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转化生长因子 β 信号转导和祖细胞扩增在肝脏再生中的作用。

Role of transforming growth factor beta signaling and expansion of progenitor cells in regenerating liver.

机构信息

Cancer Genetics, Digestive Diseases, and Developmental Molecular Biology, Department of Surgery, Lombardi Comprehensive Cancer Center, Georgetown University, Washington, DC, USA.

出版信息

Hepatology. 2010 Apr;51(4):1373-82. doi: 10.1002/hep.23449.

Abstract

UNLABELLED

Adult hepatic progenitor cells are activated during regeneration when hepatocytes and bile duct epithelium are damaged or unable to proliferate. On the basis of its role as a tumor suppressor and in the potential malignant transformation of stem cells in hepatocellular carcinoma, we investigated the role of key transforming growth factor beta (TGF-beta) signaling components, including the Smad3 adaptor protein beta2-Spectrin (beta2SP), in liver regeneration. We demonstrate a streaming hepatocyte-specific dedifferentiation process in regenerating adult human liver less than 6 weeks following living donor transplantation. We then demonstrate a spatial and temporal expansion of TGF-beta signaling components, especially beta2SP, from the periportal to the pericentral zone as regeneration nears termination via immunohistochemical analysis. This expansion is associated with an expanded remaining pool of octamer 3/4 (Oct3/4)-positive progenitor cells localized to the portal tract in adult human liver from more than 6 weeks posttransplant. Furthermore, disruption of TGF-beta signaling as in the beta2SP (beta2SP+/-) knockout mouse demonstrated a striking 2 to 4-fold (P < 0.05) expanded population of Oct3/4-positive cells with activated Wnt signaling occupying an alpha-fetoprotein (AFP)+/cytokeratin-19 (CK-19)-positive progenitor cell niche following two-thirds partial hepatectomy.

CONCLUSION

TGF-beta signaling, particularly beta2SP, plays a critical role in hepatocyte proliferation and transitional phenotype and its loss is associated with activation of hepatic progenitor cells secondary to delayed mitogenesis and activated Wnt signaling.

摘要

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当肝细胞和胆管上皮受损或无法增殖时,成年肝祖细胞在再生过程中被激活。基于其作为肿瘤抑制因子的作用,以及在肝癌干细胞的潜在恶性转化中,我们研究了关键转化生长因子β(TGF-β)信号成分的作用,包括 Smad3 衔接蛋白β2- spectrin(β2SP),在肝再生中的作用。我们在活体供体移植后不到 6 周的再生成人肝中证明了一种流动的肝细胞特异性去分化过程。然后,我们通过免疫组织化学分析证明,随着再生接近终止,TGF-β信号成分,特别是β2SP,从门脉周围区扩展到中央区。这种扩展与 Octamer 3/4(Oct3/4)阳性祖细胞的剩余池的扩大有关,这些祖细胞定位于成人肝移植后 6 周以上的门脉区。此外,TGF-β信号的破坏,如在β2SP(β2SP+/-)敲除小鼠中,在三分之二的部分肝切除术后,激活的 Wnt 信号导致 Oct3/4 阳性细胞的数量显著增加 2 到 4 倍(P<0.05),占据了α胎蛋白(AFP)+/细胞角蛋白 19(CK-19)阳性祖细胞龛。

结论

TGF-β信号,特别是β2SP,在肝细胞增殖和过渡表型中起着关键作用,其缺失与肝祖细胞的激活有关,这是由于有丝分裂延迟和激活的 Wnt 信号导致的。

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