硒蛋白PP1(SEPP1)过表达抑制786-O和769-P人肾癌细胞增殖并引起G2/M期阻滞

目的构建硒蛋白PP1(SEPP1)基因的慢病毒质粒并研究SEPP1对人肾透明细胞癌细胞增殖的影响。方法以HEK293T细胞的c DNA为模板,通过PCR法获得人SEPP1全长序列片段,并与慢病毒表达载体p LV-EGFP(2A)Puro质粒相连接,获得重组p LV-EGFP(2A)Puro-SEPP1载体并进行基因测序验证。将重组慢病毒载体与包装质粒共同转染HEK293T细胞,进行病毒包装。用病毒上清感染786-O和769-P细胞,采用Western blot法检测SEPP1蛋白表达。按照重组慢病毒感染细胞、空载体感染细胞、未感染细胞进行分组,通过MTS法检测细胞增殖活性、细胞平板克隆形成实验检测克隆形成能力、流式细胞术检测细胞周期。结果酶切后凝胶电泳得到与SEPP1的DNA大小相一致的片段与空载体片段,基因测序的结果与SEPP1序列完全一致。经p LV-EGFP(2A)Puro-SEPP1感染的786-O、769-P细胞在感染48 h后,荧光显微镜下可见EGFP明显表达,实验组与空载体组、空白对照组相比较,SEPP1蛋白表达水平均明显提高。p LV-EGFP(2A)Puro-SEPP1感染组的细胞增殖能力降低,SEPP1过表达细胞集落形成能力明显降低,SEPP1过表达引起肾癌细胞G2/M期阻滞。结论在786-O和769-P细胞过表达SEPP1显著降低细胞增殖能力,并在786-O细胞中引起G2/M期阻滞。

预知子籽提取物抑制HepG2肝癌细胞增殖作用及对SEPP1等分子表达的影响

目的:观察中药预知子籽乙醇提取物(ATKS)对HepG2肝癌细胞增殖及对SEPP1等分子表达的影响。方法:将不同浓度ATKS作用于HepG2细胞24h、48h、72h,MTT法检测HepG2细胞的细胞存活率;相差倒置显微镜下观察药物作用72h后的细胞形态;RT-qPCR方法检测SEPP1等6个基因表达量的变化;Western Blot方法检测SEPP1蛋白水平变化。结果:ATKS作用后,HepG2细胞增殖被抑制,并存在量效和时效关系,其中72h细胞半数抑制浓度为2.0mg/ml;较低浓度对细胞形态影响较小,随着浓度增加细胞数量逐渐减少,2.4 mg/ml以上细胞数量锐减,状态变差,药物细胞毒作用凸显;2.0 mg/ml作用72h后,SEPP1基因表达被显著下调,其上游基因CAPNS1、ITGA2、ITGAV、ITGB1、ITGB5却一致上调;SEPP1蛋白表达量也出现显著下降。结论:ATKS能抑制HepG2肝癌细胞增殖,并具有量效和时效关系;SEPP1等基因和蛋白表达量发生变化,可能与ATKS的抑制作用有关。

SEPP1基因与肿瘤研究进展

综述近10多年硒蛋白P(SEPP1)基因与肿瘤的研究进展,主要从血SEPP1蛋白水平与肿瘤发病风险的相关性、血DNA中SEPP1基因多态性与肿瘤遗传易感性、组织中SEPP1基因或蛋白表达变化及机制等三方面进行归纳。首先,血SEPP1蛋白水平低,推测与肿瘤慢性应激条件下肝脏及相关组织该基因表达受到抑制有关,但血SEPP1蛋白主要来源于肝脏分泌,与肿瘤组织本身直接关系并不大;其次,多种肿瘤发生后,SEPP1基因单核苷酸多态性(SNP)多见,可能会在一定程度上使其表达受限,从而与血中蛋白水平变化呈现一致性,这可能属于非特异性改变,但同时也能反映部分基因易感人群特征。再次,肿瘤组织中SEPP1基因或蛋白表达以下降居多,机制多围绕抗氧化展开,但部分机制仍待阐明。此外在后续研究中,可尝试关注SEPP1与免疫、肿瘤细胞的侵袭和转移等诸方面。

