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Effect of Hypothalamic Proline-Rich Peptide (PRP-1) on Neuronal and Bone Marrow Cell Apoptosis
Authors:Armen A Galoyan  Josef Krieglstein  Susanne Klumpp  Kristina E Danielian  Karine A Galoian  Wolfram Kremers  Kristina B Bezirganyan  Tigran K Davtyan
Institution:(1) Buniatian Institute of Biochemistry of NAS RA, Yerevan, Republic of Armenia;(2) Institute for Pharmaceutical and Medicinal Chemistry, University Muenster, Muenster, Germany;(3) Institute of Pharmacology and Toxicology, University of Marburg, Marburg, Germany;(4) Department of Orthopedics, University of Miami Miller School of Medicine, Miami, FL, USA;(5) Laboratory of Immunology and Virology, Armenicum Research Center, CJSC Armenicun, 37 Nalbandyan Street, Yerevan, 375001, Republic of Armenia
Abstract:The AGAPEPAEPAQPGVY proline-rich peptide (PRP-1) was isolated from neurosecretory granules of the bovine neurohypophysis; it is produced by N. supraopticus and N. paraventricularis. It has been shown that PRP-1 has many potentially beneficial biological effects including immunoregulatory, hematopoietic, antimicrobial and anti-neurodegenerative properties. Here we investigated the influence of PRP-1 on staurosporine-induced apoptosis of postnatal hippocampal cells and on doxorubicin-induced bone marrow granulocyte- and monocyte apoptosis. The intention was to further characterize the effect of PRP-1 on the survival rate of neurons and in context with myelopoiesis. We demonstrate that PRP-1 significantly reduced apoptosis of postnatal hippocampal cells induced by staurosporine. The protective effect of PRP-1 against apoptotic cell death was shown to be both time- and dose-dependent. Neuroprotection was more pronounced after prolonged pretreatment of the cells with PRP-1 before the induction of apoptosis with staurosporine. The related peptide arg8]vasopressin did not reveal neuroprotection. PRP-1 also significantly reduced apoptosis of bone marrow monocytes and granulocytes induced by doxorubicin. This protective effect lasted for 2-4 h and was not detectable anymore after 24 h when PRP-1 and doxorubicin were added simultaneously. Previously obtained data and results of the current studies suggested that the hypothalamic PRP-1 possibly represents an endogenous peptide whose primary functions are to regulate myelopoiesis and neuron survival as we provide evidence that PRP can differentially reduce both staurosporine- and doxorubicin-induced hippocampal and bone marrow cell apoptosis.
Keywords:Hypothalamic proline-rich polypeptide  Staurosporine- and doxorubicin-induced apoptosis  Postnatal hippocampal cells  Bone marrow granulocytes
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