酒精使用障碍且临床血清锌水平低的患者的肠道-免疫-肝脏轴

The gut-immune-liver axis in patients with alcohol use disorder and clinically low serum zinc levels.

作者信息

Thakurdesai Aishwarya, Jha Suman K, Erinkitola Iyabo, Said Aula, Joshi Thwisha, Schwandt Melanie L, Parajuli Dipendra, Singal Ashwani K, Kong Maiying, Cave Matthew C, Vatsalya Vatsalya

机构信息

Division of Gastroenterology, Hepatology, and Nutrition, Department of Medicine, Clinical Laboratory for the Intervention Development of AUD and Organ-Severity, University of Louisville, Louisville, Kentucky, USA.

Clinical Laboratory for the Intervention Development of AUD and Organ-Severity, University of Louisville, Louisville, Kentucky, USA.

出版信息

Alcohol Clin Exp Res (Hoboken). 2024 Sep;48(9):1740-1752. doi: 10.1111/acer.15408. Epub 2024 Aug 2.

DOI:10.1111/acer.15408

PMID:39095327

Abstract

BACKGROUND

Alcohol use disorder (AUD) with chronic and heavy alcohol consumption causes alcohol-associated liver disease (ALD). Early-stage ALD exhibits dyshomeostasis of zinc. We investigated the role of zinc deficiency in gut-barrier dysfunction, proinflammatory response, hepatocyte injury, and death, as well as potential sex differences in AUD patients.

METHODS

Thirty-nine male and female AUD patients were grouped by normal [≥71 μg/dL (Group 1, number (n) = 26)] and low [<71 μg/dL (Group 2, n = 13)] serum zinc levels. Demographics, alcohol intake markers [Lifetime Drinking History (LTDH), heavy drinking days in the past 90-days (HDD90), total drinks in the past 90-days (TD90), number of drinking days in the past 90-days (NDD90), average drinks per day in the past 90 days (AvgDPD90)] were collected. Blood samples were tested for complete blood count (CBC), comprehensive metabolic panel (CMP), coagulation markers, gut-barrier dysfunction markers, cytokines, and hepatocyte death markers.

RESULTS

Group 2 females exhibited lower LTDH than Group 2 males (p = 0.028), but higher recent drinking. Aspartate transaminase: alanine transaminase (AST:ALT) ratio was higher (p = 0.049) in Group 2 males compared to Group 1 males. Overall, Group 2 showed threefold higher interleukin 8 (IL-8) levels than Group 1 (p = 0.92); these were sevenfold higher in Group 2 females than Group 1 females. Group 2 females also had higher K18M65, but lower K18M30 than Group 1 females. Necrotic type of cell death (K18M65) was well-described only in Group 2 by the arrangement of lipopolysaccharide (LPS), soluble cluster of differentiation 14 (sCD14), and tumor necrosis factor alpha (TNF-α) (R = 0.633, p = 0.037).

CONCLUSION

Our findings demonstrated the role of the gut-immune-liver axis in describing hepatocyte injury and death in zinc-deficient AUD patients. These patients represented an arrangement of gut-barrier dysfunction and an exacerbated immune response. Shift in the cell-death mechanism from apoptosis in zinc-replete females to necrosis in zinc-deficient females suggests a subclinical to clinical transition of ALD associated with zinc status.

摘要

背景

慢性大量饮酒所致的酒精使用障碍（AUD）会引发酒精性肝病（ALD）。ALD早期表现为锌稳态失衡。我们研究了锌缺乏在AUD患者肠道屏障功能障碍、促炎反应、肝细胞损伤和死亡中的作用，以及潜在的性别差异。

方法

39例AUD患者按血清锌水平正常[≥71μg/dL（第1组，n = 26）]和低[<71μg/dL（第2组，n = 13）]分为两组。收集人口统计学数据、酒精摄入标志物[终生饮酒史（LTDH）、过去90天内的重度饮酒天数（HDD90）、过去90天内的饮酒总量（TD90）、过去90天内的饮酒天数（NDD90）、过去90天内的平均每日饮酒量（AvgDPD90）]。检测血样的全血细胞计数（CBC）、综合代谢指标（CMP）、凝血标志物、肠道屏障功能障碍标志物、细胞因子和肝细胞死亡标志物。

结果

第2组女性的LTDH低于第2组男性（p = 0.028），但近期饮酒量更高。与第1组男性相比，第2组男性的天冬氨酸转氨酶：丙氨酸转氨酶（AST:ALT）比值更高（p = 0.049）。总体而言，第2组的白细胞介素8（IL-8）水平比第1组高3倍（p = 0.92）；第2组女性的该水平比第1组女性高7倍。第2组女性的K18M65也高于第1组女性，但K18M30低于第1组女性。仅在第2组中，通过脂多糖（LPS）、可溶性分化簇14（sCD14）和肿瘤坏死因子α（TNF-α）的排列很好地描述了坏死型细胞死亡（K18M65）（R = 0.633，p = 0.037）。