Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance

R. Lucas; Y. Hadizamani; P. Enkhbaatar; G. Csanyi; R.W. Caldwell; H. Hundsberger; S. Sridhar; A.A. Lever; M. Hudel; D. Ash; M. Ushio-Fukai; T. Fukai; T. Chakraborty; A. Verin; D.C. Eaton; M. Romero; J. Hamacher

doi:10.3389/fphys.2021.793251

Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance

R. Lucas
, Y. Hadizamani
, P. Enkhbaatar
, G. Csanyi
, R.W. Caldwell
, H. Hundsberger
, S. Sridhar
, A.A. Lever
, M. Hudel
, D. Ash
, M. Ushio-Fukai
, T. Fukai
, T. Chakraborty
, A. Verin
, D.C. Eaton
, M. Romero
, J. Hamacher

Institute Biotechnology

Lungen-und Atmungsstiftung Bern
Saarland University
Emory University
Justus Liebig University Giessen
University of Texas Medical Branch at Galveston
Augusta University
Paracelsus Private Medical University Salzburg
Lindenhofspital Bern

Research output: Contribution to journal › Review article › peer-review

Abstract

Alveolar-capillary leak is a hallmark of the acute respiratory distress syndrome (ARDS), a potentially lethal complication of severe sepsis, trauma and pneumonia, including COVID-19. Apart from barrier dysfunction, ARDS is characterized by hyper-inflammation and impaired alveolar fluid clearance (AFC), which foster the development of pulmonary permeability edema and hamper gas exchange. Tumor Necrosis Factor (TNF) is an evolutionarily conserved pleiotropic cytokine, involved in host immune defense against pathogens and cancer. TNF exists in both membrane-bound and soluble form and its mainly -but not exclusively- pro-inflammatory and cytolytic actions are mediated by partially overlapping TNFR1 and TNFR2 binding sites situated at the interface between neighboring subunits in the homo-trimer. Whereas TNFR1 signaling can mediate hyper-inflammation and impaired barrier function and AFC in the lungs, ligand stimulation of TNFR2 can protect from ventilation-induced lung injury. Spatially distinct from the TNFR binding sites, TNF harbors within its structure a lectin-like domain that rather protects lung function in ARDS. The lectin-like domain of TNF -mimicked by the 17 residue TIP peptide- represents a physiological mediator of alveolar-capillary barrier protection. and increases AFC in both hydrostatic and permeability pulmonary edema animal models. The TIP peptide directly activates the epithelial sodium channel (ENaC) -a key mediator of fluid and blood pressure control- upon binding to its α subunit, which is also a part of the non-selective cation channel (NSC). Activity of the lectin-like domain of TNF is preserved in complexes between TNF and its soluble TNFRs and can be physiologically relevant in pneumonia. Antibody- and soluble TNFR-based therapeutic strategies show considerable success in diseases such as rheumatoid arthritis, psoriasis and inflammatory bowel disease, but their chronic use can increase susceptibility to infection. Since the lectin-like domain of TNF does not interfere with TNF’s anti-bacterial actions, while exerting protective actions in the alveolar-capillary compartments, it is currently evaluated in clinical trials in ARDS and COVID-19. A more comprehensive knowledge of the precise role of the TNFR binding sites versus the lectin-like domain of TNF in lung injury, tissue hypoxia, repair and remodeling may foster the development of novel therapeutics for ARDS.

Original language	English
Article number	793251
Pages (from-to)	793251
Journal	Frontiers in Physiology
Volume	12
DOIs	https://doi.org/10.3389/fphys.2021.793251
Publication status	Published - 21 Feb 2022

