Actions of a picomolar short-acting S1P1 agonist in S1P1-eGFP knock-in mice

Actions of a picomolar short-acting S1P1 agonist in S1P1-eGFP knock-in mice

A selective, short-acting agonist for the sphingosine-1-phosphate receptor S1P 1 and GFP-S1P 1 knock-in mouse model are used to show that both receptor degradation and receptor reserve underlie the mechanisms of lymphocyte sequestration by agonists. Sphingosine 1-phosphate receptor 1 (S1P 1 ) is cri...

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Veröffentlicht in:Nature chemical biology 2011-05, Vol.7 (5), p.254-256
Hauptverfasser: Cahalan, Stuart M, Gonzalez-Cabrera, Pedro J, Sarkisyan, Gor, Nguyen, Nhan, Schaeffer, Marie-Therese, Huang, Liming, Yeager, Adam, Clemons, Bryan, Scott, Fiona, Rosen, Hugh
Format: Artikel
Sprache:eng
Schlagworte:
631/250/1619
631/92/609
692/699/249/1313/1666
Animals
Biochemical Engineering
Biochemistry
Bioorganic Chemistry
brief-communication
Cell Biology
Cellular biology
Chemistry
Chemistry and Materials Science
Chemistry/Food Science
Down-Regulation - drug effects
Endothelium - drug effects
Endothelium - metabolism
Flow Cytometry
Fluorescent Dyes - chemistry
Fluorescent Dyes - metabolism
Gene expression
Gene Knock-In Techniques
Green Fluorescent Proteins - chemistry
Green Fluorescent Proteins - metabolism
Lymphocytes
Lymphocytes - drug effects
Lymphocytes - metabolism
Mice
Multiple sclerosis
Multiple Sclerosis - drug therapy
Multiple Sclerosis - metabolism
Multiple Sclerosis - pathology
Physiology
Receptors, Lysosphingolipid - agonists
Receptors, Lysosphingolipid - metabolism
Receptors, Lysosphingolipid - therapeutic use
Rodents
Time Factors
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Zusammenfassung:A selective, short-acting agonist for the sphingosine-1-phosphate receptor S1P 1 and GFP-S1P 1 knock-in mouse model are used to show that both receptor degradation and receptor reserve underlie the mechanisms of lymphocyte sequestration by agonists. Sphingosine 1-phosphate receptor 1 (S1P 1 ) is critical for lymphocyte recirculation and is a clinical target for treatment of multiple sclerosis. By generating a short-duration S1P 1 agonist and mice in which fluorescently tagged S1P 1 replaces wild-type receptor, we elucidate physiological and agonist-perturbed changes in expression of S1P 1 at a subcellular level in vivo . We demonstrate differential downregulation of S1P 1 on lymphocytes and endothelia after agonist treatment.
ISSN:1552-4450
1552-4469
DOI:10.1038/nchembio.547