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White spot syndrome virus (WSSV) modulates lipid metabolism in white shrimp.

Yen Siong NgCheng-Shun ChengMasahiro AndoYi-Ting TsengShu-Ting HeChun-Yuan LiShu-Wen ChengYi-Min ChenRamya KumarChun-Hung LiuHaruko TakeyamaIkuo HironoHan-Ching Wang
Published in: Communications biology (2023)
In addition to the Warburg effect, which increases the availability of energy and biosynthetic building blocks in WSSV-infected shrimp, WSSV also induces both lipolysis at the viral genome replication stage (12 hpi) to provide material and energy for the virus replication, and lipogenesis at the viral late stage (24 hpi) to complete virus morphogenesis by supplying particular species of long-chain fatty acids (LCFAs). Here, we further show that WSSV causes a reduction in lipid droplets (LDs) in hemocytes at the viral genome replication stage, and an increase in LDs in the nuclei of WSSV-infected hemocytes at the viral late stage. In the hepatopancreas, lipolysis is triggered by WSSV infection, and this leads to fatty acids being released into the hemolymph. β-oxidation inhibition experiment reveals that the fatty acids generated by WSSV-induced lipolysis can be diverted into β-oxidation for energy production. At the viral late stage, WSSV infection leads to lipogenesis in both the stomach and hepatopancreas, suggesting that fatty acids are in high demand at this stage for virion morphogenesis. Our results demonstrate that WSSV modulates lipid metabolism specifically at different stages to facilitate its replication.
Keyphrases
  • fatty acid
  • sars cov
  • adipose tissue
  • insulin resistance
  • skeletal muscle
  • genome wide
  • metabolic syndrome
  • electron transfer