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Tissue‐type plasminogen activator induces plasmin‐dependent proteolysis of intracellular neuronal nitric oxide synthase
Authors:Amandine Baron  Yannick Hommet  Frédéric Cassé  Denis Vivien
Institution:1. INSERM U919, Serine Proteases and Pathophysiology of the Neurovascular Unit (SP2U), Cyceron, Caen Cedex F‐14074, France;2. University of Caen Basse‐Normandie, Caen Cedex F‐14074, France;3. CNRS, UMR CNRS 6232 Ci‐NAPs ‘Center for Imaging—Neurosciences and Application to Pathologies’, Cyceron, Caen Cedex F‐14074, France
Abstract:Background information. Despite its pro‐fibrinolytic activity, tPA (tissue plasminogen activator) is a serine protease known to influence a number of physiological and pathological functions in the central nervous system. Accordingly, tPA was reported to mediate some of its functions in the central nervous system through NMDA (N‐methyl‐d ‐aspartate) receptors, LRP (low‐density lipoprotein receptor‐related protein) or annexin II. Results. We provide here both in vitro and in vivo evidence that tPA could mediate proteolysis and subsequent delocalization of neuronal nitric oxide synthase, thereby reducing endogenous neuronal nitric oxide release. We also demonstrate that although this effect is independent of NMDA receptors, LRP signalling and calpain‐mediated proteolysis, it is dependent on the ability of tPA to promote the conversion of plasminogen into plasmin. Conclusion. Altogether, these results demonstrate a new function for tPA in the central nervous system, which most likely contributes to its pleiotropic functions.
Keywords:neuron  neuronal nitric oxide synthase  plasmin  proteolysis  tissue‐type plasminogen activator
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