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Multiple sclerosis is a common disease of the central nervous system in which the interplay between inflammatory and neurodegenerative processes typically results in intermittent neurological disturbance followed by progressive accumulation of disability. Epidemiological studies have shown that genetic factors are primarily responsible for the substantially increased frequency of the disease seen in the relatives of affected individuals, and systematic attempts to identify linkage in multiplex families have confirmed that variation within the major histocompatibility complex (MHC) exerts the greatest individual effect on risk. Modestly powered genome-wide association studies (GWAS) have enabled more than 20 additional risk loci to be identified and have shown that multiple variants exerting modest individual effects have a key role in disease susceptibility. Most of the genetic architecture underlying susceptibility to the disease remains to be defined and is anticipated to require the analysis of sample sizes that are beyond the numbers currently available to individual research groups. In a collaborative GWAS involving 9,772 cases of European descent collected by 23 research groups working in 15 different countries, we have replicated almost all of the previously suggested associations and identified at least a further 29 novel susceptibility loci. Within the MHC we have refined the identity of the HLA-DRB1 risk alleles and confirmed that variation in the HLA-A gene underlies the independent protective effect attributable to the class I region. Immunologically relevant genes are significantly overrepresented among those mapping close to the identified loci and particularly implicate T-helper-cell differentiation in the pathogenesis of multiple sclerosis.
Genetic risk and a primary role for cell-mediated immune mechanisms in multiple sclerosis / Stephen, Sawcer; Garrett, Hellenthal; Matti, Pirinen; Chris C. A., Spencer; Nikolaos A., Patsopoulos; Loukas, Moutsianas; Alexander, Dilthey; Zhan, Su; Colin, Freeman; Sarah E., Hunt; Sarah, Edkins; Emma, Gray; David R., Booth; Simon C., Potter; An, Goris; Gavin, Band; A. B., Oturai; Amy, Strange; Janna, Saarela; Celine, Bellenguez; Bertrand, Fontaine; Matthew, Gillman; Bernhard, Hemmer; Rhian, Gwilliam; Frauke, Zipp; Alagurevathi, Jayakumar; Roland, Martin; Stephen, Leslie; Stanley, Hawkins; Eleni, Giannoulatou; Sandra, D'Alfonso; Hannah, Blackburn; F. M., Boneschi; Jennifer, Liddle; Hanne F., Harbo; Marc L., Perez; Anne, Spurkland; Matthew J., Waller; Marcin P., Mycko; Michelle, Ricketts; Manuel, Comabella; Naomi, Hammond; Ingrid, Kockum; Owen T., Mccann; Maria, Ban; Pamela, Whittaker; Anu, Kemppinen; Paul, Weston; Clive, Hawkins; Sara, Widaa; John, Zajicek; Serge, Dronov; Neil, Robertson; Suzannah J., Bumpstead; Lisa F., Barcellos; Rathi, Ravindrarajah; Roby, Abraham; Lars, Alfredsson; Kristin, Ardlie; Cristin, Aubin; Amie, Baker; Katharine, Baker; Sergio E., Baranzini; Laura, Bergamaschi; Roberto, Bergamaschi; Allan, Bernstein; Achim, Berthele; Mike, Boggild; Jonathan P., Bradfield; David, Brassat; Simon A., Broadley; Dorothea, Buck; Helmut, Butzkueven; Ruggero, Capra; William