Chemical Biology and Therapeutics Science Program, Broad Institute, 415 Main Street, Cambridge, MA, 02142, USA.
Novartis Institutes for BioMedical Research, 181 Massachusetts Avenue, Cambridge, MA, 02139, USA.
Nat Commun. 2023 Aug 15;14(1):4930. doi: 10.1038/s41467-023-40575-5.
Diversity-oriented synthesis (DOS) is a powerful strategy to prepare molecules with underrepresented features in commercial screening collections, resulting in the elucidation of novel biological mechanisms. In parallel to the development of DOS, DNA-encoded libraries (DELs) have emerged as an effective, efficient screening strategy to identify protein binders. Despite recent advancements in this field, most DEL syntheses are limited by the presence of sensitive DNA-based constructs. Here, we describe the design, synthesis, and validation experiments performed for a 3.7 million-member DEL, generated using diverse skeleton architectures with varying exit vectors and derived from DOS, to achieve structural diversity beyond what is possible by varying appendages alone. We also show screening results for three diverse protein targets. We will make this DEL available to the academic scientific community to increase access to novel structural features and accelerate early-phase drug discovery.
导向多样性合成(DOS)是一种强大的策略,可以制备在商业筛选库中代表性不足的分子,从而阐明新的生物学机制。与 DOS 的发展并行的是,DNA 编码文库(DEL)已经成为一种有效的、高效的筛选策略,可以识别蛋白质结合物。尽管该领域最近取得了进展,但大多数 DEL 合成受到存在敏感的基于 DNA 的构建体的限制。在这里,我们描述了一个 370 万成员的 DEL 的设计、合成和验证实验,该 DEL 使用不同的骨架结构和不同的出口载体生成,这些结构和载体来自于 DOS,以实现超出仅通过改变附加物所能实现的结构多样性。我们还展示了针对三个不同蛋白质靶标的筛选结果。我们将把这个 DEL 提供给学术界,以增加对新型结构特征的获取,并加速早期药物发现。
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