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Low frequency and variability of FLT3 mutations in Korean patients with acute myeloid leukemia
Authors:Bang Soo-Mee  Ahn Jeong Yeal  Park Jiyoon  Park Se Hoon  Park Jinny  Cho Eun Kyung  Shin Dong Bok  Lee Jae Hoon  Yoo Soo Jin  Jeon In Sang  Kim Yeo-Kyeoung  Kim Hyeoung Joon  Kim Hee-Nam  Lee Il-Kwon  Kang Hyoung Jin  Shin Hee Young  Ahn Hyo Seop
Affiliation:Department of Internal Medicine, Seoul National University Bundang Hospital, Seongnam, Korea.
Abstract:FLT3 mutations are common genetic changes, and are reported to have prognostic significance in acute myeloid leukemia (AML). The FLT3 internal tandem duplication (ITD) and the D835 activating mutation in the tyrosine kinase domain (TKD) were analyzed by polymerase chain reaction (PCR) in the genomic DNA of Korean patients with AML at diagnosis and during follow-up. There were 226 patients with AML enrolled between March 1996 and August 2005. The incidence of ITD and TKD at diagnosis was 13% (29/226) and 3% (6/226). When compared to Western and other Asian patients with AML, Korean patients had a lower frequency by about two-thirds of ITD and TKD. Among the non-M3 cases (N=203), the patients with an ITD had a significantly shorter event-free survival when compared with those without an ITD (p=0.0079). Among 54 relapsed patients, 9 patients had the FLT3 ITD at diagnosis. Six patients demonstrated a reappearance of the ITD and 3 patients remained negative at relapse. One patient, among 45 patients who relapsed, had a negative baseline ITD but acquired a de novo ITD at relapse. There were 101 samples from 93 patients in remission; they were all negative for an ITD. Among 34 patients who failed to achieve a remission, five patients had a persistent ITD and one patient had a de novo ITD. These results support the concept of resistance of FLT3 ITD leukemic clones to chemotherapy. Therefore, effective therapy with FLT3 targeting agents may improve the prognosis of non-M3 AML patients with the FLT3 mutation.
Keywords:FLT3 Mutations   Internal Tandem Duplication   Tyrosine Kinase Domain Mutation   Leukemia   Myeloid   Acute
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