Inhibiting 5-hydroxytryptamine receptor 3 alleviates pathological changes of a mouse model of Alzheimer's disease

Extracellular amyloid beta(Aβ) plaques are main pathological feature of Alzheimer’s disease.However,the specific type of neuro ns that produce Aβ peptides in the initial stage of Alzheimer’s disease are unknown.In this study,we found that 5-hydroxytryptamin receptor 3A subunit(HTR3A) was highly expressed in the brain tissue of transgenic amyloid precursor protein and presenilin-1 mice(an Alzheimer’s disease model) and patients with Alzheimer’s disease.To investigate whether HTR3A-positive interneurons are associated with the production of Aβ plaques,we performed double immunostaining and found that HTR3A-positive interneurons were clustered around Aβ plaques in the mouse model.Some amyloid precursor protein-positive or β-site amyloid precursor protein cleaving enzyme-1-positive neurites near Aβ plaques were co-localized with HTR3A interneurons.These results suggest that HTR3A-positive interneurons may partially contribute to the generation of Aβ peptides.We treated 5.0-5.5-month-old model mice with tro pisetron,a HTR3 antagonist,for 8 consecutive weeks.We found that the cognitive deficit of mice was partially reversed,Aβ plaques and neuroinflammation we re remarkably reduced,the expression of HTR3 was remarkably decreased and the calcineurin/nuclear factor of activated T-cell 4 signaling pathway was inhibited in treated model mice.These findings suggest that HTR3A interneurons partly contribute to generation of Aβ peptide at the initial stage of Alzheimer’s disease and inhibiting HTR3 partly reve rses the pathological changes of Alzheimer’s disease.

Mutations in Hemagglutinin of H5N1 Influenza That Switch Receptor Specificity from Avian to Human Types

Researchers have been searching for molecular features that could make avian H5N1 influenza transmissible among people since the first report of human infections with this virus in 1997. A recent study surprisingly demonstrated that only five mutations, fewer than previously estimated, are needed to make avian H5N1 influenza transmissible between ferrets through the air, raising fears that a human pandemic is possible if this virus escapes from the lab. Of the five mutations found, four of them are located in the HA gene that is responsible for the viral entry into the host cells. A crucial step for avian influenza to go across the species boundary to infect humans is the switch of its receptor binding specificity from avian to human types. The first task of this study was to quantify the individual as well as the collective effect of the known HA mutations from the previous research on receptor binding selection. Our second task was to identify new combinations of HA mutations that could change the receptor binding preference of H5N1 from avian to human types. Our findings thus deepened our understanding of the previous research and also extended its results by discovering new combinations of mutations that could enhance the binding of avian H5N1 to human type receptors while reduce that to avian types.

5-羟色胺1A受体基因多态性与精神分裂症关联性的Meta分析

目的:用Meta分析的方法综合评价人群中5-羟色胺1A(5-HT1A)受体基因多态性与精神分裂症的关联,为精神分裂症的遗传背景提供循证医学证据。方法:计算机检索PubMed、Cochorane、CNKI和万方数据库,搜集有关5-HT1A受体基因多态性与精神分裂症关联性的全文文献。以病例组和对照组5-HT1A受体基因分布的OR及其95%CI为效应指标,在全面文献回顾的基础上对文献进行筛选、评价和数据提取。应用RevMan5.0软件对各研究原始数据进行统计分析,包括异质性检验、合并效应量以及评估发表偏倚。结果:共有5篇文献被纳入分析,其中2篇研究rs6294位点与精神分裂症的关联性,3篇研究rs6295位点与精神分裂症的关联性。精神分裂症患者rs6294位点的基因型Meta分析结果,合并OR=0.35,95%CI=0.12～1.08,P=0.07;rs6294位点等位基因Meta分析结果,合并OR=0.34,95%CI=0.11～1.03,P=0.06;精神分裂症患者rs6295位点的基因型Meta分析结果,合并OR=1.78,95%CI=0.69～4.59,P=0.23;rs6295位点的等位基因Meta分析结果,合并OR=1.80,95%CI=1.03～3.16,P=0.04。结论:人群中5-HT1A受体基因多态性与精神分裂症有关联。

