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2 research outputs found

X chromosome inactivation does not necessarily determine the severity of the phenotype in Rett syndrome patients

Author: Aguirre F.J.
Aleu M.
Alonso X.
Alsius M.
Amoros M.
Antinolo G.
Aquino L.
Arellano C.
Armstrong J.
Arriola G.
Arteaga R.
Baena N.
Barcos M.
Belzunces N.
Blasco L.
Boronat S.
Brandi N.
Camacho T.
Campistol J.
Campo A.
Cancho R.
Candau R.
Canos I.
Carrascosa M.D.
Carratala-Marco F.
Casano J.
Castro P.
Cobo A.
Colomer J.
Conejo D.
Corrales M.J.
Cortes R.
Cruz G.
Csanyi G.
De Santos M.T.
De Toledo M.
del Campo M.
Del Campo M.
Del Toro M.
Domingo R.
Duat A.
Duque R.
Esparza A.M.
Fernandez R.
Fons M.C.
Fontalba A.
Galan E.
Gallano P.
Gamundi M.J.
Garcia M.D.
Garcia P.L.
Garcia-Barcina M.
Garcia-Catalan M.J.
Garcia-Cazorla A.
Garcia-Minaur S.
Garcia-Penas J.J.
Garcia-Silva M.T.
Gassio R.
Gean E.
Gerotina E.
Gil B.
Gokben S.
Gonzalez G.
Gonzalez J.
Gonzalez L.
Gonzalez V.
Guillen E.
Guitart M.
Guitet M.
Gutierrez E.
Gutierrez J.M.
Herranz J.L.
Iglesias G.
Jimenez A.M.
Karacic I.
Lahoz C.H.
Lao J.I.
Lapunzina P.
Lautre-Ecenarro M.J.
Lluch M.D.
Lopez L.
Lopez-Ariztegui A.
Macaya A.
Marin R.
Marquez C.M.L.
Martin E.
Martin-Tamayo P.
Martinez B.
Martinez F.
Martinez-Salcedo E.
Mas M.J.
Mateo G.
Mendez P.
Moreno S.
Mulas F.
Narbona J.
Nascimento A.
Nieto M.
Nunes T.F.
Nunez N.
O''Callaghan M.
Obon M.
Onsurbe I.
Ortez C.I.
Orts E.
Pacheco P.
Parrilla R.
Pascual S.I.
Pascual-Alonso A.
Patino A.
Perez-Duenas B.
Perez-Poyato M.
Pineda M.
Poo P.
Puche E.
Ramos F.
Raspall M.
Roche A.
Roldan S.
Rosell J.
Ruiz C.
Ruiz-Falco M.L.
Russi M.E.
Samarra J.
San Antonio V.
Sanchez I.
Sanmartin X.
Sans A.
Santacana A.
Scholl-Burgi S.
Serrano M.
Serrano N.
Tendero A.
Torrents J.
Tortosa D.
Trivino E.
Troncoso L.
Turon E.
Vazquez C.
Vazquez P.
Velazquez R.
Ventura C.
Verdu A.
Vernet A.
Vidal S.
Vila M.T.
Villar C.
Xiol C.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2019
Field of study

Rett syndrome (RTT) is a severe neurological disorder usually caused by mutations in the MECP2 gene. Since the MECP2 gene is located on the X chromosome, X chromosome inactivation (XCI) could play a role in the wide range of phenotypic variation of RTT patients; however, classical methylation-based protocols to evaluate XCI could not determine whether the preferentially inactivated X chromosome carried the mutant or the wild-type allele. Therefore, we developed an allele-specific methylation-based assay to evaluate methylation at the loci of several recurrent MECP2 mutations. We analyzed the XCI patterns in the blood of 174 RTT patients, but we did not find a clear correlation between XCI and the clinical presentation. We also compared XCI in blood and brain cortex samples of two patients and found differences between XCI patterns in these tissues. However, RTT mainly being a neurological disease complicates the establishment of a correlation between the XCI in blood and the clinical presentation of the patients. Furthermore, we analyzed MECP2 transcript levels and found differences from the expected levels according to XCI. Many factors other than XCI could affect the RTT phenotype, which in combination could influence the clinical presentation of RTT patients to a greater extent than slight variations in the XCI pattern

