G蛋白亲和色谱法纯化动物血清、抗体效果比较

比较 Hitrap G蛋白 Sepharose亲和色谱系统对不同动物血清或腹水的纯化效果 ,为抗体纯化提供依据。结果显示 ,G蛋白对不同动物血清 Ig G吸附能力不同 ,体现在单位体积抗体回收量明显不同 ,这一特点与 A蛋白亲和色谱系统相似。该方法简便快速 ,纯化抗体纯度高 ,免疫活性好 ,色谱柱可反复使用多次     

A Recombinant Human Cytomegalovirus with a Large Deletion in UL97 Has a Severe Replication Deficiency

Human cytomegalovirus encodes a protein kinase (UL97) that confers sensitivity to ganciclovir by phosphorylating it to the monophosphate. The function of this unusual kinase in viral replication is unknown. We constructed two independent isolates of a recombinant virus, RCDelta97, that contain large deletions in this gene and carry a 4.8-kb insertion containing a selectable genetic marker. These mutant viruses were isolated by using a population of primary cells (HEL97) that express this gene from integrated copies of a defective retroviral vector. The recombinant viruses were severely impaired in their ability to replicate in primary fibroblasts, attaining virus titers that were 2 to 3 orders of magnitude lower than those produced by the parent virus. Despite the severe replication deficit, both of these viruses retained the ability to form small, slowly growing plaques in primary fibroblasts, demonstrating that UL97 is not absolutely essential for replication in cell culture. The replication deficit was relieved when UL97 was provided in trans in the complementing cell line, showing that the phenotype was due to a deficiency in UL97. Thus, the UL97 gene product plays a very important role in viral replication in tissue culture and may be a good target for antiviral chemotherapy.     

谷氨酸及NMDA受体拮抗剂MK-801对大鼠伏核痛兴奋神经元电活动的影响

本文研究了谷氨酸(glutamic acid,Glu)及其NMDA受体拮抗剂5-甲基二氢丙环庚烯亚胺马来酸(MK-801)对人鼠伏核(nucleus accumbens,NAc)痛兴奋神经元(pain-excitation neurons,PEN)痛诱发反应的影响。电刺激坐骨神经作为伤害性刺激,用玻璃微电极记录NAc的PEN放电,观察脑室内注射Glu和NAc内注射MK-801对大鼠NAc中PEN伤害性诱发活动的影响。结果显示,伤害性刺激可使NAc的PEN电活动增强;脑室内注射Glu(10nmol／10μl)可使NAc的PEN伤害性诱发放电频率增加;NAc内注射MK-801(1．0nmol／0．5μl)可阻断这种作用;MK-801本身也可部分抑制PEN伤害性诱发反应。上述结果表明,Glu对PEN伤害性反应的易化作用是通过NMDA受体介导的：Glu和NMDA受体参与NAc伤害性信息传递的调制。     

固体介质中的重金属源解析及其在中国近海沉积物中的应用

沉积物中重金属源解析对甄别人为活动与自然变化对近海生态系统演化的影响有重要作用.本文总结了近年来污染物源解析常用的多元统计分析、地球化学方法和地质统计分析3种主要研究方法,剖析了不同方法的优劣及适用性,提出正定矩阵因子分析、Pb同位素示踪在重金属来源定量化研究中具有良好应用前景.梳理了中国近海沉积物中重金属来源的主要研究结果,发现河口和海湾是沉积物重金属受人为来源影响剧烈的典型近海区域,不同定量解析方法(多元统计分析、背景值估算、Pb同位素分析)均表明中国近海沉积物重金属的人为来源贡献率接近或超过50%.当前中国近海沉积物中重金属源解析研究还存在源识别端元模糊、解析结果缺乏相应的可靠性评价等问题.据此提出近海沉积物重金属源解析研究应使用多种解析技术手段综合、集成与优化,提高源解析的准确性;建立完善指标体系,筛选代表特定人为活动和自然过程的指标;甄别人为源重金属入海方式及过程,为沉积物数据信息的解译提供理论基础.     

