Department of Pathology, The University of Texas Medical Branch, Galveston, Texas.
Department of Internal Medicine, The University of Texas Medical Branch, Galveston, Texas.
Am J Physiol Gastrointest Liver Physiol. 2022 Mar 1;322(3):G327-G345. doi: 10.1152/ajpgi.00263.2021. Epub 2022 Jan 5.
Alcoholic chronic pancreatitis (ACP) is a fibroinflammatory disease of the pancreas. However, metabolic basis of ACP is not clearly understood. In this study, we evaluated differential pancreatic injury in hepatic alcohol dehydrogenase-deficient (ADH) deer mice fed chronic ethanol (EtOH), chronic plus binge EtOH, and chronic plus binge EtOH and fatty acid ethyl esters (FAEEs, nonoxidative metabolites of EtOH) to understand the metabolic basis of ACP. Hepatic ADH and ADH normal (ADH) deer mice were fed Lieber-DeCarli liquid diet containing 3% (wt/vol) EtOH for 3 mo. One week before the euthanization, chronic EtOH-fed mice were further administered with an oral gavage of binge EtOH with/without FAEEs. Blood alcohol concentration (BAC), pancreatic injury, and inflammatory markers were measured. Pancreatic morphology, ultrastructural changes, and endoplasmic reticulum (ER)/oxidative stress were examined using H&E staining, electron microscopy, immunostaining, and/or Western blot, respectively. Overall, BAC was substantially increased in chronic EtOH-fed groups of ADH versus ADH deer mice. A significant change in pancreatic acinar cell morphology, with mild to moderate fibrosis and ultrastructural changes evident by dilatations and disruption of ER cisternae, ER/oxidative stress along with increased levels of inflammatory markers were observed in the pancreas of chronic EtOH-fed groups of ADH versus ADH deer mice. Furthermore, chronic plus binge EtOH and FAEEs exposure elevated BAC, enhanced ER/oxidative stress, and exacerbated chronic EtOH-induced pancreatic injury in ADH deer mice suggesting a role of increased body burden of EtOH and its metabolism under reduced hepatic ADH in initiation and progression of ACP. We established a chronic EtOH feeding model of hepatic alcohol dehydrogenase-deficient (ADH) deer mice, which mimics several fibroinflammatory features of human alcoholic chronic pancreatitis (ACP). The fibroinflammatory and morphological features exacerbated by chronic plus binge EtOH and FAEEs exposure provide a strong case for metabolic basis of ACP. Most importantly, several pathological and molecular targets identified in this study provide a much broader understanding of the mechanism and avenues to develop therapeutics for ACP.
酒精性慢性胰腺炎 (ACP) 是一种胰腺的纤维炎症性疾病。然而,ACP 的代谢基础尚不清楚。在这项研究中,我们评估了慢性乙醇 (EtOH)、慢性加 binge EtOH 和慢性加 binge EtOH 和脂肪酸乙酯 (FAEEs,EtOH 的非氧化代谢物) 喂养的肝乙醇脱氢酶缺乏 (ADH) 鹿鼠的胰腺损伤差异,以了解 ACP 的代谢基础。肝 ADH 和 ADH 正常 (ADH) 的鹿鼠喂食 Lieber-DeCarli 液体饮食,其中含有 3%(wt/vol)EtOH,持续 3 个月。在安乐死前一周,慢性 EtOH 喂养的小鼠进一步接受口服 binge EtOH 灌胃,同时或不给予 FAEEs。测量血醇浓度 (BAC)、胰腺损伤和炎症标志物。使用 H&E 染色、电子显微镜、免疫染色和/或 Western blot 分别检查胰腺形态、超微结构变化和内质网 (ER)/氧化应激。总的来说,慢性 EtOH 喂养的 ADH 组的 BAC 明显高于 ADH 鹿鼠。慢性 EtOH 喂养的 ADH 组的胰腺腺泡细胞形态发生显著变化,轻度至中度纤维化,电子显微镜下可见内质网腔扩张和破坏,ER/氧化应激以及炎症标志物水平升高。此外,慢性加 binge EtOH 和 FAEEs 暴露增加了 BAC,增强了 ER/氧化应激,并加重了 ADH 鹿鼠慢性 EtOH 诱导的胰腺损伤,表明在肝 ADH 减少的情况下,体内 EtOH 负荷增加及其代谢在 ACP 的起始和进展中起作用。我们建立了一种肝乙醇脱氢酶缺乏 (ADH) 鹿鼠的慢性 EtOH 喂养模型,该模型模拟了人类酒精性慢性胰腺炎 (ACP) 的几种纤维炎症特征。慢性加 binge EtOH 和 FAEEs 暴露加剧的纤维炎症和形态特征为 ACP 的代谢基础提供了有力证据。最重要的是,本研究中确定的几个病理和分子靶点为 ACP 的发病机制和治疗方法提供了更广泛的理解。
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