M., Carroll; Paola, Cavalla; Elisabeth G., Celius; Sabine, Cepok; Rosetta, Chiavacci; Françoise Clerget, Darpoux; Katleen, Clysters; Giancarlo, Comi; Mark, Cossburn; Isabelle Cournu, Rebeix; Mathew B., Cox; Wendy, Cozen; Bruce A. C., Cree; Anne H., Cross; Daniele, Cusi; Mark J., Daly; Emma, Davis; Paul I. W., De Bakker; Marc, Debouverie; Marie Beatrice, D'Hooghe; Katherine, Dixon; Rita, Dobosi; Benedicte, Dubois; David, Ellinghaus; Irina, Elovaara; Federica, Esposito; Claire, Fontenille; Simon, Foote; Andre, Franke; Daniela, Galimberti; Angelo, Ghezzi; Joseph, Glessner; Refujia, Gomez; Olivier, Gout; Colin, Graham; Struan F. A., Grant; F. R., Guerini; Hakon, Hakonarson; Per, Hall; Anders, Hamsten; Hans Peter, Hartung; Rob N., Heard; Simon, Heath; Jeremy, Hobart; Muna, Hoshi; Carmen Infante, Duarte; Gillian, Ingram; Wendy, Ingram; Talat, Islam; Maja, Jagodic; Michael, Kabesch; Allan G., Kermode; Trevor J., Kilpatrick; Cecilia, Kim; Norman, Klopp; Keijo, Koivisto; Malin, Larsson; Mark, Lathrop; Jeannette S., Lechner Scott; Maurizio A., Leone; Virpi, Leppa; Ulrika, Liljedahl; I. L., Bomfim; Robin R., Lincoln; Jenny, Link; Jianjun, Liu; Åslaug R., Lorentzen; Sara, Lupoli; Fabio, Macciardi; Thomas, Mack; Mark, Marriott; Vittorio, Martinelli; Deborah, Mason; Jacob L., Mccauley; Frank, Mentch; Inger Lise, Mero; Tania, Mihalova; Xavier, Montalban; John, Mottershead; Kjell Morten, Myhr; Paola, Naldi; William, Ollier; Alison, Page; Aarno, Palotie; Jean, Pelletier; Laura, Piccio; Trevor, Pickersgill; Fredrik, Piehl; Susan, Pobywajlo; Hong L., Quach; Patricia P., Ramsay; Mauri, Reunanen; Richard, Reynolds; John D., Rioux; Mariaemma, Rodegher; Sabine, Roesner; Justin P., Rubio; Ina Maria, Ruckert; Salvetti, Marco; Erika, Salvi; Adam, Santaniello; Catherine A., Schaefer; Stefan, Schreiber; Christian, Schulze; Rodney J., Scott; Finn, Sellebjerg; Krzysztof W., Selmaj; David, Sexton; Ling, Shen; Brigid Simms, Acuna; Sheila, Skidmore; Patrick M. A., Sleiman; Cathrine, Smestad; P. S., Sorensen; H. B., Sondergaard; Jim, Stankovich; Richard C., Strange; Anna Maija, Sulonen; Emilie, Sundqvist; Ann Christine, Syvanen; Francesca, Taddeo; Bruce, Taylor; Jenefer M., Blackwell; Pentti, Tienari; Elvira, Bramon; Ayman, Tourbah; Matthew A., Brown; Ewa, Tronczynska; Juan P., Casas; Niall, Tubridy; Aiden, Corvin; Jane, Vickery; Janusz, Jankowski; Pablo, Villoslada; Hugh S., Markus; Kai, Wang; Christopher G., Mathew; James, Wason; Colin N. A., Palmer; H., Erich Wichmann; Robert, Plomin; Ernest, Willoughby; Anna, Rautanen; Juliane, Winkelmann; Michael, Wittig; Richard C., Trembath; Jacqueline, Yaouanq; Ananth C., Viswanathan; Haitao, Zhang; Nicholas W., Wood; Rebecca, Zuvich; Panos, Deloukas; Cordelia, Langford; Audrey, Duncanson; Jorge R., Oksenberg; Margaret A., Pericak Vance; Jonathan L., Haines; Tomas, Olsson; Jan, Hillert; Adrian J., Ivinson; Philip L., De Jager; Leena, Peltonen; Graeme J., Stewart; David A., Hafler; Stephen L., Hauser; Gil, Mcvean; Peter, Donnelly; Alastair, Compston. - In: NATURE. - ISSN 0028-0836. - 476:7359(2011), pp. 214-219. [10.1038/nature10251]
Genetic risk and a primary role for cell-mediated immune mechanisms in multiple sclerosis.
