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Cholangiocytes and blood supply.

机译:胆管细胞和血液供应。

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The microvascular supply of the biliary tree, the peribiliary plexus (PBP), stems from the hepatic artery branches and flows into the hepatic sinusoids. A detailed three-dimensional study of the PBP has been performed by using the Scanning Electron Microscopy vascular corrosion casts (SEMvcc) technique. Considering that the PBP plays a fundamental role in supporting the secretory and absorptive functions of the biliary epithelium, their organization in either normalcy and pathology is explored. The normal liver shows the PBP arranged around extra- and intrahepatic biliary tree. In the small portal tract PBP was characterized by a single layer of capillaries which progressively continued with the extrahepatic PBP where it showed a more complex vascular network. After common duct ligation (BDL), progressive modifications of bile duct and PBP proliferation are observed. The PBP presents a three-dimensional network arranged around many bile ducts and appears as bundles of vessels, composed by capillaries of homogeneous diameter with a typical round mesh structure. The PBP network is easily distinguishable from the sinusoidal network which appears normal. Considering the enormous extension of the PBP during BDL, the possible role played by the Vascular Endothelial Growth Factor (VEGF) is evaluated. VEGF-A, VEGF-C and their related receptors appeared highly immunopositive in proliferating cholangiocytes of BDL rats. The administration of anti-VEGF-A or anti-VEGF-C antibodies to BDL rats as well as hepatic artery ligation induced a reduced bile duct mass. The administration of rVEGF-A to BDL hepatic artery ligated rats prevented the decrease of cholangiocyte proliferation and VEGF-A expression as compared to BDL control rats. These data suggest the role of arterial blood supply of the biliary tree in conditions of cholangiocyte proliferation, such as it occurs during chronic cholestasis. On the other hand, the role played by VEGF as a tool of cross-talk between cholangiocytes and PBP endothelial cells suggests that manipulation of VEGF release and function could represent a therapeutic strategy for human pathological conditions characterized by damage of hepatic artery or the biliary tree.
机译:胆道树的微血管供应,即胆道丛(PBP),源于肝动脉分支,并流入肝窦。通过使用扫描电子显微镜血管腐蚀铸件(SEMvcc)技术,对PBP进行了详细的三维研究。考虑到PBP在支持胆管上皮的分泌和吸收功能中起着基本作用,因此探讨了PBP在正常性和病理性方面的组织。正常肝脏显示PBP排列在肝外和肝内胆管树周围。在小门脉中,PBP的特征是单层毛细血管,随着肝外PBP的进行逐渐发展,并显示出更为复杂的血管网络。胆总管结扎(BDL)后,观察到胆管和PBP增殖的逐步改变。 PBP提供了围绕许多胆管排列的三维网络,并显示为血管束,由直径均一且具有典型圆形网状结构的毛细管组成。 PBP网络很容易与看起来正常的正弦网络区分开。考虑到BDL期间PBP的巨大扩展,评估了血管内皮生长因子(VEGF)可能发挥的作用。 VEGF-A,VEGF-C及其相关受体在BDL大鼠的增生胆管细胞中表现出高度免疫阳性。向BDL大鼠施用抗VEGF-A或抗VEGF-C抗体以及肝动脉结扎可降低胆管质量。与BDL对照大鼠相比,向BDL肝动脉结扎大鼠施用rVEGF-A可以防止胆管细胞增殖和VEGF-A表达的降低。这些数据表明胆汁树的动脉血液供应在胆管细胞增殖的情况下的作用,例如在慢性胆汁淤积期间发生的情况。另一方面,VEGF作为胆管细胞与PBP内皮细胞之间的串扰工具发挥的作用表明,操纵VEGF的释放和功能可能代表了以肝动脉或胆道树受损为特征的人类病理疾病的治疗策略。 。

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