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纳升规模液滴微阵列上钯催化的联苯组合合成

Palladium-Catalyzed Combinatorial Synthesis of Biphenyls on Droplet Microarrays at Nanoliter Scale.

作者信息

Höpfner Julius, Brehm Marius, Levkin Pavel A

机构信息

Karlsruhe Institute of Technology (KIT), Institute of Biological and Chemical Systems (IBCS), Hermann-von Helmholtz-Platz 1, 76344, Eggenstein-Leopoldshafen, Germany.

Karlsruhe Institute of Technology (KIT), Institute of Organic Chemistry (IOC), Fritz-Haber-Weg 6, 76131, Karlsruhe, Germany.

出版信息

Small. 2024 Jan;20(4):e2304325. doi: 10.1002/smll.202304325. Epub 2023 Sep 19.

DOI:10.1002/smll.202304325
PMID:37726239
Abstract

The rising costs of pharmaceutical research are currently limiting the productivity of drug discovery and development, but can potentially be diminished via miniaturization of the synthesis and screening of new compounds. As droplet microarrays already present themselves as a versatile tool for highly miniaturized biological screening of various targets, their use for chemical synthesis is still limited. In this study, the influential palladium-catalyzed Suzuki-Miyaura reaction is successfully implemented at the nanoliter scale on droplet microarrays for the synthesis of an 800-compound library of biphenyls. Each reaction is carried out in individual 150 nL droplets. Remarkably, the synthesis of these 800 compounds requires a minimal amount of reagents, totaling 80 µmol, and a solvent volume of 400 µL. Furthermore, the cleavage kinetics and purity of the obtained biphenylic compounds are investigated. Via the solid-phase synthesis approach, the compounds could be purified from excess reactants and catalyst prior to the analysis and a UV-cleavable linker allows for fast and additive-free cleavage of each compound into the individual 100 nL droplet. This novel approach expands the toolbox of the droplet microarray for miniaturized high-throughput chemical synthesis and paves the way for future synthesis and screening of chemical compounds in a single platform.

摘要

药物研发成本的不断攀升目前正限制着药物发现与开发的效率,但通过新化合物合成与筛选的小型化,这一成本有可能降低。由于液滴微阵列已成为用于各种靶点的高度小型化生物筛选的通用工具,但其在化学合成方面的应用仍较为有限。在本研究中,具有重要影响的钯催化铃木-宫浦反应在液滴微阵列上成功实现了纳升规模的反应,用于合成一个包含800种联苯化合物的文库。每个反应在单独的150纳升液滴中进行。值得注意的是,合成这800种化合物所需的试剂用量极少,总计80微摩尔,溶剂体积为400微升。此外,还对所得联苯化合物的裂解动力学和纯度进行了研究。通过固相合成方法,在分析之前可从过量反应物和催化剂中纯化化合物,并且一个可紫外裂解的连接子能够将每种化合物快速且无添加剂地裂解到单独的100纳升液滴中。这种新方法扩展了液滴微阵列用于小型化高通量化学合成的工具库,并为未来在单一平台上进行化合物的合成与筛选铺平了道路。

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