Stephen Sawcer;Garrett Hellenthal;Matti Pirinen;Chris C. A. Spencer;Nikolaos A. Patsopoulos;Loukas Moutsianas;Alexander Dilthey;Zhan Su;Colin Freeman;Sarah E. Hunt;Sarah Edkins;Emma Gray;David R. Booth;Simon C. Potter;An Goris;Gavin Band;A. B. Oturai;Amy Strange;Janna Saarela;Celine Bellenguez;Bertrand Fontaine;Matthew Gillman;Bernhard Hemmer;Rhian Gwilliam;Frauke Zipp;Alagurevathi Jayakumar;Roland Martin;Stephen Leslie;Stanley Hawkins;Eleni Giannoulatou;Sandra D'Alfonso;Hannah Blackburn;F. M. Boneschi;Jennifer Liddle;Hanne F. Harbo;Marc L. Perez;Anne Spurkland;Matthew J. Waller;Marcin P. Mycko;Michelle Ricketts;Manuel Comabella;Naomi Hammond;Ingrid Kockum;Owen T. Mccann;Maria Ban;Pamela Whittaker;Anu Kemppinen;Paul Weston;Clive Hawkins;Sara Widaa;John Zajicek;Serge Dronov;Neil Robertson;Suzannah J. Bumpstead;Lisa F. Barcellos;Rathi Ravindrarajah;Roby Abraham;Lars Alfredsson;Kristin Ardlie;Cristin Aubin;Amie Baker;Katharine Baker;Sergio E. Baranzini;Laura Bergamaschi;Roberto Bergamaschi;Allan Bernstein;Achim Berthele;Mike Boggild;Jonathan P. Bradfield;David Brassat;Simon A. Broadley;Dorothea Buck;Helmut Butzkueven;Ruggero Capra;William M. Carroll;Paola Cavalla;Elisabeth G. Celius;Sabine Cepok;Rosetta Chiavacci;Françoise Clerget Darpoux;Katleen Clysters;Giancarlo Comi;Mark Cossburn;Isabelle Cournu Rebeix;Mathew B. Cox;Wendy Cozen;Bruce A. C. Cree;Anne H. Cross;Daniele Cusi;Mark J. Daly;Emma Davis;Paul I. W. De Bakker;Marc Debouverie;Marie Beatrice D'Hooghe;Katherine Dixon;Rita Dobosi;Benedicte Dubois;David Ellinghaus;Irina Elovaara;Federica Esposito;Claire Fontenille;Simon Foote;Andre Franke;Daniela Galimberti;Angelo Ghezzi;Joseph Glessner;Refujia Gomez;Olivier Gout;Colin Graham;Struan F. A. Grant;F. R. Guerini;Hakon Hakonarson;Per Hall;Anders Hamsten;Hans Peter Hartung;Rob N. Heard;Simon Heath;Jeremy Hobart;Muna Hoshi;Carmen Infante Duarte;Gillian Ingram;Wendy Ingram;Talat Islam;Maja Jagodic;Michael Kabesch;Allan G. Kermode;Trevor J. Kilpatrick;Cecilia Kim;Norman Klopp;Keijo Koivisto;Malin Larsson;Mark Lathrop;Jeannette S. Lechner Scott;Maurizio A. Leone;Virpi Leppa;Ulrika Liljedahl;I. L. Bomfim;Robin R. Lincoln;Jenny Link;Jianjun Liu;Åslaug R. Lorentzen;Sara Lupoli;Fabio Macciardi;Thomas Mack;Mark Marriott;Vittorio Martinelli;Deborah Mason;Jacob L. Mccauley;Frank Mentch;Inger Lise Mero;Tania Mihalova;Xavier Montalban;John Mottershead;Kjell Morten Myhr;Paola Naldi;William Ollier;Alison Page;Aarno Palotie;Jean Pelletier;Laura Piccio;Trevor Pickersgill;Fredrik Piehl;Susan Pobywajlo;Hong L. Quach;Patricia P. Ramsay;Mauri Reunanen;Richard Reynolds;John D. Rioux;Mariaemma Rodegher;Sabine Roesner;Justin P. Rubio;Ina Maria Ruckert;SALVETTI, Marco;Erika Salvi;Adam Santaniello;Catherine A. Schaefer;Stefan Schreiber;Christian Schulze;Rodney J. Scott;Finn Sellebjerg;Krzysztof W. Selmaj;David Sexton;Ling Shen;Brigid Simms Acuna;Sheila Skidmore;Patrick M. A. Sleiman;Cathrine Smestad;P. S. Sorensen;H. B. Sondergaard;Jim Stankovich;Richard C. Strange;Anna Maija Sulonen;Emilie Sundqvist;Ann Christine Syvanen;Francesca Taddeo;Bruce Taylor;Jenefer M. Blackwell;Pentti Tienari;Elvira Bramon;Ayman Tourbah;Matthew A. Brown;Ewa Tronczynska;Juan P. Casas;Niall Tubridy;Aiden Corvin;Jane Vickery;Janusz Jankowski;Pablo Villoslada;Hugh S. Markus;Kai Wang;Christopher G. Mathew;James Wason;Colin N. A. Palmer;H. Erich Wichmann;Robert Plomin;Ernest Willoughby;Anna Rautanen;Juliane Winkelmann;Michael Wittig;Richard C. Trembath;Jacqueline Yaouanq;Ananth C. Viswanathan;Haitao Zhang;Nicholas W. Wood;Rebecca Zuvich;Panos Deloukas;Cordelia Langford;Audrey Duncanson;Jorge R. Oksenberg;Margaret A. Pericak Vance;Jonathan L. Haines;Tomas Olsson;Jan Hillert;Adrian J. Ivinson;Philip L. De Jager;Leena Peltonen;Graeme J. Stewart;David A. Hafler;Stephen L. Hauser;Gil Mcvean;Peter Donnelly;Alastair Compston
