Steinbach Daniel, Schramm Alexander, Eggert Angelika, Onda Masanori, Dawczynski Kristin, Rump Andreas, Pastan Ira, Wittig Susann, Pfaffendorf Nadine, Voigt Astrid, Zintl Felix, Gruhn Bernd
University Children's Hospital Jena, Jena, Germany.
Clin Cancer Res. 2006 Apr 15;12(8):2434-41. doi: 10.1158/1078-0432.CCR-05-2552.
Monitoring of minimal residual disease (MRD) has become a strong diagnostic tool in acute lymphoblastic leukemia. It is used for risk-adapted therapy and for the recognition of pending relapses. In acute myeloid leukemia (AML), there is still a need for more suitable MRD markers.
A stepwise approach which combined genome-wide expression profiling, TaqMan low density arrays, and a TaqMan real-time PCR-based screening was used to identify new markers for the monitoring of MRD in AML. Leukemic cells from 52 children with AML and 145 follow-up samples from 25 patients were analyzed.
Seven genes were identified which are vastly overexpressed in many patients with AML compared with healthy bone marrow: CCL23, GAGED2, MSLN, SPAG6, and ST18 as well as the previously described markers WT1 and PRAME. The expression of all genes decreased to normal levels in patients who achieved a continuous complete remission. Elevated levels of at least one gene were found prior to relapse in 7 out of 10 patients who relapsed.
This set of genes should allow a sensitive and specific monitoring of MRD in AML. Notably, some of these markers could also serve as therapeutic targets or might be involved in leukemogenesis. MSLN is already used as a target for immunotherapy in clinical trials in other malignancies.
微小残留病(MRD)监测已成为急性淋巴细胞白血病的一种强大诊断工具。它用于风险适应性治疗以及识别即将发生的复发。在急性髓系白血病(AML)中,仍需要更合适的MRD标志物。
采用一种逐步方法,该方法结合全基因组表达谱分析、TaqMan低密度芯片和基于TaqMan实时PCR的筛选,以鉴定用于监测AML中MRD的新标志物。对52例AML患儿的白血病细胞和25例患者的145份随访样本进行了分析。
鉴定出7个基因,与健康骨髓相比,这些基因在许多AML患者中大量过表达:CCL23、GAGED2、MSLN、SPAG6和ST18,以及先前描述的标志物WT1和PRAME。在实现持续完全缓解的患者中,所有基因的表达均降至正常水平。在10例复发患者中,有7例在复发前发现至少一种基因水平升高。
这组基因应能对AML中的MRD进行敏感且特异的监测。值得注意的是,其中一些标志物也可作为治疗靶点或可能参与白血病发生过程。MSLN已在其他恶性肿瘤的临床试验中用作免疫治疗靶点。
