Rare Variant Burden Analysis within Enhancers Identifies CAV1 as an ALS Risk Gene

Cooper-Knock, J.; Zhang, S.; Kenna, K.P.; Moll, T.; Franklin, J.P.; Allen, S.; Nezhad, H.G.; Iacoangeli, A.; Yacovzada, N.Y.; Eitan, C.; Hornstein, E.; Ehilak, E.; Celadova, P.; Bose, D.; Farhan, S.; Fishilevich, S.; Lancet, D.; Morrison, K.E.; Shaw, C.E.; Al-Chalabi, A.; Blair, I.; Wray, N.; Kiernan, M.; Neto, M.M.; Chio, A.; Cauchi, R.; Robberecht, W.; van Damme, P.; Corcia, P.; Couratier, P.; Hardiman, O.; Mclaughlin, R.; Gotkine, M.; Drory, V.; Ticozzi, N.; Silani, V.; Veldink, J.; van den Berg, L.; de Carvalho, M.; Pardina, J.M.; Povedano, M.; Andersen, P.; Wber, M.; Basak, N.; Morrison, K.; Landers, J.; Glass, J.; Veldink, J.H.; Kirby, J.; Snyder, M.P.; Shaw, P.J.

doi:10.1016/j.celrep.2020.108456

Amyotrophic lateral sclerosis (ALS) is an incurable neurodegenerative disease. CAV1 and CAV2 organize membrane lipid rafts (MLRs) important for cell signaling and neuronal survival, and overexpression of CAV1 ameliorates ALS phenotypes in vivo. Genome-wide association studies localize a large proportion of ALS risk variants within the non-coding genome, but further characterization has been limited by lack of appropriate tools. By designing and applying a pipeline to identify pathogenic genetic variation within enhancer elements responsible for regulating gene expression, we identify disease-associated variation within CAV1/CAV2 enhancers, which replicate in an independent cohort. Discovered enhancer mutations reduce CAV1/CAV2 expression and disrupt MLRs in patient-derived cells, and CRISPR-Cas9 perturbation proximate to a patient mutation is sufficient to reduce CAV1/CAV2 expression in neurons. Additional enrichment of ALS-associated mutations within CAV1 exons positions CAV1 as an ALS risk gene. We propose CAV1/CAV2 overexpression as a personalized medicine target for ALS.

Rare Variant Burden Analysis within Enhancers Identifies CAV1 as an ALS Risk Gene / J. Cooper-Knock, S. Zhang, K.P. Kenna, T. Moll, J.P. Franklin, S. Allen, H.G. Nezhad, A. Iacoangeli, N.Y. Yacovzada, C. Eitan, E. Hornstein, E. Ehilak, P. Celadova, D. Bose, S. Farhan, S. Fishilevich, D. Lancet, K.E. Morrison, C.E. Shaw, A. Al-Chalabi, I. Blair, N. Wray, M. Kiernan, M.M. Neto, A. Chio, R. Cauchi, W. Robberecht, P. van Damme, P. Corcia, P. Couratier, O. Hardiman, R. Mclaughlin, M. Gotkine, V. Drory, N. Ticozzi, V. Silani, J. Veldink, L. van den Berg, M. de Carvalho, J.M. Pardina, M. Povedano, P. Andersen, M. Wber, N. Basak, K. Morrison, J. Landers, J. Glass, J.H. Veldink, J. Kirby, M.P. Snyder, P.J. Shaw. - In: CELL REPORTS. - ISSN 2211-1247. - 33:9(2020 Dec), pp. 108456.1-108456.16. [10.1016/j.celrep.2020.108456]

Rare Variant Burden Analysis within Enhancers Identifies CAV1 as an ALS Risk Gene

Cooper-Knock J.;Zhang S.;Kenna K. P.;Moll T.;Franklin J. P.;Allen S.;Nezhad H. G.;Iacoangeli A.;Yacovzada N. Y.;Eitan C.;Hornstein E.;Ehilak E.;Celadova P.;Bose D.;Farhan S.;Fishilevich S.;Lancet D.;Morrison K. E.;Shaw C. E.;Al-Chalabi A.;Blair I.;Wray N.;Kiernan M.;Neto M. M.;Chio A.;Cauchi R.;Robberecht W.;van Damme P.;Corcia P.;Couratier P.;Hardiman O.;McLaughlin R.;Gotkine M.;Drory V.;N. Ticozzi^{Membro del Collaboration Group};V. Silani^{Membro del Collaboration Group};Veldink J.;van den Berg L.;de Carvalho M.;Pardina J. M.;Povedano M.;Andersen P.;Wber M.;Basak N.;Morrison K.;Landers J.;Glass J.;Veldink J. H.;Kirby J.;Snyder M. P.;Shaw P. J.

2020

Abstract

Amyotrophic lateral sclerosis (ALS) is an incurable neurodegenerative disease. CAV1 and CAV2 organize membrane lipid rafts (MLRs) important for cell signaling and neuronal survival, and overexpression of CAV1 ameliorates ALS phenotypes in vivo. Genome-wide association studies localize a large proportion of ALS risk variants within the non-coding genome, but further characterization has been limited by lack of appropriate tools. By designing and applying a pipeline to identify pathogenic genetic variation within enhancer elements responsible for regulating gene expression, we identify disease-associated variation within CAV1/CAV2 enhancers, which replicate in an independent cohort. Discovered enhancer mutations reduce CAV1/CAV2 expression and disrupt MLRs in patient-derived cells, and CRISPR-Cas9 perturbation proximate to a patient mutation is sufficient to reduce CAV1/CAV2 expression in neurons. Additional enrichment of ALS-associated mutations within CAV1 exons positions CAV1 as an ALS risk gene. We propose CAV1/CAV2 overexpression as a personalized medicine target for ALS.

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Scheda completa

Scheda completa (DC)

	Parole chiave
	
				amyotrophic lateral sclerosis; CAV1; CAV2; gene enhancers; membrane lipid rafts; non-coding DNA; whole-genome sequencing
			
	Settori scientifico-disciplinari dell'articolo (validi dal 09/05/2024)
	
				Settore MEDS-12/A - Neurologia
			
	Titolo del progetto
	
	Titolo Progetto
	
									Emerging Simplex ORigins In ALS
								
	Acronimo
	
									EScORIAL
								
	Nome finanziatore
	
										European Commission
									
	Finanziamento
	
									Horizon 2020 Framework Programme
								
	N. Contratto
	
									772376
								
	Data di pubblicazione
	
				dic-2020
			
	Rivista in ANCE
	
				CELL REPORTS
			
	DOI
	
				https://dx.doi.org/10.1016/j.celrep.2020.108456
			
	Tipologia
	
				Article (author)
			
	Appare nelle tipologie:
	
				01 - Articolo su periodico

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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/1152593

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