Desensitisation of protease‐activated receptor‐1 (PAR‐1) in rat astrocytes: evidence for a novel mechanism for terminating Ca2+ signalling evoked by the tethered ligand
- 1 June 2000
- journal article
- Published by Wiley in The Journal of Physiology
- Vol. 525 (2) , 319-330
- https://doi.org/10.1111/j.1469-7793.2000.00319.x
Abstract
Protease-activated receptor-1 (PAR-1), a G-protein-coupled receptor, is activated when thrombin cleaves its N-terminal exodomain, thereby regulating morphology, growth and survival of neurones and astrocytes. We have investigated the mechanism of PAR-1 desensitisation and resensitisation after proteolytic or non-proteolytic stimulation with thrombin or thrombin receptor agonist peptide (TRag), respectively. In rat primary astrocytes, short-term stimulation with thrombin resulted in a single [Ca2+]i transient and a dose-dependent de- and resensitisation, as assessed by single-cell Ca2+ imaging of fura-2-loaded astrocytes. An initial proteolytic activation of astrocyte PAR-1 by exposure to thrombin strongly decreased the response elicited by subsequent application of a second dose of thrombin or of TRag. In contrast, after an initial non-proteolytic activation of astrocyte PAR-1 by TRag, the subsequent response to thrombin, but not to an additional application of TRag, was strongly attenuated, and the time course for desensitisation was slower. Based on this finding we hypothesised that after PAR-1 activation, the 'tethered ligand' is proteolytically destroyed. As a consequence, the receptor becomes unresponsive to a subsequent thrombin stimulus but is still capable of responding to TRag. This hypothesis was supported by applying thermolysin, which is known to cleave PAR-1 within its tethered-ligand domain, and was confirmed by incubation with soybean trypsin inhibitor. PAR-1 resensitisation occurs via new PAR-1 synthesis since resensitisation was inhibited by cycloheximide and brefeldin A. From these results, we derive a novel model wherein activation of PAR-1, in addition to initiating signal transduction, activates a protease mechanism that cleaves the N-terminus of the receptor, thus terminating the signal and probably inducing receptor internalisation.Keywords
This publication has 49 references indexed in Scilit:
- Plasmin Desensitization of the PAR1 Thrombin Receptor: Kinetics, Sites of Truncation, and Implications for Thrombolytic TherapyBiochemistry, 1999
- Thrombin is an extracellular signal that activates intracellular death protease pathways inducing apoptosis in model motor neuronsJournal of Neurobiology, 1998
- Protease-activated receptor 3 is a second thrombin receptor in humansNature, 1997
- Thrombin Attenuates Neuronal Cell Death and Modulates Astrocyte Reactivity Induced by β‐Amyloid In VitroJournal of Neurochemistry, 1996
- Differentiation of the Two Forms of GPIb Functioning as Receptors for α-Thrombin and von Willebrand Factor: Ca2+ Responses of Protease-Treated Human Platelets Activated with α-Thrombin and the Tethered Ligand PeptideBiochemistry, 1996
- Mechanisms of Thrombin Receptor Agonist SpecificityJournal of Biological Chemistry, 1995
- Regulation of Thrombin Receptors on Human Umbilical Vein Endothelial CellsPublished by Elsevier ,1995
- Specificity of the thrombin receptor for agonist peptide is defined by its extracellular surfaceNature, 1994
- Thrombin receptor peptides induce shape change in neonatal murine astrocytes in cultureJournal of Neuroscience Research, 1994
- Molecular cloning of a functional thrombin receptor reveals a novel proteolytic mechanism of receptor activationCell, 1991