默认模式网络与阿尔茨海默病

默认模式网络（default-mode network,DMN）是由在脑处于静息状态时相互联系、维持健康代谢活动的若干脑区组成的网络,主要包括楔前叶/后扣带回皮质、顶下小叶、内侧前额叶皮层的背侧和腹侧、内侧颞叶以及海马等脑区,在个体从事如自传性记忆提取、监控外界环境以及控制自身心理状态等多种事务中发挥着重要作用,且与记忆有关的结构被证实是DMN的核心成分。现已有研究表明DMN功能障碍可能会诱导β-淀粉样蛋白沉积形成老年斑,并最终导致阿尔茨海默病（Alzheimer’s disease,AD）的发病。因此,越来越多的学者将研究的重心放在了DMN功能障碍与AD发病的关系上。本文就近年来有关DMN组成、功能特别是与AD发病关系的研究作一简要回顾。     

基于纤维束追踪空间统计的内侧颞叶癫痫患者弥散张量成像研究

本研究通过分析磁共振弥散张量成像(diffusion tensor imaging,DTI)数据,观察内侧颞叶癫痫(mesial temporal lobe epilepsy,mTLE)患者大脑白质的改变。46例伴有单侧海马硬化的内侧颞叶癫痫患者(24例左侧颞叶癫痫和22例右侧颞叶癫痫),以及42例年龄和性别匹配的正常志愿者纳入本研究。采用基于纤维束追踪的空间统计分析方法(track-based spatialstatistics,TBSS),主要观察患者各向异性系数(fractionsal anisotropy,FA)的变化。结果发现,与正常志愿者相比,左侧mTLE患者FA降低的区域呈双侧分布,稍偏向患侧,胼胝体、上纵束、下纵束、内囊前肢等白质双侧都有异常,而扣带束、下额枕束只在左脑显著降低;右侧mTLE患者FA降低主要见于右脑,包括胼胝体、上纵束、下纵束和钩束等。结果表明,基于TBSS方法的DTI研究揭示了伴有海马硬化的mTLE患者的脑白质异常,有助于加深对mTLE病理生理机制的了解。     

封面图片介绍

正脑默认网络(default mode network,DMN)是由在脑处于静息状态时相互联系、维持健康代谢活动的若干脑区组成的网络,主要包括楔后扣带回/前楔叶(PCC/Precuneus)、内侧前额叶(MPFC)、双侧角回(bilateral AG)、双侧外侧颞叶(bilateral lateral temporal cortex,LTC)、双侧海马(bilateral hippocampus,HIP)等脑区,在个体从事如监控外界环境、记忆提取和控制自身心理状态等多种事务中发挥着重要作用。脑默认网络与阿兹海     

创伤后应激障碍患者脑固有连接网络研究

采用静息态功能磁共振成像方法 ,探索创伤后应激障碍(post-trauma stress disorder,PTSD)患者脑固有网络的功能异常情况。应用独立成分分析方法,提取14名PTSD患者和性别年龄均匹配的14例健康被试的脑固有连接网络。两样本检验的结果显示,PTSD患者组较健康对照组的高级认知网络有不同程度的改变。其中,默认模式网络的后扣带回、楔前叶和右侧角回功能连接呈现降低趋势;背侧注意网络和自我参考网络的功能连接呈现升高趋势,主要包括左侧顶下小叶和内侧前额叶(P0.05)。静息态下PTSD患者高级认知网络脑区之间的连接效能异常可能同其认知功能损害有关,这些异常在PTSD的病理机制中可能发挥了重要作用。     

颞叶癫痫脑“默认模式”的fMRI研究

功能磁共振成像(functional magnetic resonance imaging,fMRI)被用于检测静息时脑功能神经网络.作者运用静息fMRI检测海马硬化颞叶癫痫(temporal lobe epilepsy,TLE)脑"默认模式",采用感兴趣区域功能连接分析检测16例TLE患者和16名正常对照静息时脑的"默认模式",并进行组内和组间分析.研究发现,与正常对照相比,TLE静息时海马、颞极、额叶、颞叶、壳核及楔前叶等脑区与后扣带回的功能连接增强.研究结果表明TLE患者的固有脑功能组织模式有可能出现紊乱.这一研究将有助于从脑功能的角度了解癫痫患者某些临床症状的发病机理,为今后癫痫诊治的发展提供一定的帮助.     

