Institute of Pathology, Julius-Maximilians-University of Würzburg, Würzburg, Germany.
Comprehensive Cancer Center Mainfranke, Julius-Maximilians-University of Würzburg, Würzburg, Germany.
Autophagy. 2022 Dec;18(12):2880-2893. doi: 10.1080/15548627.2022.2052588. Epub 2022 Mar 28.
The notion that macroautophagy/autophagy is a potentially attractive therapeutic target for a variety of diseases, including cancer, largely stems from pre-clinical mouse studies. Most of these examine the effects of irreversible and organ confined autophagy deletion using site specific -loxP recombination of the essential autophagy regulating genes or . Model systems with the ability to impair autophagy systemically and reversibly at all disease stages would allow a more realistic approach to evaluate the consequences of authophagy inhibition as a therapeutic concept and its potential side effects. Here, we present shRNA transgenic mice that via doxycycline (DOX) regulable expression of a highly efficient miR30-E-based shRNA enabled knockdown of simultaneously in the majority of organs, with the brain and spleen being noteable exceptions. Induced animals deteriorated rapidly and experienced profound destruction of the exocrine pancreas, severe hypoglycemia and depletion of hepatic glycogen storages. Cessation of DOX application restored apparent health, glucose homeostasis and pancreatic integrity. In a similar knockdown model we neither observed loss of pancreatic integrity nor diminished survival after DOX treatment, but identified histological changes consistent with steatohepatitis and hepatic fibrosis in the recovery period after termination of DOX. Regulable -shRNA mice are valuable tools that will enable further studies on the role of autophagy impairment at various disease stages and thereby help to evaluate the consequences of acute autophagy inhibition as a therapeutic concept. ACTB: actin, beta; AMY: amylase complex; ATG4B: autophagy related 4B, cysteine peptidase; ATG5: autophagy related 5; ATG7: autophagy related 7; Cag: CMV early enhancer/chicken promoter; : collagen, type I, alpha 1; Cre: cre recombinase; DOX: doxycycline; GCG: glucagon; GFP: green fluorescent protein; INS: insulin; LC3: microtubule-associated protein 1 light chain 3; miR30-E: optimized microRNA backbone; NAFLD: non-alcoholic fatty liver disease; NASH: non-alcoholic steatohepatitis; PNLIP: pancreatic lipase; rtTA: reverse tetracycline transactivator protein; SQSTM1/p62: sequestome 1; TRE: tetracycline responsive element.
自噬是一种潜在的有吸引力的治疗靶点,这一观点主要源于临床前的小鼠研究。这些研究大多采用特异性 -loxP 重组关键自噬调节基因或的方法,来研究不可逆的和器官特异性的自噬缺失对多种疾病(包括癌症)的影响。具有在所有疾病阶段系统地和可逆地损害自噬能力的模型系统,将允许更现实地评估自噬抑制作为一种治疗概念的后果及其潜在的副作用。在这里,我们提供了 shRNA 转基因小鼠,通过强力霉素(DOX)可调控的表达,一种高效的基于 miR30-E 的 shRNA,能够同时在大多数器官中敲低,大脑和脾脏是显著的例外。诱导的动物迅速恶化,并经历外分泌胰腺的严重破坏、严重的低血糖和肝糖原储存的消耗。停止 DOX 的应用恢复了明显的健康、葡萄糖稳态和胰腺完整性。在类似的 敲低模型中,我们既没有观察到胰腺完整性的丧失,也没有观察到 DOX 治疗后的存活率降低,但在 DOX 治疗结束后的恢复期间,我们发现了与脂肪性肝炎和肝纤维化一致的组织学变化。可调控的 -shRNA 小鼠是非常有价值的工具,它们将使我们能够进一步研究自噬损伤在不同疾病阶段的作用,并有助于评估急性自噬抑制作为一种治疗概念的后果。ACTB:肌动蛋白,β;AMY:淀粉酶复合物;ATG4B:自噬相关 4B,半胱氨酸肽酶;ATG5:自噬相关 5;ATG7:自噬相关 7;Cag:CMV 早期增强子/鸡 启动子;:胶原蛋白,类型 I,α1;Cre:cre 重组酶;DOX:强力霉素;GCG:胰高血糖素;GFP:绿色荧光蛋白;INS:胰岛素;LC3:微管相关蛋白 1 轻链 3;miR30-E:优化的 microRNA 骨架;NAFLD:非酒精性脂肪肝疾病;NASH:非酒精性脂肪性肝炎;PNLIP:胰腺脂肪酶;rtTA:逆转录酶四环素反式激活蛋白;SQSTM1/p62:自噬体 1;TRE:四环素反应元件。
