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72 research outputs found

Loss of Ezh2 synergizes with JAK2-V617F in initiating myeloproliferative neoplasms and promoting myelofibrosis

Author: Dirnhofer Stephan
Geier Florian
Guglielmelli Paola
Hao Shen Hui
Kralovics Robert
Kubovcakova Lucia
Meyer Sara C.
Milosevic Feenstra Jelena D.
Nienhold Ronny
Orkin Stuart H.
Shimizu Takafumi
Skoda Radek C.
Vannucchi Alessandro Maria
Zmajkovic Jakub
Publication venue: 'Rockefeller University Press'
Publication date: 01/01/2016
Field of study

Genome-wide association study identifies susceptibility loci for acute myeloid leukemia

Author: Alharbi A
Allan JM
Allsup DJ
Altmann H
Andersen MK
Bodor C
Bornhauser M
Burnett AK
Cervera J
Cheok M
Clay-Gilmour AI
Cluzeau T
Collin M
Cordell HJ
Daly AK
Darlay R
Dickinson AM
Dombret H
Douglas E
Elstob C
Fitzgibbon J
Fontana MC
Fordham SE
Gaal-Wesinger J
Gale RE
Gieger C
Gilkes A
Gomez-Segui I
Grimwade D
Haferlach T
Hahn T
Heidenreich O
Hills RK
Hofmann W-K
Houlston RS
Hungate E
Ivey A
Jackson GH
Jeffries S
Jones GL
Kralovics R
Krizsan S
Kunadt D
Larson RA
Le Beau MM
Lendrem C
Lin W-Y
Linch D
Lo-Coco F
Marconi G
Marr HJ
Martinelli G
Masszi A
Meggendorfer M
Menne T
Milosevic Feenstra JD
Moreilhon C
Norden J
Nowak D
Onel K
Palm L
Park C
Piechocki K
Porkka K
Preudhomme C
Quante A
Rahman T
Raynaud S
Rollig C
Ruhnke L
Russell NH
Sanz MA
Sill H
Skol A
Stock W
Stolzel F
Strauch K
Sucheston-Campbell L
Sunter NJ
Voso MT
Wagenfuhr L
Wang J
Xu Y
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2021
Field of study

Acute myeloid leukemia (AML) is a hematological malignancy with an undefined heritable risk. Here we perform a meta-analysis of three genome-wide association studies, with replication in a fourth study, incorporating a total of 4018 AML cases and 10488 controls. We identify a genome-wide significant risk locus for AML at 11q13.2 (rs4930561; P = 2.15 × 10-8; KMT5B). We also identify a genome-wide significant risk locus for the cytogenetically normal AML sub-group (N = 1287) at 6p21.32 (rs3916765; P = 1.51 × 10-10; HLA). Our results inform on AML etiology and identify putative functional genes operating in histone methylation (KMT5B) and immune function (HLA)

UCL Discovery

PuSH

Queen Mary Research Online

Institute of Cancer Research Repository

Genome-wide association study identifies susceptibility loci for acute myeloid leukemia

Author: Alharbi A
Allan JM
Allsup DJ
Altmann H
Andersen MK
Bodor C
Bornhauser M
Burnett AK
Cervera J
Cheok M
Clay-Gilmour AI
Cluzeau T
Collin M
Cordell HJ
Daly AK
Darlay R
Dickinson AM
Dombret H
Douglas E
Elstob C
Fitzgibbon J
Fontana MC
Fordham SE
Gaal-Wesinger J
Gale RE
Gieger C
Gilkes A
Gomez-Segui I
Grimwade D
Haferlach T
Hahn T
Heidenreich O
Hills RK
Hofmann W-K
Houlston RS
Hungate E
Ivey A
Jackson GH
Jeffries S
Jones GL
Kralovics R
Krizsan S
Kunadt D
Larson RA
Le Beau MM
Lendrem C
Lin W-Y
Linch D
Lo-Coco F
Marconi G
Marr HJ
Martinelli G
Masszi A
Meggendorfer M
Menne T
Milosevic Feenstra JD
Moreilhon C
Norden J
Nowak D
Onel K
Palm L
Park C
Piechocki K
Porkka K
Preudhomme C
Quante A
Rahman T
Raynaud S
Rollig C
Ruhnke L
Russell NH
Sanz MA
Sill H
Skol A
Stock W
Stolzel F
Strauch K
Sucheston-Campbell L
Sunter NJ
Voso MT
Wagenfuhr L
Wang J
Xu Y
Publication venue: 'Nature Research Society'
Publication date: 01/01/2021
Field of study

\ua9 2021, The Author(s).Acute myeloid leukemia (AML) is a hematological malignancy with an undefined heritable risk. Here we perform a meta-analysis of three genome-wide association studies, with replication in a fourth study, incorporating a total of 4018 AML cases and 10488 controls. We identify a genome-wide significant risk locus for AML at 11q13.2 (rs4930561; P = 2.15 7 10−8; KMT5B). We also identify a genome-wide significant risk locus for the cytogenetically normal AML sub-group (N = 1287) at 6p21.32 (rs3916765; P = 1.51 7 10−10; HLA). Our results inform on AML etiology and identify putative functional genes operating in histone methylation (KMT5B) and immune function (HLA)

Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Newcastle University E-Prints

Genome-wide association study identifies susceptibility loci for acute myeloid leukemia

Author: Alharbi A
Allan JM
Allsup DJ
Altmann H
Andersen MK
Bornhäuser M
Burnett AK
Bödör C
Cervera J
Cheok M
Clay-Gilmour AI
Cluzeau T
Collin M
Cordell HJ
Daly AK
Darlay R
Dickinson AM
Dombret H
Douglas E
Elstob C
Fitzgibbon J
Fontana MC
Fordham SE
Gaal-Wesinger J
Gale RE
Gieger C
Gilkes A
Grimwade D
Gómez-Seguí I
Haferlach T
Hahn T
Heidenreich O
Hills RK
Hofmann W-K
Houlston RS
Hungate E
Ivey A
Jackson GH
Jeffries S
Jones GL
Kralovics R
Krizsán S
Kunadt D
Larson RA
Le Beau MM
Lendrem C
Lin W-Y
Linch D
Lo-Coco F
Marconi G
Marr HJ
Martinelli G
Masszi A
Meggendorfer M
Menne T
Milosevic Feenstra JD
Moreilhon C
Norden J
Nowak D
Onel K
Palm L
Park C
Piechocki K
Porkka K
Preudhomme C
Quante A
Rahman T
Raynaud S
Ruhnke L
Russell NH
Röllig C
Sanz MA
Sill H
Skol A
Stock W
Strauch K
Stölzel F
Sucheston-Campbell L
Sunter NJ
Voso MT
Wagenführ L
Wang J
Xu Y
Publication venue
Publication date: 29/10/2021
Field of study

Acute myeloid leukemia (AML) is a hematological malignancy with an undefined heritable risk. Here we perform a meta-analysis of three genome-wide association studies, with replication in a fourth study, incorporating a total of 4018 AML cases and 10488 controls. We identify a genome-wide significant risk locus for AML at 11q13.2 (rs4930561; P = 2.15 × 10^{-8}; KMT5B). We also identify a genome-wide significant risk locus for the cytogenetically normal AML sub-group (N = 1287) at 6p21.32 (rs3916765; P = 1.51 × 10^{−10}; HLA). Our results inform on AML etiology and identify putative functional genes operating in histone methylation (KMT5B) and immune function (HLA)

UCL Discovery