牛胚系基因中两种JH和Cμ抗体基因的克隆与分析

根据NCBIGenBankTM中登录的2个牛抗体重链可变区J基因(JH)(序列号为AY158087,AY149283)的序列不同之处设计PCR引物,能从同一个体的Holstein牛基因组DNA中扩增得到与以上2个基因分别相同的序列,证明这2个JH基因的差异不是由于牛个体或品种不同引起的.提取牛脾脏总RNA,RT-PCR扩增IgMcDNA,测序结果显示:序列号为AY149283的JH基因中第六外显子JH6是一个功能基因,它可以编码牛IgM的部分CDR3区和完整的FR4区,从2种IgMcDNA克隆的测序结果可以看出,其恒定区序列分别与序列号为U63637和AY230207的2种抗体重链恒定区μ基因(Cμ)cDNA序列相同.PCR扩增JH-Cμ序列,测序结果表明:序列号为AY158087的JH基因是同以上2种Cμ基因分别串连在一起的(序列号分别为AY230207和U63637).以上结果证明:序列号为U63637和AY230207的2个Cμ基因分别与AY149283的JH基因串联在一起,都能够参与牛IgM的产生,它们与AY158087的JH基因共同存在于同一个体Holstein牛胚系基因中.

中国仓鼠卵巢上皮细胞PKCμ亚型的克隆与表达

【目的】研究中国仓鼠卵巢上皮细胞(Chinese Hamster Ovary Cell,CHO cell)是否表达蛋白激酶C(Protein Kinase C,PKC)μ亚型。【方法】参照GeneBank数据库PKCμ亚型的cDNA序列;通过EMBL-EBI数据库的CLUSTALW,选取种属间同源性最高的序列;利用GENERUNNER软件设计PKCμ亚型的特异引物;RT-PCR扩增CHO细胞PKCμ亚型的cDNA序列;利用AT克隆技术将PKCμ连接到pGEM-T载体上,经蓝白斑筛选,酶切鉴定后测序;Western blotting方法检测CHO细胞中PKCμ亚型。【结果】运用RT-PCR和Western blot-ting技术证实CHO细胞表达PKCμ亚型,并经测序证实。【结论】CHO细胞中发现PKCμ亚型的存在,为深入研究PKCμ亚型的结构、功能及与细胞内信号转导通路的关系奠定基础。

Linear 6通道逻辑／SPI／I^2CμModule隔离器

近日，凌力尔特公司（Linear Technology Corporation）推出6通道SPI／数字或I^2CμModule隔离器LTM2887，该器件面向低电压组件，包括较新的DSP和微处理器。两个经过良好稳压的可调电源轨（高达5V）越过隔离势垒提供大于100mA的负载电流，并具有高达62％的效率。

