A multi-targeting pre-clinical candidate against drug-resistant tuberculosis - 27/07/21

Doi : 10.1016/j.tube.2021.102104

Parvinder Kaur ^a,^⁎ , Vijay Potluri ^a, Vijay Kamal Ahuja ^a, C.N. Naveenkumar ^a, Ramya Vadageri Krishnamurthy ^a, Shruthi Thimmalapura Gangadharaiah ^b, Prasad Shivarudraiah ^b, Sumesh Eswaran ^b, Christy Rosaline Nirmal ^c, Balasubramanian Mahizhaveni ^c, Azger Dusthackeer ^c, Rajesh Mondal ^c, Sarah M. Batt ^d, Emily J. Richardson ^d, Nicholas J. Loman ^d, Gurdyal Singh Besra ^d, Radha Krishan Shandil ^a, Shridhar Narayanan ^a
^a Foundation for Neglected Disease Research, Bangalore, India
^b Anthem BioSciences. Pvt. Ltd., No 49, Canara Bank Road, Hosur Rd, Electronics City Phase 1, Bommasandra Industrial Area, Bengaluru, Karnataka, 560099, India
^c National Institute for Research in Tuberculosis, No.1, Mayor Sathiyamoorthy St, Chetpet, Chennai, Tamil Nadu, 600031, India
^d Insitiute of Microbiology & Infection, School of Biosciences, University of Birmingham, Edgbaston, Birmingham, B15 2TT, UK

^∗Corresponding author. Foundation for Neglected Diseases Research (FNDR), Plot 20A, KIADB Industrial Area, Veerapura, Doddaballapur, Bangalore, 561203, Karnataka, India.Foundation for Neglected Diseases Research (FNDR)Plot 20A, KIADB Industrial Area, Veerapura, DoddaballapurBangaloreKarnataka561203India

Abstract

FNDR-20081 [4-{4-[5-(4-Isopropyl-phenyl)- [1,2,4]oxadiazol-3-ylmethyl]-piperazin-1-yl}-7-pyridin-3-yl-quinoline] is a novel, first in class anti-tubercular pre-clinical candidate against sensitive and drug-resistant Mycobacterium tuberculosis (Mtb). In-vitro combination studies of FNDR-20081 with first- and second-line drugs exhibited no antagonism, suggesting its compatibility for developing new combination-regimens. FNDR-20081, which is non-toxic with no CYP3A4 liability, demonstrated exposure-dependent killing of replicating-Mtb, as well as the non-replicating-Mtb, and efficacy in a mouse model of infection. Whole genome sequencing (WGS) of FNDR-20081 resistant mutants revealed the identification of pleotropic targets: marR (Rv0678), a regulator of MmpL5, a transporter/efflux pump mechanism for drug resistance; and Rv3683, a putative metalloprotease potentially involved in peptidoglycan biosynthesis. In summary, FNDR-20081 is a promising first in class compound with the potential to form a new combination regimen for MDR-TB treatment.

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Keywords : Drug resistance, Mycobacterium tuberculosis, First-in-class, Multi-target, Pre-clinical candidate

Plan

Introduction

Materials and methods

Drug metabolism and pharmacokinetics of FNDR-20081

In-vivo efficacy of FNDR-20081

Results

Target identification of FNDR-20081

Drug metabolism and pharmacokinetics

Pharmacokinetics in infected animals

In-vivo efficacy of FNDR-20081

Discussion

Funding

Declaration of competing interest

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Vol 129

Article 102104- juillet 2021 Retour au numéro

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A multi-targeting pre-clinical candidate against drug-resistant tuberculosis - 27/07/21

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