Cirrhosis Clinical Trial
Official title:
Noninvasive Tests to Predict the Presence of Esophageal Varices in Patients With Liver Cirrhosis
Liver cirrhosis is caused by chronic liver diseases, varices exist in 30 - 60% of patients with liver cirrhosis. Variceal bleeding is one of the most important complications of cirrhosis, accelerating the progression of decompensation to a stage at which the patient is at an extremely high risk of death. Endoscopy is the gold standard for the diagnosis of varices, However, periodic endoscopic screening in all cirrhotic patients might unnecessarily induce an invasive and expensive procedure, ultimately increasing not only the medical workload of endoscopy units, but also the financial burden of patients. To avoid unnecessary endoscopy in low- risk patients, some simple, non-invasive and accurate tests have been developed to identify EVs. Such as Transient elastography (TE) , which is a noninvasive tool that measures liver stiffness (LS) correlating to liver fibrosis stage. Moreover, the LS-spleen size-to-platelet ratio score (LSPS), which is a combination of three simple examination methods (LS, spleen size and platelet count) has been established to accurately predict EVs in patients with cirrhosis. Therefore, investigators design this cross-sectional study to assess these non-invasive tests in predicting the presence of EVs in patients with cirrhosis.
Liver cirrhosis is a result of excessive extracellular matrix deposition in the liver in
response to chronic inflammatory injury triggered by chronic liver diseases. And Cirrhosis is
classified in 2 distinct clinical stages, compensated (Currently, both terms : "compensated
advanced chronic liver disease(cACLD)" and "compensated cirrhosis" are acceptable) and
decompensated, defined by the presence or absence of overt clinical complications of
cirrhosis (ascites, variceal hemorrhage, hepatic encephalopathy). Portal hypertension is a
frequent complication of liver cirrhosis, a contributing fator for ascites and hepatic
encephalopathy, and a direct cause of variceal hemorrhage. An increase in portal pressure
leads to the development of portosystemic collateral circulation, of which varices are the
most important clinical feature. In accordance with the Baveno II consensus conference,
esophageal varices (EVs) were classified as absent, small (diameter < 5 mm) or large
(diameter ≥ 5 mm). The presence of red wale marks on the variceal wall in EVs was also
recorded. EVs at a high risk for bleeding were defined according to the Baveno V criteria as
large EVs or small EVs with red signs or EVs in patients with Child-Pugh class C disease.
varices exist in 30 - 60% of patients with liver cirrhosis, depending on the severity of
Portal hypertension. The yearly rate of development of new cases is 5 - 10% , whereas the
growth rate from small to large varices ranges between 5 and 30 %.
Variceal bleeding is the most important and the most lethal complication of cirrhosis,
accelerating the progression of decompensation to a stage at which the patient is at an
extremely high risk of death. Therefore, the diagnosis, prevention, and management of EVs are
important for patients with cirrhosis. And screening for EVs in all patients with cirrhosis
is also strongly recommended across guidelines and consensus statements. Endoscopy is the
gold standard for the diagnosis of varices, and is recommended as the screening method to
identify those who should undergo prophylactic treatment when the diagnosis of cirrhosis is
made. Nonselective β-blockers significantly reduce the bleeding rate in more than half of
patients with high-risk EVs (HEVs). However, as the prevalence of HEVs at any given point in
time is 15 - 25%, the majority of subjects undergoing screening endoscopy either do not have
varices, or have varices that do not require prophylactic therapy. Therefore, periodic
endoscopic screening in all cirrhotic patients, especially low-risk groups, might
unnecessarily induce an invasive and expensive procedure, ultimately increasing not only the
medical workload of endoscopy units, but also the financial burden to patients, as the number
of patients with chronic liver disease increases and their survival improves. Furthermore,
compliance may be limited, because even asymptomatic patients may be required to repeatedly
undergo an unpleasant endoscopic procedure, which usually requires conscious sedation
decreasing work productivity, It also carries rare but serious complications. Patients might
be reluctant to receive endoscopy and become discouraged in starting preventive measures. All
of these reasons lead to decline in patient compliance with treatment and follow-ups.
Meanwhile, the endoscopy-related complications reported by a related article is close to 0.1%
of incidence.
To avoid unnecessary endoscopy in low-risk patients, some simple, non-invasive and accurate
tests have been developed to identify EVs. Transient elastography (TE) is a noninvasive tool
that measures liver stiffness (LS) correlating to liver fibrosis stage. While LS also shows
potential in the prediction of EVs, its role is still under debate. Moreover, the LS-spleen
size-to-platelet ratio score (LSPS), which is a combination of three simple examination
methods (LS, spleen size and platelet count) has been established to accurately predict EVs
in patients with cirrhosis. And recent Baveno VI recommended the combination of transient
elastography and platelet count for ruling out HEVs in patients with chronic liver disease.
Although there is a correlation between these non-invasive tools and the presence of EVS or
HEVs, the optimal cut-offs and their validities vary in the different studies with different
etiologies. In addition, the qualities of EVs assessment have not been provided in these
studies. Therefore, investigators design this cross-sectional study to assess these
non-invasive tests in predicting the presence of EVs in patients with cirrhosis. This could
prevent unnecessary endoscopy with related complications and costs. And the results of
noninvasive tests will be compared with endoscopy (ie, the gold standard for diagnosing EVs).
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