C反应蛋白/白蛋白比值对2型糖尿病合并急性心肌梗死患者远期不良心脑血管事件的预测价值研究

背景急性心肌梗死(AMI)是威胁全球公众健康的主要原因之一。虽然已有相应的再灌注治疗策略,但AMI相关的主要不良心脑血管事件(MACCEs)仍然是全世界人口死亡的原因之一。尤其合并糖尿病的AMI患者,因冠状动脉病变复杂,病变程度严重,尽早发现和判断该部分患者远期预后相对困难,因此寻找相对简便、易获得的实验室指标,有利于为2型糖尿病(T2DM)合并AMI患者经皮冠状动脉介入(PCI)术后MACCEs的预测提供依据。目的探讨血清C反应蛋白(CRP)/白蛋白(Alb)比值(CAR)对T2DM合并AMI患者PCI术后远期MACCEs的预测价值。方法纳入2014—2019年就诊于宁夏医科大学总医院心血管内科1683例T2DM合并AMI患者为研究对象,收集患者的一般临床资料与检查结果。对所有患者进行电话或门诊随访,以全因死亡、非致死性心肌梗死、再发不稳定型心绞痛、非致死性脑卒中、新发心力衰竭或心力衰竭加重再入院、再次血运重建作为MACCEs。根据患者随访期间是否发生MACCEs分为MACCEs组(508例)和非MACCEs组(1175例)。采用单因素及多因素Logistic回归分析探讨T2DM合并AMI患者MACCEs事件的影响因素。采用Kaplan-Meier法绘制患者的生存曲线,生存曲线的比较采用Log-rank检验。采用受试者工作特征(ROC)曲线分析CAR对T2DM合并AMI患者远期发生MACCEs的预测效能,使用净重分类改善指标(NRI)和综合判别指数(IDI)评价CAR对T2DM合并AMI患者预后评估的改善效果。结果1683例患者中508例(30.18%)患者发生MACCEs。多因素Logistic回归分析显示高血压病[OR(95%CI)=1.994(1.142~3.483)]、冠状动脉植入支架长度[OR(95%CI)=1.031(1.002~1.062)]、CRP[OR(95%CI)=0.950(0.915~0.986)]、Alb[OR(95%CI)=0.933(0.880~0.989)]及CAR[OR(95%CI)=5.582(1.705~18.277)]是T2DM合并AMI患者PCI术后发生MACCEs的影响因素(P<0.05)。根据CAR中位表达水平(0.86),将患者分为CAR<0.86组和CAR≥0.86组,Log-rank检验结果显示,CAR≥0.86组MACCEs发生率高于CAR<0.86组(52.68%与22.92%;χ^(2)=65.65,P<0.001)。ROC曲线显示CAR预测T2DM合并AMI患者发生MACCEs的ROC曲线下面积为0.728(95%CI=0.702~0.754),最佳截断值为0.576,灵敏度为0.617,特异度为0.747。在基线模型基础上,与CRP、Alb相比,CAR能明显改善对患者发生MACCEs的预测效果(NRI=0.377,IDI=0.166,C指数=0.690;P<0.05)。结论CAR是T2DM合并AMI患者PCI术后远期MACCEs发生风险的有效预测指标。

血清可溶性CD40配体、腱糖蛋白C、甲壳质酶蛋白-40联合检测对维持性血液透析并发心血管事件的预测作用

目的:探讨血清可溶性CD40配体(sCD40L)、腱糖蛋白C(TN-C)、甲壳质酶蛋白-40(YKL-40)联合检测对维持性血液透析(MHD)并发心血管事件的预测价值。方法:选择170例MHD患者为研究对象,依据不良心血管事件(MACE)发生情况分两组,即MACE组(n=63)和非MACE组(n=107),另选同期健康体检者为对照组(n=152)。比较各组血清sCD40L、TN-C、YKL-40水平,分析以上指标与MHD发生MACE的相关性及MHD并发MACE的危险因素,绘制受试者工作曲线(ROC)分析其预测价值。结果:MHD组血清sCD40L、TN-C、YKL-40水平高于对照组(均P<0.05)。MACE组的年龄、透析龄及血清sCD40L、TN-C、YKL-40水平高于非MACE组(均P<0.05)。MHD并发MACE与年龄、透析龄及血清sCD40L、TN-C、YKL-40水平呈正相关(均P<0.05)。多因素Logistic回归分析显示,MHD并发MACE的独立危险因素包括高水平sCD40L、TN-C、YKL-40以及高年龄和透析龄(均P<0.05)。血清sCD40L、TN-C、YKL-40单独及联合预测MHD并发MACE的AUC分别为0.701、0.679、0.754、0.875,联合预测价值最高,其次为YKL-40、sCD40L、TN-C(均P<0.05)。结论:MHD并发MACE患者血清sCD40L、TN-C、YKL-40水平有升高趋势,三者均为MACE发生独立危险因素,联合检测对MHD发生MACE有一定的预测价值。

