A simple experimental model of total hepatectomy, hepatic ischemia and extrahepatic portal obstruction in rats using splenic transposition

Omokawa, Susumu; Arai, Yoshinori; Saito, Hidetomo; Furuya, Tomoki; Sato, Tsutomu; Shirayama, Kimiyuki; Ito, Masanao; Asanuma, Yoshihiro; Koyama, Kenji

doi:10.1007/bf02470866

Cited by 9 publications

(8 citation statements)

References 12 publications

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“…A second model involves PSS induced by subcutaneous transposition of the spleen [11]. This model also has been reported to be easy to create [11,28]. Since portosystemic collaterals are formed within 3 weeks after subcutaneous transposition of the spleen in rats, it takes about 3 weeks to perform the experiment.…”

Section: Figmentioning

confidence: 98%

Pathophysiological Appraisal of a Rat Model of Total Hepatic Ischemia with an Extracorporeal Portosystemic Shunt

Suzuki

Sakaguchi

Mitsuoka

et al. 1998

Journal of Surgical Research

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Section: Figmentioning

confidence: 98%

Pathophysiological Appraisal of a Rat Model of Total Hepatic Ischemia with an Extracorporeal Portosystemic Shunt

Suzuki

Sakaguchi

Mitsuoka

et al. 1998

Journal of Surgical Research

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“…Total Hepatic Ischemia. To minimize splanchnic congestion during total hepatic ischemia, we performed subcutaneous transposition of the spleen with its scarified capsule to induce development of portosystemic collaterals between the spleen and the anterior abdominal wall, as described by Omokawa et al (20). Four weeks later, after the establishment of adequate portosystemic collaterals, the animals were subjected to total hepatic ischemia.…”

Section: Animals Male Wistar Rats Each Weighing About 200 Gmmentioning

confidence: 99%

Liver Injury Following Normothermic Ischemia in Steatotic Rat Liver

et al. 1994

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The influence of normothermic ischemia on steatotic liver was compared with that on healthy liver in rats. Steatotic liver was induced with 4 wk of a choline-deficient diet. We used a procedure of subcutaneous spleen transposition to develop portosystemic collaterals to avoid splanchnic stasis during total hepatic vascular occlusion. One-week survival rates after 30, 45, and 60 min of normothermic ischemia were 75%, 20% and 0% in the steatotic liver group and 100%, 90% and 70% in the control group, respectively. Significantly poor restoration of energy metabolism was observed in the steatotic liver group. After 1 hr of reflow following 45 and 60 min of ischemia, ATP was restored to 74% and 50%, respectively, of the preischemic level in healthy liver but to only 44% and 27% respectively, in steatotic liver. Microscopically, focal hemorrhage, disruption of the sinusoidal microvasculature and occasional spotty necrosis of hepatocytes were demonstrated after 1 hr of reflow following ischemia in steatotic liver, but no significant changes were evident in healthy liver. This microcirculatory alteration seems to be responsible for the loss of organ viability in steatotic liver. We suggest that steatotic liver is more vulnerable than healthy liver to normothermic ischemia in the rat.

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“…The studies about the potential effectiveness of the portosystemic shunt on hepatic I/R injury have focused mainly on normothermic conditions (3,(11)(12)(13)(14)(15). In this regard, the portosystemic shunt leads to increased survival (12,13), extended times of sustained ischemia (3,11), and reduced levels of plasma TNF after hepatic I/R in experimental models of total normothermic ischemia (3). However, few studies (16 -18) have reported on the benefits of the portosystemic shunt in cold ischemia associated with rat liver transplantation.…”

mentioning

confidence: 99%

Role of ischemic preconditioning and the portosystemic shunt in the prevention of liver and lung damage after rat liver transplantation1

Fernández¹,

Heredia²,

Peralta

et al. 2003

Transplantation

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A simple experimental model of total hepatectomy, hepatic ischemia and extrahepatic portal obstruction in rats using splenic transposition

Cited by 9 publications

References 12 publications

Pathophysiological Appraisal of a Rat Model of Total Hepatic Ischemia with an Extracorporeal Portosystemic Shunt

Pathophysiological Appraisal of a Rat Model of Total Hepatic Ischemia with an Extracorporeal Portosystemic Shunt

Liver Injury Following Normothermic Ischemia in Steatotic Rat Liver

Role of ischemic preconditioning and the portosystemic shunt in the prevention of liver and lung damage after rat liver transplantation1

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