2009
DOI: 10.2353/ajpath.2009.081081
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IGF-1R Contributes to Stress-Induced Hepatocellular Damage in Experimental Cholestasis

Abstract: The insulin-like growth factor type 1 receptor (IGF-1R) controls aging and cellular stress, both of which play major roles in liver disease. Stimulation of insulin-like growth factor signaling can generate cell death in vitro. Here, we tested whether IGF-1R contributes to stress insult in the liver. Cholestatic liver injury was induced by bile duct ligation in control and liver-specific IGF-1R knockout (LIGFREKO) mice. LIGFREKO mice displayed less bile duct ligation-induced hepatocyte damage than controls, whi… Show more

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Cited by 10 publications
(11 citation statements)
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“…It is important to note that levels of serum ALP and hepatic PAI1 remained lower in IRS2KO mice at this final time period, suggesting that, although there were no differences in the degree of fibrosis, IRS2 deficiency protects against long-term damage induced by bile accumulation. Taken together, these data have evidenced a delay in the progression towards fibrosis in IRS2KO mice after BDL, in agreement with the work of Cadoret et al (2009) in the IGF1RKO mice. Based on that, we could hypothesize that IRS2 (this study) or IGF1R (Cadoret et al, 2009) deficiency specifically protect against IGF1-mediated HSC activation, as demonstrated here by our in vitro experiments silencing IRS2 in LX2 cells as discussed below.…”
Section: Discussionsupporting
confidence: 91%
“…It is important to note that levels of serum ALP and hepatic PAI1 remained lower in IRS2KO mice at this final time period, suggesting that, although there were no differences in the degree of fibrosis, IRS2 deficiency protects against long-term damage induced by bile accumulation. Taken together, these data have evidenced a delay in the progression towards fibrosis in IRS2KO mice after BDL, in agreement with the work of Cadoret et al (2009) in the IGF1RKO mice. Based on that, we could hypothesize that IRS2 (this study) or IGF1R (Cadoret et al, 2009) deficiency specifically protect against IGF1-mediated HSC activation, as demonstrated here by our in vitro experiments silencing IRS2 in LX2 cells as discussed below.…”
Section: Discussionsupporting
confidence: 91%
“…In the acute CCl 4 model, IGF1 did not reduce the initial damage, but caused a more rapid DNA synthesis, resulting in liver regeneration [27]. Depletion of IGF1R reduces ductular and fibrogenic responses and increased cholestasis tolerance in BDL mice [40]. The damage in the Abcb4 −/− mouse is chronic, less severe, and localized to the portal areas [16].…”
Section: Discussionmentioning
confidence: 97%
“…Toll-like receptor signaling interferes with the UPR by regulating the ATF4-CHOP pathway and the insulin-like growth factor-1 also regulates ER stress pathways. [56][57][58] Finally, XBP1 mRNA splicing in spleen B cells during plasma cell differentiation is induced by antibody-mediated CD40 activation. 59,60 The regulation of the UPR by extracellular signals may represent a mechanism by which the environment controls cell adaptation to stress.…”
Section: Discussionmentioning
confidence: 99%