Investigating the Mechanisms of Bisdemethoxycurcumin in Ulcerative Colitis: Network Pharmacology and Experimental Verification

Ulcerative colitis is a chronic inflammatory bowel disorder that is hard to cure once diagnosed. Bisdemethoxycurcumin has shown positive effects on inflammatory diseases. However, the underlying bioactive interaction between bisdemethoxycurcumin and ulcerative colitis is unclear. The objective of this study was to determine the core target and potential mechanism of action of bisdemethoxycurcumin as a therapy for ulcerative colitis. The public databases were used to identify potential targets for bisdemethoxycurcumin and ulcerative colitis. To investigate the potential mechanisms, the protein-protein interaction network, gene ontology analysis, and Kyoto encyclopedia of genes and genomes analysis have been carried out. Subsequently, experimental verification was conducted to confirm the findings. A total of 132 intersecting genes of bisdemethoxycurcumin, as well as ulcerative coli-tis-related targets, were obtained. SRC, EGFR, AKT1, and PIK3R1 were the targets of highest potential, and the PI3K/Akt and MAPK pathways may be essential for the treatment of ulcerative colitis by bisdemethoxycurcumin. Molecular docking demonstrated that bisdemethoxycurcumin combined well with SRC, EGFR, PIK3R1, and AKT1. Moreover, the in vitro experiments suggested that bisdemethoxycurcumin might reduce LPS-induced pro-inflammatory cytokines levels in RAW264.7 cells by suppressing PI3K/Akt and MAPK pathways. Our study provided a comprehensive overview of the potential targets and molecular mechanism of bisdemethoxycurcumin against ulcerative colitis. Furthermore, it also provided a theoretical basis for the clinical treatment of ulcerative colitis, as well as compelling evidence for further study on the mechanism of bisdemethoxycurcumin in the treatment of ulcerative colitis.     

Prolonged lifespan of initial-anode-free lithium-metal battery by pre-lithiation in Li-rich Li2Ni0.5Mn1.5O4 spinel cathode

Anode-free lithium metal batteries (AF-LMBs) can deliver the maximum energy density. However, achieving AF-LMBs with a long lifespan remains challenging because of the poor reversibility of Li⁺ plating/stripping on the anode. Here, coupled with a fluorine-containing electrolyte, we introduce a cathode pre-lithiation strategy to extend the lifespan of AF-LMBs. The AF-LMB is constructed with Li-rich Li₂Ni_0.5Mn_1.5O₄ cathodes as a Li-ion extender; the Li₂Ni_0.5Mn_1.5O₄ can deliver a large amount of Li⁺ in the initial charging process to offset the continuous Li⁺ consumption, which benefits the cycling performance without sacrificing energy density. Moreover, the cathode pre-lithiation design has been practically and precisely regulated using engineering methods (Li-metal contact and pre-lithiation Li-biphenyl immersion). Benefiting from the highly reversible Li metal on the Cu anode and Li₂Ni_0.5Mn_1.5O₄ cathode, the further fabricated anode-free pouch cells achieve 350 W h kg⁻¹ energy density and 97% capacity retention after 50 cycles.

Benefiting from highly reversible structure evolution of pre-lithiated Li-rich Li₂Ni_0.5Mn_1.5O₄ cathode, the corresponding anode-free pouch cell delivers a considerable energy density of 350 W h kg⁻¹ and 97% capacity retention after 50 cycles.     

基于天气数值预报模式预报高空光学湍流

介绍了天气数值预报模式的运行流程、模式安装、模拟参数设置等。结合光学湍流的参数化方案,预报了大气光学湍流强度廓线,并与探空气球实测数据对比验证。结果表明,预报的大气光学湍流强度廓线符合高空光学湍流的一般特征和变化规律,但廓线的形状与实测存在一定的差异,并分析产生差异的原因。分析表明,提高预报精度需要改进高空湍流外尺度模式。     

用于电磁驱动实验装置CQ-7的多间隙气体开关

基于电磁驱动实验装置CQ-7研制需求,设计了一套6间隙气体开关,开关高131 mm,直径108 mm,总间隙36 mm,开关电感约40 nH。采用模拟软件Ansoft Maxwell计算分析开关电场强度分布,电场分布较均匀,不均匀系数为1.14。开展了开关放电特性研究,充电100 kV条件下,开关放电电流峰值可达70 kA,放电延时约35 ns,抖动3 ns。根据开关自击穿电压值,采用正态分析开关自击穿概率,开关80%安全系数下,自放电概率小于10-4。该开关满足CQ-7实验装置研制需求。     

