Proposed pathophysiological crosstalk between MAFLD and CKD.

Proposed pathophysiological crosstalk between MAFLD and CKD.

<p>This schematic illustrates the proposed pathophysiological crosstalk between Metabolic Dysfunction-Associated Fatty Liver Disease (MAFLD) and Chronic Kidney Disease (CKD). <b>Panel A depicts organ-specific mechanisms:</b> in the <i>liver</i>, steatosis (lipid-laden h...

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書誌詳細
第一著者: Zienab M. Saad (22676502) (author)
その他の著者: Hesham K. H. Keryakos (22676505) (author), Hala A. Hassanin (22676508) (author), Mahmoud M. Higazi (22676511) (author), Manar M. Sayed (22676514) (author), Doaa E. Ismail (22676517) (author), Safaa M. Abdelhalim (21398199) (author)
出版事項: 2025
主題:
Medicine
Cell Biology
Biotechnology
Marine Biology
Cancer
Infectious Diseases
Virology
shear wave elastography
patients remains underexplored
mitigate progression risks
higher liver stiffness
56 ± 17
43 ± 17
5 ± 28
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shared metabolic abnormalities
9 ± 39
invasive fibrosis scores
45 ± 1
2 ± 5
mafld patients also
dialysis ckd patients
108 ckd patients
metabolic risk factors
5 ± 6
9 ± 1
5 ± 3
6 ± 1
xlink "> mafld
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5 %,
b ><
metabolic dysfunction
9 ml
risk populations
fibrosis severity
advanced fibrosis
1 years
2 vs
ckd severity
1 vs
6 vs
study aimed
sectional study
participants stratified
older age
nafld score
management strategies
lower egfr
integrated screening
insulin resistance
findings highlight
diagnostic criteria
bidirectional relationship
apri score
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その他の書誌記述
要約:<p>This schematic illustrates the proposed pathophysiological crosstalk between Metabolic Dysfunction-Associated Fatty Liver Disease (MAFLD) and Chronic Kidney Disease (CKD). <b>Panel A depicts organ-specific mechanisms:</b> in the <i>liver</i>, steatosis (lipid-laden hepatocytes) progresses through inflammation (Kupffer cell activation, TNF-α/IL-6 release) to fibrosis (stellate cell activation, collagen deposition); in the <i>kidney</i>, lipotoxicity (podocyte fatty acid influx) leads to podocyte injury (effacement, apoptosis) and glomerulosclerosis (collagen IV accumulation). <b>Panel B highlights systemic mediators</b>: insulin resistance (hyperinsulinemia-driven hepatic gluconeogenesis and renal sodium retention), dyslipidemia (VLDL/ApoB glomerular deposition), and key mediators (fetuin-A, adiponectin deficiency, uric acid-induced NLRP3 activation). Bidirectional interactions amplify organ damage through direct (lipotoxicity, fibrosis) and systemic (metabolic, inflammatory) pathways, suggesting shared therapeutic targets for dual hepatic-renal protection.</p>

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