Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis

Kritee Mehdiratta; Shubham Singh; Sachin Sharma; Rashmi S. Bhosale; Rahul Choudhury; Dattatraya P. Masal; Alzu Manocha; Bhushan Dilip Dhamale; Naseem Khan; Vivekanand Asokachandran; Pooja Sharma; Melanie Ikeh; Amanda C. Brown; Tanya Parish; Anil K. Ojha; Joy Sarojini Michael; Mohammed Faruq; Guruprasad R. Medigeshi; Debasisa Mohanty; D. Srinivasa Reddy; Vivek T. Natarajan; Siddhesh S. Kamat; Rajesh S. Gokhale

doi:10.1073/pnas.2110293119

Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis

Kritee Mehdiratta
, Shubham Singh
, Sachin Sharma
, Rashmi S. Bhosale
, Rahul Choudhury
, Dattatraya P. Masal
, Alzu Manocha
, Bhushan Dilip Dhamale
, Naseem Khan
, Vivekanand Asokachandran
, Pooja Sharma
, Melanie Ikeh
, Amanda C. Brown
, Tanya Parish
, Anil K. Ojha
, Joy Sarojini Michael
, Mohammed Faruq
, Guruprasad R. Medigeshi
, Debasisa Mohanty
, D. Srinivasa Reddy

Vivek T. Natarajan, Siddhesh S. Kamat, Rajesh S. Gokhale

CSIR - Institute of Genomics and Integrative Biology
Academy of Scientific and Innovative Research
Indian Institute of Science Education and Research Pune
National Institute of Immunology India
CSIR - National Chemical Laboratory
Translational Health Science and Technology Institute
Queen Mary University of London
Wadsworth Center for Laboratories and Research
SUNY Albany
Christian Medical College

Research output: Contribution to journal › Article › peer-review

32 Citations (Scopus)

Abstract

Mycobacterium tuberculosis (Mtb) endures a combination of metal scarcity and toxicity throughout the human infection cycle, contributing to complex clinical manifestations. Pathogens counteract this paradoxical dysmetallostasis by producing specialized metal trafficking systems. Capture of extracellular metal by siderophores is a widely accepted mode of iron acquisition, and Mtb iron-chelating siderophores, mycobactin, have been known since 1965. Currently, it is not known whether Mtb produces zinc scavenging molecules. Here, we characterize low-molecular-weight zinc-binding compounds secreted and imported by Mtb for zinc acquisition. These molecules, termed kupyaphores, are produced by a 10.8 kbp biosynthetic cluster and consists of a dipeptide core of ornithine and phenylalaninol, where amino groups are acylated with isonitrile-containing fatty acyl chains. Kupyaphores are stringently regulated and support Mtb survival under both nutritional deprivation and intoxication conditions. A kupyaphore-deficient Mtb strain is unable to mobilize sufficient zinc and shows reduced fitness upon infection. We observed early induction of kupyaphores in Mtb-infected mice lungs after infection, and these metabolites disappeared after 2 wk. Furthermore, we identify an Mtb-encoded isonitrile hydratase, which can possibly mediate intracellular zinc release through covalent modification of the isonitrile group of kupyaphores. Mtb clinical strains also produce kupyaphores during early passages. Our study thus uncovers a previously unknown zinc acquisition strategy of Mtb that could modulate host-pathogen interactions and disease outcome.

Original language	English
Article number	e2110293119
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	119
Issue number	8
DOIs	https://doi.org/10.1073/pnas.2110293119
Publication status	Published - 22 Feb 2022
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

metallophore
nutritional immunity
tuberculosis
zinc

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10.1073/pnas.2110293119

Cite this

Mehdiratta, K., Singh, S., Sharma, S., Bhosale, R. S., Choudhury, R., Masal, D. P., Manocha, A., Dhamale, B. D., Khan, N., Asokachandran, V., Sharma, P., Ikeh, M., Brown, A. C., Parish, T., Ojha, A. K., Michael, J. S., Faruq, M., Medigeshi, G. R., Mohanty, D., ... Gokhale, R. S. (2022). Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis. Proceedings of the National Academy of Sciences of the United States of America, 119(8), Article e2110293119. https://doi.org/10.1073/pnas.2110293119

