Sphingosine kinase 1 and sphingosine-1-phosphate receptor 2 are vital to recovery from anaphylactic shock in mice
Ana Olivera, … , Richard L. Proia, Juan Rivera
Ana Olivera, … , Richard L. Proia, Juan Rivera
Published April 19, 2010
Citation Information: J Clin Invest. 2010;120(5):1429-1440. https://doi.org/10.1172/JCI40659.
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Research Article Immunology

Sphingosine kinase 1 and sphingosine-1-phosphate receptor 2 are vital to recovery from anaphylactic shock in mice

Abstract

Sphingosine kinase 1 (SphK1) and SphK2 are ubiquitous enzymes that generate sphingosine-1-phosphate (S1P), a ligand for a family of G protein–coupled receptors (S1PR1–S1PR5) with important functions in the vascular and immune systems. Here we explore the role of these kinases and receptors in recovery from anaphylaxis in mice. We found that Sphk2–/– mice had a rapid recovery from anaphylaxis. In contrast, Sphk1–/– mice showed poor recovery from anaphylaxis and delayed histamine clearance. Injection of S1P into Sphk1–/– mice increased histamine clearance and promoted recovery from anaphylaxis. Adoptive cell transfer experiments demonstrated that SphK1 activity was required in both the hematopoietic and nonhematopoietic compartments for recovery from anaphylaxis. Mice lacking the S1P receptor S1PR2 also showed a delay in plasma histamine clearance and a poor recovery from anaphylaxis. However, S1P did not promote the recovery of S1pr2–/– mice from anaphylaxis, whereas S1pr2+/– mice showed partial recovery. Unlike Sphk2–/– mice, Sphk1–/– and S1pr2–/– mice had severe hypotension during anaphylaxis. Thus, SphK1-produced S1P regulates blood pressure, histamine clearance, and recovery from anaphylaxis in a manner that involves S1PR2. This suggests that specific S1PR2 agonists may serve to counteract the vasodilation associated with anaphylactic shock.

Authors

Ana Olivera, Christoph Eisner, Yoshiaki Kitamura, Sandra Dillahunt, Laura Allende, Galina Tuymetova, Wendy Watford, Francoise Meylan, Susanne C. Diesner, Lingli Li, Jurgen Schnermann, Richard L. Proia, Juan Rivera

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Figure 6

Clearance of plasma histamine and excretion are impaired in Sphk1–/– and S1pr2–/– mice but enhanced in Sphk2–/– mice.

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Clearance of plasma histamine and excretion are impaired in Sphk1–/– and...
(A) Histamine (5 μmol) was injected into the indicated mice, and after 60 minutes, mice were euthanized and blood was drawn. As indicated, 500 μM S1P was administered to some mice 10 minutes after induction of anaphylaxis. Plasma histamine levels were determined for all genotypes and treatments as indicated. (BD) Kinetics of plasma histamine clearance (left panels) and its appearance in urine (right panels) for (B) Sphk1–/–, (C) Sphk2–/–, and (D) S1pr2–/– mice and their corresponding WT counterparts (n = 4–7). Blood was drawn (~2 μl) from each mouse from the tail vein at the indicated times. Urine was collected (when possible) at the indicated times. Histamine was measured by competitive ELISA. *P < 0.05, **P < 0.01, ***P < 0.001, determined by Student’s t test.