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1.
我们利用基因工程的方法在大肠杆菌中制备了生物素化的膜联蛋白V。为此,我们构建了膜联蛋白V与乙酰C0A羧化产生物素受体肽DCP87的融合基因,并在大肠力中进行了表达。表达产物经HPLC检测,我们发现大约有60%的融合表达产物在大肠杆菌内进行了生物素化。生物素化的膜联蛋白V经抗生物素蛋白亲和层析化后用于吗啡诱导的下丘脑神经元细胞的凋亡检测,取得了理想的结果。  相似文献   

2.
生物素化ATP硫酸化酶的表达、固定化与应用   总被引:1,自引:0,他引:1       下载免费PDF全文
现代大规模焦测序技术的产生是DNA测序技术的一次革命,其关键技术之一是得到高活性的、固定于磁性微球表面的ATP硫酸化酶.生物素化的ATP硫酸化酶可以通过生物素与亲和素之间的特异结合特性固定在包被亲和素的磁性微球表面,但是利用化学修饰法将ATP硫酸化酶进行生物素化修饰很可能会影响酶的活性.利用融合表达策略,将大肠杆菌生物素酰基载体蛋白C端87个氨基酸肽段(BCCP87)与ATP硫酸化酶在大肠杆菌内融合表达,经SDS-PAGE和Western blot分析,表达的融合蛋白分子质量约为64 ku,并且能够在大肠杆菌内被生物素化.生物素化的ATP硫酸化酶能够与亲和素包被的磁珠结合,固定后的ATP硫酸化酶具有活性,并且能够用于定量检测焦磷酸盐(PPi)和焦测序,为今后建立高通量大规模焦测序系统提供了一个有效的工具酶.  相似文献   

3.
目的:克隆表达金黄色葡萄球菌agr系统的受体蛋白AgrC,构建人工超分子体系。方法:构建基因工程菌E.coli TOP10-pBAD-AgrC,对诱导条件进行优化,对蛋白的提取方法进行分析优化。表达产物使用Western blot鉴定,His-tag镍柱亲和层析纯化。使用肽脂质N+C5Gly2C16为膜材料制备囊泡作为载体,将纯化后的蛋白在囊泡上镶嵌。结果:构建的基因工程菌在18℃,0.002%的阿拉伯糖浓度下具有最高的表达效率,以内膜形式存在的AgrC蛋白在表面活性剂BDH中溶解效率最佳。结论:成功诱导表达并纯化了重组蛋白AgrC,成功利用其构建了人工超分子体系。  相似文献   

4.
目的:建立并优化基于Avi-tag标签技术的人胚肾细胞增强型绿色荧光蛋白(eGFP)的定点生物素化标记、纯化和检测方法。方法:分别构建具有Avi-tag标签的eGFP真核表达载体plenti-Avi-eGFP和BirA酶真核过表达载体pQCXIH-BirA,将plenti-Avi-eGFP和pQCXIH-BirA共转染人胚肾293T细胞,12 h后观察Avi-tag标签对eGFP蛋白在细胞内定位的影响;48 h后裂解细胞,用链霉亲和素珠子纯化生物素标记的eGFP,SDS-PAGE观察eGFP纯化和富集情况,并优化基于Western印迹的生物素化eGFP检测方法。结果:Avi-tag标签对eGFP在细胞内的定位无影响,同时BirA酶在293T细胞内可将带Avi-tag标签的eGFP标记上生物素;生物素化的eGFP可特异性地被链霉亲和素珠子纯化和富集,纯度可达95%;Western印迹检测生物素化蛋白的最终条件为5%的BSA作为封闭液和终浓度为100 ng/mL的链霉亲和素-HRP。结论:建立了基于Avi-tag技术的人胚肾细胞内增强型绿色荧光蛋白的生物素化标记、纯化与检测方法,为该方法的广泛应用奠定了前期技术基础。  相似文献   

5.
为探讨白藜芦醇在肿瘤细胞中的结合靶点蛋白质.采用亲和甄别磁珠法生物淘洗白藜芦醇的靶点蛋白质.在构建并优化了白藜芦醇结构模型的基础上,通过分子动力学优化分析白藜芦醇与其靶点蛋白质的结构模型,并且使用分子对接分析验证两者的结合作用.结果表明,亲和甄X别磁珠法直接筛选到的能与白藜芦醇的特异性结合的蛋白质是Myosin蛋白质和Actin蛋白质,并且成功构建得到了合理的白藜芦醇分子与Actin蛋白质的复合物的三维结构.通过分析白藜芦醇分子与Actin蛋白活性氨基酸残基结合模式发现,残基Val30,Phe31,Pro32,Thr203,Ala204,Glu205,Pro243,Asp244,等对两者的结合都有重要贡献.白藜芦醇是通过作用于肿瘤细胞的骨架结构蛋白来干扰细胞的有丝分裂过程,从而导致肿瘤细胞的体外增殖受到抑制.  相似文献   