重度OSAS患者前额叶皮质及岛叶1H—MR波谱研究

目的：利用氢质子MRS（IH-MRS）探讨重度阻塞性呼吸睡眠暂停综合症（Severeobstructivesleepapneasyndrome,S-OSAS）患者前额叶皮质及岛叶脑代谢产物特征。方法：选择18例S-OSAS患者（S-OSAS组）和15名健康志愿者（HC组）行左侧前额叶皮质及岛叶1H-MRS检查,测量两组左侧前额叶皮质区及岛叶N-乙酰天冬氨酸／肌酸（NAA／Cr）、胆碱／肌酸（Cho／Cr）值。对患S-OSAS累计时间与前额叶皮质及岛叶NAA／Cr作直线相关分析。结果：与正常对照组相比,S-OSAS患者左侧前额叶皮质、岛叶NAA／Cr比值降低,分别为1．43±0．47、1．34±0．06,对照组分别为1．51±0．65、1．45±0．07;S-OSAS组患者左侧前额叶皮质、岛叶Cho／Cr分别为0．90±0．08、1．195：0．13,对照组分别为0．87±0．07、1．09±0．02,两组差异有统计学意义。前额叶皮质及岛叶代谢物NAA／Cr与患S-OSAS累计时间成负相关性（r值分别为-0．965、-0．955,P〈0．01）。结论：1H-MRS显示S-OSAS患者前额叶皮质及岛叶病理生理变化,从该区代谢物的改变反应出S-OSAS患者执行及情感功能的异常,其NAA/Cr改变程度与患S-OSAS累计时间相关。     

重度OSAS患者前额叶皮质及岛叶1H-MR波谱研究

目的:利用氢质子MRS(1H-MRS)探讨重度阻塞性呼吸睡眠暂停综合症(Severe obstructive sleep apnea syndrome,S-OSAS)患者前额叶皮质及岛叶脑代谢产物特征。方法:选择18例S-OSAS患者(S-OSAS组)和15名健康志愿者(HC组)行左侧前额叶皮质及岛叶1H-MRS检查,测量两组左侧前额叶皮质区及岛叶N-乙酰天冬氨酸/肌酸(NAA/Cr)、胆碱/肌酸(Cho/Cr)值。对患S-OSAS累计时间与前额叶皮质及岛叶NAA/Cr作直线相关分析。结果:与正常对照组相比,S-OSAS患者左侧前额叶皮质、岛叶NAA/Cr比值降低,分别为1.43±0.47、1.34±0.06,对照组分别为1.51±0.65、1.45±0.07;S-OSAS组患者左侧前额叶皮质、岛叶Cho/Cr分别为0.90±0.08、1.19±0.13,对照组分别为0.87±0.07、1.09±0.02,两组差异有统计学意义。前额叶皮质及岛叶代谢物NAA/Cr与患S-OSAS累计时间成负相关性(r值分别为-0.965、-0.955,P<0.01)。结论:1H-MRS显示S-OSAS患者前额叶皮质及岛叶病理生理变化,从该区代谢物的改变反应出S-OSAS患者执行及情感功能的异常,其NAA/Cr改变程度与患S-OSAS累计时间相关。     

基于动脉自旋标记技术的内侧颞叶癫痫病人脑血流灌注成像研究北大核心CSCD

基于动脉自旋标记(arterial spin labeling,ASL)技术,分析内侧颞叶癫痫(mesialtemporal lobe epilepsy,mTLE)患者大脑血流灌注(perfusion)的改变情况。在静息态下,采集了30例内侧颞叶癫痫伴单侧海马硬化发作间期患者(其中左侧16例,右侧14例)及22例健康志愿者的ASL数据,并通过计算获取其相对脑血流量(relative CBF,rCBF)及灌注不对称率(asymmetric index,AI)。癫痫病人与正常人的比较结果表明:左侧mTLE患者在两侧海马旁回、梭状回、额叶、颞叶和患侧海马回及岛叶,右侧mTLE患者在两侧海马回、海马旁回、额叶、颞叶和患侧杏仁核及岛叶,rCBF均有所下降,且患侧的下降程度和范围均大于对侧。说明mTLE患者的海马硬化可能导致了痫灶区功能异常,并通过癫痫的发作影响到全脑。     

