苦瓜MAP30蛋白基因克隆、表达及其抗肿瘤活性研究

通过PCR技术,从苦瓜总DNA中扩增出编码MAP30成熟蛋白的基因,经测序鉴定后亚克隆到原核表达载体pET30a中,构建成带有N端6Histag的融合表达载体。表达载体用CaCl2介导的化学转化法转化E.coliBL21(DE3),然后利用PCR筛选阳性克隆。工程菌经1mmol/LIPTG诱导4h实现高效表达,而且在30℃时融合蛋白表达量最高,约占菌体总蛋白56%。可溶性分析表明,该融合蛋白在大肠杆菌中主要以可溶的形式存在。重组蛋白通过Ni2+鏊合亲和层析进行纯化,纯化蛋白占上清总蛋白37.2%,发酵液产率为250mg/L。Westernblot分析表明,重组蛋白可与兔抗histag多克隆抗体发生特异性反应。利用MTT法分析重组MAP30的细胞毒性,结果表明其对小鼠3T3和S180肿瘤细胞株具有明显的抑制作用,ID50分别约为50μg/ml和30mg/ml,而对人正常胚肺二倍体WI38细胞株的毒性极小。     

Structural Basis for the Biological Effects of Pr(III) Ions: Alteration of Cell Membrane Permeability

The biological effects of rare-earth ions on the organism have been studied using Pr³⁺ as a probe ion and Escherichia coli cell as a target. Atomic force microscopy (AFM) observation of the surface of E. coli cells shows that the presence of Pr³⁺ substantially changes the structure of the outer membrane. By induced coupled plasma-mass spectrometry (ICP-MS), more Cu²⁺ was found in the cells grown in the presence of Pr³⁺, indicating changes of cell permeability. Using energy dispersive X-ray spectroscopy (EDX), Ca²⁺ is found on the outer surface of the original cell. It is proposed that Pr³⁺ can replace Ca²⁺ from the binding sites because of their close ionic radii and similar ligand speciality.     

NIRF, a novel ubiquitin ligase, interacts with hepatitis B virus core protein and promotes its degradation

Hepatitis B virus (HBV) core protein (HBc) is a major component of viral nucleocapsid and a multifunctional protein involved in viral maturation and release. It is unstable and present in cells at low level because of K96 lysine residue, which is a ubiquitin acceptor site. Np95/ICBP90-like RING finger protein (NIRF) has auto-ubiquitination activity which is the hallmark of a ubiquitin ligase. In the present study, ubiquitin ligase, NIRF, binds to HBc and leads to the proteasome-mediated degradation of HBc in vivo. NIRF down-regulates HBc protein level, resulting in the decrease of the amount of HBV particles in supernatant of HepG2.2.15 cells. However knockdown of NIRF significantly increases endogenous HBc protein level, leading to HBV release. The results reveal that NIRF interacts with HBc and promotes the degradation of HBc in vivo. The pathway of NIRF-mediated ubiquitin–proteasome affects the release of HBV particles by controlling the amounts of HBc. It indicates that NIRF may participate in the maturation of HBV.     

Targeting to overexpressed glucose-regulated protein 78 in gastric cancer discovered by 2D DIGE improves the diagnostic and therapeutic efficacy of micelles-mediated system

The survivals of gastric cancer (GC) patients are associated with early diagnosis and effective treatments. Therefore, it is urgent for the discovery of early GC biomarkers and tumor-targeting therapeutics. The aim of this study was to uncover putative tissue biomarkers of GC using 2D DIGE and then apply one of these specific markers in GC treatment. We found three putative biomarkers of GC with significant differences in expression level compared to adjacent normal tissue, including glucose-regulated protein 78 (GRP78) and glutathione s-transferase pi (GSTpi) with increased expression level, and alpha-1 antitrypsin (A1AT) with reduced expression level. The overexpressed GRP78 was used as a targeted protein for guiding the drugs to tumor cells, leading to more effective treatment for GC xenografts. Our results demonstrated that the designated GRP78-binding peptide based on the sequence, WIFPWIQL, was selectively prone to recognize and bind to GC MKN45 cells in vitro, and also improve the delivery efficiency of polymeric micelles-encapsulated drugs into tumor cells and displayed better therapeutic outcome in experimental animals. This strategy of GRP78-mediated drug targeting system may bring chemotherapeutic drugs with more precise targeting to tumor cells, leading to minimize side effects on patients after chemotherapy.     

Environmental Drivers and Spatial Prediction of the Critically Endangered Species <i>Thuja sutchuenensis</i> in Sichuan-Chongqing,China

Identifying the ecological environment suitable for the growth of Thuja sutchuenensis and predicting other potential distribution areas are essential to protect this endangered species. After selecting 24 environmental factors that could affect the distribution of T. sutchuenensis, including climate, topography, soil and Normalized Difference Vegetation Index (NDVI), we adopted the Random Forest-MaxEnt integrated model to analyze our data. Based on the Random Forest study, the contribution of the mean temperature of the warmest quarter, mean temperature of the coldest quarter, annual mean temperature and mean temperature of the driest quarter was large. Based on MaxEnt model prediction outputs, the potential distribution map not only identified areas that originally recorded T. sutchuenensis, such as Xuanhan County, Kai County and Chengkou County, but also identified highly suitable distribution areas where T. sutchuenensis may exist, including Wanyuan County, Sichuan Province, and the junction of Chongqing and Hubei Province. This provides a more explicit geographic range for ex situ conservation and reintroduction of T. sutchuenensis. Our results also indicate that, in addition to climate factors, topography and soil factors are also important environmental factors that affect distribution. This provides a theoretical basis for subsequent laboratory construction to simulate the indoor growth of T. sutchuenensis.     