神经损伤诱导蛋白1在诱导细胞质膜破裂中的作用

细胞质膜破裂(plasma membrane rupture,PMR)是细胞程序性死亡的最后一步,这一过程会将细胞内容物(包括促炎细胞因子和损伤相关分子模式(damage-associated molecular patterns,DAMPs)等)释放到细胞外环境,引发或放大炎症反应。最新研究发现神经损伤诱导蛋白1(nerve injury-induced protein 1,NINJ1)是多种程序性细胞死亡中质膜破裂(plasma membrane rupture,PMR)的关键介质。本综述结合最新研究成果,聚焦于NINJ1在细胞死亡方面的关键作用,探讨NINJ1的分子结构、功能及在炎症性疾病中作为治疗靶点的潜在应用。非激活态的NINJ1具有多个α-螺旋结构,包括两个跨膜α-螺旋结构及游离在胞外的N端(1-78,包含α-螺旋结构)结构域。当NINJ1被激发后能发生寡聚并使处于胞外的α-螺旋结构插入细胞膜,从而引发细胞质膜破裂。根据已解析的NINJ1激活态分子结构,已提出2种不同的NINJ1诱发细胞质膜破裂分子机制,一种是NINJ1形成环状或拉链结构,通过其内部亲水结构切割细胞膜,另一种NINJ1也形成环状结构,但其亲水区在环外会将NINJ1跟细胞膜一起切掉。同属Ninjurin家族的NINJ2与NINJ1在结构上高度相似,却不能介导质膜破裂,揭示细微的结构差异即可改变NINJ1的溶膜功能。通过阻止NINJ1介导的质膜破裂,可减轻炎症反应。未来的研究可能会集中在开发针对NINJ1的抑制剂,以期通过调控其功能来治疗相关的炎症性疾病。

男性不育症患者血清及精浆IL-38、Ang-1水平与精液质量的相关性研究

目的探索男性不育症患者血清及精浆中白介素-38(IL-38)、血管紧张素-1(Ang-1)表达水平,并分析其与精液质量的相关性。方法选取2021年4月至2023年4月浙江中医药大学附属温州市中医院收治的108例男性不育症患者作为研究对象,依据精液质量分为少弱精子组(n=61)和正常精子组(n=47)。采用Pearson法分析患者血清及精浆IL-38、Ang-1水平与精液质量的相关性。结果少弱精子组患者精液质量及精浆果糖、中性α-葡糖苷酶(NAG)表达水平低于正常精子组,精浆IL-38及Ang-1表达水平高于正常精子组(P<0.05);男性不育症患者血清及精浆IL-38、Ang-1表达水平与精液质量及精浆果糖、NAG水平呈负相关。结论男性不育症少弱精子患者血清及精浆IL-38、Ang-1水平高于正常精子患者,且IL-38、Ang-1水平与精液质量相关。

鸡Sepp1基因及其蛋白理化性质和分子结构的生物信息学分析

硒是人和动物生命必需的微量元素,硒的生物学功能是通过硒蛋白来实现的,硒蛋白P(Selenoprotein P,Sepp1)是机体含量最多的硒蛋白。利用生物信息学相关分析软件和比较基因组学的方法,对鸡Sepp1基因序列和氨基酸序列进行理化性质和结构特征进行分析和预测,并与猪、人、鼠、羊、狗等物种进行比较。结果显示,鸡Sepp1的CDS序列和编码的蛋白质与禽类动物相似,但和哺乳类动物之间差别较大;Sepp1的功能特性与硒半胱氨酸含量有关,不同物种Sepp1中硒半胱氨酸含量存在着差异;鸡Sepp1蛋白在第170-200位氨基酸残基区域具有特定理化性质和分子结构,推测该序列可作为调控鸡Sepp1功能的靶位点。研究结果为以后深入研究鸡Sepp1的机体功能、开发富集Se的动物功能性食品提供理论参考。

