Abstract

Sepsis occurring late in the course following surgical injury, termed late onset sepsis is now the most common cause of death following trauma, burns, and elective surgery and is increasing in incidence. There is compelling evidence that loss of health promoting intestinal microbes (i.e microbiome) and its replacement by low diversity communities of healthcare associated pathogens (i.e pathobiome) plays a major contributing role in the immunopathology of sepsis and mortality. Over the last 3 continuous cycles of funding our laboratory has discovered that intestinal pathogens dynamically express virulence in a context dependent manner when they are cued by host compensatory signals (i.e opioids, cytokines, ischemic metabolites) released into the gut during surgical injury. In thi proposal we hypothesize that dynamic virulence expression among such pathogens directs them to express an immune altering phenotype that results in sepsis and mortality. In our last cycle of funding we identified a major factor that triggers a life or death signal within the virulence circuitry of several major pathogens- phosphate (Pi). When phosphate is abundant, microbial phosphoregulatory pathways override the virulence triggering effect of host signals whereas when Pi is depleted, such as occurs in the gut during injury, pathogen virulence activation is enhanced leading to the expression of immune- altering, pro-inflammatory, and lethal phenotypes. We synthesized a novel compound to maintain intestinal phosphate abundance during injury by covalently bonding Pi to a cytoprotective high MW polyethylene glycol, herein termed Pi-PEG. Here we will test the hypothesis that maintaining gut phosphate abundance with Pi-PEG during surgical injury will maintain the health promoting function of the microbiome, attenuate the virulence of the pathobiome, and prevent sepsis and mortality in mice intestinally inoculated with the actual multi- pathogen communities that are present in patients with late onset sepsis who are critically ill. Therefore we will 1. Investigate the mechanisms responsible for Pi-PEG-mediated inhibition of microbial virulence expression among virulent and resistant pathogens isolated from the gut of surgical patients with late onset sepsis 2. Define the role of dynamic microbial virulence expression on the immunopathology of sepsis and its modulation by Pi-PEG using intestinal epithelial cells (IECs) and dendritic cells DCs and 3. Elucidate the protective action of Pi-PEG by examining the systems biology of host- pathogen interactions in the gut when injured mice are exposed to human pathogen communities from patients with sepsis. Taken together, the proposed studies are highly significant for the field of sepsis research. We will leverage meta-omics to further our understanding of the systems biology involved in dynamic virulence activation when mice are colonized by actual human pathogen communities isolated from septic critically ill patients. Because Pi-PEG has no effect on microbial growth, we can gain mechanistic insight into how microbes behave in the gut when exposed to surgical injury, their effect on the immune system and how this interaction is modulated by Pi-PEG.

Public Health Relevance

We have discovered that during surgical injury, intestinal microbes dynamically express virulence in a context dependent manner by sensing and responding to host- derived physiologic 'cues' that can lead to immune activation and a lethal phenotype. In our recent funding cycle we discovered that the local concentration of phosphate (Pi) is a universal cue among hospital acquired pathogens that enhances microbial virulence expression when Pi is deficient yet inhibits virulence when Pi is abundant. Therefore as a countermeasure to prevent intestinal microbial virulence activation and its consequences during surgical injury, we have synthesized a unique phosphate based polymer (Pi-PEG) that inhibits virulence activation in intestinal pathogens and protects against mortality and now seek to determine its mechanism of action and applicability in relevant cellular and animal models of surgical injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM062344-15
Application #
9039090
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Somers, Scott D
Project Start
2001-02-01
Project End
2018-03-31
Budget Start
2016-04-01
Budget End
2017-03-31
Support Year
15
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Surgery
Type
Schools of Medicine
DUNS #
005421136
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Alverdy, John C (2018) Hypermetabolism and Nutritional Support in Sepsis. Surg Infect (Larchmt) 19:163-167
Alverdy, John C (2018) Microbiome Medicine: This Changes Everything. J Am Coll Surg 226:719-729
Gaines, S; Shao, C; Hyman, N et al. (2018) Gut microbiome influences on anastomotic leak and recurrence rates following colorectal cancer surgery. Br J Surg 105:e131-e141
Yin, Yushu; Papavasiliou, Georgia; Zaborina, Olga Y et al. (2017) De Novo Synthesis and Functional Analysis of Polyphosphate-Loaded Poly(Ethylene) Glycol Hydrogel Nanoparticles Targeting Pyocyanin and Pyoverdin Production in Pseudomonas aeruginosa as a Model Intestinal Pathogen. Ann Biomed Eng 45:1058-1068
Shakhsheer, B A; Lec, B; Zaborin, A et al. (2017) Lack of evidence for tissue hypoxia as a contributing factor in anastomotic leak following colon anastomosis and segmental devascularization in rats. Int J Colorectal Dis 32:539-547
Fleming, Irma D; Krezalek, Monika A; Belogortseva, Natalia et al. (2017) Modeling Acinetobacter baumannii wound infections: The critical role of iron. J Trauma Acute Care Surg 82:557-565
Alverdy, John C; Hyman, Neil; Gilbert, Jack et al. (2017) Preparing the Bowel for Surgery: Learning from the Past and Planning for the Future. J Am Coll Surg 225:324-332
Hyoju, Sanjiv K; Klabbers, Robin E; Aaron, Melissa et al. (2017) Oral Polyphosphate Suppresses Bacterial Collagenase Production and Prevents Anastomotic Leak Due to Serratia marcescens and Pseudomonas aeruginosa. Ann Surg :
Belogortseva, Natalia; Krezalek, Monika; Guyton, Kristina et al. (2017) Media from macrophages co-incubated with Enterococcus faecalis induces epithelial cell monolayer reassembly and altered cell morphology. PLoS One 12:e0182825
Alverdy, John C; Luo, James N (2017) The Influence of Host Stress on the Mechanism of Infection: Lost Microbiomes, Emergent Pathobiomes, and the Role of Interkingdom Signaling. Front Microbiol 8:322

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