The formyl peptide receptor agonist FPRa14 induces differentiation of Neuro2a mouse neuroblastoma cells into multiple distinct morphologies which can be specifically inhibited with FPR antagonists and FPR knockdown using siRNA

The N-formyl peptide receptors (FPRs) have been identified within neuronal tissues and may serve as yet undetermined functions within the nervous system. The FPRs have been implicated in the progression and invasiveness of neuroblastoma and other cancers. In this study the effects of the synthetic F...

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Published in	PloS one Vol. 14; no. 6; p. e0217815
Main Authors	Cussell, Peter J G, Howe, Michael S, Illingworth, Thomas A, Gomez Escalada, Margarita, Milton, Nathaniel G N, Paterson, Andrew W J
Format	Journal Article
Language	English
Published	United States Public Library of Science 06.06.2019 Public Library of Science (PLoS)
Subjects	Agonists Alzheimer's disease Animals Biology Biology and Life Sciences Cancer Cancer research Care and treatment Cell Death - drug effects Cell differentiation Cell Differentiation - drug effects Cell Line, Tumor Cell Shape - drug effects Central nervous system Differentiation (biology) Formyl peptide receptors G proteins Genetic aspects Growth factors Humans Invasiveness Kinases Ligands Medicine and Health Sciences Mice Morphology Motility Nervous system Neuralgia Neuroblastoma Neuroblastoma - pathology Neuroblastoma cells Neuroblasts Neurons Neuropathy Neutrophils Novels Oxidative stress Pain Parkinson's disease Peptides Physical Sciences Physiology Proteins Receptors Receptors, Formyl Peptide - agonists Receptors, Formyl Peptide - antagonists & inhibitors Receptors, Formyl Peptide - metabolism Regeneration Research and analysis methods Risk factors RNA interference RNA, Small Interfering - metabolism siRNA Time Factors Toxicity United Kingdom > UK
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Abstract	The N-formyl peptide receptors (FPRs) have been identified within neuronal tissues and may serve as yet undetermined functions within the nervous system. The FPRs have been implicated in the progression and invasiveness of neuroblastoma and other cancers. In this study the effects of the synthetic FPR agonist FPRa14, FPR antagonists and FPR knockdown using siRNA on mouse neuroblastoma neuro2a (N2a) cell differentiation plus toxicity were examined. The FPRa14 (1-10μM) was found to induce a significant dose-dependent differentiation response in mouse neuroblastoma N2a cells. Interestingly, three distinct differentiated morphologies were observed, with two non-archetypal forms observed at the higher FPRa14 concentrations. These three forms were also observed in the human neuroblastoma cell-lines IMR-32 and SH-SY5Y when exposed to 100μM FPRa14. In N2a cells combined knockdown of FPR1 and FPR2 using siRNA inhibited the differentiation response to FPRa14, suggesting involvement of both receptor subtypes. Pre-incubating N2a cultures with the FPR1 antagonists Boc-MLF and cyclosporin H significantly reduced FPRa14-induced differentiation to near baseline levels. Meanwhile, the FPR2 antagonist WRW4 had no significant effect on FPRa14-induced N2a differentiation. These results suggest that the N2a differentiation response observed has an FPR1-dependent component. Toxicity of FPRa14 was only observed at higher concentrations. All three antagonists used blocked FPRa14-induced toxicity, whilst only siRNA knockdown of FPR2 reduced toxicity. This suggests that the toxicity and differentiation involve different mechanisms. The demonstration of neuronal differentiation mediated via FPRs in this study represents a significant finding and suggests a role for FPRs in the CNS. This finding could potentially lead to novel therapies for a range of neurological conditions including neuroblastoma, Alzheimer's disease, Parkinson's disease and neuropathic pain. Furthermore, this could represent a potential avenue for neuronal regeneration therapies.
