药物性脂肪肝（DIFLD）的个体发生：从关键起始事件到疾病表型

IF 6.9 2区医学 Q1 TOXICOLOGY

Archives of Toxicology Pub Date : 2025-09-16 DOI:10.1007/s00204-025-04178-x

Ernesto López-Pascual, Marta Moreno-Torres, Erika Moro, Anna Rapisarda, Rita Ortega-Vallbona, Eva Serrano-Candelas, Rafael Gozalbes, Ramiro Jover, José V Castell

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引用次数: 0

摘要

我们对药物性脂肪肝（DIFLD）的临床病例报告进行专家评审，根据不同的临床表型对药物进行分类。根据反映药物毒性机制的临床、生化和组织学特征确定了7组：第0组（对照组）：没有已知脂肪变性作用或临床证据的药物。第一类：具有轻度促脂肪变性作用的药物，加剧了现有的代谢性脂肪变性，但没有显著的肝酶升高。集群2：化合物引起中度脂肪变性伴轻度肝细胞损伤，偶有酶升高和延迟发病。集群3：引起严重线粒体功能障碍、ATP消耗和乳酸酸中毒的药物，最初没有炎症。第4类：药物诱导炎症性脂肪性肝炎，肝酶（ALT， AST, ALP 90-700 U/L）中度升高，但肝功能保留。第5组：引起严重脂肪性肝炎的药物，伴有明显的酶升高（ALT, AST bbb700 U/L），表明严重的肝损伤和炎症。集群6：化合物引起脂肪性肝炎并伴有额外的胆汁淤积和胆红素升高（> 11 mg/dL）。簇1和簇2主要损害β-氧化和线粒体呼吸，与高亲脂性和通常较低的日剂量有关。集群3涉及线粒体DNA耗竭和脂质输出受损。簇4和簇5结合了线粒体和核受体的破坏，通常与较高的日剂量有关。集群6结合了脂肪变性促进机制和胆汁酸运输中断。这种分类通过将临床表现与药物理化性质和毒理学机制联系起来，提高了对DIFLD表型的理解，有助于药物性脂肪变性的诊断和风险评估。

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Ontogeny of drug-induced fatty liver disease (DIFLD): from key initiating events to disease phenotypes.

We conducted an expert review of clinical case reports on drug-induced fatty liver disease (DIFLD) to classify drugs according to distinct clinical phenotypes. Seven clusters were identified based on clinical, biochemical, and histological features reflecting drug toxic mechanisms: Cluster 0 (Control): Drugs with no known steatotic effects or clinical evidence of DIFLD. Cluster 1: Drugs with mild pro-steatotic effects, exacerbating existing metabolic steatosis without significant liver enzyme elevation. Cluster 2: Compounds causing moderate steatosis with mild hepatocellular damage, occasional enzyme increases, and delayed onset. Cluster 3: Agents causing severe mitochondrial dysfunction, ATP depletion, and lactic acidosis, initially without inflammation. Cluster 4: Drugs inducing inflammatory steatohepatitis with moderate elevations of liver enzymes (ALT, AST, ALP 90-700 U/L) but preserved liver function. Cluster 5: Drugs causing severe steatohepatitis with marked enzyme elevation (ALT, AST > 700 U/L) indicating significant liver injury and inflammation. Cluster 6: Compounds causing steatohepatitis with additional cholestasis and elevated bilirubin (> 11 mg/dL). Clusters 1 and 2 primarily impair β-oxidation and mitochondrial respiration, linked to high lipophilicity and typically lower daily doses. Cluster 3 involves mitochondrial DNA depletion and impaired lipid export. Clusters 4 and 5 combine mitochondrial and nuclear receptor disruption, often linked to higher daily doses. Cluster 6 combines steatosis-promoting mechanisms with bile acid transport disruption. This classification improves understanding of DIFLD phenotypes by linking clinical manifestations with drug physicochemical properties and toxicological mechanisms, aiding diagnosis and risk assessment of drug-induced steatosis.

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来源期刊

Archives of Toxicology 医学-毒理学

CiteScore

11.60

自引率

4.90%

发文量

218

审稿时长

1.5 months

期刊介绍： Archives of Toxicology provides up-to-date information on the latest advances in toxicology. The journal places particular emphasis on studies relating to defined effects of chemicals and mechanisms of toxicity, including toxic activities at the molecular level, in humans and experimental animals. Coverage includes new insights into analysis and toxicokinetics and into forensic toxicology. Review articles of general interest to toxicologists are an additional important feature of the journal.