Jiabing Cai scite author profile

Because of a critical shortage in suitable organs, many patients with terminal liver disease die each year before liver transplantation can be performed. Transplantation of isolated hepatocytes has been proposed for the temporary metabolic support of patients awaiting liver transplantation or spontaneous reversion of their liver disease. A major limitation of this form of therapy is the present inability to isolate an adequate number of transplantable hepatocytes. A highly differentiated cell line, NKNT-3, was generated by retroviral transfer in normal primary adult human hepatocytes of an immortalizing gene that can be subsequently and completely excised by Cre/Lox site-specific recombination. When transplanted into the spleen of rats under transient immunosuppression, reversibly immortalized NKNT-3 cells provided life-saving metabolic support during acute liver failure induced by 90% hepatectomy.

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Estimating reference evapotranspiration with the FAO Penman–Monteith equation using daily weather forecast messages

Cai

Liu

Lei

et al. 2007

Agricultural and Forest Meteorology

302

140

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Hepatocyte transplantation in rats with decompensated cirrhosis

et al. 2000

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Hepatocyte transplantation improves the survival of laboratory animals with experimentally induced acute liver failure and the physiological abnormalities associated with liver-based metabolic deficiencies. The role of hepatocyte transplantation in treating decompensated liver cirrhosis, however, has not been studied in depth. To address this issue, cirrhosis was induced using phenobarbital and carbon tetrachloride (CCL 4 ) and animals were studied only when evidence of liver failure did not improve when CCL 4 was held for 4 weeks. Animals received intrasplenic transplantation of syngeneic rat hepatocytes (G1); intraperitoneal transplantation of syngeneic rat hepatocytes (G2); intraperitoneal transplantation of a cellular homogenate of syngeneic rat hepatocytes (G3); intraperitoneal transplantation of syngeneic rat bone marrow cells (G4); or intrasplenic injection of Dulbecco's modified Eagle medium (DMEM) (G5). After transplantation, body weight and serum albumin levels deteriorated over time in all control (G2-G5) animals but did not deteriorate in animals receiving intrasplenic hepatocyte transplantation (G1) (P F .01). Prothrombin time (PT), total bilirubin, serum ammonia, and hepatic encephalopathy score were also significantly improved toward normal in animals receiving intrasplenic hepatocyte transplantation (P F .01). More importantly, survival was prolonged after a single infusion of hepatocytes and a second infusion prolonged survival from 15 to 128 days (P F .01). Thus, hepatocyte transplantation can improve liver function and prolong the survival of rats with irreversible, decompensated cirrhosis and may be useful in the treatment of cirrhosis in humans. (HEPATOLOGY 2000;31: 851-857.)

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Prolonged Survival of Porcine Hepatocytes in Cynomolgus Monkeys

et al. 2007

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Multi-scale evapotranspiration of summer maize and the controlling meteorological factors in north China

Zhang

Liu

et al. 2016

Agricultural and Forest Meteorology

162

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Jiabing Cai

Prevention of Acute Liver Failure in Rats with Reversibly Immortalized Human Hepatocytes

Estimating reference evapotranspiration with the FAO Penman–Monteith equation using daily weather forecast messages

Hepatocyte transplantation in rats with decompensated cirrhosis

Prolonged Survival of Porcine Hepatocytes in Cynomolgus Monkeys

Multi-scale evapotranspiration of summer maize and the controlling meteorological factors in north China

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