Abstract

Efficient mechanisms for the clearance of lipopolysaccharide (LPS) from the circulation are critical to prevent excessive or unwanted inflammation, particularly during infection. The observation that elevated circulating LPS levels correlate with adverse outcome in critically ill sepsis patients suggests that normal clearance mechanisms become impaired or dysfunctional in severe sepsis. Therefore, defining the physiologic mechanisms for LPS clearance is essential to understanding how this process is altered in severe infection. Our previous work supports a central role for a novel Toll-like receptor (TLR) 4-dependent signaling complex on hepatocytes (HC) for the efficient uptake of LPS. This TLR4-dependent LPS uptake pathway in HC is distinct from the canonical TLR4-dependent pathway described in macrophages for the activation of innate immune mechanisms. We have also established the models to extend our work in vivo. Using both TLR4 bone marrow chimeric mice and novel cell specific TLR4-/- mouse strains developed in our lab, we have confirmed the requirement of TLR4 for the uptake of LPS by HC and that LPS uptake in KC is TLR4- independent. These observations lead us to propose that the efficient LPS uptake mechanisms in KC clear low levels of LPS intermittently released by the gastrointestinal tract, while TLR4-dependent uptake of LPS by HC contributes to uptake of higher LPS levels, or boluses of LPS, encountered during severe infection. Our objectives in this proposal are to fully test the hypothesis that a novel TLR4-signaling complex on HC contributes to HC LPS uptake and LPS clearance from the circulation during endotoxemia and sepsis. This work will challenge the paradigm that LPS clearance is mainly dependent on KC and mostly TLR4-independent. By fully characterizing the TLR4, CD11b/CD18-dependent signaling pathways involved in HC LPS uptake, we will define and functionally characterize a TLR4-dependent signaling pathway distinct from the canonical TLR4 pathway that leads to inflammatory mediator production. For part of this work, we will exploit a novel strategy using our recently developed TLR4-loxP mouse strains to selectively delete TLR4 from specific cell populations in the liver. Utilizing these mice, we will definitively establish the role of TLR4 on specific cell populations in LPS uptake, as well as LPS clearance, and we will explore the consequences of impaired LPS uptake in our models. We expect to show that HC clear LPS in the setting of endotoxemia and sepsis, to define the signaling mechanism leading to LPS uptake in HC, and to show that impairment of this mechanism leads to an exaggerated or sustained inflammatory response. By defining the pathways leading to TLR4-dependent LPS uptake, we expect to contribute to the understanding of how the process fails during severe infection. This, in turn, could lead to strategies that promote LPS clearance and improve outcomes in critically ill septic patients.

Public Health Relevance

Elevated circulating endotoxin levels in critically ill sepsis patients correlate with a poor outcome and this suggests that normal endotoxin clearance mechanisms become impaired or dysfunctional in severe sepsis. The physiologic mechanisms for endotoxin clearance are poorly understood but understanding these mechanisms is essential to understanding how this process fails during severe infection. Our research investigating these mechanisms may lead to future treatments for critically ill sepsis patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM050441-19
Application #
8462623
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Somers, Scott D
Project Start
1994-01-01
Project End
2015-04-30
Budget Start
2013-05-01
Budget End
2014-04-30
Support Year
19
Fiscal Year
2013
Total Cost
$287,051
Indirect Cost
$94,051

  Institution

Name
University of Pittsburgh
Department
Surgery
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Li, Wenbo; Zhang, Wei; Deng, Meihong et al. (2018) Stearoyl Lysophosphatidylcholine Inhibits Endotoxin-Induced Caspase-11 Activation. Shock 50:339-345
Kang, Rui; Zeng, Ling; Zhu, Shan et al. (2018) Lipid Peroxidation Drives Gasdermin D-Mediated Pyroptosis in Lethal Polymicrobial Sepsis. Cell Host Microbe 24:97-108.e4
Zhou, Hui; Deng, Meihong; Liu, Yingjie et al. (2018) Platelet HMGB1 is required for efficient bacterial clearance in intra-abdominal bacterial sepsis in mice. Blood Adv 2:638-648
Sun, Qian; Fan, Jie; Billiar, Timothy R et al. (2017) Inflammasome and autophagy regulation - a two-way street. Mol Med 23:188-195
Cai, Jingjing; Zhong, Hua; Wu, Jinze et al. (2017) Cathepsin L promotes Vascular Intimal Hyperplasia after Arterial Injury. Mol Med 23:92-100
Xu, Hui; Turnquist, Heth R; Hoffman, Rosemary et al. (2017) Role of the IL-33-ST2 axis in sepsis. Mil Med Res 4:3
Deng, Meihong; Ma, Tao; Yan, Zhengzheng et al. (2016) Toll-like Receptor 4 Signaling on Dendritic Cells Suppresses Polymorphonuclear Leukocyte CXCR2 Expression and Trafficking via Interleukin 10 During Intra-abdominal Sepsis. J Infect Dis 213:1280-8
Sun, Qian; Wang, Qingde; Scott, Melanie J et al. (2016) Immune Activation in the Liver by Nucleic Acids. J Clin Transl Hepatol 4:151-7
Zhang, Liyong; Xiang, Wenpei; Wang, Guoliang et al. (2016) Interferon ? (IFN-?) Production during the Double-stranded RNA (dsRNA) Response in Hepatocytes Involves Coordinated and Feedforward Signaling through Toll-like Receptor 3 (TLR3), RNA-dependent Protein Kinase (PKR), Inducible Nitric Oxide Synthase (iNOS), J Biol Chem 291:15093-107
Wang, Hui; Wang, Guoliang; Zhang, Liyong et al. (2016) ADAR1 Suppresses the Activation of Cytosolic RNA-Sensing Signaling Pathways to Protect the Liver from Ischemia/Reperfusion Injury. Sci Rep 6:20248

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