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化学信息学的涵义及教育 总被引:9,自引:0,他引:9
化学信息学是近年来发展起来的新学科 ,它的产生与发展是基于化学信息量指数般增长 ,特别是组合化学及高通量筛选的迅速发展。组合化学方法能像搭积木块一样快速合成及制备大量的化合物。一个组合化学库包括数百个至数十万个化合物 ,为药物开发提供丰富的化合物源。高通量筛选能达到 1× 1 0 4~ 1× 1 0 5 个化合物 /天。组合化学及高通量筛选为药物研制提供新的技术支柱 ,同时也为化学信息学的产生与发展提供良好的机遇。 人类基因组计划为药物开发与疾病的治疗提供众多的新靶标。据 1 996年统计用于药物研制的靶标有 483个分子靶 (其… 相似文献
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化学拆分的新方法研究 总被引:8,自引:0,他引:8
主要介绍了近年来发展起来的两种化学拆分新方法,包括拆分和组合拆分;并简要论述了化学拆分中的手性识别现象,以及化学拆分方法在手性药物制备中的应用。 相似文献
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组合化学——合成化学领域的一次革命 总被引:5,自引:0,他引:5
组合化学是近十几年逐渐发展成熟起来的一个学科,它从根本上改变了化学家、生物学家以及相关学科研究人员的思维和研究方式,对科学的发展产生了革命性的影响。组合化学从创立起就与工业应用紧密联系在一起,它带动了包括新药发明和新材料研制在内的一系列高新科技产业的发展。下面简述了组合化学的起源与发展、研究方法及其对相关学科的影响和技术前景。 相似文献
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动态组合化学是组合化学的一个新兴分支,在药物先导化合物的发现中有广阔的应用前景。在动态组合化学库中,利用靶标分子的诱导结合作用,通过可逆共价反应,能够选择性的筛选到与靶标分子存在强相互作用的优势化合物。本文按照动态组合化学方法简介、动态组合化学中的可逆共价化学、动态组合化学库的分类、动态组合化学库筛选方法的研究进展及动态组合化学在药物先导化合物发现过程中的应用等5个方面对动态组合化学进行了概述。 相似文献
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《高等学校化学学报》2001,22(3):484
吉林大学组合化学研究中心是以组合化学技术研究开发为主体的跨学科的科研教学中心。主要科研方向及特色是快速合成反应的开发与应用 ;组合化学库的设计、开发及应用 ;组合化学在新药开发及新材料、新催化剂中的应用以及快速合成系统的研制和开发。该研究中心拥有近 1 0 0 0 m2的实验室 ,包括合成实验室、分析测试中心、计算中心 ;拥有目前国际上先进的自动化合成仪、高通量分析、高通量设备、LC-MS等组合化学设备和大型分析测试仪器。吉林大学组合化学研究中心现已经形成一支以留学归国人员为核心的高层次的科研和教学队伍。为进一步加强… 相似文献
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微型全化学分析系统及技术进展 总被引:9,自引:0,他引:9
对微型全化学分析系统(μ-TAS)的发展现状及其应用领域进行了综述,对μ-TAS在毛细管电泳微型化、DNA及生化分析、组合化学研究等领域的应用研究作了重点介绍. 相似文献
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组合化学是一种将计算机辅助设计、有机化学合成以及高通量筛选一体化的技术. 它以高效、微量、高度自动化的特点而受到世人瞩目, 对药物研发中加速寻找先导化合物起到了极大的推进作用. 近年来随着纳米技术的迅速发展, 组合化学策略和高通量技术也在此领域中得到应用. 为在今后的研究中能够更好地将组合化学技术应用于纳米材料和纳米技术研究领域, 本文综述了组合化学在开发新型纳米材料以及通过对纳米材料进行表面化学修饰来提高其在生物医学领域的应用研究进展, 并对目前应用于纳米技术研究的高通量筛选技术, 如磁共振成像、自动化基因芯片系统和荧光激活细胞分类术以及对纳米组合化学目前遇到的一些挑战进行了简单概括, 并对其未来的发展趋势提出了展望. 相似文献
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随着组合化学的迅速发展, 兼容固相合成和溶液相合成优点的液相合成方法已成为实现组合化学的一条重要途径. 综述了近年来聚乙二醇为可溶性聚合物载体支载的杂环化合物库的研究, 并展望了其今后的发展方向. 相似文献
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组合化学在功能材料合成方面的应用 总被引:3,自引:0,他引:3
组合化学方法是当今材料科学和化学领域的研究热点。组合化学方法首先在新药的合成领域得到应用, 很快就以其合成周期短、合成的样品数量大、节约经费等诸多优点而拓展到功能材料的合成等其它领域。组合化学的方法有许多种, 按照反应相的不同可以分为液相中的组合合成法和固相中的组合合成法, 固相组合合成又可以根据所选用的掩模方式的不同而分为二分阴影掩模法、四分阴影掩模法、可移动百叶窗式掩模法等几种, 可以根据材料合成的实际需求加以选择。 相似文献
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Recognizing the potential of combinatorial chemistry to accelerate drug discovery and development, most pharmaceutical and related industries are seriously looking toward combinatorial synthesis of compounds in order to facilitate the identification of 'lead' molecules. In particular, solid phase synthesis is the core technology for combinatorial chemistry and is widely used for generating libraries of structurally related compounds. Since many drugs contain the nitrogen heterocyclic component and since heterocycles possess a high order of structural diversity, a precise overview of recent progress in the combinatorial synthesis of nitrogen heterocycles using solid phase methodology would be useful. Since the progress in solid phase synthesis of organic molecules has been reviewed regularly from 1992 to 1998, only the development of solid phase combinatorial synthetic approaches of small nitrogen heterocycles since 1999 will be reviewed here. This review describes the solid phase synthesis of azepanes, benzodiazepines, benzimidazoles, benzothiazepines, cinnolines, indolizines, beta lactams, oxazepins, oxazoles including benzisooxazoles, hydantoins, piperidines, pyrimidines, pyrazolones, quinolones, trizolopyridazines and thiazoles. 相似文献