SR9009联合吲哚丙酸通过核因子κB信号通路减轻C2C12成肌细胞的炎症反应

背景:钟基因Rev-erbα参与调节炎症,但激活Rev-erbα会增加心脑血管疾病风险。为降低相关风险,探索Rev-erbα激动剂SR9009联合其他药物来减轻骨骼肌成肌细胞炎症,奠定治疗炎症相关性骨骼肌萎缩的理论基础。目的:探讨脂多糖刺激C2C12成肌细胞时吲哚丙酸、SR9009与核因子κB信号通路的关系。方法:①1μg/mL脂多糖刺激C2C12成肌细胞,RNA转录组测序结合KEGG通路富集分析信号通路。②CCK-8法检测C2C12成肌细胞活性,筛选吲哚丙酸的最佳给药浓度;然后将细胞分为空白对照组、脂多糖(1μg/mL)组、SR9009(10μmol/L)+脂多糖组、吲哚丙酸(80μmol/L)+脂多糖组、吲哚丙酸+SR9009+脂多糖组,ELISA检测细胞上清液中白细胞介素6水平,RT-qPCR检测白细胞介素6、肿瘤坏死因子α、Toll样受体4、CD14 mRNA表达,Western blot检测NF-κB p65、p-NF-κB p65蛋白表达。③siRNA敲减Rev-erbα,RT-qPCR评估敲减效率,检测白细胞介素6、肿瘤坏死因子αmRNA表达。结果与结论:①与空白对照组比较,脂多糖时间依赖性抑制成肌细胞融合形成肌管,白细胞介素6、肿瘤坏死因子αmRNA表达水平升高,细胞上清液中白细胞介素6水平显著升高;KEGG通路分析支持脂多糖刺激激活核因子κB信号通路。②吲哚丙酸浓度>80μmol/L时抑制C2C12成肌细胞活性;吲哚丙酸和SR9009通过抑制核因子κB信号通路发挥抗炎作用,降低白细胞介素6、肿瘤坏死因子α、Toll样受体4、CD14 mRNA表达水平,p-NF-κB p65/NF-κB p65蛋白表达比值低于脂多糖组。SR9009联合吲哚丙酸显著降低脂多糖诱导的炎症,Toll样受体4、CD14、白细胞介素6和肿瘤坏死因子αmRNA表达水平进一步下调,p-NF-κB p65/NF-κB p65蛋白表达比值显著低于吲哚丙酸+脂多糖组和SR9009+脂多糖组。③Rev-erbα随脂多糖刺激时间依赖性升高;siRNA敲减Rev-erbα效率达58%以上,成功敲减Rev-erbα后添加脂多糖,白细胞介素6和肿瘤坏死因子αmRNA表达较脂多糖组显著上调。④结果说明,Rev-erbα可以作为调节炎症反应的靶点,SR9009靶向激活Rev-erbα联合吲哚丙酸能抑制核因子κB信号通路显著减轻C2C12成肌细胞的炎症反应,联合抗炎效果优于单独干预。

骨髓间充质干细胞来源的外泌体抑制地塞米松诱导的C2C12肌管萎缩

目的研究骨髓间充质干细胞(bone marrow mesenchymal stem cells,BMSCs)来源的外泌体(exsomes,EXOs)对地塞米松(dexamethasone,DEX)诱导的C2C12肌管萎缩的影响。方法(1)分离提取培养C57BL/6J小鼠BMSCs。(2)提取并鉴定BMSCs-EXOs。(3)C2C12细胞成肌分化。(4)将肌管细胞分为对照组(Control,2%马血清培养基培养48 h)、地塞米松组(DEX、浓度为10μmol·L^(-1)的DEX干预肌管48 h)、外泌体组(EXOs、外泌体干预肌管48 h)、外泌体抑制剂组(GW4869、10μmol的GW4869干预BMSCs后提取的外泌体干预肌管48 h)。48 h后测量各组肌管直径,CCK-8法检测各组细胞活力,Western blot检测各组肌肉萎缩及成肌分化相关蛋白的表达量。结果BMSCs呈长梭形,BMSCs-EXOs在透射电镜下为圆形的双层膜结构,直径约200 nm,且高表达CD9、CD63和CD81。相比于Control组,DEX组细胞活性降低(P<0.01),肌管细胞直径减少(P<0.01),atrogin-1(P<0.05)和MuRF-1(P<0.01)的表达明显上调,MYOD(P<0.01)蛋白表达降低;相比于DEX组,BMSCs-EXOs组细胞活性升高(P<0.01),肌管细胞直径增加(P<0.01),atrogin-1(P<0.05)和MuRF-1(P<0.01)的表达明显下调,MYOD(P<0.01)蛋白表达升高;相比于BMSCs-EXOs组,BMSCs-EXOs(GW4869)组细胞活性降低(P<0.05),肌管细胞直径减少(P<0.01),atrogin-1(P<0.05)和MuRF-1(P<0.05)的表达上调,MYOD(P<0.01)蛋白表达降低。结论骨髓间充质干细胞来源的外泌体(BMSCs-EXOs)可抑制地塞米松诱导的C2C12肌管萎缩。

