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国家重点基础研究发展计划(2010CB732404)

作品数:30 被引量:63H指数:4
相关作者:陈宝安程坚夏国华鲍文王坚更多>>
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发文基金:国家重点基础研究发展计划国家自然科学基金江苏省医学重点学科基金更多>>
相关领域:医药卫生化学工程理学生物学更多>>

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30 条 记 录,以下是 1-10
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体外光化学疗法治疗慢性移植物抗宿主病的研究进展被引量:1
2015年
慢性移植物抗宿主病(c GVHD)是异基因造血干细胞移植后的主要并发症及导致患者死亡的主要原因之一。体外光化学疗法(extracorporeal photochemotherapy,ECP)已成为治疗c GVHD的一种有效手段,它是用长波紫外线照射患者的单个核细胞与光敏剂8-甲氧基补骨脂素的混合并回输至患者体内达到治疗疾病的目的。ECP治疗作用主要是通过诱导细胞凋亡、影响树突状细胞的功能及诱导免疫耐受等来实现的。它具有不增加患者的感染风险,不影响移植物抗白血病效应和副作用小等诸多优点。国外很多医学中心对ECP治疗成人及儿童c GVHD展开了大量研究,在临床上取得了较好的疗效。CD19+CD21-B淋巴细胞、血清BAFF及血清TNFα可用于衡量及早期评价ECP的治疗疗效。ECP的疗效与诸多因素相关,在治疗过程中会出现若干并发症。由于目前ECP治疗机制尚未完善明确,诸多研究治疗周期长短不一,临床研究病人例数较少等原因在一定程度上限制了其推广应用。相信在不久的将来,随着基础研究的深入、临床样本量的增多及治疗周期的规范,ECP会具有更加广泛的应用前景。本文主要针对ECP治疗c GVHD的相关研究进展展开论述。
陈润哲陈宝安程坚
关键词:异基因造血干细胞移植慢性移植物抗宿主病
Real-time detection of the interaction between anticancer drug daunorubicin and cancer cells by Au-MCNT nanocomposites modified electrodes被引量:1
2011年
In this study,we have prepared the blending of gold nanoparticles-multiwalled nanotubes (Au-MCNTs) and then applied the new nanocomposites to modify the glassy carbon electrode (GCE) for highly sensitive detection of the interaction between anticancer drug daunorubicin (DNR) and cancer cells. Electrochemical analysis indicates that the Au-MCNT modified GCE shows high sensitivity and could track the real time response of cancer cells under DNR treatments. Therefore,this new nano-interface and Au-MCNT modified electrode could be explored as a rapid,highly sensitive,and convenient real-time detection strategy in cancer related research and would have prospect in other biomedical applications.
LI QingNingWU XiaoJingZHAO JuanWU ChangYuWANG XueMei
In-situ green synthesis of highly active GSH-capped Pt–Au–Ag-hybrid nanoclusters被引量:2
2014年
Recently much attention has been paid to the application of metal hybrid nanoparticles in industrial catalytic fields because of their super-efficient catalytic activity and attractive properties. We explored a novel strategy to prepare GSH-capped Pt–Au–Ag-hybrid nanoclusters through the synergistic effect between ascorbic acid(VC) and glutathione(GSH) with chloroplatinic acid, chloroauric acid, and silver nitrate as precursors. The potential utilization of as-prepared GSH-capped Pt–Au–Aghybrid nanoclusters for catalytic applications has been evaluated through the reduction of 4-nitrophenol(4-NP) with NaBH4; we obtained the kinetic data by monitoring with UV-Vis spectroscopy. Our results illustrate that GSH-capped Pt–Au– Ag-hybrid nanoclusters could facilitate the process of reduction of 4-NP in a way that is unprecedented. This approach may offer a novel, non-cytotoxicity, efficient catalyst for industry.
CHEN DongHuaGAO ShengPingUR REHMAN FawadJIANG HuiWANG XueMei
关键词:4-NITROPHENOL
Enhanced in vitro anticancer activity of quercetin mediated by functionalized CdTe QDs被引量:2
2014年
We report in this study the effects of red-emitting CdTe QDs capped with cysteamine(Cys-CdTe) on the in vitro anticancer activity of the well-known flavenoid quercetin(Qu). Various techniques, including the methylthiazolyldiphenyl-tetrazolium bromide assay, the real-time cell electronic sensing system, the optical and fluorescence imaging, and electrochemical methods have been utilized to study the potential interactions of Cys-CdTe QDs with Qu. The observations demonstrate that the safe-dosage Cys-CdTe QDs can greatly improve the drug uptake and enhance the inhibition efficiency of Qu towards the proliferation of cancer cells such as HepG2 cells. This study implies that Cys-CdTe QDs may be used for cancer therapy and that they exert a synergic anticancer effect when bound to drug molecules.