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Combinatorial chemistry is a tool for selecting molecules with special properties. Dynamic combinatorial chemistry started off aiming to be just that. However, unlike ordinary combinatorial chemistry, the interconnectedness of dynamic libraries gives them an extra dimension. An understanding of these molecular networks at systems level is essential for their use as a selection tool and creates exciting new opportunities in systems chemistry. In this feature article we discuss selected examples and considerations related to the advanced exploitation of dynamic combinatorial libraries for their originally conceived purpose of identifying strong binding interactions. Also reviewed are examples illustrating a trend towards increasing complexity in terms of network behaviour and reversible chemistry. Finally, new applications of dynamic combinatorial chemistry in self-assembly, transport and self-replication are discussed. 相似文献
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López-Vallejo F Caulfield T Martínez-Mayorga K Giulianotti MA Nefzi A Houghten RA Medina-Franco JL 《Combinatorial chemistry & high throughput screening》2011,14(6):475-487
Virtual screening is increasingly being used in drug discovery programs with a growing number of successful applications. Experimental methodologies developed to speed up the drug discovery processes include high-throughput screening and combinatorial chemistry. The complementarities between computational and experimental screenings have been recognized and reviewed in the literature. Computational methods have also been used in the combinatorial chemistry field, in particular in library design. However, the integration of computational and combinatorial chemistry screenings has been attempted only recently. Combinatorial libraries (experimental or virtual) represent a notable source of chemically related compounds. Advances in combinatorial chemistry and deconvolution strategies, have enabled the rapid exploration of novel and dense regions in the chemical space. The present review is focused on the integration of virtual and experimental screening of combinatorial libraries. Applications of virtual screening to discover novel anticancer agents and our ongoing efforts towards the integration of virtual screening and combinatorial chemistry are also discussed. 相似文献
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Combinatorial synthesis of anti-HIV agents--a review 总被引:1,自引:0,他引:1
Sriram D Yogeeswari P Nagappa AN 《Combinatorial chemistry & high throughput screening》2005,8(5):377-385
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Solid-phase extraction for combinatorial libraries 总被引:3,自引:0,他引:3
Nilsson UJ 《Journal of chromatography. A》2000,885(1-2):305-319
Solid-phase extraction (SPE) has during the last three years emerged as a convenient method for the purification of compound libraries prepared by solution synthesis. The widespread use of SPE in combinatorial chemistry can be explained by straightforward SPE method development facilitated by the availability of numerous commercial SPE resins. High-speed automated SPE is readily accomplished by taking advantage of commercial laboratory robot systems. The present review summarizes and discusses advancements made in the use of different SPE resins and molecule tagging techniques for optimization of ion-exchange, reversed-phase, normal-phase and fluorous-phase SPE in combinatorial chemistry. 相似文献
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Pérez-Fernández R Pittelkow M Belenguer AM Sanders JK 《Chemical communications (Cambridge, England)》2008,(15):1738-1740
A two-phase approach to dynamic combinatorial chemistry is described using disulfide exchange chemistry; the use of two phases significantly increases the possibilities and the scope of dynamic combinatorial chemistry by facilitating the combination of otherwise incompatible building blocks. 相似文献