加强型Q460C方钢管间隙N型节点承载力研究

为考察加强构造对N型节点失效机理和承载力的影响规律,对加强节点和基本节点进行了主管轴压静力加载试验,试验结果表明:基本节点的破坏模式为主管上翼缘受拉鼓曲开裂,加强节点破坏模式为加劲板屈曲和覆板焊缝受拉开裂;加强节点的承载力较基本节点提高了9.4%~36.5%;增加覆板厚度,可明显提高节点承载力。采用ABAQUS软件对覆板和加劲板加强的Q460C方钢管间隙N型节点进行了有限元参数研究,考察了主管宽厚比γ、主支管厚度比η、主支管宽度比β、受拉支管与主管夹角θ、支管间距与主管宽度比ξ对节点破坏模式、应力分布、主管荷载-位移曲线和覆板焊缝断裂指数I f的影响规律。根据试验和数值模拟结果,提出了覆板和加劲板加强的Q460C方钢管间隙N型节点承载力计算式和构造设计建议。

血清降钙素原、C反应蛋白、前白蛋白联合检测评估急性胰腺炎病情进展的价值

目的 探讨血清降钙素原(PCT)、C反应蛋白(CRP)、前白蛋白(PA)联合检测评估急性胰腺炎病情进展的价值,为临床提供参考。方法 回顾性分析2019年12月至2023年12月北京市垂杨柳医院收治的92例急性胰腺炎患者的临床资料,根据病情程度分为轻症急性胰腺炎(MAP)组(68例,未合并器官衰竭)和重症急性胰腺炎(SAP)组(24例,合并器官衰竭)。比较两组患者临床资料,分析影响SAP发生的独立危险因素,分析PCT、CRP、PA水平单独及联合检测预测SAP发生的价值。结果 SAP组患者急性生理学与慢性健康状况评分系统(APACHE Ⅱ)评分、PCT、白细胞介素-6(IL-6)、CRP、D-二聚体(D-D)水平均高于MAP组,PA水平低于MAP组(均P<0.05)。多因素Logistic回归分析结果显示,APACHE Ⅱ评分升高、PCT升高、IL-6升高、CRP升高、PA降低、D-D升高均是影响SAP发生的独立危险因素(均P<0.05)。受试者操作特征(ROC)曲线分析结果显示,PCT、CRP、PA水平单独及联合检测预测SAP发生的曲线下面积(AUC)分别为0.863、0.789、0.757、0.953,灵敏度分别为0.750、0.708、0.708、0.958,特异度分别为0.853、0.824、0.271、0.912(均P<0.05)。结论 APACHE Ⅱ评分升高、PCT升高、IL-6升高、CRP升高、PA降低、D-D升高均是影响SAP发生的独立危险因素,且血清PCT、CRP、PA水平联合检测预测SAP的发生有较高价值。

白细胞介素-17C在自身免疫性皮肤病中的研究进展

白细胞介素17家族(interleukin-17s,IL-17s)具有促炎效应,参与各种自身免疫性疾病的发生发展。IL-17C是IL-17细胞因子家族中的重要成员之一,不同于广泛来源于各种免疫细胞的IL-17A,IL-17C主要由上皮细胞分泌并通过IL-17RE/A受体复合物发挥作用,在银屑病、特应性皮炎等自身免疫性皮肤病中均存在表达异常。本文综述了IL-17C与自身免疫性皮肤病之间关系的研究进展。

