Institut für Organische Chemie, Albert-Ludwigs-Universität Freiburg , Albertstraße 21, 79104 Freiburg i. Brsg., Germany.
Acc Chem Res. 2016 Aug 16;49(8):1524-36. doi: 10.1021/acs.accounts.6b00252. Epub 2016 Jul 25.
We present a new and efficient strategy for the atom-economic transformation of both alkynes and allenes to allylic functionalized structures via a Rh-catalyzed isomerization/addition reaction which has been developed in our working group. Our methodology thus grants access to an important structural class valued in modern organic chemistry for both its versatility for further functionalization and the potential for asymmetric synthesis with the construction of a new stereogenic center. This new methodology, inspired by mechanistic investigations by Werner in the late 1980s and based on preliminary work by Yamamoto and Trost, offers an attractive alternative to other established methods for allylic functionalization such as allylic substitution or allylic oxidation. The main advantage of our methodology consists of the inherent atom economy in comparison to allylic oxidation or substitution, which both produce stoichiometric amounts of waste and, in case of the substitution reaction, require prefunctionalization of the starting material. Starting out with the discovery of a highly branched-selective coupling reaction of carboxylic acids with terminal alkynes using a Rh(I)/DPEphos complex as the catalyst system, over the past 5 years we were able to continuously expand upon this chemistry, introducing various (pro)nucleophiles for the selective C-O, C-S, C-N, and C-C functionalization of both alkynes and the double-bond isomeric allenes by choosing the appropriate rhodium/bidentate phosphine catalyst. Thus, valuable compounds such as branched allylic ethers, sulfones, amines, or γ,δ-unsaturated ketones were successfully synthesized in high yields and with a broad substrate scope. Beyond the branched selectivity inherent to rhodium, many of the presented methodologies display additional degrees of selectivity in regard to regio-, diastereo-, and enantioselective transformations, with one example even proceeding via a dynamic kinetic resolution. Many advances presented in this account were driven by detailed mechanistic investigations including DFT-calculations, ESI-MS and in situ IR experiments and enabled the application of our chemistry for target-oriented syntheses demonstrated by several examples shown herein. In general, this research topic has matured over the past years into a viable option when synthesizing chiral compounds, from small molecules such as quercus lactones to complex target structures such as Homolargazole or Clavosolide A. This demonstrates the importance and utility of these coupling reactions, especially considering the ease with which carbon-heteroatom bonds can be built stereoselectively, with many of the product classes displaying motifs common in modern APIs.
我们提出了一种新的、高效的策略,通过 Rh 催化的异构化/加成反应,将炔烃和丙二烯转化为烯丙基官能化结构,这是我们小组开发的。我们的方法因此可以获得一类在现代有机化学中很有价值的重要结构,因为它具有进一步官能化的多功能性和不对称合成的潜力,可以构建新的手性中心。这种新方法的灵感来自于 Werner 在 20 世纪 80 年代末的机制研究,并基于 Yamamoto 和 Trost 的初步工作,为烯丙基官能化提供了一种有吸引力的替代方法,例如烯丙基取代或烯丙基氧化。与烯丙基氧化或取代相比,我们方法的主要优势在于其固有的原子经济性,后者会产生化学计量的废物,而且在取代反应中,需要对起始原料进行预官能化。从使用 Rh(I)/DPEphos 配合物作为催化剂体系发现羧酸与末端炔烃的高度支化选择性偶联反应开始,在过去的 5 年中,我们能够不断扩展这种化学,通过选择合适的铑/双齿膦配体催化剂,引入各种(亲核)试剂,对炔烃和双键异构丙二烯进行 C-O、C-S、C-N 和 C-C 选择性官能化。因此,成功地以高收率和广泛的底物范围合成了有价值的化合物,如支链烯丙基醚、砜、胺或γ,δ-不饱和酮。除了铑固有的支化选择性外,许多呈现的方法在区域、非对映选择性和对映选择性转化方面具有额外的选择性程度,其中一个例子甚至通过动态动力学拆分进行。本报告中介绍的许多进展是由详细的机制研究驱动的,包括 DFT 计算、ESI-MS 和原位 IR 实验,并使我们的化学能够应用于通过几个实例展示的目标导向合成。总的来说,在过去的几年中,该研究课题已经发展成为合成手性化合物的可行选择,从小分子如栎酮到复杂的靶标结构如 Homolargazole 或 Clavosolide A 都是如此。这证明了这些偶联反应的重要性和实用性,尤其是考虑到手性碳原子与杂原子键的构建具有高度的立体选择性,许多产物类别的结构都具有现代 API 中常见的结构基序。
