Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes

We have studied activation of the methyl C–H bonds in the cyclopentadienyl ligands of half-sandwich Rh(iii) complexes [η(5)-Cp(X)Rh(N,N′)Cl](+) by observing the dependence of sequential H/D exchange on variations in Cp(X) = Cp* (complexes 1 and 2), Me(4)PhCp (Cp(XPh), 3) or Me(4)PhPhCp (Cp(XPhPh), 4...

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Autores principales: Sink, Alexandra, Banerjee, Samya, Wolny, Juliusz A., Imberti, Cinzia, Lant, Edward C., Walker, Marc, Schünemann, Volker, Sadler, Peter J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2022
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9623609/
https://www.ncbi.nlm.nih.gov/pubmed/36043856
http://dx.doi.org/10.1039/d2dt02079c
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author Sink, Alexandra
Banerjee, Samya
Wolny, Juliusz A.
Imberti, Cinzia
Lant, Edward C.
Walker, Marc
Schünemann, Volker
Sadler, Peter J.
author_facet Sink, Alexandra
Banerjee, Samya
Wolny, Juliusz A.
Imberti, Cinzia
Lant, Edward C.
Walker, Marc
Schünemann, Volker
Sadler, Peter J.
author_sort Sink, Alexandra
collection PubMed
description We have studied activation of the methyl C–H bonds in the cyclopentadienyl ligands of half-sandwich Rh(iii) complexes [η(5)-Cp(X)Rh(N,N′)Cl](+) by observing the dependence of sequential H/D exchange on variations in Cp(X) = Cp* (complexes 1 and 2), Me(4)PhCp (Cp(XPh), 3) or Me(4)PhPhCp (Cp(XPhPh), 4), and chelated ligand N,N′ (bpy, 1; phen, 2–4). H/D exchange was fastest in d(4)-MeOD (t(1/2) = 10 min, 37 °C, complex 1), no H/D exchange was observed in DMSO/D(2)O, and d(4)-MeOD enhanced the rate in CD(3)CN. The proposed Rh(i)–fulvene intermediate was trapped by [4 + 2] Diels–Alder reactions with conjugated dienes and characterized. The Rh(i) oxidation state was confirmed by X-ray photoelectron spectroscopy (XPS). Influence of solvent on the mechanisms of activation and Diels–Alder adduct formation was modelled using DFT calculations with the CAM-B3LYP functional and CEP-31 g basis set, and influence on the reaction profile of the dimiine ligand and phenyl substituent using the larger qzvp basis set. The Rh(iii)–OH intemediate is stabilised by H-bonding with methanol and a Cp* CH(3) hydrogen. The Rh(i)(Me(4)fulvene) species, stabilised by interaction of methanol with a coordinated water, again by two H-bonds H(2)O–HOMe (1.49 Å) and fulvene CH(2) (1.94 Å), arises from synchronous transfer of the methanol OH proton to a Rh(iii)–OH ligand and Cp* methyl hydrogen to the methanol oxygen. Additionally, the observed trend in catalytic activity for complexes 1–4 was reproduced by DFT calculations. These complexes form a novel class of catalytic molecular motors with a tunable rate of operation that can be stalled in a given state. They provide a basis for elucidation of the effects of ligand design on the contributions of electronic, rotational and vibrational energies to each step in the reaction pathway at the atomic level, consideration of which will enhance the design principles for the next generation of molecular machines.
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spelling pubmed-96236092022-11-07 Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes Sink, Alexandra Banerjee, Samya Wolny, Juliusz A. Imberti, Cinzia Lant, Edward C. Walker, Marc Schünemann, Volker Sadler, Peter J. Dalton Trans Chemistry We have studied activation of the methyl C–H bonds in the cyclopentadienyl ligands of half-sandwich Rh(iii) complexes [η(5)-Cp(X)Rh(N,N′)Cl](+) by observing the dependence of sequential H/D exchange on variations in Cp(X) = Cp* (complexes 1 and 2), Me(4)PhCp (Cp(XPh), 3) or Me(4)PhPhCp (Cp(XPhPh), 4), and chelated ligand N,N′ (bpy, 1; phen, 2–4). H/D exchange was fastest in d(4)-MeOD (t(1/2) = 10 min, 37 °C, complex 1), no H/D exchange was observed in DMSO/D(2)O, and d(4)-MeOD enhanced the rate in CD(3)CN. The proposed Rh(i)–fulvene intermediate was trapped by [4 + 2] Diels–Alder reactions with conjugated dienes and characterized. The Rh(i) oxidation state was confirmed by X-ray photoelectron spectroscopy (XPS). Influence of solvent on the mechanisms of activation and Diels–Alder adduct formation was modelled using DFT calculations with the CAM-B3LYP functional and CEP-31 g basis set, and influence on the reaction profile of the dimiine ligand and phenyl substituent using the larger qzvp basis set. The Rh(iii)–OH intemediate is stabilised by H-bonding with methanol and a Cp* CH(3) hydrogen. The Rh(i)(Me(4)fulvene) species, stabilised by interaction of methanol with a coordinated water, again by two H-bonds H(2)O–HOMe (1.49 Å) and fulvene CH(2) (1.94 Å), arises from synchronous transfer of the methanol OH proton to a Rh(iii)–OH ligand and Cp* methyl hydrogen to the methanol oxygen. Additionally, the observed trend in catalytic activity for complexes 1–4 was reproduced by DFT calculations. These complexes form a novel class of catalytic molecular motors with a tunable rate of operation that can be stalled in a given state. They provide a basis for elucidation of the effects of ligand design on the contributions of electronic, rotational and vibrational energies to each step in the reaction pathway at the atomic level, consideration of which will enhance the design principles for the next generation of molecular machines. The Royal Society of Chemistry 2022-08-31 /pmc/articles/PMC9623609/ /pubmed/36043856 http://dx.doi.org/10.1039/d2dt02079c Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by/3.0/
spellingShingle Chemistry
Sink, Alexandra
Banerjee, Samya
Wolny, Juliusz A.
Imberti, Cinzia
Lant, Edward C.
Walker, Marc
Schünemann, Volker
Sadler, Peter J.
Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes
title Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes
title_full Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes
title_fullStr Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes
title_full_unstemmed Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes
title_short Kinetics and mechanism of sequential ring methyl C–H activation in cyclopentadienyl rhodium(iii) complexes
title_sort kinetics and mechanism of sequential ring methyl c–h activation in cyclopentadienyl rhodium(iii) complexes
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9623609/
https://www.ncbi.nlm.nih.gov/pubmed/36043856
http://dx.doi.org/10.1039/d2dt02079c
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