Top-down modulations from dorsal stream in lexical recognition: an effective connectivity FMRI study

Both the ventral and dorsal visual streams in the human brain are known to be involved in reading. However, the interaction of these two pathways and their responses to different cognitive demands remains unclear. In this study, activation of neural pathways during Chinese character reading was acquired by using a functional magnetic resonance imaging (fMRI) technique. Visual-spatial analysis (mediated by the dorsal pathway) was disassociated from lexical recognition (mediated by the ventral pathway) via a spatial-based lexical decision task and effective connectivity analysis. Connectivity results revealed that, during spatial processing, the left superior parietal lobule (SPL) positively modulated the left fusiform gyrus (FG), while during lexical processing, the left SPL received positive modulatory input from the left inferior frontal gyrus (IFG) and sent negative modulatory output to the left FG. These findings suggest that the dorsal stream is highly involved in lexical recognition and acts as a top-down modulator for lexical processing.     

2011-2017年大连市输入性卵形疟原虫感染病例的实验室诊断

目的分析大连市2011-2017年7例输入性卵形疟原虫感染病例的病原、抗原及核酸检测结果,以提高卵形疟原虫诊断的准确率和效率。方法收集7例疑似疟疾患者的血样,对血样进行血涂片镜检、快速疟疾诊断试纸条检测(RDT)及荧光定量PCR检测。结果血涂片镜检结果显示7例患者均感染卵形疟原虫。RDT检测结果显示2例阴性,另外5例为泛疟原虫抗原阳性。荧光定量PCR结果显示7例患者均检出疟原虫属和卵形疟原虫核酸。结论综合镜检、RDT及荧光定量PCR检测结果确定该7例患者均为卵形疟原虫感染。     

Spindlin1, a novel nuclear protein with a role in the transformation of NIH3T3 cells

spindlin1, a novel human gene recently isolated by our laboratory, is highly homologous to mouse spindlin gene. In this study, we cloned cDNA full-length of this novel gene and send it to GenBank database as spindlin1 (Homo sapiens spindlin1) with Accession No. AF317228. In order to investigate the function of spindlin1, we studied further the subcellular localization of Spindlin1 protein and the effects of spindlin1 overexpression in NIH3T3 cells. The results showed that the fusion protein pEGFP-N1-spindlin1 was located in the nucleus and the C-terminal is correlated with nuclear localization of Spindlin1 protein. NIH3T3 cells which could stably express spindlin1 as a result of RT-PCR analysis compared with the control cells displayed a complete morphological change; made cell growth faster; and increased the percentage of cells in G2/M and S phase. Furthermore, overexpressed spindlin1 cells formed colonies in soft agar in vitro and formed tumors in nude mice. Our findings provide direct evidence that spindlin1 gene may contribute to tumorigenesis.     

Effects of Different Sources and Levels of Zinc on H2O2-Induced Apoptosis in IEC-6 Cells

Zinc has been shown to be an inhibitor of apoptosis for many years. The present study was designed to investigate effects of three zinc chemical forms on H₂O₂-induced cell apoptosis in IEC-6 cells via analysis of cell vitality, LDH activity, apoptosis percentage, caspase-3 activity, and Bcl-2, Bax, and caspase-3, -8, and -9 gene expression. Cells were divided into H₂O₂ and zinc sources+H₂O₂ groups, and there are three different zinc sources [zinc oxide nanoparticle (nano-ZnO), zinc oxide (ZnO), and zinc sulfate (ZnSO₄)] and three concentrations (normal = 25 μM, medium = 50 μM, and high = 100 μM) used in this article. In the present study, we found the striking cytotoxicity of H₂O₂ higher than 200 μM on cell vitality, LDH activity, and apoptosis percentage in the cells using five different concentrations (50, 100, 200, 400, and 800 μM) of H₂O₂ for 4 h. Moreover, we observed that cell vitality was increased, LDH activity and apoptotic percentage were decreased, and gene expression level of Bax and caspase-3 and -9 was markedly reduced, while gene expression level of Bcl-2 and ratio of Bcl-2/Bax were increased in normal concentration groups of nano-ZnO and ZnSO₄ compared with H₂O₂ group, but no significant difference was observed in caspase-8 gene expression. Furthermore, medium or, more intensely, high concentrations of nano-ZnO and ZnSO₄ enhanced H₂O₂-induced cell apoptosis. Compared with nano-ZnO and ZnSO₄, ZnO showed weakest protective effect on H₂O₂-induced apoptosis at normal concentration and was less toxic to cells at high level. Taken together, we proposed that preventive and protective effects of zinc on H₂O₂-induced cell apoptosis varied in IEC-6 cells with its chemical forms and concentrations, and maybe for the first time, we suggested that nano-ZnO have a protective effect on H₂O₂-induced cell apoptosis in IEC-6 cells.