AbstractList	The N-formyl peptide receptors (FPRs) have been identified within neuronal tissues and may serve as yet undetermined functions within the nervous system. The FPRs have been implicated in the progression and invasiveness of neuroblastoma and other cancers. In this study the effects of the synthetic FPR agonist FPRa14, FPR antagonists and FPR knockdown using siRNA on mouse neuroblastoma neuro2a (N2a) cell differentiation plus toxicity were examined. The FPRa14 (1–10μM) was found to induce a significant dose-dependent differentiation response in mouse neuroblastoma N2a cells. Interestingly, three distinct differentiated morphologies were observed, with two non-archetypal forms observed at the higher FPRa14 concentrations. These three forms were also observed in the human neuroblastoma cell-lines IMR-32 and SH-SY5Y when exposed to 100μM FPRa14. In N2a cells combined knockdown of FPR1 and FPR2 using siRNA inhibited the differentiation response to FPRa14, suggesting involvement of both receptor subtypes. Pre-incubating N2a cultures with the FPR1 antagonists Boc-MLF and cyclosporin H significantly reduced FPRa14-induced differentiation to near baseline levels. Meanwhile, the FPR2 antagonist WRW4 had no significant effect on FPRa14-induced N2a differentiation. These results suggest that the N2a differentiation response observed has an FPR1-dependent component. Toxicity of FPRa14 was only observed at higher concentrations. All three antagonists used blocked FPRa14-induced toxicity, whilst only siRNA knockdown of FPR2 reduced toxicity. This suggests that the toxicity and differentiation involve different mechanisms. The demonstration of neuronal differentiation mediated via FPRs in this study represents a significant finding and suggests a role for FPRs in the CNS. This finding could potentially lead to novel therapies for a range of neurological conditions including neuroblastoma, Alzheimer’s disease, Parkinson’s disease and neuropathic pain. Furthermore, this could represent a potential avenue for neuronal regeneration therapies. The N-formyl peptide receptors (FPRs) have been identified within neuronal tissues and may serve as yet undetermined functions within the nervous system. The FPRs have been implicated in the progression and invasiveness of neuroblastoma and other cancers. In this study the effects of the synthetic FPR agonist FPRa14, FPR antagonists and FPR knockdown using siRNA on mouse neuroblastoma neuro2a (N2a) cell differentiation plus toxicity were examined. The FPRa14 (1-10[mu]M) was found to induce a significant dose-dependent differentiation response in mouse neuroblastoma N2a cells. Interestingly, three distinct differentiated morphologies were observed, with two non-archetypal forms observed at the higher FPRa14 concentrations. These three forms were also observed in the human neuroblastoma cell-lines IMR-32 and SH-SY5Y when exposed to 100[mu]M FPRa14. In N2a cells combined knockdown of FPR1 and FPR2 using siRNA inhibited the differentiation response to FPRa14, suggesting involvement of both receptor subtypes. Pre-incubating N2a cultures with the FPR1 antagonists Boc-MLF and cyclosporin H significantly reduced FPRa14-induced differentiation to near baseline levels. Meanwhile, the FPR2 antagonist WRW4 had no significant effect on FPRa14-induced N2a differentiation. These results suggest that the N2a differentiation response observed has an FPR1-dependent component. Toxicity of FPRa14 was only observed at higher concentrations. All three antagonists used blocked FPRa14-induced toxicity, whilst only siRNA knockdown of FPR2 reduced toxicity. This suggests that the toxicity and differentiation involve different mechanisms. The demonstration of neuronal differentiation mediated via FPRs in this study represents a significant finding and suggests a role for FPRs in the CNS. This finding could potentially lead to novel therapies for a range of neurological conditions including neuroblastoma, Alzheimer's disease, Parkinson's disease and neuropathic pain. Furthermore, this could represent a potential avenue for neuronal regeneration therapies.
Audience	Academic
Author	Paterson, Andrew W J Howe, Michael S Gomez Escalada, Margarita Illingworth, Thomas A Milton, Nathaniel G N Cussell, Peter J G
AuthorAffiliation	Universite de Rouen, FRANCE School of Clinical and Applied Sciences, Leeds Beckett University, Leeds, United Kingdom
AuthorAffiliation_xml	– name: Universite de Rouen, FRANCE – name: School of Clinical and Applied Sciences, Leeds Beckett University, Leeds, United Kingdom
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Notes	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 Competing Interests: N.G.N.M. is named as the inventor on a UK patent held by the University of Roehampton for the use of kissorphin peptides to treat Alzheimer’s disease, Creutzfeldt-Jakob disease or diabetes mellitus (Publication Numbers: GB2493313 B); under the University of Roehampton rules he could benefit financially if the patent is commercially exploited. N.G.N.M. is also a shareholder and director of NeuroDelta Ltd (Company No: 06222473; http://www.neurodelta.uk). This does not alter our adherence to PLOS ONE policies on sharing data and materials. The reference for this patent is: Milton, N. (2017) Kissorphin peptides for use in the treatment of Alzheimer's disease, Creutzfeldt-Jakob disease or diabetes mellitus. United Kingdom Patent Publication Number GB 2493313 (B).
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Snippet	The N-formyl peptide receptors (FPRs) have been identified within neuronal tissues and may serve as yet undetermined functions within the nervous system. The...
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SubjectTerms	Agonists Alzheimer's disease Animals Biology Biology and Life Sciences Cancer Cancer research Care and treatment Cell Death - drug effects Cell differentiation Cell Differentiation - drug effects Cell Line, Tumor Cell Shape - drug effects Central nervous system Differentiation (biology) Formyl peptide receptors G proteins Genetic aspects Growth factors Humans Invasiveness Kinases Ligands Medicine and Health Sciences Mice Morphology Motility Nervous system Neuralgia Neuroblastoma Neuroblastoma - pathology Neuroblastoma cells Neuroblasts Neurons Neuropathy Neutrophils Novels Oxidative stress Pain Parkinson's disease Peptides Physical Sciences Physiology Proteins Receptors Receptors, Formyl Peptide - agonists Receptors, Formyl Peptide - antagonists & inhibitors Receptors, Formyl Peptide - metabolism Regeneration Research and analysis methods Risk factors RNA interference RNA, Small Interfering - metabolism siRNA Time Factors Toxicity
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Title	The formyl peptide receptor agonist FPRa14 induces differentiation of Neuro2a mouse neuroblastoma cells into multiple distinct morphologies which can be specifically inhibited with FPR antagonists and FPR knockdown using siRNA
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