Brain Metabolite, Myo-inositol, Inhibits Catalase Activity: A Mechanism of the Distortion of the Antioxidant Defense System in Alzheimer's disease

Fasil Ali; Usma Manzoor; Reshmee Bhattacharya; Aniket Kumar Bansal; Kempohalli Sayanna Chandrashekharaiah; Laishram Rajendrakumar Singh; Suma Mohan Saraswati; Vladimir Uversky; Tanveer Ali Dar

doi:10.1021/acsomega.1c06990

Brain Metabolite, Myo-inositol, Inhibits Catalase Activity: A Mechanism of the Distortion of the Antioxidant Defense System in Alzheimer's disease

ACS Omega. 2022 Apr 7;7(15):12690-12700. doi: 10.1021/acsomega.1c06990. eCollection 2022 Apr 19.

Authors

Fasil Ali¹, Usma Manzoor², Reshmee Bhattacharya³, Aniket Kumar Bansal³, Kempohalli Sayanna Chandrashekharaiah¹, Laishram Rajendrakumar Singh³, Suma Mohan Saraswati⁴, Vladimir Uversky^{5

6}, Tanveer Ali Dar²

Affiliations

¹ Department of Studies and Research in Biochemistry, Jnana Kaveri Campus, Mangalore University, Karnataka 574199, India.
² Department of Clinical Biochemistry, University of Kashmir, Srinagar 190006, India.
³ Dr. B. R. Ambedkar Center for Biomedical Research, University of Delhi, New Delhi 110007, India.
⁴ School of Chemical & Biotechnology,SASTRA Deemed to be University, Tirumalaisamudram, Thanjavur 613401, Tamilnadu, India.
⁵ Department of Molecular Medicine and USF Health Byrd Alzheimer's Research Institute, Morsani College of Medicine, University of South Florida, Tampa, Florida 33612, United States.
⁶ Institute for Biological Instrumentation of the Russian Academy of Sciences, Federal Research Center "Pushchino Scientific Center for Biological Research of the Russian Academy of Sciences", Pushchino 142290, Russia.

Abstract

A strong correlation between brain metabolite accumulation and oxidative stress has been observed in Alzheimer's disease (AD) patients. There are two central hypotheses for this correlation: (i) coaccumulation of toxic amyloid-β and Myo-inositol (MI), a significant brain metabolite, during presymptomatic stages of AD, and (ii) enhanced expression of MI transporter in brain cells during oxidative stress-induced volume changes in the brain. Identifying specific interactive effects of MI with cellular antioxidant enzymes would represent an essential step in understanding the oxidative stress-induced AD pathogenicity. This study demonstrated that MI inhibits catalase, an essential antioxidant enzyme primarily inefficient in AD, by decreasing its k _cat (turnover number) and increasing K _m (Michaelis-Menten constant) values. This inhibition of catalase by MI under in vivo studies increased cellular H₂O₂ levels, leading to decreased cell viability. Furthermore, MI induces distortion of the active heme center with an overall loss of structure and stability of catalase. MI also alters distances of the vital active site and substrate channel residues of catalase. The present study provides evidence for the involvement of MI in the inactivation of the antioxidant defense system during oxidative stress-induced pathogenesis of AD. Regulation of MI levels, during early presymptomatic stages of AD, might serve as a potential early-on therapeutic strategy for this disease.