基于悬浮液等离子喷涂的Ba(Mg_(1/3)Ta_(2/3))O_(3)悬浮液制备及涂层组织结构

【目的】常规大气等离子喷涂制备新型热障涂层陶瓷层候选材料Ba(Mg_(1/3)Ta_(2/3))O_(3)(BMT)涂层应变容限较低。【方法】基于悬浮液等离子喷涂技术(SPS),以乙醇为分散介质,聚丙烯酸(PAA)、聚乙烯亚胺(PEI)和聚乙二醇(PEG)为分散剂,借助机械球磨制备了不同成分配比的BMT悬浮液。通过重力沉降观察法、紫外-可见分光光度计、Zeta电位仪对悬浮液的分散行为进行了研究,分析了分散剂种类及添加量对BMT悬浮液稳定性的影响;并利用SPS沉积了BMT涂层,对涂层的物相结构、表面形貌和截面组织进行了表征分析。【结果】结果表明:分散剂PEI在BMT颗粒表面吸附能够提高其Zeta电位,增强颗粒间斥力,并提供空间位阻作用,相比PAA和PEG,BMT悬浮液可以获得更好的分散效果。同时,添加PEI的BMT悬浮液黏度较低(介于1.5~2mPa·s),适用于SPS.由SPS制备的BMT涂层基本维持了BMT的物相结构,涂层呈现明显的柱状晶组织,且随悬浮液固含量的提高,涂层沉积效率增加,所形成的柱状晶体积更大,符合高应变容限涂层的组织结构特征。

PMCA1-4及其A端和C端剪接变异体在成年大鼠前庭组织中的表达

目的研究质膜钙ATP酶异构体1-4(plasma membrane Ca^(2+)-ATPase 1-4,PMCA1-4)在成年大鼠前庭组织的分布部位,及其A端和C端剪接变异体的表达类型。方法选择8周龄健康SD大鼠,解剖出内耳器官行前庭切片,同时取前庭椭圆囊斑和球囊斑提取总RNA。通过免疫荧光方法检测PMCA1-4在成年大鼠内耳前庭组织的表达部位,通过逆转录聚合酶链反应(RT-PCR)法检测PMCA1-4的A端和C端剪接变异体在成年大鼠前庭组织的表达类型。结果球囊和椭圆囊荧光染色切片中,于毛细胞和支持细胞的胞体外侧膜可见PMCA1表达,毛细胞纤毛中可见PMCA2强表达,毛细胞和支持细胞的胞体外侧膜可见PMCA3弱表达,PMCA4几乎不表达。4种PMCA亚型在球囊表达的剪接体分别为PMCA1x/b、PMCA2w/b、PMCA3z/(a,b)和PMCA4x/b,它们在椭圆囊的表达类型与球囊相同。结论PMCA1-4在成年大鼠前庭器官的表达部位存在差异,这4种PMCA亚型的剪接体类型也各不相同。这种差异性可能是为了满足前庭组织和亚细胞结构域对Ca2+调节的特殊需求。

