BACKGROUND & AIMS:Adult hepatocytes undergo cell cycle progression and proliferation in response to partial hepatectomy (PH). Transient lipid accumulation within hepatocytes preceding the peak proliferative phase is a characteristic feature of regenerating livers. However, the molecular mediators and mechanisms responsible for lipid accumulation in regenerating livers are not well understood. Adipose differentiation related protein (ADRP; Plin2) regulates hepatic triglyceride storage and Plin2-deficient (Plin2(-/-)) mice have significantly reduced triglyceride (TG) content in the liver. We sought to determine the functional significance of PLIN2 in liver regeneration in response to PH and toxic liver injury and examined whether absence of Plin2 expression modulates hepatocyte proliferation and liver regeneration. METHODS:We subjected wild-type (WT) and Plin2(-/-) mice to 70% PH or acute carbon tetrachloride (CCL4) treatment and examined the hepatic lipid content, the expression profile of lipid metabolism-related genes, the rate of cellular proliferation and the dynamics of liver regeneration in the treated animals. RESULTS:In response to PH, Plin2(-/-) mice showed decreased hepatic triglyceride accumulation and delayed cell cycle progression, which was associated with impaired liver regeneration. Fatty acid (FA) synthesis and lipid transfer gene expression profile were comparable between Plin2(-/-) and wild-type mice, while VLDL secretion rate was higher in the Plin2(-/-) mice. Downregulated β-oxidation and reduced cytosolic FA level in Plin2(-/-) mice may have contributed to the attenuation of the liver regeneration capacity in these animals. In parallel experiments, we also observed attenuated hepatic lipid accumulation and proliferation in response to CCl4-mediated acute toxic liver injury in Plin2(-/-) mice. CONCLUSIONS:We conclude that PLIN2-mediated lipid accumulation and utilization by the liver is important for efficient liver regeneration in response to PH and toxic liver injury.

译文

背景与目的:成人肝细胞响应部分肝切除术(PH)而经历细胞周期进程和增殖。在峰值增殖期之前,肝细胞内的瞬时脂质积累是再生肝脏的特征。然而,对于再生肝脏中脂质蓄积的分子介质和机制尚不十分了解。脂肪分化相关蛋白(ADRP; Plin2)调节肝甘油三酸酯的储存,Plin2缺乏(Plin2(-/-))小鼠的肝脏中甘油三酸酯(TG)含量显着降低。我们试图确定PLIN2在响应PH和中毒性肝损伤的肝再生中的功能意义,并检查Plin2表达的缺失是否调节肝细胞增殖和肝再生。
方法:我们对野生型(WT)和Plin2(-/-)小鼠进行70%PH或急性四氯化碳(CCL4)处理,并检查其肝脏脂质含量,脂质代谢相关基因的表达谱,细胞的增殖和治疗动物肝脏再生的动力学。
结果:响应PH,Plin2(-/-)小鼠肝甘油三酸酯蓄积减少,细胞周期进程延迟,这与肝再生受损有关。脂肪酸(FA)合成和脂质转移基因表达谱在Plin2(-/-)和野生型小鼠之间相当,而VLDL分泌率在Plin2(-/-)小鼠中更高。在Plin2(-/-)小鼠中β氧化的下调和胞质FA水平的降低可能有助于这些动物肝脏再生能力的减弱。在平行实验中,我们还观察到了Plin2(-/-)小鼠中CCl4介导的急性毒性肝损伤后肝脏脂质蓄积和增殖的减弱。
结论:我们得出结论,PLIN2介导的脂质在肝脏中的积累和利用对于有效响应PH和中毒性肝损伤的肝脏再生具有重要意义。

+1
+2
100研值 100研值 ¥99课程
检索文献一次
下载文献一次

去下载>

成功解锁2个技能,为你点赞

《SCI写作十大必备语法》
解决你的SCI语法难题!

技能熟练度+1

视频课《玩转文献检索》
让你成为检索达人!

恭喜完成新手挑战

手机微信扫一扫,添加好友领取

免费领《Endnote文献管理工具+教程》

微信扫码, 免费领取

手机登录

获取验证码
登录