基于动态因果模型研究盐酸哌甲酯对大脑默认网络效应连接的调制作用北大核心CSCD

本文基于静息态功能磁共振成像研究18名健康男性大学生志愿者在服用盐酸哌甲酯药物后大脑默认网络的效应连接变化。应用动态因果模型方法分析比较在服用安慰剂和盐酸哌甲酯药物两种条件下静息态默认网络的效应连接的区别。静息态的动态因果模型分析以文献研究提供的网络模型为先验基础,将低频波段信号（0.01~0.08 Hz）作为默认网络的驱动输入,再根据盐酸哌甲酯药物对节点间不同连接的调节作用设计32种动态因果可能性模型,最终通过拟合分析和贝叶斯模型选择得到最优模型及模型参数。结果表明,在静息条件下默认网络的内侧前额叶到后扣带回、两侧顶下小叶到内侧前额叶以及右侧顶下小叶到后扣带回的效应连接分别表现为促进状态,而左侧顶下小叶到后扣带回却表现为抑制连接。进一步地,根据盐酸哌甲酯药物与安慰剂条件的连接参数的配对统计比较发现,盐酸哌甲酯显著调节右侧顶下小叶到内侧前额叶皮质的连接（t=2.724,P=0.016）,使其由弱促进状态转变为抑制状态,但对其它连接无显著影响。本研究结果表明,盐酸哌甲酯药物对正常志愿者大脑静息态默认网络的效应连接具有显著的调制作用。     

基于动态因果模型研究盐酸哌甲酯对大脑默认网络效应连接的调制作用

本文基于静息态功能磁共振成像研究18名健康男性大学生志愿者在服用盐酸哌甲酯药物后大脑默认网络的效应连接变化。应用动态因果模型方法分析比较在服用安慰剂和盐酸哌甲酯药物两种条件下静息态默认网络的效应连接的区别。静息态的动态因果模型分析以文献研究提供的网络模型为先验基础,将低频波段信号(0.01~0.08 Hz)作为默认网络的驱动输入,再根据盐酸哌甲酯药物对节点间不同连接的调节作用设计32种动态因果可能性模型,最终通过拟合分析和贝叶斯模型选择得到最优模型及模型参数。结果表明,在静息条件下默认网络的内侧前额叶到后扣带回、两侧顶下小叶到内侧前额叶以及右侧顶下小叶到后扣带回的效应连接分别表现为促进状态,而左侧顶下小叶到后扣带回却表现为抑制连接。进一步地,根据盐酸哌甲酯药物与安慰剂条件的连接参数的配对统计比较发现,盐酸哌甲酯显著调节右侧顶下小叶到内侧前额叶皮质的连接(t=2.724,P=0.016),使其由弱促进状态转变为抑制状态,但对其它连接无显著影响。本研究结果表明,盐酸哌甲酯药物对正常志愿者大脑静息态默认网络的效应连接具有显著的调制作用。     

Recent advances in the study of Kaposi's sarcoma-associated herpesvirus replication and pathogenesis

It has now been over twenty years since a novel herpesviral genome was identified in Kaposi's sarcoma biopsies. Since then, the cumulative research effort by molecular biologists, virologists, clinicians, and epidemiologists alike has led to the extensive characterization of this tumor virus, Kaposi's sarcoma-associated herpesvirus(KSHV; also known as human herpesvirus 8(HHV-8)), and its associated diseases. Here we review the current knowledge of KSHV biology and pathogenesis, with a particular emphasis on new and exciting advances in the field of epigenetics. We also discuss the development and practicality of various cell culture and animal model systems to study KSHV replication and pathogenesis.     