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

alpha 1 antitrypsin
atorvastatin
baicalin
beta glucan
bms 470539
butyric acid
cation
dexamethasone
emodin
epithelial sodium channel
etanercept
infliximab
lectin
lipoxin A
monoclonal antibody
nimbolide
pentoxifylline
pravastatin
rosuvastatin
rsh 054951 5 hivmu6
simvastatin
solnatide
thalidomide
TIP peptide
tissue inhibitor of metalloproteinase 3
tumor necrosis factor
tumor necrosis factor alpha 1
tumor necrosis factor alpha 2
tumor necrosis factor alpha induced protein 3
tumor necrosis factor antibody
tumor necrosis factor monoclonal antibody
unclassified drug
adult respiratory distress syndrome
alveolar fluid clearance
antibacterial activity
binding site
blood pressure regulation
capillary leak syndrome
coronavirus disease 2019
gas exchange
human
hyperinflammation
immunity
infection sensitivity
inflammatory bowel disease
injury
lung clearance
lung edema
lung function
nonhuman
permeability barrier
pneumonia
protection
psoriasis
Review
rheumatoid arthritis
sepsis
TNF signaling
trimerization
ventilator induced lung injury
COVID-19
TNF lectin-like domain
acute respiratory distress syndrome
TNF receptor

IMC Research Focuses

Medical biotechnology

ÖFOS 2012 - Austrian Fields of Study

304005 Medical biotechnology

Access to Document

10.3389/fphys.2021.793251

Cite this

Lucas, R., Hadizamani, Y., Enkhbaatar, P., Csanyi, G., Caldwell, R. W., Hundsberger, H., Sridhar, S., Lever, A. A., Hudel, M., Ash, D., Ushio-Fukai, M., Fukai, T., Chakraborty, T., Verin, A., Eaton, D. C., Romero, M., & Hamacher, J. (2022). Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance. Frontiers in Physiology, 12, 793251. Article 793251. https://doi.org/10.3389/fphys.2021.793251

@article{8bc5d8ed5303490e8952d534a872b914,

title = "Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance",

abstract = "Alveolar-capillary leak is a hallmark of the acute respiratory distress syndrome (ARDS), a potentially lethal complication of severe sepsis, trauma and pneumonia, including COVID-19. Apart from barrier dysfunction, ARDS is characterized by hyper-inflammation and impaired alveolar fluid clearance (AFC), which foster the development of pulmonary permeability edema and hamper gas exchange. Tumor Necrosis Factor (TNF) is an evolutionarily conserved pleiotropic cytokine, involved in host immune defense against pathogens and cancer. TNF exists in both membrane-bound and soluble form and its mainly -but not exclusively- pro-inflammatory and cytolytic actions are mediated by partially overlapping TNFR1 and TNFR2 binding sites situated at the interface between neighboring subunits in the homo-trimer. Whereas TNFR1 signaling can mediate hyper-inflammation and impaired barrier function and AFC in the lungs, ligand stimulation of TNFR2 can protect from ventilation-induced lung injury. Spatially distinct from the TNFR binding sites, TNF harbors within its structure a lectin-like domain that rather protects lung function in ARDS. The lectin-like domain of TNF -mimicked by the 17 residue TIP peptide- represents a physiological mediator of alveolar-capillary barrier protection. and increases AFC in both hydrostatic and permeability pulmonary edema animal models. The TIP peptide directly activates the epithelial sodium channel (ENaC) -a key mediator of fluid and blood pressure control- upon binding to its α subunit, which is also a part of the non-selective cation channel (NSC). Activity of the lectin-like domain of TNF is preserved in complexes between TNF and its soluble TNFRs and can be physiologically relevant in pneumonia. Antibody- and soluble TNFR-based therapeutic strategies show considerable success in diseases such as rheumatoid arthritis, psoriasis and inflammatory bowel disease, but their chronic use can increase susceptibility to infection. Since the lectin-like domain of TNF does not interfere with TNF{\textquoteright}s anti-bacterial actions, while exerting protective actions in the alveolar-capillary compartments, it is currently evaluated in clinical trials in ARDS and COVID-19. A more comprehensive knowledge of the precise role of the TNFR binding sites versus the lectin-like domain of TNF in lung injury, tissue hypoxia, repair and remodeling may foster the development of novel therapeutics for ARDS.",