抑制NRF1/ABCC1提高人肺腺癌细胞系对顺铂化学治疗的敏感性

目的探讨核呼吸因子1(NRF-1)激活ATP结合盒转运蛋白C1(ABCC1)转录对肺腺癌细胞顺铂抵抗的影响及其潜在机制。方法通过癌基因组数据集分析肺腺癌肿瘤组织中ABCC1的表达水平。细胞分组:sh-NC、sh-ABCC1、sh-NC+oe-NC、sh-NRF1+oe-NC和sh-NRF1+oe-ABCC1。RT-qPCR检测ABCC1在肺腺癌细胞中的表达量。构建顺铂耐药肺腺癌细胞株,检测ABCC1的表达水平。(0、0.001,0.002,0.004、0.008、0.016和0.032 mg/mL)顺铂处理的耐药肺腺癌细胞的IC50值。Western blot检测上皮间充质转化标志物(E-cadherin、N-cadherin)蛋白的表达。双荧光素酶报告基因和ChIP实验验证NRF1与ABCC1的结合关系。结果ABCC1在肺腺癌肿瘤组织和细胞中高表达。与顺铂敏感的肺腺癌细胞相比,ABCC1在顺铂耐药肺腺癌细胞中高表达,敲低ABCC1可显著抑制细胞增殖、迁移和侵袭,并提高E-cadherin的表达(P<0.05),降低N-cadherin的表达(P<0.05)。敲低ABCC1可显著提高肺腺癌细胞对顺铂的敏感性(P<0.05)。此外,双荧光素酶报告基因和ChIP实验证实NRF1与ABCC1启动子的去结合关系,且NRF1可激活ABCC1的转录。敲低NRF1可减弱过表达ABCC1对肺腺癌细胞增殖、迁移、侵袭及顺铂抵抗的抑制作用(P<0.05)。结论NRF1/ABCC1轴在肺腺癌顺铂抵抗中具有促进作用。抑制NRF1/ABCC1轴可能是提高肺腺癌顺铂敏感性的潜在靶点。

基于质谱的脂质C=C和脂肪酰基位置鉴定方法及其在食品分析中的应用研究进展

脂质在生命体中发挥着重要作用,结构影响功能,脂质精细结构解析至关重要。但脂质结构的多样性和相似性对脂质分析提出了巨大挑战。质谱是脂质分析的重要技术之一,在脂质C=C和脂肪酰基位置结构解析中有着较好的应用。本文介绍脂质分析的前处理方法,综述基于质谱的C=C位置和脂肪酰基位置鉴定方法,并讨论该方法在食品分析中的应用,最后展望质谱在脂质化合物精确结构解析方面的发展趋势,以期为不饱和脂质C=C位置和脂肪酰基位置鉴定以及异构体识别和定量分析技术发展和应用提供参考。

