Abstract

Bacteria and humans have a complex relationship: our abundant commensal organisms provide numerous benefits, whereas pathogenic bacteria impose a large burden of morbidity and mortality. The immune system restricts bacterial growth through nutritional immunity, antimicrobial peptides, lytic enzymes, and phagocytic cells. Potential pathogens respond to these threats by the activation of specific adaptive responses, many of which are critical for virulence. We study stress responses in Bacillus subtilis, a model Gram positive bacterium. One project addresses responses to the changing availability of the essential nutrient metal ions zinc, iron, and manganese. The immune system restricts the growth of pathogens by metal sequestration, both in tissues (e.g. by calprotectin) and after phagocytosis. In addition, phagocytic cells kill cells by metal intoxication. We have demonstrated that metal ion homeostasis relies on specific metal-sensing transcription factors that respond to limitation and excess of iron (Fur and PerR), manganese (MntR), and zinc (Zur and CzrA). We will characterize the genes regulated by these transcription factors, their roles in metal homeostasis, and identify the physiological effects that result from both metal ion limitation and intoxication. This work will build upon our recent identification of the major efflux systems for both iron and manganese. The insights from these studies will be directly relevant to the similar stress responses present in human pathogens. The immune system also restricts the growth of pathogens by production of antibacterial peptides and lytic enzymes, both of which affect the integrity of the cell envelope. The cell envelope is also a target for many of our most important antibiotics. In a second project, we have defined several distinct cell envelope stress responses in B. subtilis, with a focus on those regulated by extracytoplasmic function sigma factors. We will investigate the contributions of genes activated by the antibiotic-inducible sigma-M transcription factor to cell envelope homeostasis, and more specifically to acclimation to antibiotics. In parallel, we will examine the role of a cell wall stress responsive kinase/phosphatase system and the second messenger cyclic-di-AMP. Cells with mutations in these stress response pathways are sensitive to cell wall antibiotics (e.g. beta-lactams). Selection of antibiotic resistant suppressors provides a powerful approach for delineating these responsive pathways and their interconnections. These pathways are central to cell envelope homeostasis generally, in addition to their role in sensing and responding to antibiotic-induced stress, and are implicated in the emergence of antibiotic tolerance and resistance in pathogens.

Public Health Relevance

The innate immune system restricts the growth of invading bacteria by limiting access to essential nutrient metal ions (nutritional immunity) and by production of antimicrobial peptides and enzymes that attack the cell envelope. Using Bacillus subtilis as a model system, we characterize the bacterial stress responses elicited by metal ion limitation and excess, and by antibiotics that interfere with integrity of the cell envelope. The resulting insights are relevant for understanding the mechanisms that allow bacterial cells (both beneficial and harmful) to adapt to the host environment.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Unknown (R35)
Project #
1R35GM122461-01
Application #
9274500
Study Section
Special Emphasis Panel (ZGM1-TRN-9 (MR))
Program Officer
Reddy, Michael K
Project Start
2017-06-01
Project End
2022-05-31
Budget Start
2017-06-01
Budget End
2018-05-31
Support Year
1
Fiscal Year
2017
Total Cost
$472,213
Indirect Cost
$159,499

  Institution

Name
Cornell University
Department
Microbiology/Immun/Virology
Type
Schools of Earth Sciences/Natur
DUNS #
872612445
City
Ithaca
State
NY
Country
United States
Zip Code
14850

  Publications

Patel, Vaidehi; Wu, Qun; Chandrangsu, Pete et al. (2018) A metabolic checkpoint protein GlmR is important for diverting carbon into peptidoglycan biosynthesis in Bacillus subtilis. PLoS Genet 14:e1007689
Pinochet-Barros, Azul; Helmann, John D (2018) Redox Sensing by Fe2+ in Bacterial Fur Family Metalloregulators. Antioxid Redox Signal 29:1858-1871
Chandrangsu, Pete; Loi, Vu Van; Antelmann, Haike et al. (2018) The Role of Bacillithiol in Gram-Positive Firmicutes. Antioxid Redox Signal 28:445-462
Rojas-Tapias, Daniel F; Helmann, John D (2018) Stabilization of Bacillus subtilis Spx under cell wall stress requires the anti-adaptor protein YirB. PLoS Genet 14:e1007531
Zhao, Heng; Roistacher, Daniel M; Helmann, John D (2018) Aspartate deficiency limits peptidoglycan synthesis and sensitizes cells to antibiotics targeting cell wall synthesis in Bacillus subtilis. Mol Microbiol 109:826-844
Pi, Hualiang; Helmann, John D (2018) Genome-Wide Characterization of the Fur Regulatory Network Reveals a Link between Catechol Degradation and Bacillibactin Metabolism in Bacillus subtilis. MBio 9:
Cao, Yu; Pi, Hualiang; Chandrangsu, Pete et al. (2018) Antagonism of Two Plant-Growth Promoting Bacillus velezensis Isolates Against Ralstonia solanacearum and Fusarium oxysporum. Sci Rep 8:4360
Gaballa, Ahmed; Guariglia-Oropeza, Veronica; Dürr, Franziska et al. (2018) Modulation of extracytoplasmic function (ECF) sigma factor promoter selectivity by spacer region sequence. Nucleic Acids Res 46:134-145
Rojas-Tapias, Daniel F; Helmann, John D (2018) Induction of the Spx regulon by cell wall stress reveals novel regulatory mechanisms in Bacillus subtilis. Mol Microbiol 107:659-674
Pi, Hualiang; Helmann, John D (2017) Sequential induction of Fur-regulated genes in response to iron limitation in Bacillus subtilis. Proc Natl Acad Sci U S A 114:12785-12790

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