keywords = "alpha 1 antitrypsin, atorvastatin, baicalin, beta glucan, bms 470539, butyric acid, cation, dexamethasone, emodin, epithelial sodium channel, etanercept, infliximab, lectin, lipoxin A, monoclonal antibody, nimbolide, pentoxifylline, pravastatin, rosuvastatin, rsh 054951 5 hivmu6, simvastatin, solnatide, thalidomide, TIP peptide, tissue inhibitor of metalloproteinase 3, tumor necrosis factor, tumor necrosis factor alpha 1, tumor necrosis factor alpha 2, tumor necrosis factor alpha induced protein 3, tumor necrosis factor antibody, tumor necrosis factor monoclonal antibody, unclassified drug, adult respiratory distress syndrome, alveolar fluid clearance, antibacterial activity, binding site, blood pressure regulation, capillary leak syndrome, coronavirus disease 2019, gas exchange, human, hyperinflammation, immunity, infection sensitivity, inflammatory bowel disease, injury, lung clearance, lung edema, lung function, nonhuman, permeability barrier, pneumonia, protection, psoriasis, Review, rheumatoid arthritis, sepsis, TNF signaling, trimerization, ventilator induced lung injury, COVID-19, TNF lectin-like domain, acute respiratory distress syndrome, TNF receptor",

author = "R. Lucas and Y. Hadizamani and P. Enkhbaatar and G. Csanyi and R.W. Caldwell and H. Hundsberger and S. Sridhar and A.A. Lever and M. Hudel and D. Ash and M. Ushio-Fukai and T. Fukai and T. Chakraborty and A. Verin and D.C. Eaton and M. Romero and J. Hamacher",

note = "Funding Information: Funding was obtained from R01HL138410 (to RL and DE), R01HL135584 and R01HL160014 (to MU-F), R01HL147550 (to MU-F and TF), R01HL116976 (to TF and MU-F), R01HL139562 (to GC), Veterans Administration Merit Review Award 2I01BX001232 (to TF) and by the German Scientific Research Foundation (DFG) through the Collaborative Research Center TRR84 (Project A4, to TC). The work of YH and JH was funded by the Lungen-und Atmungsstiftung, Bern, Switzerland. RL also received funding from this foundation for the preparation of this review. Publisher Copyright: Copyright {\textcopyright} 2022 Lucas, Hadizamani, Enkhbaatar, Csanyi, Caldwell, Hundsberger, Sridhar, Lever, Hudel, Ash, Ushio-Fukai, Fukai, Chakraborty, Verin, Eaton, Romero and Hamacher. Copyright {\textcopyright} 2022 Lucas, Hadizamani, Enkhbaatar, Csanyi, Caldwell, Hundsberger, Sridhar, Lever, Hudel, Ash, Ushio-Fukai, Fukai, Chakraborty, Verin, Eaton, Romero and Hamacher.",

year = "2022",

month = feb,

day = "21",

doi = "10.3389/fphys.2021.793251",

language = "English",

volume = "12",

pages = "793251",

journal = "Frontiers in Physiology",

issn = "1664-042X",

publisher = "Frontiers Media SA",

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Lucas, R, Hadizamani, Y, Enkhbaatar, P, Csanyi, G, Caldwell, RW, Hundsberger, H, Sridhar, S, Lever, AA, Hudel, M, Ash, D, Ushio-Fukai, M, Fukai, T, Chakraborty, T, Verin, A, Eaton, DC, Romero, M & Hamacher, J 2022, 'Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance', Frontiers in Physiology, vol. 12, 793251, pp. 793251. https://doi.org/10.3389/fphys.2021.793251

TY - JOUR

T1 - Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance

AU - Lucas, R.

AU - Hadizamani, Y.

AU - Enkhbaatar, P.

AU - Csanyi, G.

AU - Caldwell, R.W.

AU - Hundsberger, H.

AU - Sridhar, S.

AU - Lever, A.A.

AU - Hudel, M.

AU - Ash, D.

AU - Ushio-Fukai, M.

AU - Fukai, T.

AU - Chakraborty, T.

AU - Verin, A.

AU - Eaton, D.C.

AU - Romero, M.

AU - Hamacher, J.

