Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)

Poster by Kyung Chul Shin, Gowher Ali, Houda Yasmine Ali Moussa, Lawrence W. Stanton, and Yongsoo Park (Hamad Bin Khalifa University) Background: Autism spectrum disorder (ASD) is a complex and heterogeneous neurodevelopmental disorder, mainly...

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المؤلف الرئيسي:	Kyung Chul Shin (13913556) (author)
مؤلفون آخرون:	Gowher Ali (14152593) (author), Houda Yasmine Ali Moussa (15431071) (author), Lawrence W. Stanton (173039) (author), Yongsoo Park (14152824) (author)
منشور في:	2023
الموضوعات:	Biomedical and clinical sciences Medical biotechnology TRPC6 Cation Channel Autism Store-operated calcium entry (SOCE) Action potential Hyperactivity
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_version_	1864513531420868608
author	Kyung Chul Shin (13913556)
author2	Gowher Ali (14152593) Houda Yasmine Ali Moussa (15431071) Lawrence W. Stanton (173039) Yongsoo Park (14152824)
author2_role	author author author author
author_facet	Kyung Chul Shin (13913556) Gowher Ali (14152593) Houda Yasmine Ali Moussa (15431071) Lawrence W. Stanton (173039) Yongsoo Park (14152824)
author_role	author
dc.creator.none.fl_str_mv	Kyung Chul Shin (13913556) Gowher Ali (14152593) Houda Yasmine Ali Moussa (15431071) Lawrence W. Stanton (173039) Yongsoo Park (14152824)
dc.date.none.fl_str_mv	2023-05-17T12:13:21Z
dc.identifier.none.fl_str_mv	10.57945/manara.22785860.v1
dc.relation.none.fl_str_mv	https://figshare.com/articles/poster/Mutation_of_TRPC6_autism_candidate_gene_induces_hyperexcitability_of_neurons_by_reducing_store-operated_calcium_entry_SOCE_/22785860
dc.rights.none.fl_str_mv	CC BY 4.0 info:eu-repo/semantics/openAccess
dc.subject.none.fl_str_mv	Biomedical and clinical sciences Medical biotechnology TRPC6 Cation Channel Autism Store-operated calcium entry (SOCE) Action potential Hyperactivity
dc.title.none.fl_str_mv	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
dc.type.none.fl_str_mv	Image Poster info:eu-repo/semantics/publishedVersion image
description	<p><strong>Poster by Kyung Chul Shin, Gowher Ali, Houda Yasmine Ali Moussa, Lawrence W. Stanton, and Yongsoo Park (Hamad Bin Khalifa University)</strong></p> <p>Background: Autism spectrum disorder (ASD) is a complex and heterogeneous neurodevelopmental disorder, mainly caused by rare and de novo genetic variants and mutations. ASD co-occurs with comorbid attention-deficit hyperactivity disorder (ADHD) and epilepsy, which are associated with hyperexcitability of neurons. TRPC6 is a candidate risk factor for ASD and implicated in ASD etiology; de novo missense and nonsense mutations in TRPC6 associated with ASD etiology have been reported. Loss-of-function mutations in TRPC6 reduce calcium influx in human induced pluripotent stem cell (hiPSC)‐derived neurons cell and TRPC6 knockdown (KD) in Drosophila as a ASD animal model causes autism-like behavioral deficits and leads to the hyperactivity phenotype. However, the pathophysiology underlying hyperactivity phenotype caused by TRPC6 mutations in ASD is unclear and mains poorly understood.</p> <p>Objective: We aim to study novel pathophysiological mechanisms of ASD using human pluripotent stem cell technology that offer a platform to model pathology of ASD.</p> <p>Methods: Using hiPSC‐derived cortical neurons, single cell calcium imaging, and electrophysiological recording, we study how TRPC6 knockout (KO) leads to hyperactivity of neurons.</p> <p>Results: We show that TRPC6 KO reduces store-operated Ca2+ entry (SOCE) signaling and leads to hyperexcitability of neurons by increasing action potential frequency and network burst frequency. Our data show the molecular and cellular pathophysiology underlying hyperactivity of ASD individuals, and TRPC6 KO hiPSC-derived cortical neurons can be a good model to study hyperactive behavior of ASD. TRPC6 KO neurons will be used to screen therapeutics that rescue SOCE and reverse hyperexcitability.</p> <p>Conclusion: Our data unveil the molecular and cellular pathophysiology underlying hyperactivity of ASD individuals and TRPC6 KD hiPSC-derived cortical neurons as a platform to model neuropathology of ASD will pave the way for further studies to discover therapeutics for intervention of ASD.</p>
