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年轻的酗酒者在外周多形核细胞和单核细胞中存在免疫表型变化。

Young adult binge drinkers have immunophenotypic changes in peripheral polymorphonuclear cells and monocytes.

作者信息

Pérez-García Adolfo, Arroyo-Valerio América Guadalupe, Zaldivar-Fujigaki José Luis, Bustos-Esquivel Mayra A, Gastelum-Strozzi Alfonso, Padilla-Castañeda Miguel A, Reding-Bernal Arturo, Kershenobich David, Hernández-Ruiz Joselín

机构信息

a Laboratory of Liver, Pancreas and Motility, Experimental Medicine Unit , National Autonomous University of Mexico (UNAM) at General Hospital of Mexico "Dr. Eduardo Liceaga," Mexico City , Mexico.

b Experimental Surgery Service , General Hospital of Mexico "Dr. Eduardo Liceaga," Mexico City , Mexico.

出版信息

Am J Drug Alcohol Abuse. 2018;44(3):403-412. doi: 10.1080/00952990.2017.1316985. Epub 2017 May 8.

Abstract

BACKGROUND

High alcohol intake on weekends (binge drinking) is more frequent in young adults, who could undergo early liver damage. Alcohol-induced liver damage is characterized by polymorphonuclear cell (PMN) infiltration, which can be represented in the peripheral blood by altered trafficking and activation profiles.

OBJECTIVE

To evaluate the PMN trafficking and activation immunophenotypic profiles in people with a binge drinking pattern.

METHODS

People with binge drinking (n = 18, 8 females) or at low risk (n = 16, 13 females) based on their AUDIT and HEPCA scores were studied. Hematic biometry and liver enzyme tests were conducted. Peripheral blood leukocytes were stained for CCR5, CCR4, and CXCR4 (trafficking) and CD69 and CD127 (activation). PMNs and monocytes were analyzed by FACS. The data were analyzed using the T-test and Mann-Whitney's U-test for contrasts and principal component and Fuzzy C means analyses for clustering, with p < 0.05 considered significant.

RESULTS

Compared to the low-risk group, the binge group showed higher CCR5 expression on PMNs, decreases in the CD69 percentage and positive PMNs per microliter, and decreased CXCR4 expression on monocytes. Six immunophenotypical clusters were identified, all of which were distributed following the CCR5 and CXCR4 main vectors.

CONCLUSION

Young adult binge drinkers have differential PMN trafficking and activation immunophenotypes, which could be related to the initial onset of alcoholic liver disease and a systemic inflammatory state in response to their alcohol consumption pattern. These findings could lead to the future development of an early diagnostic tool.

摘要

背景

周末大量饮酒(暴饮)在年轻人中更为常见,他们可能会早期肝脏受损。酒精性肝损伤的特征是多形核细胞(PMN)浸润,这在外周血中可通过改变的运输和激活谱表现出来。

目的

评估暴饮模式人群中PMN的运输和激活免疫表型谱。

方法

根据酒精使用障碍识别测试(AUDIT)和肝酶谱分析(HEPCA)评分,对暴饮人群(n = 18,8名女性)或低风险人群(n = 16,13名女性)进行研究。进行血液生物测定和肝酶测试。外周血白细胞用CCR5、CCR4和CXCR4(运输)以及CD69和CD127(激活)进行染色。通过流式细胞术分析PMN和单核细胞。使用T检验和曼-惠特尼U检验进行对比分析,使用主成分分析和模糊C均值分析进行聚类分析,p < 0.05被认为具有统计学意义。

结果

与低风险组相比,暴饮组PMN上CCR5表达更高,每微升CD69百分比和阳性PMN减少,单核细胞上CXCR4表达降低。识别出六个免疫表型簇,所有这些簇均沿CCR5和CXCR4主要向量分布。

结论

年轻的暴饮者具有不同的PMN运输和激活免疫表型,这可能与酒精性肝病的初始发病以及对其饮酒模式的全身炎症状态有关。这些发现可能会导致未来早期诊断工具的开发。

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