内质网蛋白44(ERp44)通过1,4,5-三磷酸肌醇受体介导基因转录(英文)

细胞核内钙离子浓度的增加可以引起包括钙离子激活的基因转录在内的很多生理功能.运用Western blot、免疫荧光、实时定量聚合酶链反应、钙成像以及外源三磷酸腺苷刺激细胞释放钙离子等试验方法,发现1,4,5-三磷酸肌醇受体和内质网蛋白44(ERp44)在内质网和核膜上都有很好的共定位.外源三磷酸腺苷可以通过1,4,5-三磷酸肌醇受体刺激核内钙瞬变并磷酸化环磷酸腺苷反应原件结合蛋白(CREB)、刺激原癌基因c-Myc的表达.但是,这些功能都能被1,4,5-三磷酸肌醇受体抑制剂2-氨乙氧基二苯酯硼酸(2-APB)和过表达内质网蛋白44(ERp44)所抑制.这些结果均提示在子宫颈癌HeLa细胞中内质网蛋白44(ERp44)通过1,4,5-三磷酸肌醇受体而介导基因转录.

乙型肝炎病毒抑制巨噬细胞TLR3、Mda-5和RIG-I表达

目的探讨乙型肝炎病毒(HBV)与巨噬细胞上模式识别受体(PRR)的相互作用。方法以不同载量HBV刺激佛波酯(PMA)诱导的单核源巨噬细胞,实时定量PCR检测刺激2、4、12及24h后巨噬细胞Toll样受体3(TLR3)、黑色素瘤分化相关基因5(Mda-5)、视黄酸诱导基因I(RIG-I)表达;以poly I:C刺激与HBV共培养12h的巨噬细胞,酶联免疫吸附试验(ELISA)测定poly I:C刺激4h后培养上清液中β干扰素(IFNβ-)的分泌水平。结果不同病毒载量组巨噬细胞TLR3表达在2、4、12、24h较对照组下调,且高病毒载量组表达低于低病毒载量组(F值分别为123.64、24.50、6.69、7.61,P均<0.01);Mda-5和RIG-I在上述4个时间点的表达为高病毒载量组低于低病毒载量组(F值分别为36.44、48.58、46.59、12.77;67.68、74.54、18.18、17.76;P均<0.01)。IFNβ-的表达为:阳性对照组>低病毒载量组>高病毒载量组>阴性对照组(F=78.42,P<0.01),表达量分别为(497.2±43.7)、(294.2±48.4)、(92.5±12.3)、(40.4±9.9)pg/mL。结论 HBV能抑制巨噬细胞TLR3、Mda-5和RIG-I表达,致IFN-β分泌下降,可能是其逃逸机体天然免疫的机制之一。

5-杂氮-2′-脱氧胞苷对乳腺癌MCF-7细胞体外迁移能力的影响及机制探讨

目的观察5-杂氮-2′-脱氧胞苷(5-Aza-CdR)对非浸润性人乳腺癌MCF-7细胞体外迁移能力的影响,并探讨其机制。方法将MCF-7细胞分两组,观察组用含5.0μM5-Aza-CdR的培养液处理4 d,对照组加入等体积的DMSO。采用细胞划痕实验观察细胞体外迁移能力,采用RT-PCR、甲基化特异性PCR(MSP)法检测CXC趋化因子受体-4(CXCR4)、乳腺癌转移抑制基因-1(BRMS1)mRNA及其启动子区甲基化状态。结果与对照组比较,观察组36、48 h细胞划痕愈合率明显升高,MCF-7细胞的CXCR4 mRNA表达量明显增加(P<0.05);5-Aza-CdR使CXCR4启动子区甲基化的CpG岛1完全去甲基化,BRMS1启动子区CpG岛B的非甲基化状态亦无明显改变。结论 5-Aza-CdR增强了MCF-7细胞的体外迁移能力,可能与其去甲基化机制上调了促转移基因CXCR4表达有关。