WU ChunHuiSHI LiXinWU ChangYuGUO DaDongSELKE MatthiasWANG XueMei
关键词:QUERCETINNANOCOMPOSITES
The cellular labeling and pH-sensitive responsive-drug release of celastrol in cancer cells based on Cys-CdTe QDs被引量:6
2014年
As one of the active compounds derived from Traditional Chinese Medicine,Celastrol(CSL)had cytotoxicity for human leukemia cancer cells K562 and its multidrug-resistant cell line K562/A02.Here,we introduced cysteamine-modified CdTe QDs as the labeling and drug carrier into CSL research and found that the self-assembly and conjugation of anticancer molecular CSL with the Cys-CdTe QDs could significantly increase the drug’s cytotoxicity for K562 cells.More important,these CSL-Cys-CdTe nanocomposites could overcome the multidrug resistance of K562/A02 cells and efficiently inhibit the cancer cell proliferation by realizing the pH-sensitive responsive release of CSL to cancer cells.The enhanced cytotoxicity was caused by the increase of the G2/M phase arrest for K562/A02 cells as well as for K562 cells.Cys-CdTe QDs can readily bind on the cell plasma membranes and be internalized into cancer cells to trace and detect human leukemia cancer cells in real time.In addition,these Cys-CdTe QDs can facilitate the inhibition of the multidrug resistance of K562/A02 cells and readily induce apoptosis.As a good photosensitizer for the therapy,labeling,and tracing of cancer cells,the combination of CSL with Cys-CdTe QDs can optimize the use of and a new potential therapy method for CSL and yield new tools to explore the mechanisms of active compounds from Traditional Chinese Medicine.
LI JingYuanSHI LiXinSHAO YiXiangSELKE MatthiasCHEN BaoAnJIANG HuiWANG XueMei
关键词:CELASTROLLABELING
基于仿生分子识别的恶性肿瘤快速诊断与活体成像分析研究
恶性肿瘤严重威胁着人类健康,其早期诊断和治疗一直是相关学科和领域广泛关注的研究重点和难点。近年来,我们从生物医学领域有应用前景的纳米生物材料入手,运用超分子自组装技术构筑新型功能分子识别界面,采取优势互补策略制备了具有良...
王雪梅
Green photochemical synthesis of fluorescent carbon spheres in-situ enwrapped around Ag nanoparticles
2015年
Biocompatible carbon-spheres-based nanocomposites exhibit great potential in biomedical and clinical applications. In this contribution we report the first green photochemical synthesis of carbon spheres through in-situ enwrapping around silver nanoparticles(CS–Ag NPs). Since mesoporous carbon spheres can provide the location for combining Ag NPs and other agents, one-step synthesis of glutathione-stabilized CS–Ag NPs could be readily realized by photoreduction. TEM characterization of CS–Ag NPs nanocomposites illustrates that Ag NPs were superbly wrapped inside the carbon spheres and also adhered to the surfaces of the carbon spheres. These porous CS–Ag NPs show excellent fluorescence and effective antibacterial efficiency, exhibiting ideal lengthened activities against Escherichia coli and Staphylococcus aureus compared with bare Ag NPs. The relevant rationale behind it could be attributed to the fact that CS–Ag NPs nanocomposites can provide some excellent niches for the durable and slow release of silver ions. This raises the possibility of promising applications of CS–Ag NPs nanocomposites as excellent antibacterial agents for the efficient monitoring of some disease-related bacteria.
Wei GeXiaoli LiuJing YeQiwei LiHui JiangXuemei Wang
C3435T多态性与肿瘤发病风险及疗效的关系
2011年
多药耐药基因1(MDR1)C3435T多态性影响肿瘤发病风险及疗效.由于T等位基因能够使致癌物质更易在组织中积聚,因此TT基因型患者更易发生乳腺癌、胃癌、结直肠癌.并且C3435TTT基因型与KRAS基因野生型同时存在的患者化疗效果最好.但由于种族不同、地区差异、样本量不同等客观因素存在,C3435T多态性与乳腺癌、胃癌患者化疗效果的关系仍在探索中.
菅子莹陈宝安
关键词:MDR乳腺肿瘤胃肿瘤结直肠肿瘤
晚期糖基化终产物对人肝癌细胞HepG2增殖的影响
2012年
目的探讨糖尿病晚期糖基化终产物(AGEs)对肝癌细胞HepG2增殖的影响及其机制。方法体外培养人肝癌细胞HepG2,以终浓度分别为100、200和400μg/ml的AGEs处理细胞24h,并设正常对照组进行比较。运用细胞计数试剂盒8研究AGEs对HepG2增殖的影响,流式细胞术检测细胞周期的改变,Western blot检测肝癌细胞抗凋亡基因表达。结果 AGEs呈浓度依赖性显著促进HepG2细胞增殖(P<0.05)。与对照组比较,200μg/ml AGEs干预24h后可以减少HepG2细胞G1期百分率,同时增加S期百分率(P<0.05)。AGEs可致细胞抗凋亡基因B细胞淋巴瘤-白血病2(Bcl-2)相关蛋白表达增加。结论 AGEs能促进HepG2细胞的增殖,其机制可能与上调Bcl-2相关蛋白表达,加速细胞G1期向S期转换相关。
燕丹王坚陈宝安沈洁王钿钿
关键词:晚期糖基化终产物肝癌HEPG2细胞细胞增殖
DNA聚合与RNA转录联用分子机器的改进
2013年
建立了一个集成DNA聚合和RNA转录过程,能够重复产生RNA适体片段,并结合孔雀石绿产生荧光信号的分子机器,并探索了此分子机器在检测DNA方面的应用。转录产生的大量孔雀石绿适体序列被释放到溶液中,并可以与孔雀石绿结合产生荧光,实现信号的放大。85μL体系中的聚合转录的最适条件为:DNA聚合酶10IU(0.118IU·μL-1),RNA聚合酶60IU(0.706IU·μL-1),反应时间为3h。在上述条件下,荧光信号随着引发DNA用量的增加而增大。
王明印任锐
关键词:孔雀石绿RNA检测
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