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Elevated sphingosine-1-phosphate promotes sickling and sickle cell disease progression
Authors:Yujin Zhang  Vladimir Berka  Anren Song  Kaiqi Sun  Wei Wang  Weiru Zhang  Chen Ning  Chonghua Li  Qibo Zhang  Mikhail Bogdanov  Danny C Alexander  Michael V Milburn  Mostafa H Ahmed  Han Lin  Modupe Idowu  Jun Zhang  Gregory J Kato  Osheiza Y Abdulmalik  Wenzheng Zhang  William Dowhan  Rodney E Kellems  Pumin Zhang  Jianping Jin  Martin Safo  Ah-Lim Tsai  Harinder S Juneja  Yang Xia
Abstract:Sphingosine-1-phosphate (S1P) is a bioactive lipid that regulates multicellular functions through interactions with its receptors on cell surfaces. S1P is enriched and stored in erythrocytes; however, it is not clear whether alterations in S1P are involved in the prevalent and debilitating hemolytic disorder sickle cell disease (SCD). Here, using metabolomic screening, we found that S1P is highly elevated in the blood of mice and humans with SCD. In murine models of SCD, we demonstrated that elevated erythrocyte sphingosine kinase 1 (SPHK1) underlies sickling and disease progression by increasing S1P levels in the blood. Additionally, we observed elevated SPHK1 activity in erythrocytes and increased S1P in blood collected from patients with SCD and demonstrated a direct impact of elevated SPHK1-mediated production of S1P on sickling that was independent of S1P receptor activation in isolated erythrocytes. Together, our findings provide insights into erythrocyte pathophysiology, revealing that a SPHK1-mediated elevation of S1P contributes to sickling and promotes disease progression, and highlight potential therapeutic opportunities for SCD.
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