Characterization of human disease phenotypes associated with mutations in TREX1, RNASEH2A, RNASEH2B, RNASEH2C, SAMHD1, ADAR, and IFIH1

Crow, Y.; Chase, D.; Schmidt, J.; Szynkiewicz, M.; Gma, F.; Gornall, H.; Oojageer, A.; Anderson, B.; Pizzino, A.; Helman, G.; Abdel-Hamid, M.; Abdel-Salam, G.; Ackroyd, S.; Aeby, A.; Agosta, G.; Albin, C.; Allon-Shalev, S.; Arellano, M.; Ariaudo, G.; Aswani, V.; Babul-Hirji, R.; Baildam, E.; Bahi-Buisson, N.; Bailey, K.; Barnerias, C.; Barth, M.; Battini, R.; Beresford, M.; Bernard, G.; Bianchi, M.; de Villemeur TB,; Blair, E.; Bloom, M.; Burlina, A.; Carpanelli, M.; Carvalho, D.; Castro-Gago, M.; Cavallini, A.; Cereda, C.; Chandler, K.; Chitayat, D.; Collins, A.; Corcoles, C.; Njv, C.; Crichiutti, G.; Dabydeen, L.; Dale, R.; D'Arrigo, S.; De Goede CGEL,; De Laet, C.; De Waele LMH,; Denzler, I.; Desguerre, I.; Devriendt, K.; Di Rocco, M.; Fahey, M.; Fazzi, E.; Ferrie, C.; Figueiredo, A.; Gener, B.; Goizet, C.; Gowrinathan, N.; Gowrishankar, K.; Hanrahan, D.; Isidor, B.; Kara, L.; Khan, N.; King, M.; Kirk, E.; Kumar, R.; Lagae, L.; Landrieu, P.; Lauffer, H.; Laugel, V.; La Piana, R.; Lim, M.; Jpsm, L.; Linnankivi, T.; Mackay, M.; Marom, D.; Lourenco, C.; Mckee, S.; Moroni, I.; Jev, M.; Moutard, M.; Murray, K.; Nabbout, R.; Nampoothiri, S.; Nunez-Enamorado, N.; Oades, P.; Olivieri, I.; Ostergaard, J.; Perez-Duenas, B.; Prendiville, J.; Ramesh, V.; Rasmussen, M.; Regal, L.; Ricci, F.; Rio, M.; Rodriguez, D.; Roubertie, A.; Salvatici, E.; Segers, K.; Sinha, G.; Soler, D.; Spiegel, R.; Stodberg, T.; Straussberg, R.; Swoboda, K.; Suri, M.; Tacke, U.; Tan, T.; Naude, J.; Teik, K.; Thomas, M.; Till, M.; Tonduti, D.; Valente, E.; Van Coster RN,; van der Knaap MS,; Vassallo, G.; Vijzelaar, R.; Vogt, J.; Wallace, G.; Wassmer, E.; Webb, H.; Whitehouse, W.; Whitney, R.; Zaki, M.; Zuberi, S.; Livingston, J.; Rozenberg, F.; Lebon, P.; Vanderver, A.; Orcesi, S.; Rice, G.

doi:10.1002/ajmg.a.36887

Aicardi-Goutières syndrome is an inflammatory disease occurring due to mutations in any of TREX1, RNASEH2A, RNASEH2B, RNASEH2C, SAMHD1, ADAR or IFIH1. We report on 374 patients from 299 families with mutations in these seven genes. Most patients conformed to one of two fairly stereotyped clinical profiles; either exhibiting an in utero disease-onset (74 patients; 22.8% of all patients where data were available), or a post-natal presentation, usually within the first year of life (223 patients; 68.6%), characterized by a sub-acute encephalopathy and a loss of previously acquired skills. Other clinically distinct phenotypes were also observed; particularly, bilateral striatal necrosis (13 patients; 3.6%) and non-syndromic spastic paraparesis (12 patients; 3.4%). We recorded 69 deaths (19.3% of patients with follow-up data). Of 285 patients for whom data were available, 210 (73.7%) were profoundly disabled, with no useful motor, speech and intellectual function. Chilblains, glaucoma, hypothyroidism, cardiomyopathy, intracerebral vasculitis, peripheral neuropathy, bowel inflammation and systemic lupus erythematosus were seen frequently enough to be confirmed as real associations with the Aicardi-Goutieres syndrome phenotype. We observed a robust relationship between mutations in all seven genes with increased type I interferon activity in cerebrospinal fluid and serum, and the increased expression of interferon-stimulated gene transcripts in peripheral blood. We recorded a positive correlation between the level of cerebrospinal fluid interferon activity assayed within one year of disease presentation and the degree of subsequent disability. Interferon-stimulated gene transcripts remained high in most patients, indicating an ongoing disease process. On the basis of substantial morbidity and mortality, our data highlight the urgent need to define coherent treatment strategies for the phenotypes associated with mutations in the Aicardi-Goutières syndrome-related genes. Our findings also make it clear that a window of therapeutic opportunity exists relevant to the majority of affected patients and indicate that the assessment of type I interferon activity might serve as a useful biomarker in future clinical trials.

