Gianni Testino, Carmen Fucile, Maurizia Gnocchi, Gian M Rosa, Fabio Caputo
{"title":"脂肪性肝病:饮酒在其中起什么作用?","authors":"Gianni Testino, Carmen Fucile, Maurizia Gnocchi, Gian M Rosa, Fabio Caputo","doi":"10.23736/S0026-4806.25.09726-5","DOIUrl":null,"url":null,"abstract":"<p><p>Metabolic-dysfunction associated steatotic liver disease (MASLD) includes diagnostic criteria such as overweight/ obesity, metabolic syndrome (MS) and type 2 diabetes mellitus (T2DM). MASLD is a subtype of steatotic liver disease (SLD). MASLD is characterized by SLD plus one or more cardiovascular disease (CVD) risks. Metabolic and alcohol-related liver disease (MetALD) is characterized by an alcohol consumption between 20-40 g/day for females and 30-50 gr/day for males and alcohol related liver disease (ALD) is characterized by an alcohol consumption >40 g/day for females and >50 g/day for males. Synergism or a supra-additive interaction between alcohol consumption (AC) and metabolic factors is well known. The aim of this narrative review is to explore the following points: 1) it is mandatory early identification of AC and it is necessary to also identify low dosage of AC; 2) all SLD subtypes increase cardiovascular and oncologic risk; 3) fibrosis is the most important predictor of long term survival. For this reason early liver fibrosis (LF) detection is crucial to reduce hepatic and extra hepatic pathology and motivate the patient to change lifestyle. This narrative review is based on a detailed analysis of the scientific literature published before December 31, 2024 and examining the most recent guidelines on SLD (PubMed, Web of Science, Scopus, Google Scholar). From the data reported in the present narrative review, the following emerges: 1) due to the significant synergistic effect between SLD and alcohol, the cut-off to distinguish MASLD and MetALD should be reduced to 10 g/day for women and 20 g/day for men; 2) it is useful to identify even low doses of consumption. The most appropriate suggestion is total alcohol abstinence (especially in cases with high oncological risk) and even light AC increases the risk of morbidity and mortality expecially in young people; 3) it is necessary to identify LF early and improve lifestyle; 4) cardiometabolic risk factors are present in >90% of subjects with all subtypes of SLD (mainly ALD) and therefore, cardiologists and hepatologists must cooperate; 5) all subjects who come to our attention for the first time (altered liver function, MS, T2DM, CVDs) must undergo ultrasonography with elastography. Subsequent oncologic surveillance beyond rigid schemes must be decided on a case-by-case basis. In cirrhotic patients and in non-cirrhotic patients at high clinical risk, in our opinion surveillance is semi-annual (especially in the presence of T2DM and/or AC). In light of epidemiological data, in medium-low risk cases, for prudence, surveillance can be annual. It is appropriate to raise awareness among health-care professionals and the broader public that SLD is a major risk factor for liver and non-liver disease. It is necessary to combat SLD with prevention and early detection. Early detection of steatosis and fibrosis is a motivating factor for lifestyle correction. The latter represents both primary prevention and therapy in the case of early pathology. This leads to a reduction in cases of decompensated liver disease, cardiovascular and oncologic pathologies with better management of economic resources.</p>","PeriodicalId":94143,"journal":{"name":"Minerva medica","volume":" ","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2025-07-17","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Steatotic liver disease: what role does alcohol consumption play?