- 作者:G. Thakrala ; gthakral@hawaii.edu" class="auth_mail" title="E-mail the corresponding author ; K. Vierkoettera ; S. Namikib ; S. Lawickia ; X. Fernandeza ; K. Igec ; W. Kawaharad ; C. Luma
- 关键词:AML ; Gene panel ; Screening ; Next-generation sequencing ; Detection ; Prognosis
- 刊名:Pathology - Research and Practice
- 出版年:2016
- 出版时间:May 2016
- 年:2016
- 卷:212
- 期:5
- 页码:372-380
- 全文大小:827 K
bsSec_2">Methods
The genomes of 11 randomly selected patients with AML were sequenced using next generation sequencing. A narrow three gene panel and broader 50 gene panel were contrasted.
bsSec_3">Results
The expanded gene panel detected one additional pathogenic mutation in five patients and two pathogenic mutations in two patients, resulting in a change in their risk profile. Only 5/11 (45%) of AML patients demonstrated a pathogenic mutation on the 3 gene profile, however all patients had at least one detectable pathogenic mutation on the broader gene panel. The detection of a concurrent mutation by the expanded gene panel reversed the favorable risk profile for three patients.
bsSec_4">Conclusions
Detection of concurrent mutations enables rejection or validation of prognoses associated with NPM1 or CEBPA mutations. DNMT3a and TP53 mutations in AML have a pertinent prognostic and therapeutic value for patients and their addition enhances the current three gene panel. In our small study, the three gene panel changed the prognosis for three patients (3/11, 27%) with the detection of commonly occurring AML mutations.