Metabolic fate of human immunoactive sterols in Mycobacterium tuberculosis

Author:

Varaksa Tatsiana,Bukhdruker Sergey,Grabovec Irina,Marin EgorORCID,Kavaleuski Anton,Gusach AnastasiiaORCID,Kovalev KirillORCID,Maslov IvanORCID,Luginina AleksandraORCID,Zabelskiy Dmitry,Astashkin Roman,Shevtsov Mikhail,Smolskaya Sviatlana,Kavaleuskaya Anna,Shabunya Polina,Baranovsky Alexander,Dolgopalets Vladimir,Charnou Yury,Savachka Aleh,Litvinovskaya Raisa,Hurski Alakseij,Shevchenko Evgeny,Rogachev Andrey,Mishin AlexeyORCID,Gordeliy ValentinORCID,Gabrielian Andrei,Hurt Darrell E.,Nikonenko Boris,Majorov Konstantin,Apt Alexander,Rosenthal Alex,Gilep AndreiORCID,Borshchevskiy ValentinORCID,Strushkevich NatalliaORCID

Abstract

AbstractMycobacterium tuberculosis (Mtb) infection is among top ten causes of death worldwide, and the number of drug-resistant strains is increasing. The direct interception of human immune signaling molecules by Mtb remains elusive, limiting drug discovery. Oxysterols and secosteroids regulate both innate and adaptive immune responses. Here we report a functional, structural, and bioinformatics study of Mtb enzymes initiating cholesterol catabolism and demonstrated their interrelation with human immunity. We show that these enzymes metabolize human immune oxysterol messengers. Rv2266 – the most potent among them – can also metabolize vitamin D3 (VD3) derivatives. High-resolution structures show common patterns of sterols binding and reveal a site for oxidative attack during catalysis. Finally, we designed a compound that binds and inhibits three studied proteins. The compound shows activity against Mtb H37Rv residing in macrophages. Our findings contribute to molecular understanding of suppression of immunity and suggest that Mtb has its own transformation system resembling the human phase I drug-metabolizing system.

Publisher

Cold Spring Harbor Laboratory

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