6.
江年  茆灿泉 《生物信息学》2009,7(4):284-287,291
金属离子与金属结合肽(蛋白)的相互作用与应用研究,一直是生物无机化学的重点和热点,也是分子间相互作用研究领域的难点。本研究利用ClustalX、BLAST等生物信息技术与方法对大量已知的重金属结合肽进行分析与数据挖掘。确定筛选获得的重金属结合肽常富含His,无Cys,无金属结合肽模式序列,进化不保守;部分氨基酸序列结构(如六肽)可在蛋白数据库中找到相似序列。序列特征主要为Zn^2+相关的转录因子。本研究为重金属结合蛋白-重金属离子的相互作用分析简化为重金属结合肽-重金属离子的结构模拟与分析提供了重要的理论基础和研究手段。  相似文献   

7.
目的观察香菇多糖联合羟喜树碱治疗癌性胸水的临床疗效及不良反应。方法选择我院2010年1月~2013年3月确诊癌症胸水患者96例,随机分为香菇多糖联合羟喜树碱组(治疗组)48例和DDP(对照组)48例,观察香菇多糖联合羟喜树碱对癌性胸水的疗效。结果治疗组总有效率为83.3%,明显高于对照组的62.5%(P0.05)。结论香菇多糖联合羟喜树碱治疗癌性胸水具有一定的临床价值,不良反应少。  相似文献   

8.
-鹅膏毒(环)肽和二羟鬼笔毒(环)肽是剧毒的鹅膏菌和其它几种致死毒菌中由一些修饰氨基酸组成的环肽毒素。由于-鹅膏毒肽对真核生物的mRNA合成的专一性抑制和和二羟鬼笔毒肽对肌动蛋白的专一性束缚,因而它们在分子生物学和细胞学研究中具有重要应用,对其需求逐步增加。为此,作者使用了一种改良的毒素提取方法,以制备高效液相色谱从灰花纹鹅膏菌中分离制备-鹅膏毒肽和二羟鬼笔毒肽,并通过紫外吸收光谱和质谱进行鉴定,表明-鹅膏毒肽和二羟鬼笔毒肽的分离效果好,纯度高。本方法对其它毒菌中的-鹅膏毒肽和二羟鬼笔毒肽的分离制备具有同样的应用价值。  相似文献   

9.
-鹅膏毒(环)肽和二羟鬼笔毒(环)肽是剧毒的鹅膏菌和其它几种致死毒菌中由一些修饰氨基酸组成的环肽毒素。由于-鹅膏毒肽对真核生物的mRNA合成的专一性抑制和和二羟鬼笔毒肽对肌动蛋白的专一性束缚,因而它们在分子生物学和细胞学研究中具有重要应用,对其需求逐步增加。为此,作者使用了一种改良的毒素提取方法,以制备高效液相色谱从灰花纹鹅膏菌中分离制备-鹅膏毒肽和二羟鬼笔毒肽,并通过紫外吸收光谱和质谱进行鉴定,表明-鹅膏毒肽和二羟鬼笔毒肽的分离效果好,纯度高。本方法对其它毒菌中的-鹅膏毒肽和二羟鬼笔毒肽的分离制备具有同样的应用价值。  相似文献   

10.
α-鹅膏毒(环)肽和二羟鬼笔毒(环)肽是剧毒的鹅膏菌和其它几种致死毒菌中由一些修饰氨基酸组成的环肽毒素.由于α-鹅膏毒肽对真核生物的mRNA合成的专一性抑制和和二羟鬼笔毒肽对肌动蛋白的专一性束缚,因而它们在分子生物学和细胞学研究中具有重要应用,对其需求逐步增加.为此,作者使用了一种改良的毒素提取方法,以制备高效液相色谱从灰花纹鹅膏菌中分离制备α-鹅膏毒肽和二羟鬼笔毒肽,并通过紫外吸收光谱和质谱进行鉴定,表明α-鹅膏毒肽和二羟鬼笔毒肽的分离效果好,纯度高.本方法对其它毒菌中的α-鹅膏毒肽和二羟鬼笔毒肽的分离制备具有同样的应用价值.  相似文献   