无光滤波六倍频微波信号产生的系统设计

基于两个级联偏振调制器,提出了一种高频谱纯度、稳定的六倍频微波信号产生方法。该方法通过适当调整偏振片的偏振方向、射频驱动信号电压和相位,实现无光滤波器条件下、任何波段六倍频微波信号的产生。利用Optisystem平台搭建的仿真系统,以S波段4 GHz信号为例,验证了该设计系统产生的六倍频信号质量,并分析了非理想射频驱动电压和相位对六倍频信号质量的影响,结果表明：该设计系统能产生最大光边带抑制比、射频无杂散抑制比分别为21.3,15.2 dB的六倍频微波信号;且非理想驱动电压和相位差的偏离应控制在理想值5%的范围之内。     

氢氧化铝/环氧树脂复合材料的电荷衰减特性

环氧树脂电气绝缘性能优良, 但是其在脉冲功率设备中充当绝缘子时, 表面容易带电且不易衰减, 当表面电荷集聚到一定的程度会造成局部放电甚至发展为沿面闪络。为了提高环氧树脂的沿面闪络性能, 用中心粒径为1 m的氢氧化铝(ATH)无机填料来改善环氧树脂复合材料的表面性能。分别制备了ATH填料质量分数为0%(纯环氧) , 20%, 40%, 60%, 80%和100%的ATH/环氧树脂复合材料试样。用电声脉冲法研究了ATH填料对环氧树脂复合材料电荷衰减性能的影响, 对比了试样直流极化场强为10 kV/mm和30 kV/mm的试验结果。结果表明：ATH/环氧树脂复合材料电荷的衰减常数不仅与填料的质量分数有关, 而且与试样的带电量有关。     

热稳定单原子催化剂的理性构筑:从原子级结构到实际应用

80%以上的工业生产过程涉及催化,如化工生产、能源转换、制药和废物处理等等.催化剂的使用显著提高了生产效率,降低了生产成本,为国民经济、地球环境和人类文明的可持续发展做出了很大贡献.为了满足日益增长的生产需求和最大的经济效益,开发高效、稳定、低成本的新型催化剂已成为当务之急.金属中心负载在载体上的负载型金属催化剂因其较好的催化活性和相对较低的金属用量而受到广泛关注.研究发现,负载型结构可增强传热和传质并增加活性金属中心的分散度,从而影响催化性能.此外,负载金属的颗粒尺寸对催化剂的性能有很大影响.迄今为止,科学家们一直在通过减小金属颗粒尺寸和提高原子利用效率来提高催化剂的活性.原子级尺寸的颗粒通常表现出与大尺寸颗粒显着不同的物理和化学性质,而当活性位点的尺寸缩小到单个原子时,单原子催化剂的概念应运而生.对于单原子催化剂,金属原子中心通过配位被载体中的缺陷锚定,从而调整金属原子的电子云分布.这种配位调整使得单原子催化剂拥有与传统催化剂不同的性能.作为催化领域的新前沿,单原子催化剂已经在许多催化反应中表现出前所未有的活性和选择性.然而,许多报道的单原子催化剂在高温环境或长期催化应用中容易受到奥斯特瓦尔德熟化过程的影响,从而导致催化剂烧结和失活.而烧结的原因在于金属原子和载体之间较弱的相互作用.失活催化剂的再生和回收将大大增加工业生产的时间和经济成本.因此,开发具有优异热稳定性的单原子催化剂以满足工业需求是十分必要的.本综述首先总结了近年来关于热稳定型单原子催化剂合成方法的基础研究,并从原子尺度上分析了这些方法所构建的金属中心的结构形态和配位环境.此外,结合近些年的研究中新的表征技术与理论计算手段解释了热稳定性的来源.重点讨论了热稳定单原子催化剂的实际催化应用.分析了热稳定单原子催化剂在热催化应用中的独特作用机理、并尝试为确定催化过程中真正的活性中心以及通过原子级调控手段进行高活性热稳定单原子催化剂的合成提供理论指导.最后总结了热稳定单原子催化剂发展的主要问题,并简要分析了单原子催化领域的研究挑战和发展前景.     

