• Eur. J. Haematol. · Oct 2013

    Multicenter Study

    Molecular study of congenital erythrocytosis in 70 unrelated patients revealed a potential causal mutation in less than half of the cases (Where is/are the missing gene(s)?).

    • Celeste Bento, Helena Almeida, Tabita M Maia, Luís Relvas, Ana C Oliveira, Cédric Rossi, François Girodon, Carlos Fernandez-Lago, Ascension Aguado-Diaz, Cristina Fraga, Ricardo M Costa, Ana L Araújo, João Silva, Helena Vitória, Natalina Miguel, Maria Pedro Silveira, Guillermo Martin-Nuñez, and Maria Letícia Ribeiro.
    • Serviço de Hematologia, Centro Hospitalar e Universitário de Coimbra, Coimbra, Portugal.
    • Eur. J. Haematol. 2013 Oct 1; 91 (4): 361-8.

    IntroductionCongenital erythrocytosis can be classified as primary, when the defect is intrinsic to the RBC progenitors and independent of the serum erythropoietin (Epo) concentration, or secondary, when the erythrocytosis is the result of an upregulation of Epo production. Primary erythrocytosis is associated with mutations in the EPOR gene, secondary CE can de due to mutations that stabilize the hemoglobin in the oxygenated form or to mutations in the genes that control the transcriptional activation of the EPO gene - VHL, EGLN1, EPAS1. Chuvash polycythemia, caused by mutations in VHL gene, shares features of both primary and secondary erythrocytosis, with increased Epo production but also hypersensitivity of progenitors to Epo.Material And MethodsWith the main objective of describing the etiology and molecular basis of CE, we have studied 70 consecutive unrelated patients presenting with idiopathic erythrocytosis from our hematology clinic or referred from other centers. According to a study algorithm, we have sequenced all the genes described as associated with CE.Results And DiscussionErythrocytosis molecular etiology was identify in 25 (36%) of the 70 subjects. High-affinity Hb variants were the most common cause, present in 20% of the cases. New mutations were identified in the JAK2, EPOR, VHL, and EGLN1 genes.ConclusionsHigh-affinity hemoglobin variants are a very rare cause of secondary CE, but it seems likely that their incidence may be underestimated. Our experience shows that in erythrocytosis with a dominant inheritance and normal or inappropriate high Epo levels, the HBB and HBA genes should be the first to be studied. In spite of the seven genes known to be involved in CE, the majority of the cases have unknown etiology.© 2013 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.

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