11.
In this work, fluorescence spectroscopy in combination with circular dichroism spectroscopy and molecular modeling was employed to investigate the binding of 10-hydroxycamptothecin (HCPT) to human serum albumin (HSA) under simulative physiological conditions. The experiment results showed that the fluorescence quenching of HSA by HCPT was a result of the formation of HCPT–HSA complex. The corresponding association constants (K a) between HCPT and HSA at four different temperatures were determined according to the modified Stern–Volmer equation. The results of thermodynamic parameters ΔG, ΔH, and ΔS indicated that hydrogen bonds and van der Waals forces played major roles for HCPT–HSA association. Site marker competitive displacement experiment indicated that the binding of HCPT to HSA primarily took place in sub-domain IIA (site I). Molecular docking study further confirmed the binding mode and the binding site obtained by fluorescence and site marker competitive experiments. The conformational investigation showed that the presence of HCPT decreased the α-helical content of HSA and induced the slight unfolding of the polypeptides of protein, which confirmed some micro-environmental and conformational changes of HSA molecules.  相似文献   

12.

Background  

Hydroxycamptothecin (HCPT) has been shown to have activity against a broad spectrum of cancers. In order to enhance its tissue-specific delivery and anticancer activity, we prepared HCPT-loaded nanoparticles made from poly(ethylene glycol)-poly(γ-benzyl-L-glutamate) (PEG-PBLG), and then studied their release characteristics, pharmacokinetic characteristics, and anticancer effects. PEG-PBLG nanoparticles incorporating HCPT were prepared by a dialysis method. Scanning electron microscopy (SEM) was used to observe the shape and diameter of the nanoparticles. The HCPT release characteristics in vitro were evaluated by ultraviolet spectrophotometry. A high-performance liquid chromatography (HPLC) detection method for determining HCPT in rabbit plasma was established. The pharmacokinetic parameters of HCPT/PEG-PBLG nanoparticles were compared with those of HCPT.  相似文献   

13.
Fu YR  Yi ZJ  Yan YR  Qiu ZY 《Mitochondrion》2006,6(4):211-217
The camptothecin (CPT) derivative hydroxycamptothecin (HCPT) containing 10-hydroxy represents one of the most potent topoisomerase I inhibitors described. This anticancer agent, currently undergoing clinical trials on gastric tumours, has been shown more active and less toxic than conventional camptothecins. To shed light on the mechanism of action of HCPT at the cellular level, we examined cell growth, apoptosis, changes of mitochondrial membrane potential, cytochrome c and AIF translocation in cancer cells by exposing these cells to HCPT for indicated time. The effect of HCPT on cell proliferation was measured by MTT (3-[4,5-dimethylthiazol-2-yl]-2,5-diphenyl tetrazolium bromid) assay and apoptosis was measured using flow cytometry, fluorescence microscopy and electron microscopy. Changes of mitochondrial membrane potential were monitored by fluorescence microscope. Western blot analysis was used to evaluate the release of mitochondrial cytochrome c and AIF; On the other hand, translocation of cytochrome c and AIF from mitochondria to cytosol during apoptosis were confirmed by confocal microscopy. HCPT could noticeably inhibit the proliferation of SMMC-7721cells and the IC(50) dose was about 0.22muM; SMMC-7721 cells treated with HCPT showed typical characteristics of apoptosis rather than necrotic including phosphatidylserine (PS) exposed from the inner to the outer leaflet of the plasma membrane, abnormal cell morphology, chromatin condensation and nuclear fragmentation; On the other hand, during process of cell apoptosis, mitochondrial transmembrane potential was reduced; Compared with the control group, the mRNA and protein expression of cytochrome c and AIF in treated and untreated SMMC-7721 cells were not significantly changed (not shown). However, when cells were treated with HCPT, the massive translocation of cytochrome c and AIF to the nucleus was evident. Our results indicate that HCPT can inhibit proliferation and induce apoptosis of human hepatoma SMMC-7721 cells. Mitochondrial pathway of apoptosis, especially for cytochrome c and AIF translocation, may play an important role in apoptosis induced by HCPT.  相似文献   

