Statin-associated regulation of hepatic PNPLA3 in patients without known liver disease.

IF 9 2区 医学 Q1 MEDICINE, GENERAL & INTERNAL
Osman Ahmed, Vladimir S Shavva, Laura Tarnawski, Wanmin Dai, Filip Borg, Viggo V Olofsson, Ting Liu, Peter Saliba-Gustafsson, Christian Simini, Matteo Pedrelli, Otto Bergman, Giuseppe Danilo Norata, Paolo Parini, Anders Franco-Cereceda, Per Eriksson, Stephen G Malin, Hanna M Björck, Peder S Olofsson
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引用次数: 0

Abstract

Background and objectives: Statins are used for metabolic dysfunction-associated steatotic liver disease (MASLD) (NAFLD) treatment, but their role in this context is unclear. Genetic variants of patatin-like phospholipase domain containing 3 (PNPLA3) are associated with MASLD susceptibility and statin treatment efficacy. Access to liver biopsies before established MASLD is limited, and statins and PNPLA3 in early liver steatosis are thus difficult to study.

Methods: Liver biopsies were collected from 261 patients without known liver disease at surgery and stratified based on statin use and criteria for the metabolic syndrome (MS). Genotypes and transcript levels were measured using Illumina and Affymetrix arrays, and metabolic and lipoprotein profiles by clinical assays. Statin effects on PNPLA3, de novo lipogenesis (DNL), and lipid accumulation were further studied in vitro.

Results: The PNPLA3I148M genetic variant was associated with significantly lower hepatic levels of cholesterol synthesis-associated transcripts. Patients with MS had significantly higher hepatic levels of MASLD and lipogenesis-associated transcripts than non-MS patients. Patients with MS on statin therapy had significantly higher hepatic levels of PNPLA3, acetyl-CoA carboxylase alpha, and ATP citrate lyase, and statin use was associated with higher plasma fasting glucose, insulin, and HbA1c. Exposure of hepatocyte-like HepG2 cells to atorvastatin promoted intracellular accumulation of triglycerides and lipogenesis-associated transcripts. Atorvastatin-exposure of HepG2, sterol O-acyltransferase (SOAT) 2-only-HepG2, primary human hepatic stellate, and hepatic stellate cell-like LX2 cells significantly increased levels of PNPLA3 and SREBF2-target genes, whereas knockdown of SREBF2 attenuated this effect.

Conclusions: Collectively, these observations suggest statin-associated regulation of PNPLA3 and DNL in liver. The potential interaction between PNPLA3 genotype and metabolic status should be considered in future studies in the context of statin therapy for MASLD.

他汀类药物对无已知肝病患者肝脏 PNPLA3 的相关调节。
背景和目的:他汀类药物用于代谢功能障碍相关性脂肪性肝病(MASLD)(NAFLD)的治疗,但其在这方面的作用尚不清楚。含帕他丁样磷脂酶域 3 (PNPLA3) 的基因变异与 MASLD 易感性和他汀类药物的疗效有关。在确诊 MASLD 之前进行肝活检的机会有限,因此很难对他汀类药物和 PNPLA3 在早期肝脏脂肪变性中的作用进行研究:方法:收集了261名手术时未发现肝病的患者的肝活检组织,并根据他汀类药物的使用情况和代谢综合征(MS)的标准进行了分层。使用 Illumina 和 Affymetrix 阵列测量基因型和转录本水平,并使用临床检测方法测量代谢和脂蛋白概况。在体外进一步研究了他汀类药物对 PNPLA3、新生脂肪生成(DNL)和脂质累积的影响:结果:PNPLA3I148M 基因变异与肝脏胆固醇合成相关转录物水平显著降低有关。与非多发性硬化症患者相比,多发性硬化症患者肝脏中的 MASLD 和脂肪生成相关转录本水平明显较高。接受他汀类药物治疗的多发性硬化症患者的肝脏中 PNPLA3、乙酰-CoA 羧化酶 alpha 和 ATP 柠檬酸酶的水平明显较高,他汀类药物的使用与较高的血浆空腹血糖、胰岛素和 HbA1c 有关。将肝细胞样 HepG2 细胞暴露于阿托伐他汀可促进细胞内甘油三酯和脂肪生成相关转录物的积累。将阿托伐他汀暴露于HepG2、固醇O-酰基转移酶(SOAT)2-only-HepG2、原代人类肝星状细胞和肝星状细胞样LX2细胞可显著增加PNPLA3和SREBF2靶基因的水平,而敲除SREBF2可减轻这种影响:总之,这些观察结果表明他汀类药物对肝脏中的 PNPLA3 和 DNL 有相关调控作用。在他汀类药物治疗MASLD的背景下,未来的研究应考虑PNPLA3基因型与代谢状态之间的潜在相互作用。
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来源期刊
Journal of Internal Medicine
Journal of Internal Medicine 医学-医学:内科
CiteScore
22.00
自引率
0.90%
发文量
176
审稿时长
4-8 weeks
期刊介绍: JIM – The Journal of Internal Medicine, in continuous publication since 1863, is an international, peer-reviewed scientific journal. It publishes original work in clinical science, spanning from bench to bedside, encompassing a wide range of internal medicine and its subspecialties. JIM showcases original articles, reviews, brief reports, and research letters in the field of internal medicine.
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