Communications Biology (Jul 2024)

Activation of AMPD2 drives metabolic dysregulation and liver disease in mice with hereditary fructose intolerance

  • Ana Andres-Hernando,
  • David J. Orlicky,
  • Masanari Kuwabara,
  • Mehdi A. Fini,
  • Dean R. Tolan,
  • Richard J. Johnson,
  • Miguel A. Lanaspa

DOI
https://doi.org/10.1038/s42003-024-06539-1
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 12

Abstract

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Abstract Hereditary fructose intolerance (HFI) is a painful and potentially lethal genetic disease caused by a mutation in aldolase B resulting in accumulation of fructose-1-phosphate (F1P). No cure exists for HFI and treatment is limited to avoid exposure to fructose and sugar. Using aldolase B deficient mice, here we identify a yet unrecognized metabolic event activated in HFI and associated with the progression of the disease. Besides the accumulation of F1P, here we show that the activation of the purine degradation pathway is a common feature in aldolase B deficient mice exposed to fructose. The purine degradation pathway is a metabolic route initiated by adenosine monophosphate deaminase 2 (AMPD2) that regulates overall energy balance. We demonstrate that very low amounts of fructose are sufficient to activate AMPD2 in these mice via a phosphate trap. While blocking AMPD2 do not impact F1P accumulation and the risk of hypoglycemia, its deletion in hepatocytes markedly improves the metabolic dysregulation induced by fructose and corrects fat and glycogen storage while significantly increasing the voluntary tolerance of these mice to fructose. In summary, we provide evidence for a critical pathway activated in HFI that could be targeted to improve the metabolic consequences associated with fructose consumption.