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Dive into the research topics where Pierre Heimann is active.

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Featured researches published by Pierre Heimann.


Nature Genetics | 2004

Fusion of NUP214 to ABL1 on amplified episomes in T-cell acute lymphoblastic leukemia.

C Graux; Jan Cools; Cindy Melotte; Hilmar Quentmeier; A Ferrando; Robert A. Levine; Joris Vermeesch; Michel Stul; B Dutta; Nancy Boeckx; André Bosly; Pierre Heimann; Anne Uyttebroeck; Nicole Mentens; René Somers; R A F Macleod; Hans G. Drexler; At Look; Dwight Gary Gilliland; Lucienne Michaux; Peter Vandenberghe; Iwona Wlodarska; Peter Marynen; Anne Hagemeijer

In T-cell acute lymphoblastic leukemia (T-ALL), transcription factors are known to be deregulated by chromosomal translocations, but mutations in protein tyrosine kinases have only rarely been identified. Here we describe the extrachromosomal (episomal) amplification of ABL1 in 5 of 90 (5.6%) individuals with T-ALL, an aberration that is not detectable by conventional cytogenetics. Molecular analyses delineated the amplicon as a 500-kb region from chromosome band 9q34, containing the oncogenes ABL1 and NUP214 (refs. 5,6). We identified a previously undescribed mechanism for activation of tyrosine kinases in cancer: the formation of episomes resulting in a fusion between NUP214 and ABL1. We detected the NUP214-ABL1 transcript in five individuals with the ABL1 amplification, in 5 of 85 (5.8%) additional individuals with T-ALL and in 3 of 22 T-ALL cell lines. The constitutively phosphorylated tyrosine kinase NUP214-ABL1 is sensitive to the tyrosine kinase inhibitor imatinib. The recurrent cryptic NUP214-ABL1 rearrangement is associated with increased HOX expression and deletion of CDKN2A, consistent with a multistep pathogenesis of T-ALL. NUP214-ABL1 expression defines a new subgroup of individuals with T-ALL who could benefit from treatment with imatinib.


Leukemia | 2006

The JAK2V617F mutation is detectable at very low level in peripheral blood of healthy donors

Pierre Sidon; H El Housni; Barbara Dessars; Pierre Heimann

The JAK2 V617F mutation is detectable at very low level in peripheral blood of healthy donors


Acta Clinica Belgica | 2009

Guidelines for an integrated diagnostic approach of chronic lymphoproliferative disorders in the routine laboratory of haematology in Belgium.

Jan Philippé; Friedel Nollet; Marleen Bakkus; P Meeus; Christian Demanet; N Schaaf-Lafontaine; S Franke; Bernard Chatelain; K Vermeulen; E. Boone; H El Housni; Pierre Heimann; B Husson; Frédéric Lambert; P Vannuffel; Pascale Saussoy; B Maes; P Deschouwer

Abstract This paper summarizes the minimal workout of chronic lymphoproliferative disorders in a routine laboratory of haematology as recommended by a team of experienced laboratory supervisors in Belgium, taking into account the specific organisation of healthcare in Belgium, the innovations in the field of molecular analyses and related reimbursement. The starting point was essentially based upon clinical and/or haematological indications and it is emphasized that conclusions should be drawn in close dialogue with the clinician and experts in cytogenetics and histopathology. Reports made in the laboratory should be based upon an integration of cytomorphological, immunophenotypical and molecular data. These guidelines are not intended to be used as universal ‘diagnostic pathways’, but should be useful in developing local diagnostic pathways. It is well understood that this consensus, being valid anno 2009, may rapidly change with new technologies being introduced and new targets discovered.


The Journal of Molecular Diagnostics | 2007

A Case of FIP1L1-PDGFRA-Positive Chronic Eosinophilic Leukemia with a Rare FIP1L1 Breakpoint

Frédéric Lambert; Pierre Heimann; Christian Herens; Alain Chariot; Vincent Bours


Leukemia | 2007

The JAK2 V617F mutation is detectable in granulocyte populations at greater than two copies per cell among individuals with myeloproliferative disorders

Hakim El Housni; Pierre Sidon; Barbara Dessars; Pierre Heimann


Blood | 2004

Fusion of NUP214 to ABL1 on amplified extrachromosomal elements in T-ALL.

Jan Cools; Lucienne Michaux; Carlos Graux; C Melotte; Hilmar Quentmeier; Adolfo A. Ferrando; Robert A. Levine; Vermeesch; M. Stul; B Dutta; Nancy Boeckx; André Bosly; Pierre Heimann; Anne Uyttebroeck; Nicole Mentens; R. Somers; Raf MacLeod; Hans G. Drexler; At Look; D G Gilliland; Peter Vandenberghe; W Wlodarska; Peter Marynen; Anne Hagemeijer


Haematologica-the Hematology Journal | 2009

Microrna-29c and 223 and Their Prognostic Value in Chronic Lymphocytic Leukemia

Basile Stamatopoulos; Pascale Saussoy; Eric Van Den Neste; Lucienne Michaux; N Meuleman; Benjamin Haibe-Kains; Pierre Heimann; P. Martiat; D. Bron; Laurence Lagneaux


Haematologica-the Hematology Journal | 2009

MICRORNA SIGNATURES IN GENETIC SUBTYPES OF T-CELL ACUTE LYMPHOBLASTIC LEUKEMIA

Joni Van der Meulen; Pieter Van Vlierberghe; Pieter Mestdagh; Jo Vandesompele; Bruce Poppe; Nadine Van Roy; Tom Taghon; Jean Plum; Barbara Cauwelier; Dld Selleslag; Pierre Heimann; Peter Vandenberghe; Nicole Dastugue; Eric Delabesse; Carine Gervais; Mj Gregoire; M J Mozziconacci; Christine Lefebvre; J P P Meijerink; Jessica Buijs-Gladdines; Barbara De Moerloose; Yves Benoit; Anne De Paepe; Franki Speleman


Archive | 2008

Etude génotypique et phénotypique du Naevus Congénital, de taille moyenne et large

Barbara Dessars; Pierre Heimann; Gilbert Vassart


Archive | 2006

Consultations in Molecular Diagnostics Limitations and Practical Procedure in BclII-Ig Heavy Chain Gene Rearrangement Real-Time Quantitative Polymerase Chain Reaction

Barbara Dessars; Pierre Heimann; Hakim El Housni

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Barbara Dessars

Free University of Brussels

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Anne Hagemeijer

Katholieke Universiteit Leuven

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Lucienne Michaux

Katholieke Universiteit Leuven

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Peter Vandenberghe

Katholieke Universiteit Leuven

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Yves Benoit

Ghent University Hospital

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André Bosly

Université catholique de Louvain

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Anne Uyttebroeck

Katholieke Universiteit Leuven

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B Dutta

Katholieke Universiteit Leuven

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