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Directed evolution unlocks oxygen reactivity for a nicotine-degrading flavoenzyme

Medicine and Health

Directed evolution unlocks oxygen reactivity for a nicotine-degrading flavoenzyme

M. Dulchavsky, R. Mitra, et al.

Unlock the potential of nicotine oxidoreductase (NicA2) with groundbreaking research by Mark Dulchavsky and team, revealing variants that dramatically enhance its capacity to degrade nicotine in blood. This advancement paves the way for more effective smoking cessation therapies.... show more
Abstract
The flavoenzyme nicotine oxidoreductase (NicA2) is a promising injectable treatment to aid in the cessation of smoking, a behavior responsible for one in ten deaths worldwide. NicA2 acts by degrading nicotine in the bloodstream before it reaches the brain. Clinical use of NicA2 is limited by its poor catalytic activity in the absence of its natural electron acceptor CycN. Without CycN, NicA2 is instead oxidized slowly by dioxygen (O2), necessitating unfeasibly large doses in a therapeutic setting. Here, we report a genetic selection strategy that directly links CycN-independent activity of NicA2 to growth of Pseudomonas putida S16. This selection enabled us to evolve NicA2 variants with substantial improvement in their rate of oxidation by O2. The encoded mutations cluster around a putative O2 tunnel, increasing flexibility and accessibility to O2 in this region. These mutations further confer desirable clinical properties. A variant form of NicA2 is tenfold more effective than the wild type at degrading nicotine in the bloodstream of rats.
Publisher
Nature Chemical Biology
Published On
Sep 28, 2023
Authors
Mark Dulchavsky, Rishav Mitra, Kevin Wu, Joshua Li, Karli Boer, Xiaomeng Liu, Zhiyao Zhang, Cristian Vasquez, Christopher T. Clark, Kaitrin Funckes, Kokila Shankar, Selene Bonnet-Zahedi, Mohammad Siddiq, Yadira Sepulveda, Raymond T. Suhandynata, Jeremiah D. Momper, Antonio N. Calabrese, Oliver George, Frederick Stull, James C. A. Bardwell
Tags
Nicotine oxidoreductase
CycN
smoking cessation
genetic selection
oxidation
O2 tunnel
NicA2 v320
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