Harnessing Rhodium-Catalyzed C–H Activation: Regioselective Cascade Annulation for Fused Polyheterocycles

Singam, Maneesh Kumar Reddy; Babu, Undamatla Suri; Nagireddy, Attunuri; Nanubolu, Jagadeesh Babu; Reddy, Maddi Sridhar

doi:10.1021/acs.joc.1c00477

Cited by 19 publications

(14 citation statements)

References 48 publications

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“…Then, coordination of 4-hydroxy-2-alkynoate with B followed by sequential regioselective insertion, reductive elimination and lactonization provided the final product 205 (Scheme 58). [122] Indazole derivatives are one of the prominent heterocyclic scaffolds widely found in nature possessing potential biological activity. [123a,b] Over the past decade transition metal catalyzed CÀ H activation was found to be a robust and efficient synthetic tool for the construction of CÀ N and CÀ C bond.…”

Section: Rhodium Catalyzed C-h/c-c Activationmentioning

confidence: 99%

“…Regioselective cascade annulation for fused polyheterocycles via rhodium-catalyzed CÀ H activation. [122] ylides emerged as a novel carbene substituent in Rhodium catalyzed CÀ H functionalization serving both as C1 and C2 synthons to access heterocyclic products. [125d-g] Previously, Cheng group developed a novel route for the synthesis of indoloindolones via rhodium-catalyzed [4 + 1] annulation reaction between sulfoxonium ylides and anthranils.…”

Section: Rhodium Catalyzed C-h/c-c Activationmentioning

confidence: 99%

“…Then, coordination of 4‐hydroxy‐2‐alkynoate with B followed by sequential regioselective insertion, reductive elimination and lactonization provided the final product 205 (Scheme 58). [122] …”

Section: Introductionmentioning

confidence: 99%

“… Regioselective cascade annulation for fused polyheterocycles via rhodium‐catalyzed C−H activation [122] …”

Section: Introductionmentioning

confidence: 99%

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Recent Advances in the Synthesis of 5‐MemberedN‐Heterocycles via Rhodium Catalysed Cascade Reactions

et al. 2022

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Five membered N-heterocycles are significant targets in organic synthesis because of their ubiquitous existence in bioactive natural products and pharmaceuticals. Over the past decade a compelling attractiveness has grown to develop rhodium complex catalysed efficient and atom-economic chemistry to access structurally diverse N-heterocyclic frameworks. This present review enlightens notable progresses and advances in synthesis of 5-membered N-heterocycles via rhodium catalysed cascade reactions (annulations, CÀ H/CÀ C activation, cycloaddition, rearrangement, cyclization, metathesis) from 2018-2021.[a] D.

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Section: Rhodium Catalyzed C-h/c-c Activationmentioning

confidence: 99%

Section: Rhodium Catalyzed C-h/c-c Activationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

“… Regioselective cascade annulation for fused polyheterocycles via rhodium‐catalyzed C−H activation [122] …”

Section: Introductionmentioning

confidence: 99%

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Recent Advances in the Synthesis of 5‐MemberedN‐Heterocycles via Rhodium Catalysed Cascade Reactions

et al. 2022

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“…Inert C–H activation has been gradually recognized as a reliable dimension of organic synthesis after the discovery of various catalytic systems to functionalize many C–H bonds that were previously regarded as being passive for the reactions. Among various metals, ,,, rhodium-catalyzed C–H functionalizations ,,,− , display unique reactivity patterns for the orchestration of multifaceted carbo/heterocycles in an operationally simple and synthetically convenient manner. Distinguished by its exceptional functional group tolerance and cryptic reactivity, rhodium catalysis could profusely expand the choice of feedstocks.…”

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confidence: 99%

Rhodium-Catalyzed Coordination-Assisted Regioselective and Migratory Three-Point Double Annulation of o-Alkenyl Phenols with Tertiary Propargyl Alcohols

et al. 2022

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We disclose herein a Rh(III)-catalyzed migratory three-point double annulation of o-alkenyl phenols with propargyl alcohols for de novo construction of naphtho furan derivatives in a regio-and chemoselective manner. The protocol orchestrates two new rings with four new bonds in one operation without the need for any additive. Necessary labeled and control experiments are conducted to elucidate the reaction mechanism. A tertiary hydroxyl group is found to be crucial both for controlling the regioselective insertion of alkyne through chelation with rhodium to form a key spiro cyclic intermediate and for forcing ring expansion via unusual and selective olefin reshuffling, apart from forming an extra (furan) ring. The protocol is scalable and shows tolerance for late stage functionalization of natural products.

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Rhodium‐Catalyzed Dual C−H Activation for Regioselective Triple Annulation of Enaminones: Access to Polycyclic Naphthopyran Derivatives

et al. 2023

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Rh‐catalyzed C−H activation of arenes for oxidative annulations with alkynes stands out as a protocol for polycyclic scaffolds. This perspective drives us to disclose herein a rhodium catalyzed regioselective triple annulation of enaminones with hydroxyl‐alkynoates via double C−H functionalization for polycyclic naphtho‐pyran scaffolds. Secondary coordination of OH in alkynoate dictated the regioselectivity. Initial lactonization occurred chemoselectively on to enamine part via carbo rhodation followed by reductive elimination. This protocol was scalable and has shown high functionality tolerance. KIE studies were done to get insight in to the mechanism, and some downstream transformations were achieved to show the synthetic potential of the method.

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Harnessing Rhodium-Catalyzed C–H Activation: Regioselective Cascade Annulation for Fused Polyheterocycles

Cited by 19 publications

References 48 publications

Recent Advances in the Synthesis of 5‐MemberedN‐Heterocycles via Rhodium Catalysed Cascade Reactions

Recent Advances in the Synthesis of 5‐MemberedN‐Heterocycles via Rhodium Catalysed Cascade Reactions

Rhodium-Catalyzed Coordination-Assisted Regioselective and Migratory Three-Point Double Annulation of o-Alkenyl Phenols with Tertiary Propargyl Alcohols

Rhodium‐Catalyzed Dual C−H Activation for Regioselective Triple Annulation of Enaminones: Access to Polycyclic Naphthopyran Derivatives

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