Thermal decomposition of syn- and anti-dihydropyrenes; functional group-dependent decomposition pathway

Bibi Saima; Yan Alexander Wang; Riaz Hussain; Shabbir Muhammad; Khurshid Ayub

doi:10.1007/s00894-019-4052-1

Thermal decomposition of syn- and anti-dihydropyrenes; functional group-dependent decomposition pathway

J Mol Model. 2019 Jul 10;25(8):215. doi: 10.1007/s00894-019-4052-1.

Authors

Bibi Saima¹, Yan Alexander Wang², Riaz Hussain³, Shabbir Muhammad^{4

5}, Khurshid Ayub⁶

Affiliations

¹ Department of Chemistry, COMSATS University, Abbottabad Campus, Abbottabad, 22060, Pakistan.
² Department of Chemistry, University of British Columbia, Vancouver, V6T 1Z1, Canada.
³ Department of Chemistry, University of Okara, Okara, Punjab, Pakistan.
⁴ Department of Physics, College of Science, King Khalid University, Abha, Saudi Arabia.
⁵ Research Center for Advanced Materials Science (RCAMS), King Khalid University, Abha, Saudi Arabia.
⁶ Department of Chemistry, COMSATS University, Abbottabad Campus, Abbottabad, 22060, Pakistan. [email protected].

PMID: 31292739
DOI: 10.1007/s00894-019-4052-1

Abstract

Syn and anti dihydropyrene (DHP) are excellent thermochromes, and therefore extensively studied for their thermochromic and photochromic properties, respectively. However, they suffer from thermal decomposition due to thermal instability. In this study, we thoroughly investigated pathways for the thermal decomposition of anti- and syn- dihydropyrenes through computational methods. The decomposition pathways include sigmatropic shift and hemolytic and heterolytic (cationic and anionic) cleavages. The decomposition pathway is influenced not only by the dihydropyrene (syn- or anti-) but also by the functional groups present. For anti-dihydropyrenes, sigmatropic shift is the most plausible pathways for CN and CHO internal groups. The cascade of sigmatropic shifts is followed by elimination to deliver substituted pyrenes. For CH₃- and H- dihydropyrenes, hemolytic cleavage of the internal groups is the most plausible pathway for decomposition to pyrenes. The pathway is changed to heterolytic cleavage when the internal groups on the dihydropyrenes are Cl^-, Br^-, and SMe^-. Comparison of the activation barriers for syn (30.18 kcal mol^-1) and anti (32.10 kcal mol^-1) dimethyldihydropyrenes for radical pathway reveal that decomposition of syn- DHP is more facile over anti-, which is consistent with the experimental observation. The decomposition pathway for syn-dihydropyrene is also hemolytic in cleavage when the internal groups are methyl and hydrogen. Syn-dihydropyrenes (symmetrical or unsymmetrical) bearing CN group do not follow sigmatropic shift, quite contrary to the anti-dihydropyrene. The lack of tendency of the syn-dihydropyrene for sigmatropic shift is rationalized on the planarity of the scaffold. The results of the theoretical study are consistent with the experimental observations. The results here help in understanding the behavior of substituents on the dihydropyrene scaffold, which will be useful in designing new molecules with improved thermal stabilities. Graphical abstract Functional group dependent decomposition pathways of dihydropyrenes.

Keywords: Cyclophanediene; Decomposition pathways; Density functional theory; Dihydropyrene; Sigmatropic shift.

Grants and funding

1899, 2469, 2981/Higher Education Commission, Pakistan