2011
Abstract
Multiple sclerosis is a common disease of the central nervous system in which the interplay between inflammatory and neurodegenerative processes typically results in intermittent neurological disturbance followed by progressive accumulation of disability. Epidemiological studies have shown that genetic factors are primarily responsible for the substantially increased frequency of the disease seen in the relatives of affected individuals, and systematic attempts to identify linkage in multiplex families have confirmed that variation within the major histocompatibility complex (MHC) exerts the greatest individual effect on risk. Modestly powered genome-wide association studies (GWAS) have enabled more than 20 additional risk loci to be identified and have shown that multiple variants exerting modest individual effects have a key role in disease susceptibility. Most of the genetic architecture underlying susceptibility to the disease remains to be defined and is anticipated to require the analysis of sample sizes that are beyond the numbers currently available to individual research groups. In a collaborative GWAS involving 9,772 cases of European descent collected by 23 research groups working in 15 different countries, we have replicated almost all of the previously suggested associations and identified at least a further 29 novel susceptibility loci. Within the MHC we have refined the identity of the HLA-DRB1 risk alleles and confirmed that variation in the HLA-A gene underlies the independent protective effect attributable to the class I region. Immunologically relevant genes are significantly overrepresented among those mapping close to the identified loci and particularly implicate T-helper-cell differentiation in the pathogenesis of multiple sclerosis.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/393536
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simulazione ASN
Il report seguente simula gli indicatori relativi alla propria produzione scientifica in relazione alle soglie ASN 2023-2025 del proprio SC/SSD. Si ricorda che il superamento dei valori soglia (almeno 2 su 3) è requisito necessario ma non sufficiente al conseguimento dell'abilitazione. La simulazione si basa sui dati IRIS e sugli indicatori bibliometrici alla data indicata e non tiene conto di eventuali periodi di congedo obbligatorio, che in sede di domanda ASN danno diritto a incrementi percentuali dei valori. La simulazione può differire dall'esito di un’eventuale domanda ASN sia per errori di catalogazione e/o dati mancanti in IRIS, sia per la variabilità dei dati bibliometrici nel tempo. Si consideri che Anvur calcola i valori degli indicatori all'ultima data utile per la presentazione delle domande.
La presente simulazione è stata realizzata sulla base delle specifiche raccolte sul tavolo ER del Focus Group IRIS coordinato dall’Università di Modena e Reggio Emilia e delle regole riportate nel DM 589/2018 e allegata Tabella A. Cineca, l’Università di Modena e Reggio Emilia e il Focus Group IRIS non si assumono alcuna responsabilità in merito all’uso che il diretto interessato o terzi faranno della simulazione. Si specifica inoltre che la simulazione contiene calcoli effettuati con dati e algoritmi di pubblico dominio e deve quindi essere considerata come un mero ausilio al calcolo svolgibile manualmente o con strumenti equivalenti.
