Literature DB >> 24056343

A strategy for the diversity-oriented synthesis of macrocyclic scaffolds using multidimensional coupling.

Henning S G Beckmann1, Feilin Nie, Caroline E Hagerman, Henrik Johansson, Yaw Sing Tan, David Wilcke, David R Spring.   

Abstract

A prerequisite for successful screening campaigns in drug discovery or chemical genetics is the availability of structurally and thus functionally diverse compound libraries. Diversity-oriented synthesis (DOS) provides strategies for the generation of such libraries, of which the build/couple/pair (B/C/P) algorithm is the most frequently used. We have developed an advanced B/C/P strategy that incorporates multidimensional coupling. In this approach, structural diversity is not only defined by the nature of the building blocks employed, but also by the linking motif installed during the coupling reaction. We applied this step-efficient approach in a DOS of a library that consisted of 73 macrocyclic compounds based around 59 discrete scaffolds. The macrocycles prepared cover a broad range of different molecular shapes, as illustrated by principal moment-of-inertia analysis. This demonstrates the capability of the advanced B/C/P strategy using multidimensional coupling for the preparation of structurally diverse compound collections.

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Year:  2013        PMID: 24056343     DOI: 10.1038/nchem.1729

Source DB:  PubMed          Journal:  Nat Chem        ISSN: 1755-4330            Impact factor:   24.427


  41 in total

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  29 in total

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Review 4.  Macrocycles as protein-protein interaction inhibitors.

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6.  Cyclization and Docking Protocol for Cyclic Peptide-Protein Modeling Using HADDOCK2.4.

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8.  High content screening of diverse compound libraries identifies potent modulators of tubulin dynamics.

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9.  A diversity-oriented synthesis strategy enabling the combinatorial-type variation of macrocyclic peptidomimetic scaffolds.

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10.  Modular, One-Pot, Sequential Aziridine Ring Opening-S(N)Ar Strategy to 7-, 10-, and 11-Membered Benzo-Fused Sultams.

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