\",\"authors\":\"Gianni Testino, Carmen Fucile, Maurizia Gnocchi, Gian M Rosa, Fabio Caputo\",\"doi\":\"10.23736/S0026-4806.25.09726-5\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Metabolic-dysfunction associated steatotic liver disease (MASLD) includes diagnostic criteria such as overweight/ obesity, metabolic syndrome (MS) and type 2 diabetes mellitus (T2DM). MASLD is a subtype of steatotic liver disease (SLD). MASLD is characterized by SLD plus one or more cardiovascular disease (CVD) risks. Metabolic and alcohol-related liver disease (MetALD) is characterized by an alcohol consumption between 20-40 g/day for females and 30-50 gr/day for males and alcohol related liver disease (ALD) is characterized by an alcohol consumption >40 g/day for females and >50 g/day for males. Synergism or a supra-additive interaction between alcohol consumption (AC) and metabolic factors is well known. The aim of this narrative review is to explore the following points: 1) it is mandatory early identification of AC and it is necessary to also identify low dosage of AC; 2) all SLD subtypes increase cardiovascular and oncologic risk; 3) fibrosis is the most important predictor of long term survival. For this reason early liver fibrosis (LF) detection is crucial to reduce hepatic and extra hepatic pathology and motivate the patient to change lifestyle. This narrative review is based on a detailed analysis of the scientific literature published before December 31, 2024 and examining the most recent guidelines on SLD (PubMed, Web of Science, Scopus, Google Scholar). From the data reported in the present narrative review, the following emerges: 1) due to the significant synergistic effect between SLD and alcohol, the cut-off to distinguish MASLD and MetALD should be reduced to 10 g/day for women and 20 g/day for men; 2) it is useful to identify even low doses of consumption. The most appropriate suggestion is total alcohol abstinence (especially in cases with high oncological risk) and even light AC increases the risk of morbidity and mortality expecially in young people; 3) it is necessary to identify LF early and improve lifestyle; 4) cardiometabolic risk factors are present in >90% of subjects with all subtypes of SLD (mainly ALD) and therefore, cardiologists and hepatologists must cooperate; 5) all subjects who come to our attention for the first time (altered liver function, MS, T2DM, CVDs) must undergo ultrasonography with elastography. Subsequent oncologic surveillance beyond rigid schemes must be decided on a case-by-case basis. In cirrhotic patients and in non-cirrhotic patients at high clinical risk, in our opinion surveillance is semi-annual (especially in the presence of T2DM and/or AC). In light of epidemiological data, in medium-low risk cases, for prudence, surveillance can be annual. It is appropriate to raise awareness among health-care professionals and the broader public that SLD is a major risk factor for liver and non-liver disease. It is necessary to combat SLD with prevention and early detection. Early detection of steatosis and fibrosis is a motivating factor for lifestyle correction. The latter represents both primary prevention and therapy in the case of early pathology. 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引用次数: 0
摘要
代谢功能障碍相关的脂肪变性肝病(MASLD)包括超重/肥胖、代谢综合征(MS)和2型糖尿病(T2DM)等诊断标准。MASLD是脂肪变性肝病(SLD)的一种亚型。MASLD的特征是SLD加上一种或多种心血管疾病(CVD)风险。代谢性和酒精相关肝病(MetALD)的特征是女性每天饮酒20-40克,男性每天饮酒30-50克;酒精相关肝病(ALD)的特征是女性每天饮酒40克,男性每天饮酒50克。协同作用或酒精消耗(AC)和代谢因素之间的超加性相互作用是众所周知的。本文的目的是探讨以下几点:1)AC的早期识别是强制性的,同时也有必要识别低剂量AC;2)所有SLD亚型均增加心血管和肿瘤风险;3)纤维化是长期生存最重要的预测指标。因此,早期肝纤维化(LF)检测对于减少肝脏和肝外病理以及激励患者改变生活方式至关重要。这篇叙述性综述是基于对2024年12月31日之前发表的科学文献的详细分析,并检查了SLD的最新指南(PubMed, Web of Science, Scopus, b谷歌Scholar)。从本叙述性综述报告的数据中可以得出以下结论:1)由于SLD和酒精之间存在显著的协同效应,区分MASLD和MetALD的截止值应降至女性10克/天,男性20克/天;2)查明即使是低剂量的摄入也是有用的。最适当的建议是完全戒酒(特别是在肿瘤风险高的病例中),甚至轻度饮酒也会增加发病和死亡的风险,特别是在年轻人中;3)早期发现LF,改善生活方式;4)在所有SLD亚型(主要是ALD)患者中,有90%以上的患者存在心脏代谢危险因素,因此,心脏病专家和肝病专家必须合作;5)所有首次发现的患者(肝功能改变、多发性硬化症、2型糖尿病、心血管疾病)均需行超声弹性成像检查。在严格计划之外的后续肿瘤监测必须根据具体情况决定。在肝硬化患者和临床风险较高的非肝硬化患者中,我们认为监测是半年一次(特别是在存在T2DM和/或AC的情况下)。根据流行病学数据,在中低风险病例中,为谨慎起见,可每年监测一次。应当提高卫生保健专业人员和广大公众的认识,即SLD是肝脏和非肝脏疾病的一个主要危险因素。有必要通过预防和早期发现来对抗SLD。早期发现脂肪变性和纤维化是纠正生活方式的一个激励因素。后者在早期病理的情况下代表初级预防和治疗。通过更好地管理经济资源,可以减少失代偿性肝病、心血管疾病和肿瘤疾病的病例。
Steatotic liver disease: what role does alcohol consumption play?