血清可溶性生长刺激表达基因2蛋白、胱抑素C、C反应蛋白与冠状动脉病变严重程度的相关性及预后影响因素分析

目的:探究血清可溶性生长刺激表达基因2蛋白(sST2)、胱抑素C(Cys C)、C反应蛋白(CRP)与冠状动脉病变严重程度的相关性并分析预后的影响因素。方法:选取170例冠状动脉病变患者为观察组,以冠状动脉病变严重程度分为轻度狭窄组(53例)、中度狭窄组(62例)、重度狭窄组(55例),并选同期100例健康体检者为对照组。比较不同组别患者血清sST2、CysC、CRP水平差异,Pearson相关性分析其与冠状动脉病变严重程度的关系。对所有患者进行6个月随访,预后良好(118例)、预后不良(52例),以多元Logistic回归分析影响预后的危险因素。结果:观察组血清sST2、CysC、CRP水平较对照组升高(均P<0.05)。重度狭窄组患者血清sST2、CysC、CRP水平高于轻度、中度狭窄组,中度狭窄组高于轻度狭窄组(均P<0.05)。Pearson相关性分析显示,冠状动脉病变严重程度与血清sST2(r=0.727)、CysC(r=0.644)、CRP(r=0.889)均表现为显著正相关(均P<0.05)。多元Logistic回归分析显示,高血压史、糖尿病史、高血脂症、病变血管、经皮冠状动脉介入术使用支架类型、sST2与CysC均为影响预后的独立危险因素(均P<0.05)。结论:冠状动脉病变程度越严重,患者血清sST2、CysC、CRP水平越高,且高血压史、糖尿病史、高血脂症、病变血管、经皮冠状动脉介入术使用支架类型、sST2与CysC均是影响患者预后的独立危险因素。

lncRNA-TNFRSF13C调控miR-1246对牙周细胞低氧诱导因子1α的作用

背景:LncRNA-TNFRSF13C是B细胞发育和功能中的一个重要因子,在牙周炎患者牙周组织中高表达,但具体机制还不清楚。目的:探讨lncRNA-TNFRSF13C调控miR-1246对牙周细胞低氧诱导因子1α的作用机制。方法:人牙周膜细胞经过脂多糖处理后分为7组:A组(无转染的人牙周膜细胞株)、B组(人牙周膜细胞株转染TNFRSF13C NC-siRNA)、C组(人牙周膜细胞株转染TNFRSF13C-siRNA)、D组(人牙周膜细胞株转染miR-1246 mimics)、E组(人牙周膜细胞株转染miR-1246 siRNA)、F组(人牙周膜细胞株转染TNFRSF13C-siRNA+miR-1246 mimics)及G组(人牙周膜细胞株转染TNFRSF13C-siRNA+miR-1246 siRNA)。采用qRT-PCR检测各组细胞lncRNA-TNFRSF13C、miR-1246相对表达;CCK-8检测细胞活性;流式细胞仪检测细胞凋亡率;免疫印迹检测细胞中低氧诱导因子1α、血管内皮生长因子蛋白的表达;Pearson分析lncRNA-TNFRSF13C与miR-1246相关性,双荧光素酶分析靶向关系。结果与结论:①A、B两组人牙周膜细胞活性、凋亡率及蛋白指标比较差异均无显著性意义(P>0.05),与B组相比,C组细胞活性升高、凋亡率及低氧诱导因子1α、血管内皮生长因子蛋白降低(P<0.05),与C组相比,D组细胞活性降低,凋亡率及低氧诱导因子1α、血管内皮生长因子蛋白均升高(P<0.05),D组相比,E组细胞活性升高(P<0.05),F组细胞活性低于E组,E、F组细胞凋亡率降低(P<0.05),与F组相比,G组细胞活性升高、凋亡率及低氧诱导因子1α、血管内皮生长因子蛋白降低(P<0.05)。②lncRNA-TNFRSF13C与miR-1246呈现正相关(P<0.05)。③TNFRSF13C-siRNA组与TNFRSF13C-NC组在miR-1246-wt荧光活性降低(P<0.05);与miR-1246-NC组相比,miR-1246 mimics组低氧诱导因子1α-wt、血管内皮生长因子-wt荧光活性升高(P<0.05)。④结果说明,下调lncRNA-TNFRSF13C对脂多糖处理的牙周细胞具有促进活性、降低凋亡的作用,同时也可抑制低氧诱导因子1α、血管内皮生长因子的表达,其机制与调控miR-1246活性相关。

Repetitive traumatic brain injury–induced complement C1–related inflammation impairs long-term hippocampal neurogenesis

