Catalysis by the Non-Heme Iron(II) Histone Demethylase PHF8 Involves Iron Center Rearrangement and Conformational Modulation of Substrate Orientation

Shobhit S Chaturvedi; Rajeev Ramanan; Nicolai Lehnert; Christopher J Schofield; Tatyana G Karabencheva-Christova; Christo Z Christov

doi:10.1021/acscatal.9b04907

Catalysis by the Non-Heme Iron(II) Histone Demethylase PHF8 Involves Iron Center Rearrangement and Conformational Modulation of Substrate Orientation

ACS Catal. 2020 Jan 17;10(2):1195-1209. doi: 10.1021/acscatal.9b04907. Epub 2019 Dec 11.

Authors

Shobhit S Chaturvedi¹, Rajeev Ramanan¹, Nicolai Lehnert², Christopher J Schofield³, Tatyana G Karabencheva-Christova¹, Christo Z Christov¹

Affiliations

¹ Department of Chemistry, Michigan Technological University, Houghton, Michigan 49931, United States.
² Department of Chemistry and Department of Biophysics, University of Michigan, Ann Arbor, Michigan 48109, United States.
³ The Chemistry Research Laboratory, University of Oxford, Mansfield Road, Oxford OX1 5JJ, U.K.

Abstract

PHF8 (KDM7B) is a human non-heme 2-oxoglutarate (2OG) JmjC domain oxygenase that catalyzes the demethylation of the di/mono-N^ε-methylated K9 residue of histone H3. Altered PHF8 activity is linked to genetic diseases and cancer; thus, it is an interesting target for epigenetic modulation. We describe the use of combined quantum mechanics/molecular mechanics (QM/MM) and molecular dynamics (MD) simulations to explore the mechanism of PHF8, including dioxygen activation, 2OG binding modes, and substrate demethylation steps. A PHF8 crystal structure manifests the 2OG C-1 carboxylate bound to iron in a nonproductive orientation, i.e., trans to His247. A ferryl-oxo intermediate formed by activating dioxygen bound to the vacant site in this complex would be nonproductive, i.e., "off-line" with respect to reaction with N^ε-methylated K9. We show rearrangement of the "off-line" ferryl-oxo intermediate to a productive "in-line" geometry via a solvent exchange reaction (called "ferryl-flip") is energetically unfavorable. The calculations imply that movement of the 2OG C-1 carboxylate prior to dioxygen binding at a five-coordination stage in catalysis proceeds with a low barrier, suggesting that two possible 2OG C-1 carboxylate geometries can coexist at room temperature. We explored alternative mechanisms for hydrogen atom transfer and show that second sphere interactions orient the N^ε-methylated lysine in a conformation where hydrogen abstraction from a methyl C-H bond is energetically more favorable than hydrogen abstraction from the N-H bond of the protonated N^ε-methyl group. Using multiple HAT reaction path calculations, we demonstrate the crucial role of conformational flexibility in effective hydrogen transfer. Subsequent hydroxylation occurs through a rebound mechanism, which is energetically preferred compared to desaturation, due to second sphere interactions. The overall mechanistic insights reveal the crucial role of iron-center rearrangement, second sphere interactions, and conformational flexibility in PHF8 catalysis and provide knowledge useful for the design of mechanism-based PHF8 inhibitors.

Grants and funding

18245/CRUK_/Cancer Research UK/United Kingdom