14.
Peptides with both an affinity for ZnO and the ability to generate ZnO nanoparticles have attracted attention for the self‐assembly and templating of nanoscale building blocks under ambient conditions with compositional uniformity. In this study, we have analyzed the specific binding sites of the ZnO‐binding peptide, EAHVMHKVAPRP, which was identified using a phage display peptide library. The peptide binding assay against ZnO nanoparticles was performed using peptides synthesized on a cellulose membrane using the spot method. Using randomized rotation of amino acids in the ZnO‐binding peptide, 125 spot‐synthesized peptides were assayed. The peptide binding activity against ZnO nanoparticles varied greatly. This indicates that ZnO binding does not depend on total hydrophobicity or other physical parameters of these peptides, but rather that ZnO recognizes the specific amino acid alignment of these peptides. In addition, several peptides were found to show higher binding ability compared with that of the original peptides. Identification of important binding sites in the EAHVMHKVAPRP peptide was investigated by shortened, stepwise sequence from both termini. Interestingly, two ZnO‐binding sites were found as 6‐mer peptides: HVMHKV and HKVAPR. The peptides identified by amino acid substitution of HKVAPR were found to show high affinity and specificity for ZnO nanoparticles. Biotechnol. Bioeng. 2010;106: 845–851. © 2010 Wiley Periodicals, Inc.  相似文献   

15.
Antiangiogenic potential of 10-hydroxycamptothecin   总被引:12,自引:0,他引:12  
Xiao D  Tan W  Li M  Ding J 《Life sciences》2001,69(14):1619-1628
To investigate the antiangiogenic potential of 10-hydroxycamptothecin (HCPT), the proliferation of human microvascular endothelial cells (HMEC) and seven human tumor cell lines were detected by SRB assay, and the endothelial cell migration and tube formation were assessed using two in vitro model systems. Also, inhibition of angiogenesis was determined with a modification of the chick embryo chorioallantoic membrane (CAM) assay in vivo. Morphological assessment of apoptosis was performed by fluorescence microscope. HCPT 0.313-5 micromol x L(-1) treatment resulted in a dose-dependent inhibition of proliferation, migration and tube formation in HMEC cells, and HCPT 6.25-25 nmol x egg(-1) inhibited angiogenesis in CAM assay. HCPT 1.25-5 micromol x L(-1) elicited typical morphological changes of apoptosis including condensed chromatin, nuclear fragmentation, and reduction in volume in HMEC cells. HCPT significantly inhibited angiogenesis both in vitro and in vivo at relatively low concentrations, and this effect was related with induction of apoptosis in HMEC cells. These results taken collectively suggest that HCPT may be a potent antiangiogenetic and cytotoxic drug and further investigation is warranted.  相似文献   

16.
Specificities of three mouse major histocompatibility complex (MHC) class I molecules, Kb, Db, and Ld, were analyzed by positional scanning using combinatorial peptide libraries. The result of the analysis was used to create a scoring program to predict MHC-binding peptides in proteins. The capacity of the scoring was then challenged with a number of peptides by comparing the prediction with the experimental binding. The score and the experimental binding exhibited a linear correlation but with substantial deviations of data points. Statistically, for approximately 80% of randomly chosen peptides, MHC-binding capacity could be predicted within one log concentration of peptides for a half-maximal binding. Known cytotoxic T-lymphocyte epitope peptides could be predicted, with a few exceptions. In addition, frequent findings of MHC-binding peptides with incomplete or no anchor amino acid(s) suggested a substantial bias introduced by natural antigen processing in peptide selection by MHC class I molecules.  相似文献   

17.
10-hydroxycamptothecin (HCPT), a natural plant extract, exerts anticancer capacity. HCPT has been reported to induce apoptosis and autophagy in human cancer cells. The interaction between autophagy and apoptosis induced by HCPT and the molecular mechanism in bladder cancer cells were investigated in this study. Our results confirmed that HCPT suppressed cell viability and migration and caused cell-cycle arrest in T24 and 5637. Then, we used Z-VAD(OMe)-FMK to clarify that apoptosis induced by HCPT was mediated by caspase. Moreover, HCPT boosted autophagy through activating the AMPK/mTOR/ULK1 pathway. Blocking autophagy by 3-methyladenine, the adenosine monophosphate-activated protein kinase (AMPK) inhibitor dorsomorphin and siATG7 reversed HCPT-induced cytotoxicity. Conversely, rapamycin and the AMPK activator AICAR enhanced growth inhibition and cell apoptosis, suggesting that autophagy played a proapoptosis role. Taken together, our findings showed that HCPT-induced autophagy mediated by the AMPK pathway in T24 and 5637 cell lines, which reinforced the apoptosis, indicating that HCPT together with autophagy activator would be a novel strategy for clinical treatment in bladder cancer.  相似文献   

