酒精性肝炎患者的肠上皮损伤再生胰岛衍生蛋白 3α 和三叶因子 3 的血液生物标志物持续升高。
Blood Biomarkers of Intestinal Epithelium Damage Regenerating Islet-derived Protein 3α and Trefoil Factor 3 Are Persistently Elevated in Patients with Alcoholic Hepatitis.
机构信息
School of Laboratory Medicine and Life Sciences, Wenzhou Medical University, Wenzhou, Zhejiang, China.
Department of Microbiology and Immunology, Indiana University School of Medicine, Indianapolis, Indiana, USA.
出版信息
Alcohol Clin Exp Res. 2021 Apr;45(4):720-731. doi: 10.1111/acer.14579. Epub 2021 Mar 11.
BACKGROUND
Heavy alcohol consumption disrupts gut epithelial integrity, leading to increased permeability of the gastrointestinal tract and subsequent translocation of microbes. Regenerating islet-derived protein 3α (REG3α) and Trefoil factor 3 (TFF3) are mainly secreted to the gut lumen by Paneth and Goblet cells, respectively, and are functionally linked to gut barrier integrity. Circulating levels of REG3α and TFF3 have been identified as biomarkers for gut damage in several human diseases. We examined whether plasma levels of REG3α and TFF3 were dysregulated and correlated with conventional markers of microbial translocation (MT) and pro-inflammatory mediators in heavy drinkers with and without alcoholic hepatitis (AH).
METHODS
Cross-sectional and longitudinal studies were performed to monitor plasma levels of REG3α and TFF3 in 79 AH patients, 66 heavy drinkers without liver disease (HDC), and 46 healthy controls (HC) at enrollment and at 6- and 12-month follow-ups. Spearman correlation was used to measure the relationships of REG3α and TFF3 levels with MT, disease severity, inflammation, and effects of abstinence from alcohol.
RESULTS
At enrollment, AH patients had significantly higher levels of REG3α and TFF3 than HDC and HC. The elevated REG3α levels were positively correlated with the 30-day fatality rate. Plasma levels of REG3α and TFF3 in AH patients differentially correlated with conventional MT markers (sCD14, sCD163, and LBP) and several highly up-regulated inflammatory cytokines/chemokines/growth factors. At follow-ups, although REG3α and TFF3 levels were decreased in AH patients with alcohol abstinence, they did not fully return to baseline levels.
CONCLUSIONS
Circulating levels of REG3α and TFF3 were highly elevated in AH patients and differentially correlated with AH disease severity, MT, and inflammation, thereby serving as potential biomarkers of MT and gut epithelial damage in AH patients.
背景
大量饮酒会破坏肠道上皮完整性,导致胃肠道通透性增加,随后微生物易位。再生胰岛衍生蛋白 3α(REG3α)和三叶因子 3(TFF3)主要由 Paneth 和 Goblet 细胞分别分泌到肠道腔中,其功能与肠道屏障完整性相关。在几种人类疾病中,REG3α 和 TFF3 的循环水平已被确定为肠道损伤的生物标志物。我们研究了大量饮酒者(包括有和没有酒精性肝炎[AH]的患者)的 REG3α 和 TFF3 血浆水平是否失调,并与微生物易位(MT)的常规标志物和促炎介质相关。
方法
进行了横断面和纵向研究,以监测 79 名 AH 患者、66 名无肝病的大量饮酒者(HDC)和 46 名健康对照者(HC)在入组时以及 6 个月和 12 个月随访时的 REG3α 和 TFF3 血浆水平。采用 Spearman 相关分析来测量 REG3α 和 TFF3 水平与 MT、疾病严重程度、炎症以及戒酒效果的关系。
结果
入组时,AH 患者的 REG3α 和 TFF3 水平明显高于 HDC 和 HC。升高的 REG3α 水平与 30 天病死率呈正相关。AH 患者的 REG3α 和 TFF3 血浆水平与常规 MT 标志物(sCD14、sCD163 和 LBP)以及几种高度上调的炎症细胞因子/趋化因子/生长因子呈不同相关性。在随访中,尽管 AH 患者在戒酒时 REG3α 和 TFF3 水平降低,但并未完全恢复到基线水平。
结论
AH 患者的循环 REG3α 和 TFF3 水平明显升高,与 AH 疾病严重程度、MT 和炎症呈不同相关性,因此可作为 AH 患者 MT 和肠道上皮损伤的潜在生物标志物。
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