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成体海鳗通过改变胆汁盐组成和肾脏排泄来耐受胆道闭锁。

Adult sea lamprey tolerates biliary atresia by altering bile salt composition and renal excretion.

机构信息

Department of Internal Medicine and Liver Center, Yale University School of Medicine, New Haven, CT; Mount Desert Island Biological Laboratory, Salisbury Cove, ME, USA.

出版信息

Hepatology. 2013 Jun;57(6):2418-26. doi: 10.1002/hep.26161.

Abstract

The sea lamprey (Petromyzon marinus) is a genetically programmed animal model for biliary atresia, as it loses its bile ducts and gallbladder during metamorphosis. However, in contrast to patients with biliary atresia or other forms of cholestasis who develop progressive disease, the postmetamorphosis lampreys grow normally to adult size. To understand how the adult lamprey thrives without the ability to secrete bile, we examined bile salt homeostasis in larval and adult lampreys. Adult livers were severely cholestatic, with levels of bile salts >1 mM, but no evidence of necrosis, fibrosis, or inflammation. Interestingly, both larvae and adults had normal plasma levels (∼10 μM) of bile salts. In larvae, petromyzonol sulfate (PZS) was the predominant bile salt, whereas the major bile salts in adult liver were sulfated C27 bile alcohols. Cytotoxicity assays revealed that PZS was highly toxic. Pharmacokinetic studies in free-swimming adults revealed that ∼35% of intravenously injected bromosulfophthalein (BSP) was eliminated over a 72-hour period. Collection of urine and feces demonstrated that both endogenous and exogenous organic anions, including biliverdin, bile salts, and BSP, were predominantly excreted by way of the kidney, with minor amounts also detected in feces. Gene expression analysis detected marked up-regulation of orthologs of known organic anion and bile salt transporters in the kidney, with lesser effects in the intestine and gills in adults compared to larvae. These findings indicate that adult lampreys tolerate cholestasis by altering hepatic bile salt composition, while maintaining normal plasma bile salt levels predominantly through renal excretion of bile products. Therefore, we conclude that strategies to accelerate renal excretion of bile salt and other toxins should be beneficial for patients with cholestasis. (HEPATOLOGY 2013;57:2418-2426).

摘要

海七鳃鳗(Petromyzon marinus)是一种具有遗传编程的先天性胆道闭锁动物模型,因为它在变态过程中会失去胆管和胆囊。然而,与患有先天性胆道闭锁或其他形式的胆汁淤积症的患者不同,这些患者的疾病会逐渐发展,变态后的七鳃鳗会正常生长至成年体型。为了了解没有分泌胆汁能力的成年七鳃鳗是如何茁壮成长的,我们研究了幼体和成年七鳃鳗的胆汁盐动态平衡。成年七鳃鳗的肝脏严重胆汁淤积,胆汁盐水平>1mM,但没有坏死、纤维化或炎症的证据。有趣的是,幼体和成年七鳃鳗的血浆胆汁盐水平都正常(∼10μM)。在幼体中,主要的胆汁盐是 petromyzonol 硫酸盐(PZS),而成年七鳃鳗肝脏中的主要胆汁盐是硫酸化 C27 胆汁醇。细胞毒性测定表明 PZS 具有高度毒性。在自由游动的成年七鳃鳗中进行的药代动力学研究表明,静脉注射的溴磺酞(BSP)约有 35%在 72 小时内被消除。尿液和粪便的收集表明,内源性和外源性有机阴离子,包括胆红素、胆汁盐和 BSP,主要通过肾脏排泄,粪便中也检测到少量。基因表达分析发现,在成年七鳃鳗的肾脏中,已知的有机阴离子和胆汁盐转运蛋白的同源物明显上调,而在幼体中,肠道和鳃中的效应较小。这些发现表明,成年七鳃鳗通过改变肝脏胆汁盐组成来耐受胆汁淤积,同时通过肾脏主要排泄胆汁产物来维持正常的血浆胆汁盐水平。因此,我们得出结论,加速胆汁盐和其他毒素的肾脏排泄的策略应该对胆汁淤积症患者有益。(HEPATOLOGY 2013;57:2418-2426)。

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