Mechanisms of decompensation and organ failure in cirrhosis: From peripheral arterial vasodilation to systemic inflammation hypothesis

Mechanisms of decompensation and organ failure in cirrhosis: From peripheral arterial vasodilation to systemic inflammation hypothesis

Summary The peripheral arterial vasodilation hypothesis has been most influential in the field of cirrhosis and its complications. It has given rise to hundreds of pathophysiological studies in experimental and human cirrhosis and is the theoretical basis of life-saving treatments. It is undisputed...

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Bibliographic Details
Published in:Journal of hepatology Vol. 63; no. 5; pp. 1272 - 1284
Main Authors: Bernardi, Mauro, Moreau, Richard, Angeli, Paolo, Schnabl, Bernd, Arroyo, Vicente
Format: Journal Article
Language:English
Published: Netherlands Elsevier B.V 01-11-2015
Subjects:
Animals
Arteries - physiopathology
Ascites
Bacterial translocation
Cardiovascular dysfunction
Cirrhosis
Cytokines - metabolism
Gastroenterology and Hepatology
Humans
Inflammation - complications
Inflammation - metabolism
Inflammation - physiopathology
Liver Cirrhosis - complications
Liver Failure - etiology
Liver Failure - metabolism
Liver Failure - physiopathology
Peripheral arterial vasodilation hypothesis
Pro-inflammatory cytokines
Renal dysfunction
Systemic inflammation
Vasodilation - physiology
plasma renin activity
ACLF
GTP
toll-like receptors
systemic inflammation hypothesis
HRS
TNF
CX3CL1
TLR(s)
mesenteric lymph nodes
C-RP
K ATP
PAMPs
nitric oxide synthase
nitric oxide
IL
HSP
relative adrenal insufficiency
guanosine 5′ monophosphate
carbon monoxide
GMP
acute-on-chronic liver failure
BH4
adenosine triphosphate-sensitive potassium channels
Cirrhosis
pathogen-associated molecular patterns
NOS
SIH
receptor tyrosine kinases
hepatorenal syndrome
ROS
IPVD
VEGFs
acute kidney injury
peripheral arterial vasodilation hypothesis
lipopolysaccharide
Ascites
Systemic inflammation
PICD
NO
tetrahydrobiopterin
PAVH
PRRs
Renal dysfunction
plasma C-reactive protein
vascular endothelial growth factors
heat shock protein
HPS
LPS
DAMPs
BT
reactive oxygen species
hepatic encephalopathy
danger-associated molecular patterns
SNS
bacterial translocation
interleukin
AKI
MLNs
SBP
hepatopulmonary syndrome
sympathetic nervous system
fractaline chemokine
guanosine 5′ triphosphate
CO
RTKs
paracentesis-induced circulatory dysfunction
ECM
pattern recognition receptors
tumor necrosis factor
intrapulmonary vasodilatation
Cardiovascular dysfunction
Pro-inflammatory cytokines
RAI
spontaneous bacterial peritonitis
HE
PRA
extracellular matrix
Peripheral arterial vasodilation hypothesis
Bacterial translocation
KATP
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Summary:Summary The peripheral arterial vasodilation hypothesis has been most influential in the field of cirrhosis and its complications. It has given rise to hundreds of pathophysiological studies in experimental and human cirrhosis and is the theoretical basis of life-saving treatments. It is undisputed that splanchnic arterial vasodilation contributes to portal hypertension and is the basis for manifestations such as ascites and hepatorenal syndrome, but the body of research generated by the hypothesis has revealed gaps in the original pathophysiological interpretation of these complications. The expansion of our knowledge on the mechanisms regulating vascular tone, inflammation and the host-microbiota interaction require a broader approach to advanced cirrhosis encompassing the whole spectrum of its manifestations. Indeed, multiorgan dysfunction and failure likely result from a complex interplay where the systemic spread of bacterial products represents the primary event. The consequent activation of the host innate immune response triggers endothelial molecular mechanisms responsible for arterial vasodilation, and also jeopardizes organ integrity with a storm of pro-inflammatory cytokines and reactive oxygen and nitrogen species. Thus, the picture of advanced cirrhosis could be seen as the result of an inflammatory syndrome in contradiction with a simple hemodynamic disturbance.
Bibliography:ObjectType-Article-2
SourceType-Scholarly Journals-1
ObjectType-Feature-3
content type line 23
ObjectType-Review-1
ISSN:0168-8278
1600-0641
DOI:10.1016/j.jhep.2015.07.004