@article{277a895f2f7f4cd9808be76cd16ad2f6,

title = "Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis",

abstract = "Mycobacterium tuberculosis (Mtb) endures a combination of metal scarcity and toxicity throughout the human infection cycle, contributing to complex clinical manifestations. Pathogens counteract this paradoxical dysmetallostasis by producing specialized metal trafficking systems. Capture of extracellular metal by siderophores is a widely accepted mode of iron acquisition, and Mtb iron-chelating siderophores, mycobactin, have been known since 1965. Currently, it is not known whether Mtb produces zinc scavenging molecules. Here, we characterize low-molecular-weight zinc-binding compounds secreted and imported by Mtb for zinc acquisition. These molecules, termed kupyaphores, are produced by a 10.8 kbp biosynthetic cluster and consists of a dipeptide core of ornithine and phenylalaninol, where amino groups are acylated with isonitrile-containing fatty acyl chains. Kupyaphores are stringently regulated and support Mtb survival under both nutritional deprivation and intoxication conditions. A kupyaphore-deficient Mtb strain is unable to mobilize sufficient zinc and shows reduced fitness upon infection. We observed early induction of kupyaphores in Mtb-infected mice lungs after infection, and these metabolites disappeared after 2 wk. Furthermore, we identify an Mtb-encoded isonitrile hydratase, which can possibly mediate intracellular zinc release through covalent modification of the isonitrile group of kupyaphores. Mtb clinical strains also produce kupyaphores during early passages. Our study thus uncovers a previously unknown zinc acquisition strategy of Mtb that could modulate host-pathogen interactions and disease outcome.",

keywords = "metallophore, nutritional immunity, tuberculosis, zinc",

author = "Kritee Mehdiratta and Shubham Singh and Sachin Sharma and Bhosale, \{Rashmi S.\} and Rahul Choudhury and Masal, \{Dattatraya P.\} and Alzu Manocha and Dhamale, \{Bhushan Dilip\} and Naseem Khan and Vivekanand Asokachandran and Pooja Sharma and Melanie Ikeh and Brown, \{Amanda C.\} and Tanya Parish and Ojha, \{Anil K.\} and Michael, \{Joy Sarojini\} and Mohammed Faruq and Medigeshi, \{Guruprasad R.\} and Debasisa Mohanty and Reddy, \{D. Srinivasa\} and Natarajan, \{Vivek T.\} and Kamat, \{Siddhesh S.\} and Gokhale, \{Rajesh S.\}",

year = "2022",

month = feb,

day = "22",

doi = "10.1073/pnas.2110293119",

language = "English",

volume = "119",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

issn = "0027-8424",

publisher = "National Academy of Sciences",

number = "8",

}

Mehdiratta, K, Singh, S, Sharma, S, Bhosale, RS, Choudhury, R, Masal, DP, Manocha, A, Dhamale, BD, Khan, N, Asokachandran, V, Sharma, P, Ikeh, M, Brown, AC, Parish, T, Ojha, AK, Michael, JS, Faruq, M, Medigeshi, GR, Mohanty, D, Reddy, DS, Natarajan, VT, Kamat, SS & Gokhale, RS 2022, 'Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis', Proceedings of the National Academy of Sciences of the United States of America, vol. 119, no. 8, e2110293119. https://doi.org/10.1073/pnas.2110293119

TY - JOUR

T1 - Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis

AU - Mehdiratta, Kritee

AU - Singh, Shubham

AU - Sharma, Sachin

AU - Bhosale, Rashmi S.

AU - Choudhury, Rahul

AU - Masal, Dattatraya P.

AU - Manocha, Alzu

AU - Dhamale, Bhushan Dilip

AU - Khan, Naseem

AU - Asokachandran, Vivekanand

AU - Sharma, Pooja

AU - Ikeh, Melanie

AU - Brown, Amanda C.