食物源距离对中华姬鼠贮藏策略的影响

在围栏条件下, 检验食物源距离对中华姬鼠贮藏策略的影响,并检验根据快速隔离假说和最优贮藏空间分布模型做出的两个预测：（1）3个释放点无论距离远近,种子均先被大量分散贮藏在各个释放点周围;（2）随着释放点远离巢穴,种子被集中贮藏的比例下降。结果发现: 分散贮藏是中华姬鼠的主要贮藏方式,3个释放点种子被分散贮藏的数量无显著差异,这个结果支持预测（1）;3个种子释放点（1m,5m,13m）被集中贮藏的比例分别为(1m: 6.25%; 5m: 1.88%; 13m: 1.25%),说明被集中贮藏的种子数量随种子释放点与巢穴距离的增大而逐渐减少,这个结果支持预测（2）。本研究表明中华姬鼠应对捕食风险升高的策略是降低取食量和贮藏量。     

Krüppel样因子7(KLF7)生物学功能研究进展

Krüppel样因子7(Krüppel-like factor 7,KLF7)是Sp1样或Krüppel样转录因子家族(specificity protein/Krüppel-like factor,SP/KLF)成员,在多种生物学过程中发挥重要作用,该基因完全敲除小鼠出生时大部分死亡.KLF7是肥胖症、Ⅱ型糖尿病、心血管疾病、癌症、面部发育异常、氧化磷酸化缺陷和Ⅰ型自身免疫性胰腺炎等疾病的相关基因.功能分析显示,KLF7是神经系统发育和脂肪形成的关键因子,同时也在肌肉再生和造血作用中发挥功能.在SP/KLF家族中,KLF7研究相对较少,大部分作用机制尚不清楚.本文从结构和功能方面详述了KLF7的最新研究进展,为其和KLFs家族深入研究提供重要的科学依据.     

贵州省发现翼手目动物——高颅鼠耳蝠

2015年7~9月在贵州省兴仁县、平坝县和兴义市的五屯镇及敬南镇捕获鼠耳蝠33只,鉴定为高颅鼠耳蝠(Myotis siligorensis),为贵州省新纪录物种。标本保存于贵州师范大学生命科学学院生态实验室。主要特征:体型较小,前臂长(36.03±1.50)mm(32.66~38.98 mm,n=33);耳狭长;耳屏直而细长;第Ⅲ掌骨最长,第Ⅴ掌骨最短;阴茎长(4.52±0.84)mm(2.85~5.75 mm,n=21);头骨狭长,颅骨凸显;颅全长(13.87±0.74)mm(13.00~14.88 mm,n=8),颅高(6.36±0.24)mm(6.03~6.74 mm,n=8);听泡较小;矢状脊细弱;上颌第1、2门齿向中央倾斜,上颌第1门齿有1个主尖和1个附尖;上颌第2门齿较第1门齿小,且与犬齿分离;上颌第2前臼齿(P3)位于齿列中。基于Cyt b基因(1 141 bp)序列进行的分子系统学分析显示,此次捕获鼠耳蝠物种与高颅鼠耳蝠聚在一起,二者遗传距离最近(仅为0.03),进一步确认所采集物种为高颅鼠耳蝠。     

Structure of a Pancreatic ATP-Sensitive Potassium Channel

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Neuroprotective Effect of Chitosan Oligosaccharide on Hypoxic-Ischemic Brain Damage in Neonatal Rats

Neonatal hypoxic-ischemic brain damage (HIBD) is one of the leading causes of neonatal mortality and permanent neurological disability worldwide and the effective treatment strategies are not yet available. It has been demonstrated that Chitosan oligosaccharide (COS) exerts protective effect in vitro ischemic brain injury. However, no information is available on possible effects of COS on neonatal HIBD. To investigate the hypothesis of the potential neuroprotective effect of COS on the brain injury due to HIBD, 7-day-old Sprague–Dawley rats were treated with left carotid artery ligation followed by exposure to 8% oxygen (balanced with nitrogen) for 2.5 h at 37?°C. After COS treatment, the cerebral damage was measured by behavior tasks, 2,3,5-triphenyltetrazolium chloride(TTC), Hematoxyline-Eosin(HE), Nissl and Fluoro-Jade B(FJB)staining. In addition, the oxidative stress were assayed with ipsilateral hemisphere homogenates. Immunofluorescence staining were used to examine the activation of the astrocyte and microglia. Expression of inflammatory-related proteins were analyzed by western-blot analysis. In this study we found that administration of COS ameliorated early neurological reflex behavior, significantly reduce brain infarct volume and attenuated neuronal cell injury and degeneration. Furthermore, COS markedly decreased the level of MDA, lactic acid and increased SOD, GSH-Px and T-AOC. COS attenuated hypoxic-ischemic induced up-regulation of expressions of interleukin-1β (IL-1β), tumor necrosis factor alpha (TNF-α), meanwhile it dramatically increased the interleukin-10 (IL-10). These results suggest that COS exerts neuroprotection on hypoxic-ischemic brain damage in neonatal rats, it implies COS might be a potential therapeutic for the treatment of HIBD.