急性大血管闭塞性脑卒中桥接治疗后再灌注损伤sCD40L、ET-1、ICAM-1因子相关性研究

目的探讨血清细胞间黏附分子(ICAM-1)、内皮素-1(ET-1)、血浆可溶性CD40配体(sCD40L)与急性大血管闭塞性脑卒中桥接治疗后再灌注损伤的关系。方法选取湖南省脑科医院2021年12月至2022年12月间接受桥接治疗的急性大血管闭塞性脑卒中患者90例。按照术后是否出现再灌注损伤并发症进行分组,分为再灌注损伤组和未再灌注损伤组:运用ELISA法检测桥接治疗前和治疗开始后30 min、1h、2h、6h、24 h、5d的患者血清sCD40L、ICAM-1、ET-1的水平,并分析两组之间的差异以及治疗前后这3种因子水平的变化。结果治疗前再灌注损伤组和未再灌注损伤组患者血清中sCD40L、ICAM-1、ET-1水平比较差异无统计学意义(P>0.05)。未再灌注损伤组患者的治疗前及治疗后30 min、1 h、2h、6h、24 h、5d的血清中sCD40L、ICAM-1、ET-1水平随时间推移的变化急性大血管闭塞性脑卒中桥接治疗后再灌注损伤组患者的血清sCD40L、ICAM-1、ET-1水平增高,并且随时间推移逐渐升高。均不显著(P>0.05),各指标间无差异:再灌注损伤组患者治疗后各时间点血清中sCD40L、ICAM-1、ET-1水平均显著高于治疗前(均P<0.05),且在治疗后30 min、1h、2h、6 h、24 h、5d的时间点,患者血清中sCD40L、ICAM-1、ET-1水平均随时间变化而升高,不同时间亚组间比较差异均有统计学意义(~均P<0.05)。再灌注损伤组患者治疗后各时间点血清中sCD40L、ICAM-1、ET-1水平均高于未再灌注损伤组相同时间点(~均P<0.05)。结论急性大血管闭塞性脑卒中桥接治疗后再灌注损伤组患者的血清sCD40L、ICAM-1、ET-1水平增高,并且5d内随时间推移逐渐升高。

血清PAPP-A、PP13和sFlt-1/PlGF比值检测对子痫前期高危孕妇患病的预测价值

目的分析血清妊娠相关α血浆蛋白(PAPP-A)、胎盘蛋白13(PP13)和可溶性胎盘血管内皮生长因子受体-1(sFlt-1)/胎盘生长因子(PlGF)比值检测对子痫前期(PE)高危因素孕妇PE发生的预测价值。方法选取2021年3月至2023年3月合肥市第二人民医院收治的187例具有PE高危因素的孕妇,根据妊娠20周后是否发生PE分为患病组(28例)和未患病组(159例)。收集所有孕妇一般资料,并采用酶联免疫吸附试验检测所有孕妇血清PAPP-A、PP13、sFlt-1、PlGF水平,采用Pearson相关分析各指标的关系,绘制受试者工作特征(ROC)曲线评估各项指标对PE发生的预测价值。结果妊娠16周及分娩前患病组血清PAPP-A水平均低于未患病组,血清PP13水平均高于未患病组,sFlt-1/PlGF比值均高于未患病组,差异有统计学意义(t值介于4.198~8.173之间,P<0.05);患病组孕妇经干预治疗后血清PAPP-A水平升高,血清PP13水平降低,sFlt-1/PlGF比值降低,差异有统计学意义(t值介于2.024~3.671之间,P<0.05);血清PAPP-A水平与PP13、sFlt-1/PlGF比值均呈负相关性(r值分别为-0.836、-0.775,P<0.05),血清PP13水平与sFlt-1/PlGF比值呈正相关性(r=0.670,P<0.05);ROC分析结果显示,血清PAPP-A、PP13、sFlt-1/PlGF预测PE发生的曲线下面积(AUC)分别为0.810、0.805、0.798,均有一定的预测价值(P<0.05)。结论血清PAPP-A、PP13和sFlt-1/PlGF比值对PE高危因素孕妇发生PE有较高的预测价值。