Repetitive traumatic brain injury impacts adult neurogenesis in the hippocampal dentate gyrus,leading to long-term cognitive impairment.However,the mechanism underlying this neurogenesis impairment remains unknown.In this study,we established a male mouse model of repetitive traumatic brain injury and performed long-term evaluation of neurogenesis of the hippocampal dentate gyrus after repetitive traumatic brain injury.Our results showed that repetitive traumatic brain injury inhibited neural stem cell proliferation and development,delayed neuronal maturation,and reduced the complexity of neuronal dendrites and spines.Mice with repetitive traumatic brain injuryalso showed deficits in spatial memory retrieval.Moreover,following repetitive traumatic brain injury,neuroinflammation was enhanced in the neurogenesis microenvironment where C1q levels were increased,C1q binding protein levels were decreased,and canonical Wnt/β-catenin signaling was downregulated.An inhibitor of C1 reversed the long-term impairment of neurogenesis induced by repetitive traumatic brain injury and improved neurological function.These findings suggest that repetitive traumatic brain injury–induced C1-related inflammation impairs long-term neurogenesis in the dentate gyrus and contributes to spatial memory retrieval dysfunction.

Crystallization Modulation and Holistic Passivation Enables Efficient Two‑Terminal Perovskite/CuIn(Ga)Se_(2)Tandem Solar Cells

Two-terminal(2-T)perovskite(PVK)/CuIn(Ga)Se_(2)(CIGS)tandem solar cells(TSCs)have been considered as an ideal tandem cell because of their best bandgap matching regarding to Shockley–Queisser(S–Q)limits.However,the nature of the irregular rough morphology of commercial CIGS prevents people from improving tandem device performances.In this paper,D-homoserine lactone hydrochloride is proven to improve coverage of PVK materials on irregular rough CIGS surfaces and also passivate bulk defects by modulating the growth of PVK crystals.In addition,the minority carriers near the PVK/C60 interface and the incompletely passivated trap states caused interface recombination.A surface reconstruction with 2-thiopheneethylammonium iodide and N,N-dimethylformamide assisted passivates the defect sites located at the surface and grain boundaries.Meanwhile,LiF is used to create this field effect,repelling hole carriers away from the PVK and C60 interface and thus reducing recombination.As a result,a 2-T PVK/CIGS tandem yielded a power conversion efficiency of 24.6%(0.16 cm^(2)),one of the highest results for 2-T PVK/CIGS TSCs to our knowledge.This validation underscores the potential of our methodology in achieving superior performance in PVK/CIGS tandem solar cells.

Spectrum of venous thromboembolism in adult patients with ulcerative colitis in Pakistan:A single center retrospective study

BACKGROUND Patients with inflammatory bowel disease are at a 2-8-fold higher risk of deve-loping venous thromboembolism(VTE)as compared to the general population.Although the exact pathogenesis is unclear,the literature suggests that increased risk of thromboembolic events in such patients occurs as a result of increased coagulation factors,inflammatory cytokines,and reduction in anticoagulants leading to a prothrombotic state.AIM To assess the prevalence,risk factors,management,and outcome of ulcerative colitis(UC)patients who develop VTE.METHODS This was a retrospective chart review done in The Gastroenterology Department of The Aga Khan University Hospital.Data was collected from medical records for all patients admitted with a diagnosis of UC from January 2012 to December 2022.RESULTS Seventy-four patients fulfilled the inclusion criteria.The mean±SD of age at presentation of all UC patients was 45 years±10 years whereas for those who developed VTE,it was 47.6 years±14.7 years.Hypertension and diabetes were the most common co-morbid seen among UC patients with a frequency of 17(22.9%)and 12(16.2%),respectively.A total of 5(6.7%)patients developed VTE.Deep venous thrombosis was the most common thromboembolic phenomenon seen in 3(60%)patients.All the patients with UC and concomitant VTE were discharged home(5;100%).CONCLUSION The prevalence of VTE with UC in Pakistani patients corresponds with the international literature.However,multi-centric studies are required to further explore these results.

