Department of Chemistry, University of Wisconsin , Madison, Wisconsin 53706, United States.
Acc Chem Res. 2017 Sep 19;50(9):2147-2158. doi: 10.1021/acs.accounts.7b00178. Epub 2017 Aug 8.
Carbon-nitrogen (C-N) bonds are ubiquitous in pharmaceuticals, agrochemicals, diverse bioactive natural products, and ligands for transition metal catalysts. An effective strategy for introducing a new C-N bond into a molecule is through transition metal-catalyzed nitrene transfer chemistry. In these reactions, a metal-supported nitrene can either add across a C═C bond to form an aziridine or insert into a C-H bond to furnish the corresponding amine. Typical catalysts for nitrene transfer include RhL and RuL complexes supported by bridging carboxylate and related ligands, as well as complexes based on Cu, Co, Ir, Fe, and Mn supported by porphyrins and related ligands. A limitation of metal-catalyzed nitrene transfer is the ability to predictably select which specific site will undergo amination in the presence of multiple reactive groups; thus, many reactions rely primarily on substrate control. Achieving true catalyst-control over nitrene transfer would open up exciting possibilities for flexible installation of new C-N bonds into hydrocarbons, natural product-inspired scaffolds, existing pharmaceuticals or biorenewable building blocks. Silver-catalyzed nitrene transfer enables flexible control over the position at which a new C-N bond is introduced. Ag(I) supported by simple N-donor ligands accommodates a diverse range of coordination geometries, from linear to tetrahedral to seesaw, enabling the electronic and steric parameters of the catalyst to be tuned independently. In addition, the ligand, Ag salt counteranion, Ag/ligand ratio and the solvent all influence the fluxional and dynamic behavior of Ag(I) complexes in solution. Understanding the interplay of these parameters to manipulate the behavior of Ag-nitrenes in a predictable manner is a key design feature of our work. In this Account, we describe successful applications of a variety of design principles to tunable, Ag-catalyzed aminations, including (1) changing Ag/ligand ratios to influence chemoselectivity, (2) manipulating the steric environment of the catalyst to achieve site-selective C-H bond amination, (3) promoting noncovalent interactions between Ag/substrate or substrate/ligand to direct C-H functionalization, and (4) dictating the substrate's trajectory of approach to the Ag-nitrene. Our catalysts distinguish between the aminations of various types of C-H bonds, including tertiary C(sp)-H, benzylic, allylic, and propargylic C-H bonds. Efforts in asymmetric nitrene transfer reactions catalyzed by Ag(I) complexes are also described.
碳-氮(C-N)键在药物、农用化学品、各种生物活性天然产物以及过渡金属催化剂配体中普遍存在。将新的 C-N 键引入分子中的有效策略是通过过渡金属催化的氮烯转移化学。在这些反应中,金属支持的氮烯可以加成到 C═C 键上形成氮丙啶,或者插入 C-H 键中得到相应的胺。氮烯转移的典型催化剂包括 RhL 和 RuL 配合物,它们由桥连的羧酸盐和相关配体支持,以及基于 Cu、Co、Ir、Fe 和 Mn 的配合物,它们由卟啉和相关配体支持。金属催化的氮烯转移的一个限制是能够可预测地选择在存在多个反应性基团的情况下哪个特定位置将进行胺化;因此,许多反应主要依赖于底物控制。实现对氮烯转移的真正催化剂控制将为灵活地在碳氢化合物、受天然产物启发的支架、现有药物或生物可再生构建块中引入新的 C-N 键开辟令人兴奋的可能性。银催化的氮烯转移能够灵活控制引入新 C-N 键的位置。由简单的 N-供体配体支持的 Ag(I) 可以容纳从线性到四面体形到跷跷板式的各种配位几何形状,从而可以独立调节催化剂的电子和空间参数。此外,配体、Ag 盐抗衡阴离子、Ag/配体比和溶剂都影响 Ag(I) 配合物在溶液中的动态和动态行为。理解这些参数的相互作用以可预测的方式控制 Ag-氮烯的行为是我们工作的关键设计特征。在本报告中,我们描述了各种设计原则在可调谐的 Ag 催化胺化中的成功应用,包括(1)改变 Ag/配体比以影响化学选择性,(2)操纵催化剂的空间环境以实现选择性 C-H 键胺化,(3)促进 Ag/底物或底物/配体之间的非共价相互作用以引导 C-H 官能化,以及(4)决定底物接近 Ag-氮烯的轨迹。我们的催化剂可以区分各种类型的 C-H 键的胺化,包括叔 C(sp)-H、苄基、烯丙基和炔丙基 C-H 键。还描述了 Ag(I) 配合物催化的不对称氮烯转移反应的努力。