eu_rights_str_mv	openAccess
id	Manara2_40ad337ca9b510c80249e55b8d839099
identifier_str_mv	10.57945/manara.22785860.v1
network_acronym_str	Manara2
network_name_str	Manara2
oai_identifier_str	oai:figshare.com:article/22785860
publishDate	2023
repository.mail.fl_str_mv
repository.name.fl_str_mv
repository_id_str
rights_invalid_str_mv	CC BY 4.0
spelling	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)Kyung Chul Shin (13913556)Gowher Ali (14152593)Houda Yasmine Ali Moussa (15431071)Lawrence W. Stanton (173039)Yongsoo Park (14152824)Biomedical and clinical sciencesMedical biotechnologyTRPC6 Cation ChannelAutismStore-operated calcium entry (SOCE)Action potentialHyperactivity<p><strong>Poster by Kyung Chul Shin, Gowher Ali, Houda Yasmine Ali Moussa, Lawrence W. Stanton, and Yongsoo Park (Hamad Bin Khalifa University)</strong></p> <p>Background: Autism spectrum disorder (ASD) is a complex and heterogeneous neurodevelopmental disorder, mainly caused by rare and de novo genetic variants and mutations. ASD co-occurs with comorbid attention-deficit hyperactivity disorder (ADHD) and epilepsy, which are associated with hyperexcitability of neurons. TRPC6 is a candidate risk factor for ASD and implicated in ASD etiology; de novo missense and nonsense mutations in TRPC6 associated with ASD etiology have been reported. Loss-of-function mutations in TRPC6 reduce calcium influx in human induced pluripotent stem cell (hiPSC)‐derived neurons cell and TRPC6 knockdown (KD) in Drosophila as a ASD animal model causes autism-like behavioral deficits and leads to the hyperactivity phenotype. However, the pathophysiology underlying hyperactivity phenotype caused by TRPC6 mutations in ASD is unclear and mains poorly understood.</p> <p>Objective: We aim to study novel pathophysiological mechanisms of ASD using human pluripotent stem cell technology that offer a platform to model pathology of ASD.</p> <p>Methods: Using hiPSC‐derived cortical neurons, single cell calcium imaging, and electrophysiological recording, we study how TRPC6 knockout (KO) leads to hyperactivity of neurons.</p> <p>Results: We show that TRPC6 KO reduces store-operated Ca2+ entry (SOCE) signaling and leads to hyperexcitability of neurons by increasing action potential frequency and network burst frequency. Our data show the molecular and cellular pathophysiology underlying hyperactivity of ASD individuals, and TRPC6 KO hiPSC-derived cortical neurons can be a good model to study hyperactive behavior of ASD. TRPC6 KO neurons will be used to screen therapeutics that rescue SOCE and reverse hyperexcitability.</p> <p>Conclusion: Our data unveil the molecular and cellular pathophysiology underlying hyperactivity of ASD individuals and TRPC6 KD hiPSC-derived cortical neurons as a platform to model neuropathology of ASD will pave the way for further studies to discover therapeutics for intervention of ASD.</p>2023-05-17T12:13:21ZImagePosterinfo:eu-repo/semantics/publishedVersionimage10.57945/manara.22785860.v1https://figshare.com/articles/poster/Mutation_of_TRPC6_autism_candidate_gene_induces_hyperexcitability_of_neurons_by_reducing_store-operated_calcium_entry_SOCE_/22785860CC BY 4.0info:eu-repo/semantics/openAccessoai:figshare.com:article/227858602023-05-17T12:13:21Z
spellingShingle	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE) Kyung Chul Shin (13913556) Biomedical and clinical sciences Medical biotechnology TRPC6 Cation Channel Autism Store-operated calcium entry (SOCE) Action potential Hyperactivity
status_str	publishedVersion
title	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
title_full	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
title_fullStr	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
title_full_unstemmed	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
title_short	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
title_sort	Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)
topic	Biomedical and clinical sciences Medical biotechnology TRPC6 Cation Channel Autism Store-operated calcium entry (SOCE) Action potential Hyperactivity

Mutation of TRPC6, autism candidate gene, induces hyperexcitability of neurons by reducing store-operated calcium entry (SOCE)

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