Endoplasmic reticulum stress and autophagy in cerebral ischemia/reperfusion injury:PERK as a potential target for intervention

Several studies have shown that activation of unfolded protein response and endoplasmic reticulum(ER)stress plays a crucial role in severe cerebral ischemia/reperfusion injury.Autophagy occurs within hours after cerebral ischemia,but the relationship between ER stress and autophagy remains unclear.In this study,we established experimental models using oxygen-glucose deprivation/reoxygenation in PC12 cells and primary neurons to simulate cerebral ischemia/reperfusion injury.We found that prolongation of oxygen-glucose deprivation activated the ER stress pathway protein kinase-like endoplasmic reticulum kinase(PERK)/eukaryotic translation initiation factor 2 subunit alpha(e IF2α)-activating transcription factor 4(ATF4)-C/EBP homologous protein(CHOP),increased neuronal apoptosis,and induced autophagy.Furthermore,inhibition of ER stress using inhibitors or by si RNA knockdown of the PERK gene significantly attenuated excessive autophagy and neuronal apoptosis,indicating an interaction between autophagy and ER stress and suggesting PERK as an essential target for regulating autophagy.Blocking autophagy with chloroquine exacerbated ER stress-induced apoptosis,indicating that normal levels of autophagy play a protective role in neuronal injury following cerebral ischemia/reperfusion injury.Findings from this study indicate that cerebral ischemia/reperfusion injury can trigger neuronal ER stress and promote autophagy,and suggest that PERK is a possible target for inhibiting excessive autophagy in cerebral ischemia/reperfusion injury.

Activin A receptor type 1C single nucleotide polymorphisms associated with esophageal squamous cell carcinoma risk in Chinese population

BACKGROUND Transforming growth factor-β(TGF-β)superfamily plays an important role in tumor progression and metastasis.Activin A receptor type 1C(ACVR1C)is a TGF-βtype I receptor that is involved in tumorigenesis through binding to dif-ferent ligands.AIM To evaluate the correlation between single nucleotide polymorphisms(SNPs)of ACVR1C and susceptibility to esophageal squamous cell carcinoma(ESCC)in Chinese Han population.METHODS In this hospital-based cohort study,1043 ESCC patients and 1143 healthy controls were enrolled.Five SNPs(rs4664229,rs4556933,rs77886248,rs77263459,rs6734630)of ACVR1C were assessed by the ligation detection reaction method.Hardy-Weinberg equilibrium test,genetic model analysis,stratified analysis,linkage disequi-librium test,and haplotype analysis were conducted.RESULTS Participants carrying ACVR1C rs4556933 GA mutant had significantly decreased risk of ESCC,and those with rs77886248 TA mutant were related with higher risk,especially in older male smokers.In the haplotype analysis,ACVR1C Trs4664229Ars4556933Trs77886248Crs77263459Ars6734630 increased risk of ESCC,while Trs4664229Grs4556933Trs77886248Crs77263459Ars6734630 was associated with lower susceptibility to ESCC.CONCLUSION ACVR1C rs4556933 and rs77886248 SNPs were associated with the susceptibility to ESCC,which could provide a potential target for early diagnosis and treatment of ESCC in Chinese Han population.

Netrin-1 signaling pathway mechanisms in neurodegenerative diseases

Netrin-1 and its receptors play crucial roles in inducing axonal growth and neuronal migration during neuronal development.Their profound impacts then extend into adulthood to encompass the maintenance of neuronal survival and synaptic function.Increasing amounts of evidence highlight several key points:(1)Diminished Netrin-1 levels exacerbate pathological progression in animal models of Alzheimer’s disease and Parkinson’s disease,and potentially,similar alterations occur in humans.(2)Genetic mutations of Netrin-1 receptors increase an individuals’susceptibility to neurodegenerative disorders.(3)Therapeutic approaches targeting Netrin-1 and its receptors offer the benefits of enhancing memory and motor function.(4)Netrin-1 and its receptors show genetic and epigenetic alterations in a variety of cancers.These findings provide compelling evidence that Netrin-1 and its receptors are crucial targets in neurodegenerative diseases.Through a comprehensive review of Netrin-1 signaling pathways,our objective is to uncover potential therapeutic avenues for neurodegenerative disorders.