛选,得到了具有高预测活性的6个N-型和19个P/Q-型钙离子通道拮抗剂,为进一步的合成和活性评价奠定了理论基础.同时,本文建立的多肽QSAR预测模型和虚拟筛选策略,为其它多肽类化合物的定量构效关系研究和虚拟筛选提供了参考.     

钛表面生物活性榍石/氧化钛复合涂层的结构和磷灰石形成机理(英文)

采用微弧氧化和热处理复合技术,在钛表面制备了具有双层结构的榍石/氧化钛复合涂层。榍石/氧化钛复合涂层的外层是由微弧氧化涂层经热处理后晶化生成;而内层是由钛基底的氧化生成,并且氧化钛表现出不同的Ti,O原子比。由于钛基底的氧化,孔径在50~500 nm的微孔呈层状结构分布在涂层内层。与微弧氧化涂层相比,该复合涂层具有很好的磷灰石诱导能力,这是由于榍石沿着特定晶面和晶向与羟基磷灰石表现出良好的晶体学匹配关系,从而为磷灰石的成核和取向沉积过程提供良好的位点。