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2 research outputs found

Nat Genet

Author: Adams D. (D) J. (J)
Adams N. (N) C. (C)
Adler T. (T)
Aguilar-Pimentel A. (A)
Ali-Hadji D. (Dalila)
Amann G. (Grégory)
Andre P. (Philippe)
Atkins S. (S)
Auburtin A. (Aurélie)
Ayadi A. (Abdelkader)
Becker J. (Julien)
Becker L. (L)
Bedu E. (Elodie)
Bekeredjian R. (R)
Birling M. (Marie-Christine)
Blake A. (A)
Bottomley J. (J)
Bowl M. (M) R. (R)
Brault V. (Véronique)
Brown S. (S) D. (D)
Busch D. (D) H. (H)
Bussell J. (J) N. (N)
Calzada-Wack J. (J)
Cater H. (H)
Champy M. (Marie-France)
Charles P. (Philippe)
Chevalier C. (Claire)
Chiani F. (F)
Codner G. (G) F. (F)
Combe R. (R)
Consortium E. (Eumodic)
Cox R. (R)
Da Cruz I. (I) G. (G)
Dalloneau E. (E)
Di Fenza A. (A)
Dierich A. (A)
Doe B. (B)
Duchon A. (Arnaud)
Eickelberg O. (O)
Emelyanova I. (I)
Esapa C. (C) T. (T)
Estabel J. (J)
Favor J. (J)
Feigel T. (T)
Fertak L. (L) E. (E)
Flenniken A. (A)
Fray M. (M)
Fuchs H. (H)
Gailus-Durner V. (V)
Gambadoro A. (A)
Garrett L. (L)
Gates H. (H)
Gerdin A. (A) K. (K)
Gkoutos G. (G)
Glasl L. (L)
Goetz P. (P)
Gotz A. (A)
Graw J. (J)
Greenaway S. (S)
Guimond A. (Alain)
Hancock J. (J) M. (M)
Hans W. (W)
Herault Y. (Yann)
Hicks G. (G)
Hoehndorf R. (R)
Hofler H. (H)
Holmes C. (C)
Holter S. (S) M. (M)
Hough T. (T)
Houghton R. (R)
Hrabe de Angelis M. (M)
Hurt A. (A)
Ivandic B. (B)
Jacobs H. (Hugues)
Jacquot S. (Sylvie)
Jones N. (N)
Karp N. (N) A. (A)
Katus H. (H) A. (A)
Kitchen S. (S)
Klein-Rodewald T. (T)
Klingenspor M. (M)
Klopstock T. (T)
Lalanne V. (Valérie)
le Marchand E. (Elise)
Leblanc S. (Sophie)
Lengger C. (C)
Ludwig T. (T)
Lux A. (Aline)
Maier H. (H)
Mallon A. (A) M. (M)
Mandel J. (Jean-Louis)
Mark M. (Manuel)
Marschall S. (S)
McKerlie C. (C)
Melvin D. (D) G. (G)
Meziane H. (Hamid)
Micklich K. (K)
Mittelhauser C. (C)
Monassier L. (Laurent)
Morgan H. (H)
Moulaert D. (David)
Muller S. (S)
Naton B. (B)
Neff F. (F)
Nicholson G. (G)
Nolan P. (P) M. (M)
Nutter L. (L) M. (M)
Ollert M. (M)
Pavlovic G. (Guillaume)
Pellegata N. (N) S. (S)
Peter E. (E)
Petit-Demouliere B. (Benoît)
Pickard A. (A)
Podrini C. (C)
Potter P. (P)
Pouilly L. (Laurent)
Puk O. (O)
Quintanilla-Fend L. (L)
Quwailid M. (M) M. (M)
Racz I. (I)
Ramirez-Solis R. (R)
Rathkolb B. (B)
Richardson D. (D)
Riet F. (Fabrice)
Rossant J. (J)
Rousseau S. (Stéphane)
Roux M. (Michel)
Rozman J. (J)
Ryder E. (E)
Salisbury J. (J)
Santos L. (L)
Schable K. (K) H. (H)
Schiller E. (E)
Schrewe A. (A)
Schulz H. (H)
Selloum M. (Mohammed)
Simon M. (M)
Sorg T. (Tania)
Steel K. (K) P. (P)
Steinkamp R. (R)
Stewart M. (M)
Stoger C. (C)
Stoger T. (T)
Sun M. (M)
Sunter D. (D)
Teboul L. (L)
Tilly I. (I)
Tocchini-Valentini G. (G) P. (P)
Tost M. (M)
Treise I. (I)
Vasseur L. (Laurent)
Velot E. (E)
Vogt-Weisenhorn D. (D)
Wagner C. (Christel)
Walling A. (A)
Wattenhofer-Donze M. (Marie)
Weber B. (Bruno)
Wells S. (S)
Wendling O. (Olivia)
Westerberg H. (H)
White J. (J) K. (K)
Willershauser M. (M)
Wolf E. (E)
Wolter A. (A)
Wood J. (J)
Wurst W. (W)
Yildirim A. (A) O. (O)
Zeh R. (R)
Zimmer A. (A)
Zimprich A. (A)
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 27/07/2015
Field of study

The function of the majority of genes in the mouse and human genomes remains unknown. The mouse embryonic stem cell knockout resource provides a basis for the characterization of relationships between genes and phenotypes. The EUMODIC consortium developed and validated robust methodologies for the broad-based phenotyping of knockouts through a pipeline comprising 20 disease-oriented platforms. We developed new statistical methods for pipeline design and data analysis aimed at detecting reproducible phenotypes with high power. We acquired phenotype data from 449 mutant alleles, representing 320 unique genes, of which half had no previous functional annotation. We captured data from over 27,000 mice, finding that 83% of the mutant lines are phenodeviant, with 65% demonstrating pleiotropy. Surprisingly, we found significant differences in phenotype annotation according to zygosity. New phenotypes were uncovered for many genes with previously unknown function, providing a powerful basis for hypothesis generation and further investigation in diverse systems.Comment in : Genetic differential calculus. [Nat Genet. 2015] Comment in : Scaling up phenotyping studies. [Nat Biotechnol. 2015

univOAK

Using ancestry-informative markers to identify fine structure across 15 populations of European origin.

Author: Boraska V.
Bulik C.M.
Collier D.A.
EUMODIC Consortium (Wichmann H.-E.
Floyd J.A.B.
Franklin C.S.
Huckins L.M.
Southam L.
Sullivan P.F.
Tachmazidou I.
Tyler-Smith C.
Zeggini E.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2014
Field of study

The Wellcome Trust Case Control Consortium 3 anorexia nervosa genome-wide association scan includes 2907 cases from 15 different populations of European origin genotyped on the Illumina 670K chip. We compared methods for identifying population stratification, and suggest list of markers that may help to counter this problem. It is usual to identify population structure in such studies using only common variants with minor allele frequency (MAF) >5%; we find that this may result in highly informative SNPs being discarded, and suggest that instead all SNPs with MAF >1% may be used. We established informative axes of variation identified via principal component analysis and highlight important features of the genetic structure of diverse European-descent populations, some studied for the first time at this scale. Finally, we investigated the substructure within each of these 15 populations and identified SNPs that help capture hidden stratification. This work can provide information regarding the designing and interpretation of association results in the International Consortia

PuSH