A Unique Protease Cleavage Site Predicted in the Spike Protein of the Novel Pneumonia Coronavirus (2019-nCoV) Potentially Related to Viral Transmissibility

正Dear Editor,In December 2019, a novel human coronavirus caused an epidemic of severe pneumonia(Coronavirus Disease 2019,COVID-19) in Wuhan, Hubei, China(Wu et al. 2020; Zhu et al. 2020). So far, this virus has spread to all areas of China and even to other countries. The epidemic has caused 67,102 confirmed infections with 1526 fatal cases     

Curcuminoids as inhibitors of thioredoxin reductase: A receptor based pharmacophore study with distance mapping of the active site

Curcumin is the yellow pigment of turmeric that interacts irreversibly forming an adduct with thioredoxin reductase (TrxR), an enzyme responsible for redox control of cell and defence against oxidative stress. Docking at both the active sites of TrxR was performed to compare the potency of three naturally occurring curcuminoids, namely curcumin, demethoxy curcumin and bis-demethoxy curcumin. Results show that active sites of TrxR occur at the junction of E and F chains. Volume and area of both cavities is predicted. It has been concluded by distance mapping of the most active conformations that Se atom of catalytic residue SeCYS498, is at a distance of 3.56 from C13 of demethoxy curcumin at the E chain active site, whereas C13 carbon atom forms adduct with Se atom of SeCys 498. We report that at least one methoxy group in curcuminoids is necessary for interation with catalytic residues of thioredoxin. Pharmacophore of both active sites of the TrxR receptor for curcumin and demethoxy curcumin molecules has been drawn and proposed for design and synthesis of most probable potent antiproliferative synthetic drugs.     

Comparative morphology of the carpel in the Liliaceae: Hewardieae, Petrosavieae, and Tricyrteae

The young pistils in the melanthioid tribes, Hewardieae, Petrosavieae and Tricyrteae, are uniformly tricarpellate and syncarpous. They lack raphide idioblasts. All are multiovulate, with bitegmic ovules. The Petrosavieae are marked by the presence of septal glands and incomplete syncarpy. Tepals and stamens adhere to the ovary in the Hewardieae and the Petrosavieae but not in the Tricyrteae. Two vascular bundles occur in the stamens of the Hewartlieae and Tricyrtis latifolia. Ventral bundles in the upper part of the ovary of the Hewardieae are continuous with compound septal bundles and placental bundles in the lower part. Putative ventral bundles occur in the alternate position in the Tricyrteae and putative placental bundles in the opposite. position in the Petrosavieae. The dichtomously branched stigma in each carpel of the Tricyrteae is supplied by a bifurcated dorsal bundle.     

Synthesis and antimicrobial studies of hydrazone derivatives of 4-[3-(2,4-difluorophenyl)-4-formyl-1H-pyrazol-1-yl]benzoic acid and 4-[3-(3,4-difluorophenyl)-4-formyl-1H-pyrazol-1-yl]benzoic acid

Microbial resistance to antibiotics is an unresolved global concern, which needs urgent and coordinated action. One of the guidelines of the Centers for Disease Control and Preventions (CDC) to combat antibiotic resistance is the development of new antibiotics to treat drug-resistant bacteria. In our effort to find new antibiotics, we report the synthesis and antimicrobial studies of 30 new pyrazole derivatives. These novel molecules have been synthesized by using readily available starting materials and benign reaction conditions. Some of these molecules have shown activity with MIC values as low as 0.78?µg/mL against four bacterial strains; Staphylococcus aureus, methicillin-resistant S. aureus, Bacillus subtilis, and Acinetobacter baumannii. Furthermore, active molecules are non-toxic to mammalian cell line.

     

Novel compounds with potent CDK9 inhibitory activity for the treatment of myeloma

Cyclin-dependent kinases (CDKs) and Polo-like kinases (PLKs) play key role in the regulation of the cell cycle. The aim of our study was originally the further development of our recently discovered polo-like kinase 1 (PLK1) inhibitors. A series of new 2,4-disubstituted pyrimidine derivatives were synthesized around the original hit, but their PLK1 inhibitory activity was very poor. However the novel compounds showed nanomolar CDK9 inhibitory activity and very good antiproliferative effect on multiple myeloma cell lines (RPMI-8226).