TY - JOUR
T1 - A Population-based and Clinical Cohort Validation of the Novel Consensus Definition of Metabolic Hyperferritinemia
AU - Liu, Wen-Yue
AU - Lian, Li-You
AU - Zhang, Huai
AU - Chen, Sui-Dan
AU - Jin, Xin-Zhe
AU - Zhang, Ni
AU - Ye, Chen-Hui
AU - Chen, Wen-Ying
AU - Bee, George Goh Boon
AU - Wang, Fu-Di
AU - Miele, Luca
AU - Corradini, Elena
AU - Valenti, Luca
AU - Zheng, Ming-Hua
PY - 2024
Y1 - 2024
N2 - Context: There is limited data on the clinical significance of metabolic hyperferritinemia (MHF) based on the most recent consensus.Objective: We aimed to validate the clinical outcomes of MHF in the general population and patients with biopsy-proven metabolic dysfunction-associated fatty liver disease (MAFLD).Methods: The NHANES database and PERSONS cohort were included. MHF was defined as elevated serum ferritin with metabolic dysfunction (MD) and stratified into different grades according to ferritin (grade 1: 200 [females]/300 [males]-550 ng/mL; grade 2: 550-1000 ng/mL; grade 3: >1000 ng/mL). The clinical outcomes, including all-cause death, comorbidities, and liver histology, were compared between non-MHF and MHF in adjusted models.Results: In NHANES, compared with non-MHF with MD, MHF was related to higher risks of advanced fibrosis (P = .036), elevated albumin-creatinine ratio (UACR, P = .001), and sarcopenia (P = .013). Although the association between all grades of MHF and mortality was insignificant (P = .122), grades 2/3 was associated with increased mortality (P = .029). When comparing with non-MHF without MD, the harmful effects of MHF were more significant in mortality (P < .001), elevated UACR (P < .001), cardiovascular disease (P = .028), and sarcopenia (P < .001). In the PERSONS cohort, MHF was associated with more advanced grades of steatosis (P < .001), lobular inflammation (P < .001), advanced fibrosis (P = .017), and more severe hepatocellular iron deposition (P < .001).Conclusion: Both in the general population and in at-risk individuals with MAFLD, MHF was related with poorer clinical outcomes.
AB - Context: There is limited data on the clinical significance of metabolic hyperferritinemia (MHF) based on the most recent consensus.Objective: We aimed to validate the clinical outcomes of MHF in the general population and patients with biopsy-proven metabolic dysfunction-associated fatty liver disease (MAFLD).Methods: The NHANES database and PERSONS cohort were included. MHF was defined as elevated serum ferritin with metabolic dysfunction (MD) and stratified into different grades according to ferritin (grade 1: 200 [females]/300 [males]-550 ng/mL; grade 2: 550-1000 ng/mL; grade 3: >1000 ng/mL). The clinical outcomes, including all-cause death, comorbidities, and liver histology, were compared between non-MHF and MHF in adjusted models.Results: In NHANES, compared with non-MHF with MD, MHF was related to higher risks of advanced fibrosis (P = .036), elevated albumin-creatinine ratio (UACR, P = .001), and sarcopenia (P = .013). Although the association between all grades of MHF and mortality was insignificant (P = .122), grades 2/3 was associated with increased mortality (P = .029). When comparing with non-MHF without MD, the harmful effects of MHF were more significant in mortality (P < .001), elevated UACR (P < .001), cardiovascular disease (P = .028), and sarcopenia (P < .001). In the PERSONS cohort, MHF was associated with more advanced grades of steatosis (P < .001), lobular inflammation (P < .001), advanced fibrosis (P = .017), and more severe hepatocellular iron deposition (P < .001).Conclusion: Both in the general population and in at-risk individuals with MAFLD, MHF was related with poorer clinical outcomes.
KW - Iron overload
KW - Metabolic dysfunction-associated fatty liver disease
KW - Metabolic hyperferritinemia
KW - Metabolic syndrome
KW - Iron overload
KW - Metabolic dysfunction-associated fatty liver disease
KW - Metabolic hyperferritinemia
KW - Metabolic syndrome
UR - http://hdl.handle.net/10807/273456
U2 - 10.1210/clinem/dgad749
DO - 10.1210/clinem/dgad749
M3 - Article
SN - 0021-972X
VL - 109
SP - 1540
EP - 1549
JO - THE JOURNAL OF CLINICAL ENDOCRINOLOGY AND METABOLISM
JF - THE JOURNAL OF CLINICAL ENDOCRINOLOGY AND METABOLISM
ER -