Molecular diagnostics of myeloproliferative neoplasms

Langabeer, Stephen E.; Andrikovics, Hajnalka; Asp, Julia; Bellosillo, Beatríz; Carillo, Serge; Haslam, Karl; Kjær, Lasse; Lippert, Éric; Mansier, Olivier; Leibundgut, Elisabeth Oppliger; Percy, Melanie J.; Porret, Naomi; Palmqvist, Lars; Schwarz, Jiřı́; McMullin, Mary Frances; Schnittger, Susanne; Pallisgaard, Niels; Hermouet, Sylvie

doi:10.1111/ejh.12578

Cited by 75 publications

(69 citation statements)

References 90 publications

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“…TET2, DNMT3A and ASXL1. 10 In the current study, mutations were found in 35 additional genes (Figure 3 and Online Supplementary Table S3). All but one patient with MPL mutated ET had additional mutations, while in 39% of ET cases with JAK2 mutation (n=7) and 28% with CALR mutation (n=5) no additional mutations were found.…”

Section: 4mentioning

confidence: 53%

Mutation status of essential thrombocythemia and primary myelofibrosis defines clinical outcome

et al. 2016

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Section: 4mentioning

confidence: 53%

Mutation status of essential thrombocythemia and primary myelofibrosis defines clinical outcome

et al. 2016

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“…Indeed, apart from JAK2 V617F , MPL , and CALR mutations, several other gene mutations have been described: TET2 (in 5% of cases), DNMT3A (in 1–5%), and ASXL1 (in 2–5%) [16]. Thirty-five other gene mutations have been reported [7].…”

Section: Discussionmentioning

confidence: 99%

JAK2V617F, CALR, and MPL Mutations and Bone Marrow Histology in Patients with Essential Thrombocythaemia

et al. 2018

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Introduction: Mutations in the JAK2, CALR, and MPL genes have been shown to have prognostic value in essential thrombocythaemia (ET), but no clear association with morphological changes has been reported so far. We investigated the possible correlation between gene mutations and histopathological features in bone marrow (BM) biopsies of patients with ET. Methods: Marrow cellularity, fibrosis, and the number of total and dysmorphic megakaryocytes and clusters of megakaryocytes were compared to gene mutations in 90 cases of ET at diagnosis. Results: The JAK2^V617F mutation was found in 58.9%, CALR in 28.9%, and MPL in 4.4% of the cases, and 7.8% were triple-negative. JAK2^V617F-mutated ET showed a high BM cellularity, the lowest number of clusters of megakaryocytes and the highest number of dysmorphic megakaryocytes; CALR-mutated ET showed a reduced BM cellularity, many clusters of large megakaryocytes, and very few dysmorphic megakaryocytes; MPL-mutated ET showed the lowest BM cellularity, the highest number of clustered and large megakaryocytes, and the lowest number of dysmorphic megakaryocytes. Triple-negative ET cases had the highest BM cellularity. Conclusions: Distinct morphological patterns were associated with gene mutations in ET, supporting the classification of ET into different subtypes.

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“…A Philadelphia-negatív klasszikus myeloproliferativ neoplasiák (MPN) köré-be tartozik az essentialis thrombocythaemiával (ET) és a primer myelofibrosissal (PMF) együtt. A kórkép kialakulására jellemző a JAK-STAT jelátviteli útvonal folyamatos, konstitucionális aktivációja, amely a myeloproliferatióhoz vezet [1,2].…”

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Philadelphia-negatív krónikus Myeloproliferativ Neoplasia Magyarországi Regiszter. Polycythaemia verás betegeink adatainak elemzése

et al. 2017

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Bevezetés és célkitűzés:A HUMYPRON munkacsoport által 2013-ban létrehozott Philadelphia-negatív myeloproliferativ neoplasiás betegek magyar regiszteréből a polycythaemia verás betegek adatait elemezzük. Módszer: A 15 hematológiai centrumból regisztrált 351 JAK2 V617F -és exon-12-mutációpozitív polycythaemia verás beteg epidemiológiai, klinikai, diagnosztikus és kezelési jellemzőit, vascularis és transzformációs eseményeit dolgoztuk fel. A diagnózist megelőző és azt követő thromboemboliás eseményeket a Landolfi szerinti rizikófelmérés alapján értelmeztük. Eredmények: A diagnózist megelőzően 106 betegben 116, a diagnózist követő időszakban 106 betegben 152 thromboemboliás eseményt regisztráltunk. A major artériás események szignifikánsan csökkentek (p<0,0001), a minor vé-nás események szignifikánsan fokozódtak (p<0,0001) a diagnózist követően. A betegség transzformációját 26 esetben, a major vérzést 25 esetben észleltük. Következtetések: Online regiszterünk könnyen kezelhető, lehetővé teszi a hazai betegek jellemzőinek felmérését és az eredmények gyors kiértékelését. A Landolfi-rizikóbecslés eredményesnek bizonyult. Kérdőívünket a kiértékelést kö-vetően pontosítottuk. A diagnosztikus kritériumok, a rizikóbecslés és az ennek megfelelő kezelési ajánlás pontosabb betartása szükséges, amelyre ajánlásokat tettünk. Orv Hetil. 2017; 158(23): 901-909. Kulcsszavak: polycythaemia vera, regiszter, myeloproliferativ neoplasia, cardiovascularis rizikófaktor, Landolfirizikóbecslés Hungarian Philadelphia negative chronic myeloproliferative neoplasia registry Evaluation of the polycythemia vera patientsIntruduction and aim: The Hungarian National Registry for Philadelphia chromosome negative myeloproliferative neoplasms has been developed. The aim of the recent study is to assess the clinical characteristics of Hungarian patients with polycythemia vera. Method: Data of 351 JAK2 V617F and exon 12 mutation positive polycythemia vera patients were collected online from 15 haematology centres reporting epidemiologic, clinical characteristics, diagnostic tools, therapeutic interventions, thromboembolic complications, disease transformations. Vascular events prior to and after diagnosis were evaluated upon the Landolfi risk assessment scale. Results: 116 thromboembolic events were reported in 106 PV patients prior to diagnosis and 152 occasions in 102 patients during follow-up. The frequency of major arterial events were significantly reduced (p<0.0001) and the minor venous events were significantly elevated (p<0.0001) after the diagnosis. Major hemorrhagic complications were found in 25 and transformation in 26 cases.

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Molecular diagnostics of myeloproliferative neoplasms

Cited by 75 publications

References 90 publications

Mutation status of essential thrombocythemia and primary myelofibrosis defines clinical outcome

Mutation status of essential thrombocythemia and primary myelofibrosis defines clinical outcome

<b><i>JAK2</i></b><sup>V617F</sup>, <b><i>CALR</i></b>, and <b><i>MPL</i></b> Mutations and Bone Marrow Histology in Patients with Essential Thrombocythaemia

Philadelphia-negatív krónikus Myeloproliferativ Neoplasia Magyarországi Regiszter. Polycythaemia verás betegeink adatainak elemzése

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