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Copyright ©The Author(s) 2021.
World J Stem Cells. Sep 26, 2021; 13(9): 1349-1359
Published online Sep 26, 2021. doi: 10.4252/wjsc.v13.i9.1349
Table 1 Experiments using mesenchymal stem cell transplantation in animals
Disease
Treatment
Source
Animal
Main results
Mechanism
Ref.
ALFAPAPHuman UC-MSCsMiceAlleviate hepatic injury and improve survival ratesMediate paracrine effects, regulate inflammatory responseLiu et al[38], 2014
ALFLPSHuman UC-MSCsMonkeysImprove the hepatic histology, systemic homeostasis, and survivalSuppress the hepatic aggregation and maturation of circulating monocytes and their IL-6 secretionGuo et al[40], 2019
LCCCl4Human UC-MSCsRatsImprove liver transaminases and synthetic function, reduce liver histopathology, and reverse hepatobiliary fibrosisDifferentiate into hepatocytesZhang et al[3], 2017
LCCCl4Monkey BM-MSCsMiceDecrease liver fibrosis, progression, and hepatocyte necrosisMediate paracrine effectsFu et al[42], 2018
LCTAAHuman BM-MSCsRatsDecrease collagen proportionate area and the content of hepatic hydroxyprolineMediate TGF-β1/Smad signaling pathwayJang et al[41], 2014
NAFLDHFDMice BM-MSCsMiceDecrease fibrosis markers and pro-inflammatory cytokinesRegulate inflammatory processEzquer et al[46], 2011
NAFLDHFDMice BM-MSCsMiceDecrease weight gain, expansion of subcutaneous adipose tissue, steatosis, lobular inflammation, and liver fibrosisSuppress the proliferation of CD 4+ T cellsWang et al[47], 2018
MSCs: Mesenchymal stem cells; AFL: Acute liver failure; LC: Liver cirrhosis; NAFLD: Non-alcoholic fatty liver disease; APAP: Acetaminophen; LPS: α-amatoxin and lipopolysaccharide; TAA: Thioacetamide; HFD: High-fat diet; BM-MSCs: Bone marrow-derived MSCs; UC-MSCs: Umbilical cord-derived MSCs.
Table 2 Clinical trials using mesenchymal stem cells to treat liver disease
Disease
Phase
No.
Stage
Source
Dose
Route of delivery
Main results
Ref.
LCI–II8MELD score ≥ 10Autologous BM-MSCs30-50 million cellsPeripheral or the portal veinReduce volumes of ascites; improve MELD scores, INR, and serum creatinineKharaziha et al[64], 2009
LCI–II30MELD Na score approximately 14UC-MSCs0.5 × 106 cells/kgPeripheralReduce volumes; improve ALB, TBIL, PTA, and MELD Na scoresZhang et al[65], 2012
ALCII48Child-Pugh B/CBM-MSCs5 × 107 cells/kgHepatic arteryImprove Child-Pugh scores and histologic fibrosisSuk et al[66], 2016
Liver failureII53MELD score: CG: 29.15 ± 3.72; EG: 30.01 ± 3.99Autologous BM-MSCsNoneHepatic arteryImprove ALB, TBIL, PT, and MELD scoresPeng et al[67], 2011
ACLFII5617 ≤ MELD score ≤ 30Allogeneic BM-MSCs1.0-10 × 105 cells/kgPeripheral veinsImprove ALT, ALB, TBIL, and MELD scores; decrease mortalityLin et al[69], 2017
ACLFII24MELD score: CG: 26.32; EG: 24.05UC-MSCs0.5 × 106 cells/kgCubital veinImprove ALB, CHE, PTA, and MELD score; increase survival rateShi et al[70], 2012
LC: Liver cirrhosis; ALC: Alcoholic liver cirrhosis; ACLF: Acute-on-chronic liver failure; CG: Control group; EG: Experimental group; BM-MSCs: Bone marrow-derived MSCs; UC-MSCs: Umbilical cord-derived MSCs; MELD: End-stage liver disease; ALB: Albumin; ALT: Alanine aminotransferase; TBIL: Total bilirubin; PT: Prothrombin time; PTA: Prothrombin time activity; INR: International normalized ratio; CHE: Cholinesterase.