circPVT1靶向调控miR-195-5p/SOX9轴影响结肠癌细胞增殖、凋亡及上皮间质转化

目的:探究环状RNA浆细胞瘤变体易位1(circPVT1)靶向调控微小RNA-195-5p(miR-195-5p)/性别决定区Y框蛋白9(SOX9)轴对结肠癌细胞增殖、凋亡及上皮间质转化(EMT)的影响。方法:体外培养人正常结肠上皮细胞NCM-460、人结肠癌细胞系(SW480、HCT116、HCT29、LOVO、SW620)至对数期,将SW480细胞分为对照组(正常培养SW480细胞不进行转染)、空载质粒组(转染空载质粒)、circPVT1沉默组[转染circPVT1小干扰RNA(siRNA)质粒]、miR-195-5p过表达组[转染miR-195-5p模拟物(mimics)质粒]、SOX9沉默组(转染SOX9 siRNA质粒)、circPVT1沉默+miR-195-5p低表达组(转染circPVT1 siRNA和miR-195-5p siRNA质粒)。各组转染相应质粒后培养48 h。荧光定量PCR法检测NCM-460细胞、人结肠癌细胞系(SW480、HCT116、HCT29、LOVO、SW620)和各组SW480细胞circPVT1、miR-195-5p、SOX9 mRNA的表达;噻唑蓝和流式细胞仪分别检测各组SW480细胞增殖和凋亡;蛋白印迹法检测各组SW480细胞SOX9、凋亡和EMT相关蛋白表达;双荧光素酶报告基因实验检测circPVT1与miR-195-5p、miR-195-5p与SOX9的靶向关系。结果:与NCM-460细胞比较,SW480细胞、HCT116细胞、HCT29细胞、LOVO细胞、SW620细胞中circPVT1、SOX9 mRNA表达显著升高,miR-195-5p表达显著降低(P<0.05);其中,SW480细胞中circPVT1、SOX9 mRNA表达最高,miR-195-5p表达最低;故选择SW480细胞进行后续实验。与对照组和空载质粒组比较,circPVT1沉默组circPVT1、SOX9 mRNA及蛋白表达显著降低,miR-195-5p表达显著升高(P<0.05);miR-195-5p过表达组miR-195-5p表达显著升高,SOX9 mRNA及蛋白表达显著降低(P<0.05);SOX9沉默组SOX9 mRNA及蛋白表达显著降低(P<0.05)。与对照组和空载质粒组比较,circPVT1沉默组、miR-195-5p过表达组、SOX9沉默组细胞增殖率、Bcl-2、Vimentin蛋白表达显著降低,凋亡率、Bax、E-cadherin蛋白表达显著升高(P<0.05)。与circPVT1沉默组比较,circPVT1沉默+miR-195-5p低表达组miR-195-5p、凋亡率、Bax、E-cadherin蛋白表达显著降低,SOX9 mRNA及蛋白、细胞增殖率、Bcl-2、Vimentin蛋白表达显著升高(P<0.05)。circPVT1与miR-195-5p、miR-195-5p与SOX9存在靶向调控关系。结论:沉默circPVT1可以靶向上调miR-195-5p表达,抑制SOX9表达,进而抑制SW480细胞增殖和EMT进程,促进其凋亡。

富血小板血浆治疗膝骨关节炎的临床疗效及对血清胃饥饿素、HMGB1水平的影响

目的 探讨富血小板血浆(PRP)治疗膝骨关节炎的临床疗效及对患者血清胃饥饿素、高迁移率族蛋白1(HMGB1)水平的影响。方法 选取2021年1月至2023年1月自贡市第一人民医院收治的膝骨关节炎患者106例为研究对象,根据治疗方法分为PRP治疗组和透明质酸治疗组,各53例。比较两组治疗效果及血清胃饥饿素、HMGB1水平。结果 PRP组治疗后1、3个月膝关节损伤及骨关节炎调查问卷(KOOS)评分、Lysholm评分、骨密度高于透明质酸组,差异有统计学意义(t=3.235、10.437、5.494、3.863、4.183、10.268,P<0.05);PRP组治疗后1、3个月胃饥饿素水平高于透明质酸组,差异有统计学意义(t=2.065、3.611,P<0.05);HMGB1水平低于透明质酸组,差异有统计学意义(t=2.193、6.146,P<0.05);PRP组治疗后1、3个月视觉模拟评分(VAS)评分低于透明质酸组,生活质量评价量表(SF-36)评分高于透明质酸组,差异有统计学意义(t=3.119、6.661、2.713、3.550,P<0.05);PRP组及透明质酸组总不良反应发生率分别为9.43%、13.21%,两组不良反应发生率比较差异无统计学意义(χ^(2)=0.376,P>0.05)。结论 PRP可以提高血清胃饥饿素水平,降低HMGB1水平,改善膝骨关节炎患者关节功能,缓解疼痛提高生活质量。

