The large and growing problem of drug resistance of Mtb in humans requires new approaches to determine the mechanism of multi-drug resistance and markers of the resistant state in humans. Using 116 drug resistant Mtb isolates, we used whole genome sequencing to identify Mtb mutations stastically associated to drug resistance during natural infection of humans. This unbiased and broad approach identified all of the known genes that promote drug resistance and identified 11 genes of known function with no known connection to drug resistance. Three of these genes (ppsA, polyketide synthase 12 and polyketide synthase 3) produce polykefides with inter-related functions in outer membrane integrity of Mtb. An independent, mass spectromety analysis of molecules changed in a strain evolving drug resistance in vivo identified mannosyl phosphomycoketide, the product of polyeketide synthase 12, as being inversely correlated with resistance. Based on independent genetic and metabolomic discovery of altered polyketide synthesis function in drug resistant strains, we will test a new model in which altered polykefide function controls cell wall integrity and drug resistance. Using patient derived strains from Lima, Peru, we seek independent validation of altered polykefide biosynthetic genes in human populations. In the laboratory, we will test whether polykefide synthase genes and the lipids they produce influence molecular remodeling of the cell wall, Mtb permeability changes and drug resistance. To determine if genes showing strong statistical associations are actually causal of the drug resistant state or altered fitness, we will test measure the cell wall components and an in vivo fitness of polyketide deficient and drug-resistanct Mtb. Finally, taking advantage of whole organism screens that identify the particular bacterial metabolites changed in polyketide-deficient or drug resistant states, we will identify the changed molecules to give insight to the mechanism of resistance and to identify biomarkers of the drug resistant state.

Public Health Relevance

The emergence of multi-drug resistant TB undermines the ability to control the TB epidemic worldwide. By identifying the genes and molecules that are most frequently changed in drug-resistant TB cultures taken in natural clinic settings, we seek to identify new genes that cause resistance, so that their effects can be neutralized and drug resistant Mtb can be more rapidly recognized in the clinic.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI111224-07
Application #
10089388
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2015-02-01
Project End
2022-01-31
Budget Start
2021-02-01
Budget End
2022-01-31
Support Year
7
Fiscal Year
2021
Total Cost
Indirect Cost
Name
Brigham and Women's Hospital
Department
Type
DUNS #
030811269
City
Boston
State
MA
Country
United States
Zip Code
02115
James, Charlotte A; Yu, Krystle K Q; Gilleron, Martine et al. (2018) CD1b Tetramers Identify T Cells that Recognize Natural and Synthetic Diacylated Sulfoglycolipids from Mycobacterium tuberculosis. Cell Chem Biol 25:392-402.e14
Mizoguchi, Fumitaka; Slowikowski, Kamil; Wei, Kevin et al. (2018) Functionally distinct disease-associated fibroblast subsets in rheumatoid arthritis. Nat Commun 9:789
Davenport, Emma E; Amariuta, Tiffany; Gutierrez-Arcelus, Maria et al. (2018) Discovering in vivo cytokine-eQTL interactions from a lupus clinical trial. Genome Biol 19:168
Carette, Xavier; Platig, John; Young, David C et al. (2018) Multisystem Analysis of Mycobacterium tuberculosis Reveals Kinase-Dependent Remodeling of the Pathogen-Environment Interface. MBio 9:
Lehmann, Johannes; Cheng, Tan-Yun; Aggarwal, Anup et al. (2018) An Antibacterial ?-Lactone Kills Mycobacterium tuberculosis by Disrupting Mycolic Acid Biosynthesis. Angew Chem Int Ed Engl 57:348-353
Wun, Kwok S; Reijneveld, Josephine F; Cheng, Tan-Yun et al. (2018) T cell autoreactivity directed toward CD1c itself rather than toward carried self lipids. Nat Immunol 19:397-406
Jeon, Albert B; Obregón-Henao, Andrés; Ackart, David F et al. (2017) 2-aminoimidazoles potentiate ß-lactam antimicrobial activity against Mycobacterium tuberculosis by reducing ß-lactamase secretion and increasing cell envelope permeability. PLoS One 12:e0180925
Moody, D Branch; Suliman, Sara (2017) CD1: From Molecules to Diseases. F1000Res 6:1909
Van Rhijn, Ildiko; Iwany, Sarah K; Fodran, Peter et al. (2017) CD1b-mycolic acid tetramers demonstrate T-cell fine specificity for mycobacterial lipid tails. Eur J Immunol 47:1525-1534
Madigan, Cressida A; Cambier, C J; Kelly-Scumpia, Kindra M et al. (2017) A Macrophage Response to Mycobacterium leprae Phenolic Glycolipid Initiates Nerve Damage in Leprosy. Cell 170:973-985.e10

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