TRAF1/C5和TNF-α基因多态性与结核病易感性分析

目的分析肿瘤坏死因子受体相关蛋白1(tumor necrosis factor receptor-associated factor 1,TRAF1)/补体5(complement component 5,C5)rs10818488和肿瘤坏死因子-α(tumor necrosis factor-alpha,TNF-α)rs1800629基因多态性、环境因素及其交互作用对结核病(tuberculosis,TB)易感性的影响。方法选取TB多发家庭中TB确诊患者作为TB病例组,当地社区同期体检的健康志愿者作为健康对照(healthy controls,HC)组,与TB组有血缘关系且共同居住者组成家庭密切接触(healthy household contacts,HHC)组。采用logistic回归分析模型分析基因型和环境因素与TB的关联,叉生分析结合logistic回归分析模型分析基因与环境交互作用。结果年龄>45岁(χ^(2)=7.90,OR=2.28,95%CI:1.28~4.04,P=0.005)、吸烟(χ^(2)=15.27,OR=4.70,95%CI:2.16~10.22,P<0.001)增加HHC组TB发病风险。吸烟(χ^(2)=13.94,OR=3.58,95%CI:1.83~7.01,P<0.001)、居住地为农村(χ^(2)=25.05,OR=3.81,95%CI:2.26~6.42,P<0.001)和居室环境卫生较差(χ^(2)=15.31,OR=3.20,95%CI:1.79~5.73,P<0.001)增加HC组TB发病风险。TRAF1/C5 rs10818488位点中,携带AG基因型(共显性及超显性模型)、GG基因型(共显性模型)和AG-GG基因型(显性模型)增加HHC组和HC组患TB风险。TNF-αrs1800629位点与TB易感性暂未显示存在关联。分析基因与环境交互作用,在TB组和HHC组间,TRAF1/C5 rs10818488位点AG-GG基因型与吸烟存在协同作用;而在TB组和HC组间,rs10818488位点AG-GG基因型与吸烟和居室环境卫生较差存在协同作用,与居住地存在相乘交互作用,均使TB发病风险提高。结论TRAF1/C5 rs10818488位点的基因多态性可能与TB发病风险有关,且其与吸烟、居住地、居室环境卫生存在交互作用,共同影响TB的易感性。

H_1受体基因敲除模型鼠的评价及其疼痛感受性低下的探讨

目的 :通过对H1受体基因敲除模型鼠 [(- / - ) (HIKO) ]进行的评价性研究 ,更进一步探索组胺H1受体的生理意义。方法 :对 (- / - )鼠及野生型鼠 (+ / + )进行了 3项评价性实验 :即PCR检测、标记配体 [3H]Pyrilamine的H1受体结合实验及福尔马林疼痛感觉试验 ,并进行了小鼠脑各部位单胺含量的测定。结果 :PCR检测的结果是变异基因为 90 0bp、野生型鼠 (+ / + )基因为12 0 0bp。受体结合实验 (+ / + )鼠与 (- / - )鼠比较其具结合能有显著性差异 (P <0 .0 5 )。福尔马林试验两者比较 ,第二时相 (- / - )鼠的舔、咬注射部位的行为的减少与 (+ / + )鼠比较有显著差异 (P <0 .0 5 )。用高效液相色谱分析仪测定的脑中单胺含量的结果显示 :(- / - )鼠与 (+ / + )鼠比较 ,(- / - )鼠的 5 HT的代谢回转率 (5 HIAA/ 5 HT)在丘脑、大脑皮质、海马、脑干部都有显著地增加 (P <0 .0 5 )。结论 :从 (- / - )鼠首次观察到的疼痛感受性低下及 5