富血小板血浆联合膝痹1号方治疗寒湿痹阻型膝骨关节炎临床研究

目的 观察富血小板血浆(PRP)联合膝痹1号方治疗寒湿痹阻型膝骨关节炎的临床疗效。方法 将90例寒湿痹阻型膝骨关节炎患者随机分为A、B、C组,A组予以PRP关节腔内注射联合膝痹1号方治疗,B组单纯PRP关节腔注射治疗,C组膝痹1号方治疗。于治疗前及治疗1、3、6个月比较3组膝关节疼痛视觉模拟量表(VAS)评分、西安大略和麦克马斯特大学(WOMAC)骨关节炎指数量表评分、Lysholm量表评分、临床疗效。结果 治疗后,三组VAS评分比较,差异有统计学意义(P<0.05);与治疗前比较,三组VAS评分均降低(P<0.05);治疗3、6个月,A组VAS评分均低于B组(P<0.05);治疗6个月,A组VAS评分低于C组(P<0.05)。治疗后,三组WOMAC评分比较,差异有统计学意义(P<0.05);治疗1、3、6个月,A、C组WOMAC评分均低于治疗前(P<0.05),B组治疗6个月WOMAC评分低于治疗前(P<0.05);与B组比较,治疗后3、6个月,A组WOMAC评分均低于B组(P<0.05);与C组比较,治疗3、6个月,A组WOMAC评分均低于同期C组(P<0.05)。治疗后,三组Lysholm评分比较,差异有统计学意义(P<0.05);治疗3、6个月,三组Lysholm评分均高于治疗前(P<0.05);与B组比较,治疗3、6个月,A组Lysholm评分均高于同期B组(P<0.05);与C组比较,治疗3、6个月,A组Lysholm评分均明显高于同期C组(P<0.05)。A组治疗后临床总有效率86.67%,B组总有效率76.67%,C组总有效率73.33%,三组比较,差异有统计学意义(P<0.05)。结论 采用PRP关节腔注射联合膝痹1号方与单纯PRP关节腔注射、膝痹1号方治疗寒湿痹阻型膝骨关节炎,均能缓解膝关节疼痛和促进膝关节功能恢复,但联合治疗的疗效优于单一治疗。

Increased plasma galectin-1 correlates with advanced glycation end products and interleukin-1β in patients with proliferative diabetic retinopathy

Dear Editor,Galectin-1, one of galactoside-binding lectin family proteins, has been shown to regulate cell growth, migration, and proliferation, where it binds many receptors depending on their glycosylation profile, rather than its specific receptors.

Single-cell analysis of tumor microenvironment and cell adhesion reveals that interleukin-1 beta promotes cancer cell proliferation in breast cancer

Background: Triple-negative breast cancer(TNBC), which is so called because of the lack of estrogen receptors(ER), progesterone receptors(PR), and human epidermal growth factor receptor 2(HER2) receptors on the cancer cells, accounts for 10%–15% of all breast cancers. The heterogeneity of the tumor microenvironment is high.However, the role of plasma cells controlling the tumor migration progression in TNBC is still not fully understood.Methods: We analyzed single-cell RNA sequencing data from five HER2 positive, 12ER positive/PR positive, and nine TNBC samples. The potential targets were validated by immunohistochemistry.Results: Plasma cells were enriched in TNBC samples, which was consistent with validation using data from The Cancer Genome Atlas. Cell communication analysis revealed that plasma cells interact with T cells through the intercellular adhesion molecule 2–integrin–aLb2 complex, and then release interleukin 1 beta(IL1B), as verified by immunohistochemistry, ultimately promoting tumor growth.Conclusion: Our results revealed the role of plasma cells in TNBC and identified IL1B as a new prognostic marker for TNBC.