Metabolic-dysfunction associated steatotic liver disease (MASLD) includes diagnostic criteria such as overweight/ obesity, metabolic syndrome (MS) and type 2 diabetes mellitus (T2DM). MASLD is a subtype of steatotic liver disease (SLD). MASLD is characterized by SLD plus one or more cardiovascular disease (CVD) risks. Metabolic and alcohol-related liver disease (MetALD) is characterized by an alcohol consumption between 20-40 g/day for females and 30-50 gr/day for males and alcohol related liver disease (ALD) is characterized by an alcohol consumption >40 g/day for females and >50 g/day for males. Synergism or a supra-additive interaction between alcohol consumption (AC) and metabolic factors is well known. The aim of this narrative review is to explore the following points: 1) it is mandatory early identification of AC and it is necessary to also identify low dosage of AC; 2) all SLD subtypes increase cardiovascular and oncologic risk; 3) fibrosis is the most important predictor of long term survival. For this reason early liver fibrosis (LF) detection is crucial to reduce hepatic and extra hepatic pathology and motivate the patient to change lifestyle. This narrative review is based on a detailed analysis of the scientific literature published before December 31, 2024 and examining the most recent guidelines on SLD (PubMed, Web of Science, Scopus, Google Scholar). From the data reported in the present narrative review, the following emerges: 1) due to the significant synergistic effect between SLD and alcohol, the cut-off to distinguish MASLD and MetALD should be reduced to 10 g/day for women and 20 g/day for men; 2) it is useful to identify even low doses of consumption. The most appropriate suggestion is total alcohol abstinence (especially in cases with high oncological risk) and even light AC increases the risk of morbidity and mortality expecially in young people; 3) it is necessary to identify LF early and improve lifestyle; 4) cardiometabolic risk factors are present in >90% of subjects with all subtypes of SLD (mainly ALD) and therefore, cardiologists and hepatologists must cooperate; 5) all subjects who come to our attention for the first time (altered liver function, MS, T2DM, CVDs) must undergo ultrasonography with elastography. Subsequent oncologic surveillance beyond rigid schemes must be decided on a case-by-case basis. In cirrhotic patients and in non-cirrhotic patients at high clinical risk, in our opinion surveillance is semi-annual (especially in the presence of T2DM and/or AC). In light of epidemiological data, in medium-low risk cases, for prudence, surveillance can be annual. It is appropriate to raise awareness among health-care professionals and the broader public that SLD is a major risk factor for liver and non-liver disease. It is necessary to combat SLD with prevention and early detection. Early detection of steatosis and fibrosis is a motivating factor for lifestyle correction. The latter represents both primary prevention and therapy in the case of early pathology. This leads to a reduction in cases of decompensated liver disease, cardiovascular and oncologic pathologies with better management of economic resources.