N1 - Funding Information: Funding was obtained from R01HL138410 (to RL and DE), R01HL135584 and R01HL160014 (to MU-F), R01HL147550 (to MU-F and TF), R01HL116976 (to TF and MU-F), R01HL139562 (to GC), Veterans Administration Merit Review Award 2I01BX001232 (to TF) and by the German Scientific Research Foundation (DFG) through the Collaborative Research Center TRR84 (Project A4, to TC). The work of YH and JH was funded by the Lungen-und Atmungsstiftung, Bern, Switzerland. RL also received funding from this foundation for the preparation of this review. Publisher Copyright: Copyright © 2022 Lucas, Hadizamani, Enkhbaatar, Csanyi, Caldwell, Hundsberger, Sridhar, Lever, Hudel, Ash, Ushio-Fukai, Fukai, Chakraborty, Verin, Eaton, Romero and Hamacher. Copyright © 2022 Lucas, Hadizamani, Enkhbaatar, Csanyi, Caldwell, Hundsberger, Sridhar, Lever, Hudel, Ash, Ushio-Fukai, Fukai, Chakraborty, Verin, Eaton, Romero and Hamacher.

PY - 2022/2/21

Y1 - 2022/2/21

N2 - Alveolar-capillary leak is a hallmark of the acute respiratory distress syndrome (ARDS), a potentially lethal complication of severe sepsis, trauma and pneumonia, including COVID-19. Apart from barrier dysfunction, ARDS is characterized by hyper-inflammation and impaired alveolar fluid clearance (AFC), which foster the development of pulmonary permeability edema and hamper gas exchange. Tumor Necrosis Factor (TNF) is an evolutionarily conserved pleiotropic cytokine, involved in host immune defense against pathogens and cancer. TNF exists in both membrane-bound and soluble form and its mainly -but not exclusively- pro-inflammatory and cytolytic actions are mediated by partially overlapping TNFR1 and TNFR2 binding sites situated at the interface between neighboring subunits in the homo-trimer. Whereas TNFR1 signaling can mediate hyper-inflammation and impaired barrier function and AFC in the lungs, ligand stimulation of TNFR2 can protect from ventilation-induced lung injury. Spatially distinct from the TNFR binding sites, TNF harbors within its structure a lectin-like domain that rather protects lung function in ARDS. The lectin-like domain of TNF -mimicked by the 17 residue TIP peptide- represents a physiological mediator of alveolar-capillary barrier protection. and increases AFC in both hydrostatic and permeability pulmonary edema animal models. The TIP peptide directly activates the epithelial sodium channel (ENaC) -a key mediator of fluid and blood pressure control- upon binding to its α subunit, which is also a part of the non-selective cation channel (NSC). Activity of the lectin-like domain of TNF is preserved in complexes between TNF and its soluble TNFRs and can be physiologically relevant in pneumonia. Antibody- and soluble TNFR-based therapeutic strategies show considerable success in diseases such as rheumatoid arthritis, psoriasis and inflammatory bowel disease, but their chronic use can increase susceptibility to infection. Since the lectin-like domain of TNF does not interfere with TNF’s anti-bacterial actions, while exerting protective actions in the alveolar-capillary compartments, it is currently evaluated in clinical trials in ARDS and COVID-19. A more comprehensive knowledge of the precise role of the TNFR binding sites versus the lectin-like domain of TNF in lung injury, tissue hypoxia, repair and remodeling may foster the development of novel therapeutics for ARDS.