AU - Parish, Tanya

AU - Ojha, Anil K.

AU - Michael, Joy Sarojini

AU - Faruq, Mohammed

AU - Medigeshi, Guruprasad R.

AU - Mohanty, Debasisa

AU - Reddy, D. Srinivasa

AU - Natarajan, Vivek T.

AU - Kamat, Siddhesh S.

AU - Gokhale, Rajesh S.

PY - 2022/2/22

Y1 - 2022/2/22

N2 - Mycobacterium tuberculosis (Mtb) endures a combination of metal scarcity and toxicity throughout the human infection cycle, contributing to complex clinical manifestations. Pathogens counteract this paradoxical dysmetallostasis by producing specialized metal trafficking systems. Capture of extracellular metal by siderophores is a widely accepted mode of iron acquisition, and Mtb iron-chelating siderophores, mycobactin, have been known since 1965. Currently, it is not known whether Mtb produces zinc scavenging molecules. Here, we characterize low-molecular-weight zinc-binding compounds secreted and imported by Mtb for zinc acquisition. These molecules, termed kupyaphores, are produced by a 10.8 kbp biosynthetic cluster and consists of a dipeptide core of ornithine and phenylalaninol, where amino groups are acylated with isonitrile-containing fatty acyl chains. Kupyaphores are stringently regulated and support Mtb survival under both nutritional deprivation and intoxication conditions. A kupyaphore-deficient Mtb strain is unable to mobilize sufficient zinc and shows reduced fitness upon infection. We observed early induction of kupyaphores in Mtb-infected mice lungs after infection, and these metabolites disappeared after 2 wk. Furthermore, we identify an Mtb-encoded isonitrile hydratase, which can possibly mediate intracellular zinc release through covalent modification of the isonitrile group of kupyaphores. Mtb clinical strains also produce kupyaphores during early passages. Our study thus uncovers a previously unknown zinc acquisition strategy of Mtb that could modulate host-pathogen interactions and disease outcome.

AB - Mycobacterium tuberculosis (Mtb) endures a combination of metal scarcity and toxicity throughout the human infection cycle, contributing to complex clinical manifestations. Pathogens counteract this paradoxical dysmetallostasis by producing specialized metal trafficking systems. Capture of extracellular metal by siderophores is a widely accepted mode of iron acquisition, and Mtb iron-chelating siderophores, mycobactin, have been known since 1965. Currently, it is not known whether Mtb produces zinc scavenging molecules. Here, we characterize low-molecular-weight zinc-binding compounds secreted and imported by Mtb for zinc acquisition. These molecules, termed kupyaphores, are produced by a 10.8 kbp biosynthetic cluster and consists of a dipeptide core of ornithine and phenylalaninol, where amino groups are acylated with isonitrile-containing fatty acyl chains. Kupyaphores are stringently regulated and support Mtb survival under both nutritional deprivation and intoxication conditions. A kupyaphore-deficient Mtb strain is unable to mobilize sufficient zinc and shows reduced fitness upon infection. We observed early induction of kupyaphores in Mtb-infected mice lungs after infection, and these metabolites disappeared after 2 wk. Furthermore, we identify an Mtb-encoded isonitrile hydratase, which can possibly mediate intracellular zinc release through covalent modification of the isonitrile group of kupyaphores. Mtb clinical strains also produce kupyaphores during early passages. Our study thus uncovers a previously unknown zinc acquisition strategy of Mtb that could modulate host-pathogen interactions and disease outcome.

KW - metallophore

KW - nutritional immunity

KW - tuberculosis

KW - zinc

U2 - 10.1073/pnas.2110293119

DO - 10.1073/pnas.2110293119

M3 - Article

C2 - 35193957

AN - SCOPUS:85125154470

SN - 0027-8424

VL - 119

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 8

M1 - e2110293119

ER -

Kupyaphores are zinc homeostatic metallophores required for colonization of Mycobacterium tuberculosis

Abstract

UN SDGs

Keywords

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