Characterization of human disease phenotypes associated with mutations in TREX1, RNASEH2A, RNASEH2B, RNASEH2C, SAMHD1, ADAR, and IFIH1 / Y. Crow, D. Chase, J. Schmidt, M. Szynkiewicz, G. Forte, H. Gornall, A. Oojageer, B. Anderson, A. Pizzino, G. Helman, M. Abdel-Hamid, G. Abdel-Salam, S. Ackroyd, A. Aeby, G. Agosta, C. Albin, S. Allon-Shalev, M. Arellano, G. Ariaudo, V. Aswani, R. Babul-Hirji, E. Baildam, N. Bahi-Buisson, K. Bailey, C. Barnerias, M. Barth, R. Battini, M. Beresford, G. Bernard, M. Bianchi, T. de Villemeur, E. Blair, M. Bloom, A. Burlina, M. Carpanelli, D. Carvalho, M. Castro-Gago, A. Cavallini, C. Cereda, K. Chandler, D. Chitayat, A. Collins, C. Corcoles, N. Cordeiro, G. Crichiutti, L. Dabydeen, R. Dale, S. D'Arrigo, C. De Goede, C. De Laet, L. De Waele, I. Denzler, I. Desguerre, K. Devriendt, M. Di Rocco, M. Fahey, E. Fazzi, C. Ferrie, A. Figueiredo, B. Gener, C. Goizet, N. Gowrinathan, K. Gowrishankar, D. Hanrahan, B. Isidor, L. Kara, N. Khan, M. King, E. Kirk, R. Kumar, L. Lagae, P. Landrieu, H. Lauffer, V. Laugel, R. La Piana, M. Lim, J. Lin, T. Linnankivi, M. Mackay, D. Marom, C. Lourenco, S. Mckee, I. Moroni, J. Morton, M. Moutard, K. Murray, R. Nabbout, S. Nampoothiri, N. Nunez-Enamorado, P. Oades, I. Olivieri, J. Ostergaard, B. Perez-Duenas, J. Prendiville, V. Ramesh, M. Rasmussen, L. Regal, F. Ricci, M. Rio, D. Rodriguez, A. Roubertie, E. Salvatici, K. Segers, G. Sinha, D. Soler, R. Spiegel, T. Stodberg, R. Straussberg, K. Swoboda, M. Suri, U. Tacke, T. Tan, J. Naude, K. Teik, M. Thomas, M. Till, D. Tonduti, E. Valente, R. Van Coster, M. van der Knaap, G. Vassallo, R. Vijzelaar, J. Vogt, G. Wallace, E. Wassmer, H. Webb, W. Whitehouse, R. Whitney, M. Zaki, S. Zuberi, J. Livingston, F. Rozenberg, P. Lebon, A. Vanderver, S. Orcesi, G. Rice. - In: AMERICAN JOURNAL OF MEDICAL GENETICS. PART A. - ISSN 1552-4825. - 167:2(2015 Feb), pp. 296-312. [10.1002/ajmg.a.36887]

Characterization of human disease phenotypes associated with mutations in TREX1, RNASEH2A, RNASEH2B, RNASEH2C, SAMHD1, ADAR, and IFIH1