Recent advances in non-thermal plasma(NTP)catalysis towards C1 chemistry

C1 chemistrymainly involves the catalytic transformation of C1molecules(i.e.,CO,CO2,CH4 and CH3OH),which usually encounters thermodynamic and/or kinetic limitations.To address these limitations,non-thermal plasma(NTP)activated heterogeneous catalysis offers a number of advantages,such as relatively mild reaction conditions and energy efficiency,in comparison to the conventional thermal catalysis.This review presents the state-of-the-art for the application of NTP-catalysis towards C1 chemistry,including the CO2 hydrogenation,reforming of CH4 and CH3OH,and water-gas shift(WGS)reaction.In the hybrid NTP-catalyst system,the plasma-catalyst interactions aremultifaceted.Accordingly,this reviewalso includes a brief discussion on the fundamental research into themechanisms of NTP activated catalytic C1 chemistry,such as the advanced characterisation methods(e.g.,in situ diffuse reflectance infrared Fourier transform spectroscopy,DRIFTS),temperatureprogrammed plasma surface reaction(TPPSR),kinetic studies.Finally,prospects for the future research on the development of tailor-made catalysts for NTP-catalysis systems(which will enable the further understanding of its mechanism)and the translation of the hybrid technique to practical applications of catalytic C1 chemistry are discussed.

Development and Integration of a Data Acquisition System for SST-1 Phase-1 Plasma Diagnostics

Long pulse （of the order of 1000 s or more） SST-1 tokamak experiments demand a data acquisition system that is capable of acquiring data from various diagnostics channels without losing useful data （and hence physics information） while avoiding unnecessary generation of a large volume data. SST-1 Phase-1 tokamak operation has been envisaged with data acquisition of several essential diagnostics channels. These channels demand data acquisition at a sampling rate ranging from 1 kilo samples per second （KSPS） to 1 mega samples per second （MSPS）. Considering the technical characteristics and requirements of the diagnostics, a data acquisition system based on PXI and CAMAC has been developed for SST-1 plasma diagnostics. Both these data acquisition systems are scalable. Present data acquisition needs involving slow plasma diagnostics are catered by the PXI based data acquisition system. On the other hand, CAMAC data acquisition hardware meets all requirements of the SST-1 Phase-1 fast plasma diagnostics channels. A graphical user interface for both data acquisition systems （PXI and CAMAC） has been developed using LabVIEW application development software. The collected data on the local hard disk are directly streaming to the central server through a dedicated network for post-shot data analysis. This paper describes the development and integration of the data acquisition system for SST-1 Phase-1 plasma diagnostics. The integrated testing of the developed data acquisition system has been performed using SST-1 central control and diagnostics signal conditioning units. In the absence of plasma shots, the integrated testing of the data acquisition system for the initial diagnostics of SST-1 Phase-1 operation has been performed with simulated physical signals. The primary engineering objective of this integrated testing is to validate the performance of the developed data acquisition system under simulated conditions close to that of actual tokamak operation. The data acquisition is synchronized with a clock and trigger provided by the central timing system.

Shi-pi-xiao-ji formula suppresses hepatocellular carcinoma by reducing cellular stiffness through upregulation of acetyl-coA acetyltransferase 1

