Kottaridis Panagiotis D, Gale Rosemary E, Langabeer Stephen E, Frew Marion E, Bowen David T, Linch David C
Department of Haematology, University College London, London, United Kingdom.
Blood. 2002 Oct 1;100(7):2393-8. doi: 10.1182/blood-2002-02-0420.
FLT3 mutations, either internal tandem duplications (ITDs) or aspartate residue 835 (D835) point mutations, are present in approximately one third of patients with acute myeloid leukemia (AML) and have been associated with an increased relapse rate. We have studied FLT3 mutations in paired presentation and relapse samples to ascertain the biology of these mutations and to evaluate whether they can be used as markers of minimal residual disease. At diagnosis, 24 patients were wild-type FLT3, and 4 acquired a FLT3 mutation at relapse (2 D835(+), 2 ITD(+)), with a further patient acquiring an ITD at second relapse. Of 20 patients positive at diagnosis (18 ITD(+), 2 D835(+)), 5 who were all originally ITD(+) had no detectable mutation at relapse, as determined by a sensitive radioactive polymerase chain reaction. One of these patients had acquired an N-Ras mutation not detectable at presentation. Furthermore, another patient had a completely different ITD at relapse, which could not be detected in the presentation sample. These results indicate that FLT3 mutations are secondary events in leukemogenesis, are unstable, and thus should be used cautiously for the detection of minimal residual disease.
FMS样酪氨酸激酶3(FLT3)突变,即内部串联重复(ITD)或天冬氨酸残基835(D835)点突变,大约存在于三分之一的急性髓系白血病(AML)患者中,并与复发率增加相关。我们研究了配对的初诊和复发样本中的FLT3突变,以确定这些突变的生物学特性,并评估它们是否可用作微小残留病的标志物。诊断时,24例患者为FLT3野生型,4例在复发时获得FLT3突变(2例D835阳性,2例ITD阳性),另有1例患者在第二次复发时获得ITD。在诊断时为阳性的20例患者中(18例ITD阳性,2例D835阳性),5例最初均为ITD阳性的患者在复发时未检测到突变,这是通过敏感的放射性聚合酶链反应确定的。其中1例患者获得了初诊时未检测到的N-Ras突变。此外,另1例患者在复发时出现了完全不同的ITD,在初诊样本中未检测到。这些结果表明,FLT3突变是白血病发生过程中的继发事件,具有不稳定性,因此在检测微小残留病时应谨慎使用。
