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正常肝细胞在对接受照射/部分切除的冈恩大鼠肝脏进行再填充后可纠正血清胆红素水平。

Normal hepatocytes correct serum bilirubin after repopulation of Gunn rat liver subjected to irradiation/partial resection.

作者信息

Guha Chandan, Parashar Bhupesh, Deb Niloy J, Garg Madhur, Gorla Giridhar R, Singh Anupam, Roy-Chowdhury Namita, Vikram Bhadrasain, Roy-Chowdhury Jayanta

机构信息

Departments of Radiation Oncology, Medicine, Pathology, and Molecular Genetics and The Marion Bessin Liver Research Center, Albert Einstein College of Medicine, Bronx, NY.

出版信息

Hepatology. 2002 Aug;36(2):354-62. doi: 10.1053/jhep.2002.34516.

Abstract

The treatment of inherited metabolic liver diseases by hepatocyte transplantation (HT) would be greatly facilitated if the transplanted normal hepatocytes could be induced to proliferate preferentially over the host liver cells. We hypothesized that preparative hepatic irradiation (HIR) should inhibit host hepatocyte proliferation in response to partial hepatectomy (PH). Normal nonirradiated hepatocytes transplanted in this setting should have a selective growth advantage over the host liver cells and should progressively repopulate the liver. To test this hypothesis, we transplanted 5 million hepatocytes from normal Wistar-Roman High Avoidance (RHA) rats into the livers of congeneic bilirubin-uridine 5'-diphosphoglucuronate glucuronosyltransferase (UGT1A1)-deficient jaundiced Gunn rats by intrasplenic injection after one of the following treatments: (1) 68% PH, (2) HIR (50 Gy), or (3) HIR + PH. In rats receiving either PH or HIR alone before HT, serum bilirubin concentrations declined by 25% to 30% in 28 weeks. In contrast, serum bilirubin levels were normalized completely in rats receiving HIR + PH before HT. Massive repopulation of the Gunn rat liver by the UGT1A1-positive Wistar-RHA hepatocytes was shown by UGT1A1 enzyme assay, immunoblot analysis, and immunohistochemical staining of the recipient liver. High-performance liquid chromatography analysis of the bile collected from Gunn rats 5 months after PH, HIR, and HT showed normalization of the pigment profile, with bilirubin diglucuronide and monoglucuronide as the predominant pigments. In conclusion, a preparative regimen of HIR + PH results in massive repopulation of the liver with functionally normal transplanted hepatocytes, resulting in complete correction of a metabolic deficiency. Noninvasive strategies to replace PH for providing proliferative stimuli to the transplanted cells should make this regimen valuable in augmenting the effects of HT for the treatment of liver diseases.

摘要

如果移植的正常肝细胞能够被诱导优先于宿主肝细胞增殖,那么肝细胞移植(HT)对遗传性代谢性肝病的治疗将会得到极大的促进。我们推测,术前肝脏照射(HIR)应能抑制宿主肝细胞在部分肝切除(PH)后的增殖。在此情况下移植的正常未照射肝细胞应比宿主肝细胞具有选择性生长优势,并应逐渐重新填充肝脏。为了验证这一假设,我们在以下处理之一后,通过脾内注射将500万个来自正常Wistar-Roman高回避(RHA)大鼠的肝细胞移植到同基因胆红素-尿苷5'-二磷酸葡萄糖醛酸转移酶(UGT1A1)缺陷的黄疸Gunn大鼠的肝脏中:(1)68% PH,(2)HIR(50 Gy),或(3)HIR + PH。在HT前单独接受PH或HIR的大鼠中,血清胆红素浓度在28周内下降了25%至30%。相比之下,在HT前接受HIR + PH的大鼠中,血清胆红素水平完全恢复正常。通过UGT1A1酶分析、免疫印迹分析和受体肝脏的免疫组织化学染色显示,UGT1A1阳性的Wistar-RHA肝细胞大量重新填充了Gunn大鼠肝脏。对接受PH、HIR和HT 5个月后的Gunn大鼠胆汁进行的高效液相色谱分析显示,色素谱正常化,以胆红素二葡萄糖醛酸酯和单葡萄糖醛酸酯为主要色素。总之,HIR + PH的预处理方案导致功能正常的移植肝细胞大量重新填充肝脏,从而完全纠正代谢缺陷。用于替代PH以向移植细胞提供增殖刺激的非侵入性策略应使该方案在增强HT治疗肝病的效果方面具有价值。

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