TY - JOUR
T1 - Synergistic lethality of a binary inhibitor of mycobacterium tuberculosis kasA
AU - Kumar, Pradeep
AU - Capodagli, Glenn C.
AU - Awasthi, Divya
AU - Shrestha, Riju
AU - Maharaja, Karishma
AU - Sukheja, Paridhi
AU - Li, Shao Gang
AU - Inoyama, Daigo
AU - Zimmerman, Matthew
AU - Liang, Hsin Pin Ho
AU - Sarathy, Jansy
AU - Mina, Marizel
AU - Rasic, George
AU - Russo, Riccardo
AU - Perryman, Alexander L.
AU - Richmann, Todd
AU - Gupta, Aditi
AU - Singleton, Eric
AU - Verma, Sheetal
AU - Husain, Seema
AU - Soteropoulos, Patricia
AU - Wang, Zhe
AU - Morris, Roxanne
AU - Porter, Gene
AU - Agnihotri, Gautam
AU - Salgame, Padmini
AU - Ekins, Sean
AU - Rhee, Kyu Y.
AU - Connell, Nancy
AU - Dartois, Veronique
AU - Neiditch, Matthew B.
AU - Freundlich, Joel S.
AU - Alland, David
N1 - Publisher Copyright:
© 2018 Kumar et al.
PY - 2018/11/1
Y1 - 2018/11/1
N2 - We report GSK3011724A (DG167) as a binary inhibitor of β-ketoacyl-ACP synthase (KasA) in Mycobacterium tuberculosis. Genetic and biochemical studies established KasA as the primary target. The X-ray crystal structure of the KasA-DG167 complex refined to 2.0-Å resolution revealed two interacting DG167 molecules occupying nonidentical sites in the substrate-binding channel of KasA. The binding affinities of KasA to DG167 and its analog, 5g, which binds only once in the substrate-binding channel, were determined, along with the KasA-5g X-ray crystal structure. DG167 strongly augmented the in vitro activity of isoniazid (INH), leading to synergistic lethality, and also synergized in an acute mouse model of M. tuberculosis infection. Synergistic lethality correlated with a unique transcriptional signature, including upregulation of oxidoreductases and downregulation of molecular chaperones. The lead structure-activity relationships (SAR), pharmacokinetic profile, and detailed interactions with the KasA protein that we describe may be applied to evolve a next-generation therapeutic strategy for tuberculosis (TB). IMPORTANCE Cell wall biosynthesis inhibitors have proven highly effective for treating tuberculosis (TB). We discovered and validated members of the indazole sulfon-amide class of small molecules as inhibitors of Mycobacterium tuberculosis KasA—a key component for biosynthesis of the mycolic acid layer of the bacterium’s cell wall and the same pathway as that inhibited by the first-line antitubercular drug isoniazid (INH). One lead compound, DG167, demonstrated synergistic lethality in combination with INH and a transcriptional pattern consistent with bactericidality and loss of persisters. Our results also detail a novel dual-binding mechanism for this compound as well as substantial structure-activity relationships (SAR) that may help in lead optimization activities. Together, these results suggest that KasA inhibition, spe-cifically, that shown by the DG167 series, may be developed into a potent therapy that can synergize with existing antituberculars.
AB - We report GSK3011724A (DG167) as a binary inhibitor of β-ketoacyl-ACP synthase (KasA) in Mycobacterium tuberculosis. Genetic and biochemical studies established KasA as the primary target. The X-ray crystal structure of the KasA-DG167 complex refined to 2.0-Å resolution revealed two interacting DG167 molecules occupying nonidentical sites in the substrate-binding channel of KasA. The binding affinities of KasA to DG167 and its analog, 5g, which binds only once in the substrate-binding channel, were determined, along with the KasA-5g X-ray crystal structure. DG167 strongly augmented the in vitro activity of isoniazid (INH), leading to synergistic lethality, and also synergized in an acute mouse model of M. tuberculosis infection. Synergistic lethality correlated with a unique transcriptional signature, including upregulation of oxidoreductases and downregulation of molecular chaperones. The lead structure-activity relationships (SAR), pharmacokinetic profile, and detailed interactions with the KasA protein that we describe may be applied to evolve a next-generation therapeutic strategy for tuberculosis (TB). IMPORTANCE Cell wall biosynthesis inhibitors have proven highly effective for treating tuberculosis (TB). We discovered and validated members of the indazole sulfon-amide class of small molecules as inhibitors of Mycobacterium tuberculosis KasA—a key component for biosynthesis of the mycolic acid layer of the bacterium’s cell wall and the same pathway as that inhibited by the first-line antitubercular drug isoniazid (INH). One lead compound, DG167, demonstrated synergistic lethality in combination with INH and a transcriptional pattern consistent with bactericidality and loss of persisters. Our results also detail a novel dual-binding mechanism for this compound as well as substantial structure-activity relationships (SAR) that may help in lead optimization activities. Together, these results suggest that KasA inhibition, spe-cifically, that shown by the DG167 series, may be developed into a potent therapy that can synergize with existing antituberculars.
KW - Antitubercular
KW - DG167
KW - Drug development
KW - Isoniazid
KW - KasA
KW - Mycobacterium tuberculosis
KW - Mycolic acid biosynthesis
KW - Synergistic lethality
UR - http://www.scopus.com/inward/record.url?scp=85058876242&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85058876242&partnerID=8YFLogxK
U2 - 10.1128/mBio.02101-17
DO - 10.1128/mBio.02101-17
M3 - Article
C2 - 30563908
AN - SCOPUS:85058876242
SN - 2161-2129
VL - 9
JO - mBio
JF - mBio
IS - 6
M1 - e02101-17
ER -