Repositorio Universidad de Zaragoza

The design, construction, and commissioning of the KATRIN experiment

Author: Aker M.
Altenmüller K.
Amsbaugh J.F.
Arenz M.
Babutzka M.
Barrero D. Díaz
Bast J.
Bauer S.
Bechtler H.
Beck M.
Beglarian A.
Behrens J.
BENDER B.
Berendes R.
Berlev A.
Besserer U.
Bettin C.
Bieringer B.
Blaum K.
Block F.
Bobien S.
Bohn J.
Bokeloh K.
Bolz H.
Bornschein B.
Bornschein L.
Bouquet H.
Boyd N.M.
Brunst T.
Burritt T.H.
Böttcher M.
Caldwell T.S.
Chaoui Z.
Chilingaryan S.
Choi W.
Corona T.J.
Cox G.A.
Debowski K.
Deffert M.
Descher M.
Doe P.J.
Dragoun O.
Drexlin G.
Dunmore J.A.
Dyba S.
Edzards F.
Eichelhardt F.
Eitel K.
Ellinger E.
Engel R.
Enomoto S.
Erhard M.
Eversheim D.
Fedkevych M.
Felden A.
Fischer S.
Formaggio J.A.
Franklin G.B.
Frenzel H.
Friedel F.
Fränkle F.M.
Fulst A.
Gauda K.
Gehring R.
Gil W.
Glück F.
Grimm J.
Groh S.
Grohmann S.
Grössle R.
Gumbsheimer R.
Görhardt S.
Hackenjos M.
Hannen V.
Harms F.
Harper G.C.
Hartmann J.
Haußmann N.
Heizmann F.
Helbing K.
Held M.
Hernández A.P. Vizcaya
Hickford S.
Hilk D.
Hillen B.
Hiller R.
Hillesheimer D.
Hinz D.
Holzmann S.
Horn S.
Houdy T.
Howe M.A.
Huber A.
Häßler D.
Höhn T.
Hötzel M.
James T.
Jansen A.
Kaiser M.
Karl C.
Kazachenko O.
Kellerer J.
Kippenbrock L.
Kleesiek M.
Kleifges M.
Klein M.
Kleinfeller J.
Kopmann A.
Korzeczek M.
Kosmider A.
Kovalík A.
Krasch B.
Kraus M.
Krause H.
Kuckert L.
Kumb A.
Kunka N.
Käfer W.
Köllenberger L.
La Cascio L.
Lasserre T.
Le T.L.
Lebeda O.
Leber M.L.
Lehnert B.
Leiber B.
Letnev J.
Lewis R.J.
Lichter S.
Lokhov A.
Machatschek M.
Malcherek E.
Mark M.
Marsteller A.
Martin E.L.
Mehret K.
Meloni M.
Melzer C.
Menshikov A.
Mertens S.
Minter L.I.
Monreal B.
Mostafa J.
Myers A.W.
Müller K.
Naumann U.
Neumann H.
Niemes S.
Oelpmann P.
Off A.
Ortjohann H.-W.
Osipowicz A.
Ostrick B.
Parno D.S.
Peterson D.A.
Plischke P.
Poon A.W.P.
Poyato J.M. Lopez
Prall M.
Priester F.
Ranitzsch P.C.-O.
Reich J.
Renschler P.
Rest O.
Rinderspacher R.
Robertson R.G.H.
Rodejohann W.
Rodenbeck C.
Rohr P.
Rupp S.
Ryšavý M.
Röllig M.
Röttele C.
Sack R.
Saenz A.
Sagawe M.
Schaller A.
Schimpf L.
Schlösser K.
Schlösser M.
Schlüter L.
Schneidewind S.
Schrank M.
Schulz B.
Schwarz J.
Schäfer P.
Schön H.
Schönung K.
Seitz-Moskaliuk H.
Seller W.
Sibille V.
Siegmann D.
Slezák M.
Spanier F.
Steidl M.
Sturm M.
Sun M.
Tcherniakhovski D.
Telle H.H.
Thorne L.A.
Thümmler T.
Titov N.
Tkachev I.
Trost N.
Valerius K.
Van Wechel T.D.
VanDevender B.A.
Verbeek A.
Vianden R.
Vogt K.
Vénos D.
Wall B.L.
Wandkowsky N.
Weber M.
Weingardt H.
Weinheimer C.
Weiss C.
Welte S.
Wendel J.
Wierman K.J.
Wilkerson J.F.
Wolf J.
Wüstling S.
Xu W.
Yen Y.-R.
Zacher M.
Zadoroghny S.
Zboril M.
Zeller G.
Šefčík M.
Publication venue: 'IOP Publishing'
Publication date: 01/01/2021
Field of study

The KArlsruhe TRItium Neutrino (KATRIN) experiment, which aims to make a direct and model-independent determination of the absolute neutrino mass scale, is a complex experiment with many components. More than 15 years ago, we published a technical design report (TDR) [1] to describe the hardware design and requirements to achieve our sensitivity goal of 0.2 eV at 90% C.L. on the neutrino mass. Since then there has been considerable progress, culminating in the publication of first neutrino mass results with the entire beamline operating [2]. In this paper, we document the current state of all completed beamline components (as of the first neutrino mass measurement campaign), demonstrate our ability to reliably and stably control them over long times, and present details on their respective commissioning campaigns

arXiv.org e-Print Archive

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