Crow YJ^Primo;Chase DS;Schmidt JL;Szynkiewicz M;Forte GMA;Gornall HL;Oojageer A;Anderson B;Pizzino A;Helman G;Abdel-Hamid MS;Abdel-Salam GM;Ackroyd S;Aeby A;Agosta G;Albin C;Allon-Shalev S;Arellano M;Ariaudo G;Aswani V;Babul-Hirji R;Baildam EM;Bahi-Buisson N;Bailey KM;Barnerias C;Barth M;Battini R;Beresford MW;Bernard G;Bianchi M;de Villemeur TB;Blair EM;Bloom M;Burlina AB;Carpanelli ML;Carvalho DR;Castro-Gago M;Cavallini A;Cereda C;Chandler KE;Chitayat DA;Collins AE;Corcoles CS;Cordeiro NJV;Crichiutti G;Dabydeen L;Dale RC;D'Arrigo S;De Goede CGEL;De Laet C;De Waele LMH;Denzler I;Desguerre I;Devriendt K;Di Rocco M;Fahey MC;Fazzi E;Ferrie CD;Figueiredo A;Gener B;Goizet C;Gowrinathan NR;Gowrishankar K;Hanrahan D;Isidor B;Kara L;Khan N;King MD;Kirk EP;Kumar R;Lagae L;Landrieu P;Lauffer H;Laugel V;La Piana R;Lim MJ;Lin JPSM;Linnankivi T;Mackay MT;Marom DR;Lourenco CM;McKee SA;Moroni I;Morton JEV;Moutard ML;Murray K;Nabbout R;Nampoothiri S;Nunez-Enamorado N;Oades PJ;Olivieri I;Ostergaard JR;Perez-Duenas B;Prendiville JS;Ramesh V;Rasmussen M;Regal L;Ricci F;Rio M;Rodriguez D;Roubertie A;Salvatici E;Segers KA;Sinha GP;Soler D;Spiegel R;Stodberg TI;Straussberg R;Swoboda KJ;Suri M;Tacke U;Tan TY;Naude JT;Teik KW;Thomas MM;Till M;D. Tonduti;Valente EM;Van Coster RN;van der Knaap MS;Vassallo G;Vijzelaar R;Vogt J;Wallace GB;Wassmer E;Webb HJ;Whitehouse WP;Whitney RN;Zaki MS;Zuberi SM;Livingston JH;Rozenberg F;Lebon P;Vanderver A;Orcesi S;Rice GI

2015

Abstract

Aicardi-Goutières syndrome is an inflammatory disease occurring due to mutations in any of TREX1, RNASEH2A, RNASEH2B, RNASEH2C, SAMHD1, ADAR or IFIH1. We report on 374 patients from 299 families with mutations in these seven genes. Most patients conformed to one of two fairly stereotyped clinical profiles; either exhibiting an in utero disease-onset (74 patients; 22.8% of all patients where data were available), or a post-natal presentation, usually within the first year of life (223 patients; 68.6%), characterized by a sub-acute encephalopathy and a loss of previously acquired skills. Other clinically distinct phenotypes were also observed; particularly, bilateral striatal necrosis (13 patients; 3.6%) and non-syndromic spastic paraparesis (12 patients; 3.4%). We recorded 69 deaths (19.3% of patients with follow-up data). Of 285 patients for whom data were available, 210 (73.7%) were profoundly disabled, with no useful motor, speech and intellectual function. Chilblains, glaucoma, hypothyroidism, cardiomyopathy, intracerebral vasculitis, peripheral neuropathy, bowel inflammation and systemic lupus erythematosus were seen frequently enough to be confirmed as real associations with the Aicardi-Goutieres syndrome phenotype. We observed a robust relationship between mutations in all seven genes with increased type I interferon activity in cerebrospinal fluid and serum, and the increased expression of interferon-stimulated gene transcripts in peripheral blood. We recorded a positive correlation between the level of cerebrospinal fluid interferon activity assayed within one year of disease presentation and the degree of subsequent disability. Interferon-stimulated gene transcripts remained high in most patients, indicating an ongoing disease process. On the basis of substantial morbidity and mortality, our data highlight the urgent need to define coherent treatment strategies for the phenotypes associated with mutations in the Aicardi-Goutières syndrome-related genes. Our findings also make it clear that a window of therapeutic opportunity exists relevant to the majority of affected patients and indicate that the assessment of type I interferon activity might serve as a useful biomarker in future clinical trials.

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	Parole chiave
	
			Aicardi–Goutie`res syndrome; bilateral striatal necrosis; spastic paraparesis; type I interferon; interferon signature
		
	Settori scientifico-disciplinari dell'articolo
	
			Settore MED/39 - Neuropsichiatria Infantile
		
	Data di pubblicazione
	
			feb-2015
		
	Rivista in ANCE
	
			AMERICAN JOURNAL OF MEDICAL GENETICS. PART A
		
	DOI
	
			https://dx.doi.org/10.1002/ajmg.a.36887
		
	Tipologia
	
			Article (author)
		
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			01 - Articolo su periodico

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