Inhibition of mitochondrial complex I improves glucose metabolism independently of AMPK activation

Accumulating evidences showed metformin and berberine, well‐known glucose‐lowering agents, were able to inhibit mitochondrial electron transport chain at complex I. In this study, we aimed to explore the antihyperglycaemic effect of complex I inhibition. Rotenone, amobarbital and gene silence of NDUFA13 were used to inhibit complex I. Intraperitoneal glucose tolerance test and insulin tolerance test were performed in db/db mice. Lactate release and glucose consumption were measured to investigate glucose metabolism in HepG2 hepatocytes and C2C12 myotubes. Glucose output was measured in primary hepatocytes. Compound C and adenoviruses expressing dominant negative AMP‐activated protein kinase (AMPK) α1/2 were exploited to inactivate AMPK pathway. Cellular NAD⁺/NADH ratio was assayed to evaluate energy transforming and redox state. Rotenone ameliorated hyperglycaemia and insulin resistance in db/db mice. It induced glucose consumption and glycolysis and reduced hepatic glucose output. Rotenone also activated AMPK. Furthermore, it remained effective with AMPK inactivation. The enhanced glycolysis and repressed gluconeogenesis correlated with a reduction in cellular NAD⁺/NADH ratio, which resulted from complex I suppression. Amobarbital, another representative complex I inhibitor, stimulated glucose consumption and decreased hepatic glucose output in vitro, too. Similar changes were observed while expression of NDUFA13, a subunit of complex I, was knocked down with gene silencing. These findings reveal mitochondrial complex I emerges as a key drug target for diabetes treatment. Inhibition of complex I improves glucose homoeostasis via non‐AMPK pathway, which may relate to the suppression of the cellular NAD⁺/NADH ratio.     

The variation of 15 autosomal microsatellite DNA loci in five indigenous populations of South Siberia

The allele frequencies of 15 autosomal STR loci (D3S1358, vWA, FGA, TH01, TPOX, CSF1PO, D5S818, D13S317, D7S820, D16S539, D2S1338, D8S1179, D21S11, D18S51, and D19S433) included into the AmpFlSTR SGM Plus and AmpFlSTR Profiler Plus kits (Applied Biosystems, United States) were determined for five indigenous populations of South Siberia: Buryats, Altaians, Tofalars, Sojots, and Khakassians (N = 261). No significant differences in allele frequencies were found between the populations. The combined power of discrimination of the STR loci was determined for every population.     

阿胶冲剂与阿胶的化学成分对比分析研究

阿胶在我国有着悠久的历史,是常用滋补中药,具有许多特殊的功效,国内外享有盛誉。据《本草纲目》及《本草纲目拾遗》等介绍,阿胶在明代以前系用(沙牛)牛,水牛,驴皮或猪、马、驼皮等杂皮熬制而成。自清代始一律采用黑驴皮熬制。以往服用阿胶必须将阿胶先用水浸泡后,然后加热溶解后才能服用.为了克服这一缺点,山东化工学院研制了一种用开水冲服的阿胶新制剂——阿胶冲剂.为了弄清阿胶经物理方法处理后的化学组成成份与原阿谱的化学组成成分的不同变化。我们对其所含微量元素、氨基酸进行了对比分析.另外,本文首次报道了阿胶及阿胶冲剂的红外光谱分析结果.     

次磷酸钠的急性毒性研究

目的本研究旨在探讨次磷酸钠对小鼠经口的急性毒性作用,评价其安全性,为其在食品工业中的广泛应用提供理论依据;方法受试物采用经口灌胃途径,观察不同剂量组给予小鼠后的死亡率,并按照寇式法计算半数致死量;结果经实验结果统计,计算出次磷酸钠的LD50为7.67g/kg体重,95%置信区间上限是7.943g/kg体重,下限是6.166g/kg体重;结论按化学物经口急性毒性分级标准,次磷酸钠毒性为2级,属于实际无毒物质。     

广东本地及移民学龄儿童饮食结构和肠道菌群差异分析

[目的]探究广东本地及移民学龄儿童的饮食结构及肠道菌群分布的差异.[方法]以广东深圳为采样点,随机抽样选取48名广东本地儿童和34名移民儿童,进行膳食问卷调查和晨便采集.采用Mann-Whitney U test分析本地及移民儿童饮食因子摄入频率的差异,并使用Illumina Miseq高通量测序技术对儿童的肠道菌群进...     

