[HTML][HTML] A functional role of GAS6/TAM in nonalcoholic steatohepatitis progression implicates AXL as therapeutic target
A Tutusaus, E de Gregorio, B Cucarull… - Cellular and molecular …, 2020 - Elsevier
A Tutusaus, E de Gregorio, B Cucarull, H Cristóbal, C Aresté, I Graupera, M Coll, A Colell…
Cellular and molecular gastroenterology and hepatology, 2020•ElsevierBackground and Aims GAS6 signaling, through the TAM receptor tyrosine kinases AXL and
MERTK, participates in chronic liver pathologies. Here, we addressed GAS6/TAM
involvement in Non-Alcoholic SteatoHepatitis (NASH) development. Methods GAS6/TAM
signaling was analyzed in cultured primary hepatocytes, hepatic stellate cells (HSC) and
Kupffer cells (KCs). Axl-/-, Mertk-/-and wild-type C57BL/6 mice were fed with Chow, High Fat
Choline-Deficient Methionine-Restricted (HFD) or methionine-choline-deficient (MCD) diet …
MERTK, participates in chronic liver pathologies. Here, we addressed GAS6/TAM
involvement in Non-Alcoholic SteatoHepatitis (NASH) development. Methods GAS6/TAM
signaling was analyzed in cultured primary hepatocytes, hepatic stellate cells (HSC) and
Kupffer cells (KCs). Axl-/-, Mertk-/-and wild-type C57BL/6 mice were fed with Chow, High Fat
Choline-Deficient Methionine-Restricted (HFD) or methionine-choline-deficient (MCD) diet …
Background and Aims
GAS6 signaling, through the TAM receptor tyrosine kinases AXL and MERTK, participates in chronic liver pathologies. Here, we addressed GAS6/TAM involvement in Non-Alcoholic SteatoHepatitis (NASH) development.
Methods
GAS6/TAM signaling was analyzed in cultured primary hepatocytes, hepatic stellate cells (HSC) and Kupffer cells (KCs). Axl-/-, Mertk-/- and wild-type C57BL/6 mice were fed with Chow, High Fat Choline-Deficient Methionine-Restricted (HFD) or methionine-choline-deficient (MCD) diet. HSC activation, liver inflammation and cytokine/chemokine production were measured by qPCR, mRNA Array analysis, western blotting and ELISA. GAS6, soluble AXL (sAXL) and MERTK (sMERTK) levels were analyzed in control individuals, steatotic and NASH patients.
Results
In primary mouse cultures, GAS6 or MERTK activation protected primary hepatocytes against lipid toxicity via AKT/STAT-3 signaling, while bemcentinib (small molecule AXL inhibitor BGB324) blocked AXL-induced fibrogenesis in primary HSCs and cytokine production in LPS-treated KCs. Accordingly; bemcentinib diminished liver inflammation and fibrosis in MCD- and HFD-fed mice. Upregulation of AXL and ADAM10/ADAM17 metalloproteinases increased sAXL in HFD-fed mice. Transcriptome profiling revealed major reduction in fibrotic- and inflammatory-related genes in HFD-fed mice after bemcentinib administration. HFD-fed Mertk-/- mice exhibited enhanced NASH, while Axl-/- mice were partially protected. In human serum, sAXL levels augmented even at initial stages, whereas GAS6 and sMERTK increased only in cirrhotic NASH patients. In agreement, sAXL increased in HFD-fed mice before fibrosis establishment, while bemcentinib prevented liver fibrosis/inflammation in early NASH.
Conclusion
AXL signaling, increased in NASH patients, promotes fibrosis in HSCs and inflammation in KCs, while GAS6 protects cultured hepatocytes against lipotoxicity via MERTK. Bemcentinib, by blocking AXL signaling and increasing GAS6 levels, reduces experimental NASH, revealing AXL as an effective therapeutic target for clinical practice.
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