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Drosophila immune cells transport oxygen through PPO2 protein phase transitionopen access

Authors
Shin, MingyuChang, EunjiLee, DaewonKim, NayunCho, BumsikCha, NuriKoranteng, FerdinandSong, Ji-JoonShim, Jiwon
Issue Date
Jul-2024
Publisher
Nature Research
Citation
Nature, v.631, no.8020, pp 350 - 359
Pages
10
Indexed
SCIE
SCOPUS
Journal Title
Nature
Volume
631
Number
8020
Start Page
350
End Page
359
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/194923
DOI
10.1038/s41586-024-07583-x
ISSN
0028-0836
1476-4687
Abstract
Insect respiration has long been thought to be solely dependent on an elaborate tracheal system without assistance from the circulatory system or immune cells1,2. Here we describe that Drosophila crystal cells—myeloid-like immune cells called haemocytes—control respiration by oxygenating Prophenoloxidase 2 (PPO2) proteins. Crystal cells direct the movement of haemocytes between the trachea of the larval body wall and the circulation to collect oxygen. Aided by copper and a neutral pH, oxygen is trapped in the crystalline structures of PPO2 in crystal cells. Conversely, PPO2 crystals can be dissolved when carbonic anhydrase lowers the intracellular pH and then reassembled into crystals in cellulo by adhering to the trachea. Physiologically, larvae lacking crystal cells or PPO2, or those expressing a copper-binding mutant of PPO2, display hypoxic responses under normoxic conditions and are susceptible to hypoxia. These hypoxic phenotypes can be rescued by hyperoxia, expression of arthropod haemocyanin or prevention of larval burrowing activity to expose their respiratory organs. Thus, we propose that insect immune cells collaborate with the tracheal system to reserve and transport oxygen through the phase transition of PPO2 crystals, facilitating internal oxygen homeostasis in a process that is comparable to vertebrate respiration.
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