世界胃肠病学杂志(英文版)
世界胃腸病學雜誌(英文版)
세계위장병학잡지(영문판)
WORLD JOURNAL OF GASTROENTEROLOGY
2008年
24期
3841-3848
,共8页
Chronic liver disease%Portal hypertension,Portosystemic shunts%Per-rectal portal scintigraphy%Angioscintigraphy
AIM: To explore portal hypertension and portosystemic shunts and to stage chronic liver disease (CLD)based on the pathophysiology of portal hemodynamics.METHODS: Per-rectal portal scintigraphy (PRPS) was performed on 312 patients with CLD and liver angioscintigraphy (LAS) on 231 of them.The control group included 25 healthy subjects.We developed a new model of PRPS interpretation by introducing two new parameters,the liver transit time (LIT) and the circulation time between right heart and liver (RHLT).LTT for each lobe was used to evaluate the early portal hypertension.RHLT is useful in cirrhosis to detect liver areas missing portal inflow.We calculated the classical per-rectal portal shunt index (PRSI) at PRPS and the hepatic perfusion index (HPI) at LAS.RESULTS: The normal LTT value was 24 ±1 s.Abnormal LTT had PPV = 100% for CLD.Twenty-seven noncirrhotic patients had L-IT increased up to 35 s (median 27 s).RHLT (42 ±1 s) was not related to liver disease.Cirrhosis could be excluded in all patients with PRSI< 5% (P < 0.01).PRSI > 30% had PPV = 100% for cirrhosis.Based on PRPS and LAS we propose the classification of CLD in 5 hemodynamic stages.Stage 0 is normal (LIT = 24 s,PRSI < 5%).In stage 1,LIT is increased,while PRSI remains normal.In stage 2,LIT is decreased between 16 s and 23 s,whereas PRSI is increased between 5% and 10%.In stage 3,PRSI is increased to 10%-30%,and LTT becomes undetectable by PRPS due to the portosystemic shunts.Stage 4 includes the patients with PRSI > 30%.RHLT and HPI were used to subtype stage 4.In our study stage 0 had NPV = 100% for CLD,stage 1 had PPV = 100% for non-cirrhotic CLD,stages 2 and 3 represented the transition from chronic hepatitis to cirrhosis,stage 4 had PPV = 100% for cirrhosis.CONCLUSION: LTT allows the detection of early portal hypertension and of opening of transhepatic shunts.PRSI is useful in CLD with extrahepatic portosystemic shunts.Our hemodynamic model stages the evolution of portal hypertension and portosystemic shunts.It may be of use in the selection of patients for interferon therapy.
