Department of Chemistry and Applied Biosciences, ETH Zurich, 8093 Zurich, Switzerland.
Department of Biology, ETH Zurich, 8093 Zurich, Switzerland.
Science. 2024 Jun 14;384(6701):1259-1265. doi: 10.1126/science.adn3412. Epub 2024 Jun 13.
The first drugs discovered using DNA-encoded chemical library (DEL) screens have entered late-stage clinical development. However, DEL technology as a whole still suffers from poor chemical purity resulting in suboptimal performance. In this work, we report a technique to overcome this issue through self-purifying release of the DEL after magnetic bead-based synthesis. Both the first and last building blocks of each assembled library member were linked to the beads by tethers that could be cleaved by mutually orthogonal chemistry. Sequential cleavage of the first and last tether, with washing in between, ensured that the final library comprises only the fully complete compounds. The outstanding purity attained by this approach enables a direct correlation of chemical display and encoding, allows for an increased chemical reaction scope, and facilitates the use of more diversity elements while achieving greatly improved signal-to-noise ratios in selections.
利用 DNA 编码化学库 (DEL) 筛选发现的首批药物已进入后期临床开发阶段。然而,整体而言,DEL 技术仍然存在较差的化学纯度问题,导致性能不佳。在这项工作中,我们报告了一种通过基于磁珠合成后 DEL 自动纯化释放来克服这一问题的技术。每个组装文库成员的第一个和最后一个构建块都通过可以通过正交化学切割的连接物连接到珠上。通过依次切割第一个和最后一个连接物,并在中间进行洗涤,确保最终文库仅包含完全完整的化合物。该方法达到的出色纯度可实现化学显示和编码的直接相关,允许增加化学反应范围,并促进使用更多的多样性元素,同时在筛选中实现大大提高的信噪比。
