Post-coordination of Ru(II) Controlled Regioselective B(4)–H Acylmethylation of o-Carboranes with Sulfoxonium Ylides

IF 7.6 1区化学 Q1 CHEMISTRY, MULTIDISCIPLINARY

Chemical Science Pub Date : 2025-04-24 DOI:10.1039/d5sc01576f

Hou-Ji Cao, Jia-Xin Li, Jia-Hui Yan, Miao-Xin Liu, Qianyi Zhao, Jie Zhang, Ju Zhang, Hong Yan

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引用次数: 0

Abstract

Despite significant progress in the B–H functionalization of carboranes, the development of cost-effective catalytic systems devoid of noble metals, coupled with mechanistic validation of regioselectivity control, remains a formidable challenge. Herein, we disclose an Ag salt-free, redox-neutral, and inexpensive ruthenium(II)-catalyzed protocol that enables exclusive B(4)–H acylmethylation of o-carboranes through a novel post-coordination strategy. By exploiting weakly coordinating carboxylic acid as a traceless directing group, this method achieves excellent mono-site selectivity for B–C(sp³) bond formation using diverse sulfoxonium ylides, demonstrating both functional group tolerance and synthetic scalability. This work not only establishes a practical synthetic platform but also addresses critical mechanistic questions unresolved in prior analogous studies. Through deuterium labeling, in situ high-resolution mass spectrometry (HRMS) tracking, and single-crystal X-ray analysis of critical Ru intermediates, we unequivocally demonstrate that the mono-site selectivity originates from a unique post-coordination mode of Ru(II). The Ru catalyst simultaneously engages both the carboxylic acid and the enolizable acylmethyl moiety in the mono-acylated intermediate, thereby dictating the B(4)–H activation trajectory. Our findings establish a generalizable platform for regiocontrolled carborane functionalization while defining mechanistic paradigms in transition metal-mediated B–H activation chemistry.

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邻碳硼烷与亚砜酰化调控区域选择性B(4) -H酰基甲基化后配位

尽管碳硼烷的B-H功能化取得了重大进展，但开发不含贵金属的低成本催化体系，以及对区域选择性控制的机理验证，仍然是一个艰巨的挑战。在此，我们公开了一种无银盐、氧化还原中性、廉价的钌（II）催化方案，该方案通过一种新颖的后配位策略实现邻碳硼烷的B(4) -H酰甲基化。通过利用弱配位羧酸作为无迹导向基团，该方法实现了不同亚砜基化合物对B-C （sp³）键形成的良好单位点选择性，证明了官能团耐受性和合成可扩展性。这项工作不仅建立了一个实用的合成平台，而且还解决了先前类似研究中未解决的关键机制问题。通过氘标记，原位高分辨率质谱（HRMS）跟踪和关键Ru中间体的单晶x射线分析，我们明确地证明了单位点选择性源于Ru（II）独特的后配位模式。Ru催化剂同时作用于单酰基化中间体中的羧酸和可烯化的酰基甲基部分，从而决定了B(4) -H的活化轨迹。我们的发现为区域控制碳硼烷功能化建立了一个可推广的平台，同时定义了过渡金属介导的B-H活化化学的机制范式。

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来源期刊

Chemical Science CHEMISTRY, MULTIDISCIPLINARY-

CiteScore

14.40

自引率

4.80%

发文量

1352

审稿时长

2.1 months

期刊介绍： Chemical Science is a journal that encompasses various disciplines within the chemical sciences. Its scope includes publishing ground-breaking research with significant implications for its respective field, as well as appealing to a wider audience in related areas. To be considered for publication, articles must showcase innovative and original advances in their field of study and be presented in a manner that is understandable to scientists from diverse backgrounds. However, the journal generally does not publish highly specialized research.