8 research outputs found

    Overall survival in IGP model subgroups.

    Full text link
    <p>A. Overall survival by cytogenetics and mutational profiles. Among patients with intermediate cytogenetics, three-year overall survival was 59% for those with favorable mutational profiles (A), 33% for those with intermediate mutational profiles (B), 51% for those who were <i>FLT3-</i>ITD negative with high-risk mutations (C) and 11% for those who were <i>FLT3-</i>ITD positive with high-risk mutations (D). Three-year overall survival was 77% among patients with favorable cytogenetics (favorable) and 21% among patients with unfavorable cytogenetics (unfavorable). B. Overall survival among patients with favorable mutational profiles. The overall survival curve for patients with intermediate cytogenetics and mutant <i>NPM1</i> plus mutant <i>IDH1</i> or <i>IDH2</i> was similar to the survival curve for patients with favorable cytogenetics (adjusted p = 0.697) and different from the survival curve for patients in the intermediate IGP risk group (adjusted p = 0.028). C. Overall survival among patients with <i>FLT3-</i>ITD negative AML and high-risk mutations. The overall survival curve for patients with <i>FLT3</i>-ITD negative (<i>FLT3-</i>ITD-) AML and co-occurring high-risk mutations (<i>TET2</i>, <i>ASXL1</i> and/or <i>PHF6</i>) was not significantly different from the survival curves for patients with unfavorable cytogenetics or patients with intermediate IGP risk (adjusted p = 0.111 and p = 0.919, respectively). D. Overall survival among patients with <i>FLT3</i>-ITD positive AML and high-risk mutations. The overall survival curve for patients with <i>FLT3</i>-ITD positive (<i>FLT3</i>-ITD+) AML and co-occurring high-risk mutations (trisomy 8, <i>TET2</i> and/or <i>DNMT3A</i>) was similar to the survival curve for patients with unfavorable cytogenetics (adjusted p = 0.793) and different from the survival curve for patients in the intermediate IGP risk group (adjusted p = 0.022).</p

    A Modified Integrated Genetic Model for Risk Prediction in Younger Patients with Acute Myeloid Leukemia

    Full text link
    <div><p>Background</p><p>Although cytogenetics-based prognostication systems are well described in acute myeloid leukemia (AML), overall survival (OS) remains highly variable within risk groups. An integrated genetic prognostic (IGP) model using cytogenetics plus mutations in nine genes was recently proposed for patients ≤60 years to improve classification. This model has not been validated in clinical practice.</p><p>Methods and Findings</p><p>We retrospectively studied 197 patients with newly diagnosed de novo AML. We compared OS curves among the mutational profiles defined by the IGP model. The IGP model assigned patients with intermediate cytogenetics as having favorable, intermediate or unfavorable mutational profiles. The IGP model reassigned 50 of 137 patients with intermediate cytogenetics to favorable or unfavorable mutational profiles. Median OS was 2.8 years among 14 patients with intermediate cytogenetics and favorable mutational profiles (mutant <i>NPM1</i> and mutant <i>IDH1</i> or <i>IDH2</i>) and 1.3 years among patients with intermediate mutational profiles. Among patients with intermediate cytogenetics labeled as having unfavorable mutational profiles, median OS was 0.8 years among 24 patients with <i>FLT3</i>-ITD positive AML and high-risk genetic changes (trisomy 8, <i>TET2</i> and/or <i>DNMT3A</i>) and 1.7 years among 12 patients with <i>FLT3</i>-ITD negative AML and high-risk mutations (<i>TET2</i>, <i>ASXL1</i> and/or <i>PHF6</i>). OS for patients with intermediate cytogenetics and favorable mutational profiles was similar to OS for patients with favorable cytogenetics (p = 0.697) and different from patients with intermediate cytogenetics and intermediate mutational profiles (p = 0.028). OS among patients with <i>FLT3</i>-ITD positive AML and high-risk genetic changes was similar to patients with unfavorable cytogenetics (p = 0.793) and different from patients with intermediate IGP profile (p = 0.022). Patients with <i>FLT3</i>-ITD negative AML and high-risk mutations, defined as ‘unfavorable’ in the IGP model, had OS similar to patients with intermediate IGP profile (p = 0.919).</p><p>Conclusions</p><p>The IGP model was not completely validated in our cohort. However, mutations in six out of the nine genes can be used to characterize survival (<i>NPMI</i>, <i>IDH1</i>, <i>IDH2</i>, <i>FLT3-</i>ITD, <i>TET2</i>, <i>DNMT3A</i>) and allow for more robust prognostication in the patients who are re-categorized by the IGP model. These mutations should be incorporated into clinical testing for younger patients outside of clinical trials, in order to guide therapy.</p></div

    Overall survival by integrated genetic prognostic (IGP) profile (n = 197).

    Full text link
    <p>The overall survival curve for patients with favorable IGP risk was significantly different from the curve for patients with unfavorable IGP risk (adjusted p<0.001). There was no significant difference in survival curves between patients with favorable IGP risk and patients with intermediate IGP risk (adjusted p = 0.055), or between patients with unfavorable IGP risk and patients with intermediate IGP risk (adjusted p = 0.596).</p

    Overall survival by modified IGP profile (n = 197).

    Full text link
    <p>The overall survival curve for patients with favorable M-IGP risk was significantly different from the survival curve for patients with unfavorable IGP risk (adjusted p<0.001). There was no significant difference in survival curves between patients with favorable M-IGP profiles and patients with intermediate M-IGP profiles (adjusted p = 0.178), or between patients with unfavorable M-IGP profiles and patients with intermediate M-IGP profiles (adjusted p = 0.100).</p
    corecore