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Hypoxia‐driven Hif2a coordinates mouse liver regeneration by coupling parenchymal growth to vascular expansion
Author(s) -
Kron Philipp,
Linecker Michael,
Limani Perparim,
Schlegel Andrea,
Kambakamba Patryk,
Lehn JeanMarie,
Nicolau Claude,
Graf Rolf,
Humar Bostjan,
Clavien PierreAlain
Publication year - 2016
Publication title -
hepatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.488
H-Index - 361
eISSN - 1527-3350
pISSN - 0270-9139
DOI - 10.1002/hep.28809
Subject(s) - hepatocyte , liver regeneration , microbiology and biotechnology , mitosis , biology , hepatocyte growth factor , hypoxia (environmental) , regeneration (biology) , sinusoid , hepatectomy , chemistry , immunology , biochemistry , medicine , oxygen , receptor , surgery , organic chemistry , resection , in vitro
Interaction between sinusoidal endothelial cells and hepatocytes is a prerequisite for liver function. Upon tissue loss, both liver cell populations need to be regenerated. Repopulation occurs in a coordinated pattern, first through the regeneration of parenchyme (hepatocytes), which then produces vascular endothelial growth factor (VEGF) to enable the subsequent angiogenic phase. The signals that instruct hepatocytes to induce timely VEGF remain unidentified. Given that liver is highly vascularized, we reasoned that fluctuations in oxygenation after tissue loss may contribute to the coordination between hepatocyte and sinusoidal endothelial cell proliferation. To prevent drops in oxygen after hepatectomy, mice were pretreated with inositol trispyrophosphate (ITPP), an allosteric effector of hemoglobin causing increased O 2 release from heme under hypoxic conditions. ITPP treatment delayed liver weight gain after hepatectomy. Comparison with controls revealed the presence of a hypoxic period around the peak of hepatocyte mitosis. Inhibition of hypoxia led to deficient hepatocyte mitosis, suppressed the regenerative Vegf wave, and abrogated the subsequent reconstruction of the sinusoidal network. These ITPP effects were ongoing with the reduction in hepatocellular hypoxia inducible factor 2a (Hif2a). In contrast, Hif1a was unaffected by ITPP. Hif2a knockdown phenocopied all effects of ITPP, including the mitotic deficiencies, Vegf suppression, and angiogenic failure. Conclusions: Oxygen is a key regulator of liver regeneration. Hypoxia—inherent to the expansion of parenchyme—activates Hif2a to couple hepatocyte mitosis with the angiogenic phase. Hif2a acts as a safeguard to initiate sinusoidal reconstruction only upon successful hepatocyte mitosis, thereby enforcing a timely order onto cell type‐specific regeneration patterns. These findings portray the hypoxia‐driven Hif2a‐Vegf axis as a prime node in coordinating sinusoidal endothelial cell‐hepatocyte crosstalk during liver regeneration. (H epatology 2016;64:2198‐2209).