4 research outputs found

    <i>TP53</i> alterations in primary and secondary SĂ©zary syndrome: A diagnostic tool for the assessment of malignancy in patients with erythroderma

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    <div><p>Recent massive parallel sequencing data have evidenced the genetic diversity and complexity of SĂ©zary syndrome mutational landscape with <i>TP53</i> alterations being the most prevalent genetic abnormality. We analyzed a cohort of 35 patients with SS and a control group of 8 patients with chronic inflammatory dermatoses. <i>TP53</i> status was analyzed at different clinical stages especially in 9 patients with a past-history of mycosis fungoides (MF), coined secondary SS. <i>TP53</i> mutations were only detected in 10 patients with either primary or secondary SS (29%) corresponding to point mutations, small insertions and deletions which were unique in each case. Interestingly, <i>TP53</i> mutations were both detected in sequential unselected blood mononuclear cells and in skin specimens. Cytogenetic analysis of blood specimens of 32 patients with SS showed a <i>TP53</i> deletion in 27 cases (84%). Altogether 29 out of 35 cases exhibited <i>TP53</i> mutation and/or deletion (83%). No difference in prognosis was observed according to <i>TP53</i> status while patients with secondary SS had a worse prognosis than patients with primary SS. Interestingly, patients with <i>TP53</i> alterations displayed a younger age and the presence of <i>TP53</i> alteration at initial diagnosis stage supports a pivotal oncogenic role for <i>TP53</i> mutation in SS as well as in erythrodermic MF making <i>TP53</i> assessment an ancillary method for the diagnosis of patients with erythroderma as patients with inflammatory dermatoses did not display <i>TP53</i> alteration.</p></div

    Clinical data and somatic alterations of <i>TP53</i> gene in SĂ©zary syndrome.

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    <p>Age at diagnosis (years), Clinical status means survival time in months after diagnosis of Sézary syndrome until the death or last clinical status, ⱡ data determined by fluorescence <i>in situ</i> hybridization, ¥ data determined by quantitative fluorescence <i>in situ</i> hybridization.</p
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