Bioinformatic analysis of human nuclear receptor nr5a2(hb1f) genomic sequence

We have cloned the cDNA of human nuclear receptor nr5a2(hb1f) gene and obtained its whole genomic sequence previously. In this work we carried out in-depth bioinformatic analysis on the genomic sequence of nr5a2(hb1f) gene. Sequence comparison and prediction algorithms implicated that there might be additional coding regions in the 210 kb genomic sequence besides known exons, especially in the two largest introns. Comparison of the structures of nr5a loci in different species revealed distinguishable conservation and apparent gene duplication during evolution. The remarkable conservation among promoters of zebrafish, mouse and human nr5a2 genes suggested that they would be regulated by the same transcription factors.

8-hydroxy-dipropylaminotetralin promotes neural plasticity in epileptic rats with depression

Rats with chronic pilocarpine-induced temporal lobe epilepsy complicated with depression were studied. Anti-5-bromodeoxyuridine immunofluorescence staining and Timms staining showed that neurogenesis within the hippocampal dentate gyrus and mossy fiber sprouting were increased in model rats. Neurogenesis within the hippocampal dentate gyrus was further enhanced, while mossy fiber sprouting was decreased in model rats administered carbamazepine alone or in combination with the 5-hydroxytryptamine 1A receptor agonist, 8-hydroxy-dipropylaminotetralin （0.1 and 1 mg/kg）. Among the groups, the effect was the most significant in rats receiving carbamazepine in conjunction with 1 mg/kg 8-hydroxy-dipropylaminotetralin. Thus, high dose 8-hydroxy-dipropylaminotetralin can improve neural plasticity in epileptic rats with depression.

Interaction of the major inflammatory bowel disease susceptibility alleles in Crohn’s disease patients

AIM:To investigate the interaction of interleukin-23 receptor(IL23R)(rs1004819 and rs2201841),autophagy-related 16-like 1(ATG16L1)(rs2241880), caspase recruitment domain-containing protein 15 (CARD15)genes,and IBD5 locus in Crohn's disease(CD) patients. METHODS:A total of 315 unrelated subjects with CD and 314 healthy controls were genotyped.Interactions and specific genotype combinations of a total of eight variants were tested.The variants of IBD5locus(IGR2198a_1 rs11739135 and IGR2096a_1 rs12521868),CARD15(R702W rs2066845 and L1007fs rs2066847),ATG16L1(rs2241880)and IL23R (rs1004819,rs2201841)genes were genotyped by PCR-RFLP,the G908R(rs2066844)in CARD15 was determined by direct sequencing. RESULTS:The association of ATG16L1 T300A with CD was confirmed[P=0.004,odds ratio(OR)=1.69, 95%CI:1.19-2.41],and both IL23R variants were found to represent significant risk for the disease(P= 0.008,OR=2.05,95%CI:1.20-3.50 for rs1004819 AA;P<0.001,OR=2.97,95%CI:1.65-5.33 for rs2201841 CC).Logistic regression analysis of pairwise interaction of the inflammatory bowel disease (IBD)loci indicated that IL23R,ATG16L1,CARD15 and IBD5(IGR2198a_1)contribute independently to disease risk.We also analysed the specific combina- tions by pair of individual ATG16L1,IL23R rs1004819, rs2201841,IGR2198a_1,IGR2096a_1 and CARD15 genotypes for disease risk influence.In almost all cases,the combined risk of susceptibility pairs was higher in patients carrying two different risk-associated gene variants together than individuals with just one polymorphism.The highest OR was found for IL23R rs2201841 homozygous genotype with combination of positive CARD15 status(P<0.001,OR=9.15,95% CI:2.05-40.74). CONCLUSION:The present study suggests a cumulative effect of individual IBD susceptibility loci.