预测肝纤维化进展的因素及纤维化评分的表现:瘦型与非瘦型代谢相关脂肪性肝病(MASLD)患者的比较。
Predictors of advanced liver fibrosis and the performance of fibrosis scores: lean compared to non-lean metabolic dysfunction-associated steatotic liver disease (MASLD) patients.
机构信息
Liver Diseases Center, Sheba Medical Center, Ramat Gan, Israel -
Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel -
出版信息
Minerva Gastroenterol (Torino). 2024 Sep;70(3):322-331. doi: 10.23736/S2724-5985.23.03518-0. Epub 2023 Oct 27.
BACKGROUND
Non-alcoholic fatty liver disease (NAFLD) in lean patients differs from that of NAFLD in non-lean patients. However, current data regarding predictors of advanced fibrosis and the performance of fibrosis-4 index (FIB-4) and NAFLD fibrosis score (NFS) in lean compared to non-lean metabolic dysfunction-associated steatotic liver disease (MASLD) patients is insufficient.
METHODS
This was a cross-sectional study. Lean was defined as Body Mass Index <25 kg/m. Advanced fibrosis (F3-F4) was detected by liver biopsy or two-dimension shear wave elastography (2D-SWE). Predictors of advanced fibrosis were identified using logistic regression and area under ROC curves (AUROC) were derived for FIB-4 and NFS.
RESULTS
Lean patients (N.=153) comprised 19.2% of the MASLD cohort. Advanced fibrosis was associated with the number of cardiometabolic risk factors (CMRF) in lean (OR=2.06, P=0.011) and non-lean (OR=1.58, P<0.001) patients, however, hypertension and diabetes or impaired fasting glucose were significant only among non-lean. Age was associated with advanced fibrosis in both subgroups with age ≥65 showing higher odds in lean compared to non-lean patients (P=0.016). Non-lean patients had higher odds for advanced fibrosis relative to lean patients (OR=4.8, P=0.048). FIB-4 and NFS predicted advanced fibrosis among lean (AUROC=0.79 and AUROC=0.85, respectively) and non-lean (AUROC=0.79 and AUROC=0.76, respectively) patients. NFS ≥-1.445 showed higher specificity among lean compared to non-lean (P<0.001) and compared to that of FIB-4 ≥1.3 in lean patients (P<0.001).
CONCLUSIONS
The number of CMRF was predictive of advanced fibrosis in both subgroups while age ≥65 showed higher odds among lean patients. NFS ≥-1.445 is more specific than FIB-4 ≥1.3 for advanced fibrosis prediction in lean patients. These findings may help identify high-risk lean MASLD patients for further liver fibrosis stage assessment.
背景
瘦型非酒精性脂肪性肝病(NAFLD)与非瘦型患者的 NAFLD 不同。然而,目前关于预测因子的先进纤维化和纤维化-4 指数(FIB-4)和 NAFLD 纤维化评分(NFS)在瘦型与非瘦型代谢功能障碍相关脂肪性肝病(MASLD)患者中的表现的数据不足。
方法
这是一项横断面研究。瘦型定义为体重指数<25kg/m。先进的纤维化(F3-F4)通过肝活检或二维剪切波弹性成像(2D-SWE)检测。使用逻辑回归识别先进纤维化的预测因子,并为 FIB-4 和 NFS 得出 ROC 曲线下面积(AUROC)。
结果
瘦型患者(N=153)占 MASLD 队列的 19.2%。先进的纤维化与瘦型(OR=2.06,P=0.011)和非瘦型(OR=1.58,P<0.001)患者的代谢相关心血管危险因素(CMRF)数量相关,但高血压、糖尿病或空腹血糖受损仅在非瘦型患者中显著。年龄与两个亚组的先进纤维化相关,年龄≥65 岁的瘦型患者发生先进纤维化的几率高于非瘦型患者(P=0.016)。与瘦型患者相比,非瘦型患者发生先进纤维化的几率更高(OR=4.8,P=0.048)。FIB-4 和 NFS 预测瘦型(AUROC=0.79 和 AUROC=0.85)和非瘦型(AUROC=0.79 和 AUROC=0.76)患者的先进纤维化。NFS≥-1.445 在瘦型患者中的特异性高于非瘦型(P<0.001),也高于 FIB-4≥1.3 在瘦型患者中的特异性(P<0.001)。
结论
CMRF 的数量在两个亚组中均预测先进纤维化,而年龄≥65 岁的瘦型患者发生先进纤维化的几率更高。NFS≥-1.445 对预测瘦型患者的先进纤维化比 FIB-4≥1.3 更特异。这些发现可能有助于识别高危瘦型 MASLD 患者,以进一步评估肝纤维化分期。
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