Adeno-associated viruses (AAV)

Recombinant adeno-associated virus derived vectors (rAAV) a thought to be a most promising candidates for gene therapy applications. Their nonpathogenic nature as well as the encouraging capability to infect both proliferating and non proliferating cells are advantages for gene therapy applications. Here, we summarize the potential mechanisms responsible for AAV maintenance and site-specific integration to human genome. The role of Rep proteins, inverted terminal repeats and p5 promotor sequences for chromosomal incorporation of AAV are discussed. Making the site-specific integrative recombinant AAV vectors for gene therapy seems to be closely dependent on the development of viral vectorology.     

克山病是一种“心肌线粒体病(Mitochondrial Cardiomyopathy)”

亚急克病人心肌线粒体内膜电子传递链的琥珀酸氧化酶系,琥珀酸脱氢酶和细胞色素氧化酶活性明显低于对照。H~ -ATP酶的活性及其对寡霉素的敏感性都明显下降。ATP能量化后线粒体膜电位的变化也比对照明显降低。膜脂流动性低于对照。亚急克病人心肌线粒体内观察到较多的电子致密无定形物质,经电镜X射线微区等方法分析,认为这些物质不是Ca_3(PO_4)_2,而可能是一种蛋白质凝聚物。此外,心肌线粒体的硒含量远低于对照,而Ca含量明显高于对照。上述结果都反映亚急克病人心肌线粒体明显损伤。根据克山病患者心肌细胞线粒体结构与功能方面呈现的如此广泛与明显的异常,可将克山病称为“心肌线粒体病(Mitochondrial Cardiomyopathy)”。     

聚赖氨酸修饰丝素蛋白膜对神经干细胞生长和分化的影响

利用聚赖氨酸修饰丝素蛋白膜,观察其对神经干细胞(NSCs)生长及分化的影响,为中枢神经系统损伤修复材料的选择提供实验基础和理论依据。文中首先制备聚赖氨酸修饰的丝素蛋白膜,并通过核磁共振图谱和紫外-可见光谱进行验证。NSCs分别接种在单纯丝蛋白膜(Silk)、聚赖氨酸修饰的丝蛋白膜(Silk-PIL)和多聚赖氨酸(PLL)上进行培养,分别在1、3、5、7 d时用CCK-8检测NSCs增殖活性。在第7天时,用免疫荧光染色检测NSCs分化情况,Western blotting和TUNEL检测细胞凋亡水平,Real-time PCR检测脑源性神经营养因子(BDNF)mRNA水平。结果表明,核磁共振图谱和紫外-可见光谱证明聚赖氨酸成功地接枝到了丝素蛋白膜上,CCK-8检测显示:从第3天开始一直到第7天,NSCs在Silk-PIL上的增殖活性要显著高于Silk组(P0.05),而与PLL组无显著性差异(P0.05)。免疫荧光观察显示,NSCs在Silk-PIL上分化成神经元的细胞显著多于Silk组(P0.05),而与PLL组无显著性差异,3个组之间分化为星型胶质细胞的数量并无显著性差异。Western blotting和TUNEL检测结果表明Silk-PIL组NSCs凋亡程度显著小于Silk组(P0.05),但与PLL组无显著性差异(P0.05)。RT-PCR结果显示,NSCs在Silk-PIL和PLL组的BDNFmRNA表达水平显著高于Silk组(P0.05)。结果表明,聚赖氨酸修饰的丝素蛋白膜能够促进NSCs的增殖活性并减少NSCs细胞凋亡,同时促进NSCs向神经元方向分化,有望成为新型组织工程支架材料搭载NSCs移植修复中枢神经系统损伤。     

Synthesis,receptor binding studies,optical spectroscopic and in silico structural characterization of morphiceptin analogs with cis‐4‐amino‐L‐proline residues

Three novel morphiceptin analogs, in which Pro in position 2 and/or 4 was replaced by cis‐4‐aminoproline connected with the preceding amino acid through the primary amino group, were synthesized. The opioid receptor affinities, functional assay results, enzymatic degradation studies and experimental and in silico structural analysis of such analogs are presented. Copyright © 2017 European Peptide Society and John Wiley & Sons, Ltd.