Purification Process and In Vitro and In Vivo Bioactivity Evaluation of Pectolinarin and Linarin from Cirsium japonicum

Pectolinarin and linarin are two major flavone O-glycosides of Cirsium japonicum, which has been used for thousands of years in traditional Chinese medicine. Pharmacological research on pectolinarin and linarin is meaningful and necessary. Here, a process for the purification of pectolinarin and linarin from C. japonicum was established using macroporous resin enrichment followed by prep-HPLC separation. The results show the purity of pectolinarin and linarin reached 97.39% and 96.65%, respectively. The in vitro bioactivities result shows the ORAC values of pectolinarin and linarin are 4543 and 1441 µmol TE/g, respectively, meanwhile their inhibition rate of BSA-MGO-derived AGEs is 63.58% and 19.31% at 2 mg/mL, which is 56.03% and 30.73% in the BSA-fructose system, respectively. The COX-2 inhibition rate at 50 µg/mL of linarin and pectolinarin reached 55.35% and 40.40%, respectively. Furthermore, the in vivo bioassay combining of histopathologic evaluation and biochemical analysis of liver glutamic oxaloacetic transaminase, serum creatinine and TNF-α show pectolinarin can alleviate lipopolysaccharide (LPS)-induced acute liver and kidney injury in mice. Metabolomics analysis shows that pectolinarin attenuates LPS-challenged liver and kidney stress through regulating the arachidonic acid metabolism and glutathione synthesis pathways. Collectively, our work presents a solid process for pectolinarin and linarin purification and has discovered a promising natural therapeutic agent—pectolinarin.     

Non-Covalent Dimer as Donor Chromophore for Constructing Artificial Light-Harvesting System in Water

Dynamic emissive materials in aqueous media have received much attention owing to their ease of preparation, tunable luminescence and environmental friendliness. However, hydrophobic fluorophores usually suffer from aggregation-caused quenching in water. In this work, we constructed an artificial light-harvesting system by using a non-covalent aggregation-induced emission dimer as antenna and energy donor. The dimer is quadruple hydrogen bonded from a ureidopyrimidinone derivative (M) containing a tetraphenylethylene group. The dispersed nano-assemblies based on the dimer in aqueous media were fabricated with the help of surfactant. By loading a hydrophobic acceptor molecule DBT into the nano-assemblies, man-made light-harvesting nanoparticles were fabricated, showing considerable energy transfer efficiency and a relatively high antenna effect. Additionally, the fluorescence color of the system can be gradually tuned by varying the content of the acceptors. This study provides a general way for the construction of an aqueous light-harvesting system based on a supramolecular dimer, which is important for potential application in luminescent materials.     

Efficient Degradation of Tetracycline Antibiotics by Engineered Myoglobin with High Peroxidase Activity

Tetracyclines are one class of widely used antibiotics. Meanwhile, due to abuse and improper disposal, they are often detected in wastewater, which causes a series of environmental problems and poses a threat to human health and safety. As an efficient and environmentally friendly method, enzymatic catalysis has attracted much attention. In previous studies, we have designed an efficient peroxidase (F43Y/P88W/F138W Mb, termed YWW Mb) based on the protein scaffold of myoglobin (Mb), an O₂ carrier, by modifying the heme active center and introducing two Trp residues. In this study, we further applied it to degrade the tetracycline antibiotics. Both UV-Vis and HPLC studies showed that the triple mutant YWW Mb was able to catalyze the degradation of tetracycline, oxytetracycline, doxycycline, and chlortetracycline effectively, with a degradation rate of ~100%, ~98%, ~94%, and ~90%, respectively, within 5 min by using H₂O₂ as an oxidant. These activities are much higher than those of wild-type Mb and other heme enzymes such as manganese peroxidase. As further analyzed by UPLC-ESI-MS, we identified multiple degradation products and thus proposed possible degradation mechanisms. In addition, the toxicity of the products was analyzed by using in vitro antibacterial experiments of E. coli. Therefore, this study indicates that the engineered heme enzyme has potential applications for environmental remediation by degradation of tetracycline antibiotics.