TDP-43 loss and ALS-risk SNPs drive mis-splicing and depletion of UNC13A

Brown A.-L., Wilkins O.G., Keuss M.J., Hill S.E., Zanovello M., Lee W.C., Bampton A., Lee F.C.Y., Masino L., Qi Y.A., Bryce-Smith S., Gatt A., Hallegger M., Fagegaltier D., Phatnani H., Phatnani H., Kwan J., Sareen D., Broach J.R., Simmons Z., Arcila-Londono X., Lee E.B., Van Deerlin V.M., Shneider N.A., Fraenkel E., Ostrow L.W., Baas F., Zaitlen N., Berry J.D., Malaspina A., Fratta P., Cox G.A., Thompson L.M., Finkbeiner S., Dardiotis E., Miller T.M., Chandran S., Pal S., Hornstein E., MacGowan D.J., Heiman-Patterson T., Hammell M.G., Patsopoulos N.A., Butovsky O., Dubnau J., Nath A., Bowser R., Harms M., Aronica E., Poss M., Phillips-Cremins J., Crary J., Atassi N., Lange D.J., Adams D.J., Stefanis L., Gotkine M., Baloh R.H., Babu S., Raj T., Paganoni S., Shalem O., Smith C., Zhang B., Harris B., Broce I., Drory V., Ravits J., McMillan C., Menon V., Wu L., Altschuler S., Lerner Y., Sattler R., Van Keuren-Jensen K., Rozenblatt-Rosen O., Lindblad-Toh K., Nicholson K., Gregersen P., Lee J.-H., Kokos S., Muljo S., Newcombe J., Gustavsson E.K., Seddighi S., Reyes J.F., Coon S.L., Ramos D., Schiavo G., Fisher E.M.C., Raj T., Secrier M., Lashley T., Ule J., Buratti E., Humphrey J., Ward M.E., Fratta P., NYGC ALS Consortium

dc.creator	Brown A.-L., Wilkins O.G., Keuss M.J., Hill S.E., Zanovello M., Lee W.C., Bampton A., Lee F.C.Y., Masino L., Qi Y.A., Bryce-Smith S., Gatt A., Hallegger M., Fagegaltier D., Phatnani H., Phatnani H., Kwan J., Sareen D., Broach J.R., Simmons Z., Arcila-Londono X., Lee E.B., Van Deerlin V.M., Shneider N.A., Fraenkel E., Ostrow L.W., Baas F., Zaitlen N., Berry J.D., Malaspina A., Fratta P., Cox G.A., Thompson L.M., Finkbeiner S., Dardiotis E., Miller T.M., Chandran S., Pal S., Hornstein E., MacGowan D.J., Heiman-Patterson T., Hammell M.G., Patsopoulos N.A., Butovsky O., Dubnau J., Nath A., Bowser R., Harms M., Aronica E., Poss M., Phillips-Cremins J., Crary J., Atassi N., Lange D.J., Adams D.J., Stefanis L., Gotkine M., Baloh R.H., Babu S., Raj T., Paganoni S., Shalem O., Smith C., Zhang B., Harris B., Broce I., Drory V., Ravits J., McMillan C., Menon V., Wu L., Altschuler S., Lerner Y., Sattler R., Van Keuren-Jensen K., Rozenblatt-Rosen O., Lindblad-Toh K., Nicholson K., Gregersen P., Lee J.-H., Kokos S., Muljo S., Newcombe J., Gustavsson E.K., Seddighi S., Reyes J.F., Coon S.L., Ramos D., Schiavo G., Fisher E.M.C., Raj T., Secrier M., Lashley T., Ule J., Buratti E., Humphrey J., Ward M.E., Fratta P., NYGC ALS Consortium	en
dc.date.accessioned	2023-01-31T07:40:52Z
dc.date.available	2023-01-31T07:40:52Z
dc.date.issued	2022
dc.identifier	10.1038/s41586-022-04436-3
dc.identifier.issn	00280836
dc.identifier.uri	http://hdl.handle.net/11615/72164
dc.description.abstract	Variants of UNC13A, a critical gene for synapse function, increase the risk of amyotrophic lateral sclerosis and frontotemporal dementia1–3, two related neurodegenerative diseases defined by mislocalization of the RNA-binding protein TDP-434,5. Here we show that TDP-43 depletion induces robust inclusion of a cryptic exon in UNC13A, resulting in nonsense-mediated decay and loss of UNC13A protein. Two common intronic UNC13A polymorphisms strongly associated with amyotrophic lateral sclerosis and frontotemporal dementia risk overlap with TDP-43 binding sites. These polymorphisms potentiate cryptic exon inclusion, both in cultured cells and in brains and spinal cords from patients with these conditions. Our findings, which demonstrate a genetic link between loss of nuclear TDP-43 function and disease, reveal the mechanism by which UNC13A variants exacerbate the effects of decreased TDP-43 function. They further provide a promising therapeutic target for TDP-43 proteinopathies. © 2022, The Author(s).	en
dc.language.iso	en	en
dc.source	Nature	en
dc.source.uri	https://www.scopus.com/inward/record.uri?eid=2-s2.0-85125039190&doi=10.1038%2fs41586-022-04436-3&partnerID=40&md5=6afcbfa9edcc1f8c16aba4b224a8e20f
dc.subject	TAR DNA binding protein	en
dc.subject	DNA binding protein	en
dc.subject	cell component	en
dc.subject	enzyme	en
dc.subject	enzyme activity	en
dc.subject	nervous system disorder	en
dc.subject	polymorphism	en
dc.subject	protein	en
dc.subject	adult	en
dc.subject	amyotrophic lateral sclerosis	en
dc.subject	Article	en
dc.subject	clinical article	en
dc.subject	down regulation	en
dc.subject	exon	en
dc.subject	gene	en
dc.subject	gene knockdown	en
dc.subject	genetic risk	en
dc.subject	human	en
dc.subject	human cell	en
dc.subject	male	en
dc.subject	nerve cell	en
dc.subject	RNA splicing	en
dc.subject	single nucleotide polymorphism	en
dc.subject	UNC13A gene	en
dc.subject	frontotemporal dementia	en
dc.subject	genetics	en
dc.subject	metabolism	en
dc.subject	single nucleotide polymorphism	en
dc.subject	TDP 43 proteinopathy	en
dc.subject	Amyotrophic Lateral Sclerosis	en
dc.subject	DNA-Binding Proteins	en
dc.subject	Frontotemporal Dementia	en
dc.subject	Humans	en
dc.subject	Polymorphism, Single Nucleotide	en
dc.subject	TDP-43 Proteinopathies	en
dc.subject	Nature Research	en
dc.title	TDP-43 loss and ALS-risk SNPs drive mis-splicing and depletion of UNC13A	en
dc.type	journalArticle	en

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