BACKGROUND Previous studies have shown that the Shi-pi-xiao-ji(SPXJ)herbal decoction formula is effective in suppressing hepatocellular carcinoma(HCC),but the underlying mechanisms are not known.Therefore,this study investigated whether the antitumor effects of the SPXJ formula in treating HCC were mediated by acetyl-coA acetyltransferase 1(ACAT1)-regulated cellular stiffness.Through a series of experiments,we concluded that SPXJ inhibits the progression of HCC by upregulating the expression level of ACAT1,lowering the level of cholesterol in the cell membrane,and altering the cellular stiffness,which provides a new idea for the research of traditional Chinese medicine against HCC.AIM To investigate the anti-tumor effects of the SPXJ formula on the malignant progression of HCC.METHODS HCC cells were cultured in vitro with SPXJ-containing serum prepared by injecting SPXJ formula into wild-type mice.The apoptotic rate and proliferative,invasive,and migratory abilities of control and SPXJ-treated HCC cells were compared.Atomic force microscopy was used to determine the cell surface morphology and the Young’s modulus values of the control and SPXJ-treated HCC cells.Plasma membrane cholesterol levels in HCC cells were detected using the Amplex Red cholesterol detection kit.ACAT1 protein levels were estimated using western blotting.RESULTS Compared with the vehicle group,SPXJ serum considerably reduced proliferation of HCC cells,increased stiffness and apoptosis of HCC cells,inhibited migration and invasion of HCC cells,decreased plasma membrane cholesterol levels,and upregulated ACAT1 protein levels.However,treatment of HCC cells with the water-soluble cholesterol promoted proliferation,migration,and invasion of HCC cells as well as decreased cell stiffness and plasma membrane cholesterol levels,but did not alter the apoptotic rate and ACAT1 protein expression levels compared with the vehicle control.CONCLUSION SPXJ formula inhibited proliferation,invasion,and migration of HCC cells by decreasing plasma membrane cholesterol levels and altering cellular stiffness through upregulation of ACAT1 protein expression.

A new discovered ABCA1 gene polymorphisms and the association of ABCA1 SNPs with coronary artery disease and plasma lipids in Chinese population

Single nucleotide polymorphisms （SNP） of ATP-binding cassette transporter A1 （ABCA1） gene are related to plasma lipid and susceptibility to coronary artery disease （CAD）. Our first goal was to screen all 50 coding regions of ABCA1 to find new SNPs. Our second goal was to investigate the frequency distribution of R1587K and M883I polymorphisms of ABCA1 gene, which are the variant occurred most frequently, in Chinese people and to evaluate their association with the CAD phenotype and plasma lipids. Methods： Single-strand conformation polymorphism （SSCP） and DNA sequence were used for confirming new SNP of ABCA1, and restriction fragment length polymorphism （RFLP） were applied for confirming genotypes of R1587K and M883I in 112 CAD cases and 108 healthy people. Results： We discovered a new ABCA1 SNP in Chinese population, which converse 233 amino acids from Methionine to Valine （M233V）. This new ABCA1 SNP located in exon7, and might potentially modulate the biological function of lipid metabolism. For R1587K and M883I SNPs, the K allele and I allele frequency was 28.9% and 31.1%, respectively. The K allele at R1587K conferred lower mean values of HDL-C in a dose-dependent manner in both CAD patients and healthy people. However, 883I allele was not associated with plasma lipid level. Neither 1587KK nor 883II associated with increased risk of CAD. Conclusion： Our study finds a potential functional ABCA1 SNPs and revealed K allele of R1587K associated decreased HDL-C level in Chinese population.

Experiments and Studies of Edge Plasma Radial Transport and Confinement Property on the HL-1M Tokamak

This paper describes a Mach/Langmuir probe array with five pins and six pins, which can measure not only parallel flows and the flow perpendicular to the magnetic field but also the radial and the poloidal electric field E. arid E as well. Experimental measurements of the edge fluctuations, velocities of the toroidal, the poloidal flow and electric field have been carried out on both of SOL and the boundary region of HL-1M for Ohmic, biased H-mode, Lower Hybrid Current Drive (LHCD), Supersonic Molecular Beam Injection (MBI), Multi-shot Pellet Injection (MPI), Neutral Beam Injection (NBI), Ion Cyclotron Resonance Heating (ICRH) and Electric Cyclotron Resonance Heating (ECRH) discharges. The results show that the suppressions of the fluctuations are related to poloidal rotations produced by different discharge modes in the improved particle confinement property, simultaneously the change of the radial and poloidal electric field is generated and becomes more negative at the Tokamak plasma edge, and the sheared poloidal flow is related to the reduction in fluctuation level, and the poloidal velocity is mainly dominated by the E × B drift.