AB - Alveolar-capillary leak is a hallmark of the acute respiratory distress syndrome (ARDS), a potentially lethal complication of severe sepsis, trauma and pneumonia, including COVID-19. Apart from barrier dysfunction, ARDS is characterized by hyper-inflammation and impaired alveolar fluid clearance (AFC), which foster the development of pulmonary permeability edema and hamper gas exchange. Tumor Necrosis Factor (TNF) is an evolutionarily conserved pleiotropic cytokine, involved in host immune defense against pathogens and cancer. TNF exists in both membrane-bound and soluble form and its mainly -but not exclusively- pro-inflammatory and cytolytic actions are mediated by partially overlapping TNFR1 and TNFR2 binding sites situated at the interface between neighboring subunits in the homo-trimer. Whereas TNFR1 signaling can mediate hyper-inflammation and impaired barrier function and AFC in the lungs, ligand stimulation of TNFR2 can protect from ventilation-induced lung injury. Spatially distinct from the TNFR binding sites, TNF harbors within its structure a lectin-like domain that rather protects lung function in ARDS. The lectin-like domain of TNF -mimicked by the 17 residue TIP peptide- represents a physiological mediator of alveolar-capillary barrier protection. and increases AFC in both hydrostatic and permeability pulmonary edema animal models. The TIP peptide directly activates the epithelial sodium channel (ENaC) -a key mediator of fluid and blood pressure control- upon binding to its α subunit, which is also a part of the non-selective cation channel (NSC). Activity of the lectin-like domain of TNF is preserved in complexes between TNF and its soluble TNFRs and can be physiologically relevant in pneumonia. Antibody- and soluble TNFR-based therapeutic strategies show considerable success in diseases such as rheumatoid arthritis, psoriasis and inflammatory bowel disease, but their chronic use can increase susceptibility to infection. Since the lectin-like domain of TNF does not interfere with TNF’s anti-bacterial actions, while exerting protective actions in the alveolar-capillary compartments, it is currently evaluated in clinical trials in ARDS and COVID-19. A more comprehensive knowledge of the precise role of the TNFR binding sites versus the lectin-like domain of TNF in lung injury, tissue hypoxia, repair and remodeling may foster the development of novel therapeutics for ARDS.

KW - alpha 1 antitrypsin

KW - atorvastatin

KW - baicalin

KW - beta glucan

KW - bms 470539

KW - butyric acid

KW - cation

KW - dexamethasone

KW - emodin

KW - epithelial sodium channel

KW - etanercept

KW - infliximab

KW - lectin

KW - lipoxin A

KW - monoclonal antibody

KW - nimbolide

KW - pentoxifylline

KW - pravastatin

KW - rosuvastatin

KW - rsh 054951 5 hivmu6

KW - simvastatin

KW - solnatide

KW - thalidomide

KW - TIP peptide

KW - tissue inhibitor of metalloproteinase 3

KW - tumor necrosis factor

KW - tumor necrosis factor alpha 1

KW - tumor necrosis factor alpha 2

KW - tumor necrosis factor alpha induced protein 3

KW - tumor necrosis factor antibody

KW - tumor necrosis factor monoclonal antibody

KW - unclassified drug

KW - adult respiratory distress syndrome

KW - alveolar fluid clearance

KW - antibacterial activity

KW - binding site

KW - blood pressure regulation

KW - capillary leak syndrome

KW - coronavirus disease 2019

KW - gas exchange

KW - human

KW - hyperinflammation

KW - immunity

KW - infection sensitivity

KW - inflammatory bowel disease

KW - injury

KW - lung clearance

KW - lung edema

KW - lung function

KW - nonhuman

KW - permeability barrier

KW - pneumonia

KW - protection

KW - psoriasis

KW - Review

KW - rheumatoid arthritis

KW - sepsis

KW - TNF signaling

KW - trimerization

KW - ventilator induced lung injury

KW - COVID-19

KW - TNF lectin-like domain

KW - acute respiratory distress syndrome

KW - TNF receptor

UR - https://www.scopus.com/pages/publications/85125880134

U2 - 10.3389/fphys.2021.793251

DO - 10.3389/fphys.2021.793251

M3 - Review article

C2 - 35264975

SN - 1664-042X

VL - 12

SP - 793251

JO - Frontiers in Physiology

JF - Frontiers in Physiology

M1 - 793251

ER -

Dichotomous Role of Tumor Necrosis Factor in Pulmonary Barrier Function and Alveolar Fluid Clearance

Abstract

UN SDGs

Keywords

IMC Research Focuses

ÖFOS 2012 - Austrian Fields of Study

Access to Document

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