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DFT Investigation of the η6⇌ η6-Inter-ring Haptotropic Rearrangement of the Group 8 Metals Complexes [(graphene)MCp]+(M = Fe, Ru, Os)

Authors :
Gloriozov, Igor P.
Dem’yanov, Piotr I.
Zhulyaev, Nikolay S.
Nechaev, Mikhail S.
Oprunenko, Yuri F.
Gam, Franck
Saillard, Jean-Yves
Kuznetsov, Aleksey E.
Source :
The Journal of Physical Chemistry - Part A; January 2021, Vol. 125 Issue: 1 p366-375, 10p
Publication Year :
2021

Abstract

Metalcyclopentadienyl complexes (MCp)+(M = Fe, Ru, Os) bound to the large polyaromatic hydrogenated hydrocarbon (PAH) C96H24used as a model for pristine graphene have been studied using a density functional theory (DFT) generalized gradient approximation (PBE functional) to reveal their structural features and dynamic behavior. The inter-ring haptotropic rearrangements (IRHRs) for these complexes were shown to occur via two transition states and one intermediate. The energy barriers of the η6⇌ η6IRHRs of the (MCp)+unit were found to be 30, 27, and 29 kcal/mol for M = Fe, Ru, and Os, respectively. These values are significantly lower than the values found previously for smaller PAHs. Both polar and nonpolar solvents were found not to affect significantly the energy barrier heights. Investigated transition metal complexes could be used in general as catalysts in the design of novel derivatives or materials with promising properties. Metalcyclopentadienyl complexes (MCp)+of PAHs show catalytic properties mainly due to their structural details as well as their important characteristic of inter-ring haptotropic rearrangement. IRHRs take place usually by intramolecular mechanisms. During IRHRs, the MLnorganometallic groups (OMGs) undergo shifting along the PAH plane and could coordinate additional reagents, which is important for catalysis. Large PAHs such as graphene, fullerenes, and nanotubes possess intrinsic anticancer activity, and numerous arene complexes of Ru and Os have been proven to have anticancer properties as well. We suppose that coordinating Ru or Os to very large PAHs could synergistically increase the anticancer activity of resulting complexes.

Details

Language :
English
ISSN :
10895639 and 15205215
Volume :
125
Issue :
1
Database :
Supplemental Index
Journal :
The Journal of Physical Chemistry - Part A
Publication Type :
Periodical
Accession number :
ejs54935576
Full Text :
https://doi.org/10.1021/acs.jpca.0c08251