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Tumor progression locus 2 ablation suppressed hepatocellular carcinoma development by inhibiting hepatic inflammation and steatosis in mice
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نویسنده
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li x. ,liu c. ,ip b.c. ,hu k.-q. ,smith d.e. ,greenberg a.s. ,wang x.-d.
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منبع
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journal of experimental and clinical cancer research - 2015 - دوره : 34 - شماره : 1
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چکیده
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Background: tumor progression locus 2 (tpl2),a serine-threonine kinase,functions as a critical regulator of inflammatory pathways and mediates oncogenic events. the potential role of tpl2 in nonalcoholic fatty liver disease (nafld) associated hepatocellular carcinoma (hcc) development remains unknown. methods: both wild-type and tpl2 knockout male mice were initiated by a hepatic carcinogen (diethylnitrosamine,i.p. with a single dose of 25 mg.kg-1)at 2 weeks of age,and then were given the high carbohydrate diet feeding to induce hepatic steatosis,inflammation,adenoma and hcc for 24 weeks. results: tpl2 knockout mice had significantly lower incidences of liver tumor and developed hepatocellular adenoma only,which is contrast to wild-type mice where they all developed hcc. tpl2 knockout mice had significantly down-regulated phosphorylation of jnk and erk,and levels of mrna expression of pro-inflammatory cytokines (il-1β,il-18,mcp-1 and nalp3),which correlated with the reduced incidence and number of hepatic inflammatory foci. furthermore,tpl2 ablation resulted in decreased hepatic steatosis and expression of de novo lipogenesis related markers (acc,scd1,srebp1c and akt phosphorylation),as well as reduction of endoplasmic reticulum stress biomarkers perk and eif-2a. conclusion: the study revealed for the first time that tpl2 plays a significant role in promoting hcc development by its pro-inflammatory effect,which suggested that tpl2 could be a molecular target for hcc prevention. © 2015 li et al.
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کلیدواژه
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HCC; Inflammation; Steatosis; TPL2; Tumorigenesis
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آدرس
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nutrition and cancer biology laboratory,jean mayer usda human nutrition research center on aging,tufts university,711 washington street,boston,ma 02111,united states,school of public health,medical college,soochow university,suzhouyy,jiangsu,215123, China, nutrition and cancer biology laboratory,jean mayer usda human nutrition research center on aging,tufts university,711 washington street,boston,ma 02111, United States, nutrition and cancer biology laboratory,jean mayer usda human nutrition research center on aging,tufts university,711 washington street,boston,ma 02111, United States, nutrition and cancer biology laboratory,jean mayer usda human nutrition research center on aging,tufts university,711 washington street,boston,ma 02111, United States, comparative biology unit,boston,ma, United States, obesity and metabolism laboratory,jean mayer usda human nutrition research center on aging,tufts university,boston,ma 02111, United States, nutrition and cancer biology laboratory,jean mayer usda human nutrition research center on aging,tufts university,711 washington street,boston,ma 02111, United States
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Authors
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