经颈静脉肝内门体分流术矫正门静脉高压症后外周血浆肽组成分的变化

Giulia Ilaria Bagarolo, Shruti Bhargava, Robert Schierwagen, Wenyi Gu, Vera Jankowski, Josefin Soppert, Emona Barzakova, Federica Cascone, Olaf Tyc, Christiane Kuhl, Heidi Noels, Jonel Trebicka, Joachim Jankowski
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摘要

晚期慢性肝病(CLD)患者,尤其是肝硬化患者会出现门静脉高压症,并伴有消化道出血和腹水等并发症,死亡率很高。经颈静脉肝内门体分流术(TIPS)是治疗门静脉高压症的一种方法,其目的是通过为胃肠道到肝静脉的血液建立一条人工通道来降低门静脉压力。本研究重点研究门静脉高压症患者血浆样本在 TIPS 干预前后的分子组成差异,以确定影响肠道-肝脏交叉对话的潜在介质并描述其特征。在 TIPS 治疗前后,从外周静脉采集了 23 名门静脉高压症晚期 CLD 患者的血浆,并采用成熟的非靶向色谱-质谱(LC-MS)方法进行了分析。经鉴定,TIPS 治疗后,Sialomucin 核心蛋白 24(CD164)(160-180)、meckelin(99-118)、组蛋白-赖氨酸 N-甲基转移酶(MLL3)(3019-3045)和瞬时受体电位阳离子通道 V 亚家族成员 5(TRPV5)(614-630)被下调。此外,3-羧基-4-甲基-5-丙基-2-呋喃丙酸(CMPF)、尿酸、多巴胺、高精氨酸、白脯氨酸和 5-甲基尿苷等代谢物在 TIPS 治疗后显著减少,而一种尚未确定的低分子量代谢物在治疗后增加。总之,这些物质是慢性肝病患者门静脉高压症的新型潜在生物标志物,具有参与调节病理肠肝交叉对话的机理线索。
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Alterations of the peptidomic composition of peripheral plasma after portal hypertension correction by transjugular intrahepatic portosystemic shunt
Portal hypertension develops in patients with advanced chronic liver diseases (CLD), especially cirrhosis and is associated with complications, such as gastrointestinal bleeding and ascites resulting in high mortality. The transjugular intrahepatic portosystemic shunt (TIPS) is a treatment option for portal hypertension, aiming to decrease portal venous pressure by establishing an artificial passage for blood from the gastrointestinal tract to the liver vein. This study focuses on the differences in the molecular composition of plasma samples from patients with portal hypertension before and after TIPS intervention to identify and characterise potential mediators influencing gut-liver cross-talk. The plasma of 23 patients displaying advanced CLD with portal hypertension was collected from peripheral veins before and after TIPS treatment and analysed using a well-established non-targeted chromatography-mass spectrometric (LC-MS) approach. Sialomucin core protein 24(CD164)(160–180), meckelin(99-118), Histone-lysine N-methyltransferase(MLL3)(3019-3045) and transient receptor potential cation channel subfamily V member 5(TRPV5)(614-630) were identified to be downregulated after the TIPS treatment. In addition, the metabolites 3-carboxy-4-methyl-5-propyl-2-furanpropionic acid (CMPF), uric acid, dopamine, homoarginine, leucylproline and 5-methyluridine were significantly decreased after TIPS, whereas one yet unidentified low molecular-weight metabolite showed an increase after the medical procedure. In conclusion, these substances are novel potential biomarkers for portal hypertension in patients with CLD, with mechanistic clues of involvement in regulating pathological gut-liver cross-talk.
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