18.
The effect of plant growth regulators (PGRs) on the accumulation of the alkaloid camptothecin (CPT) and its analogue 10-hydroxycamptothecin (HCPT) in tender leaves of Camptotheca acuminata saplings was studied. In screening experiments for PGRs, 40?mg/L dose of thiourea, triacontanol, and ascorbic acid (VC) had no positive effects on the accumulation of the alkaloids. However, treatments with 40?mg/L of chlormequat chloride (CCC), choline chloride, paclobutrazol (PBZ), and daminozide (B9) induced CPT and HCPT accumulation in both pre-harvest and postharvest stages. On that basis, five levels of PGRs at 0, 20, 40, 60, 80?mg/L were sprayed on tender leaves of C. acuminata saplings at pre-harvest and postharvest stages. Treatment by 40?mg/L CCC dramatically enhanced HCPT production by 308?% in pre-harvest, treatment by 60?mg/L CCC enhanced HCPT production by 100?% in postharvest. Spraying the leaves with 60?mg/L choline chloride resulted in 94?% increase of CPT and spraying with 40?mg/L of the PGRs reached 167?% increase of HCPT in the pre-harvest treatment, respectively; treatments with 60?mg/L choline chloride resulted in 64?% increase of CPT and 525?% increase of HCPT in postharvest, respectively. 52?% increase of CPT and 86?% increase of HCPT in pre-harvest, 22?% increase of CPT and 33?% increase of HCPT in postharvest were obtained by spraying leaves with 60?mg/L PBZ. Treatments with 40?mg/L B9 had the highest impact on CPT (12?% increase in pre-harvest, 11?% increase in postharvest) and HCPT (167?% increase in pre-harvest, 173?% increase in postharvest) accumulation. The optimal PGR for obtaining the highest levels of CPT and HCPT was treatment with 60?mg/L choline chloride. In most case, the pre-harvest treatment was better than the postharvest one. These preliminary results suggest that the application of PGRs may be a useful and feasible method to increase CPT and HCPT levels in C. acuminata.  相似文献   

19.
Prostate specific antigen (PSA) is a member of kallikrein family having serine protease-like activity and acts as a prognostic marker of prostate carcinoma. Various studies have been performed on inhibition of PSA and such targeting requires the identification of highly selective peptide inhibitors. PSA was purified from human seminal plasma by rapid and efficient methods, and binding studies for various peptides were carried out by fluorescence spectroscopy and SPR. The 'S' of PSA is predominated by hydrophobic residues, and hence many hydrophobic peptides were used to determine their binding affinity to PSA by fluorescence spectroscopy. We observed that LLFW, FFKW, and KFW binds strongly to PSA, among them LLFW showed strong binding. SPR also showed strong binding affinity of PSA toward peptides with hydrophobic and basic residues. Among the peptides used, FWYS showed dramatic increase in binding affinity (10(-10) M). The peptides analyzed for binding studies, suggests that peptide with Trp residue along with basic or hydrophobic amino acids may be useful for designing specific inhibitors for PSA. The strong affinities of designed peptides for PSA can be a valuable tool for designing therapeutic agents for prostate carcinomas.  相似文献   

20.
范莲  袁志兰  陈琴  田寅辉  顾洛 《生物磁学》2011,(16):3067-3070
目的:研究羟基喜树碱(HCPT)对体外培养的人眼Tenon囊成纤维细胞(Human Tenon's capsule fibroblasts,HTFs)增殖、移行的影响。方法:取正常供体新鲜的Tenon囊组织,采用组织块培养法,进行成纤维细胞的体外培养,并用光镜、免疫荧光法观察鉴定;MTT法、划痕法检测不同浓度的HCPT(0、0.031、0.062、0.125、0.25、0.5、1、2、4mg/1)对HTFs增殖、移行的影响,并与MMC对比。结果:HTFs体外生长良好,经光镜和免疫荧光法观察鉴定为成纤维细胞;与空白对照组比较,HCPT(0.031-4mg/1)、MMC(0.0031-0.4mg/1)均能有效抑制HTFs的增殖,且呈一定的剂量、时间依赖性,HCPT作用24h、48h、72h的IC50分别为2.24mg/1、O.76mg/1、0.39mg/1,MMC作用24h、48h、72h的IC50分别为0.34mg/1、0.24mg/1、0.07mg/1;与空白对照组比较,HCPT(0.031-4mg/1)、MMC(O.0031-0.4mg/1)均能抑制HTFs迁移,呈剂量依赖性,而与时间无显著相关。结论:HCPT、MMC均能有效抑制HTFs的增殖和移行,其效应MMC约为HCPT的10倍。  相似文献   

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