Tutaeva V, Misurin A V, Michiels J J, Rozenberg J M, Sokolova M A, Ivanova V L, Kolosheinova T I, Manakova T E, Levina A A, Semenova E A, Khoroshko N D
National Hematology Research Centre, Moscow, Russia.
Hematology. 2007 Dec;12(6):473-9. doi: 10.1080/10245330701384005.
Increased PRV-1 mRNA expression and the presence of Jak2(V617F) mutation in peripheral blood granulocytes are specific markers for chronic myeloproliferative disorders (MPD), which facilitate the differential diagnosis between polycythemia vera (PV) and secondary erythrocytosis (SE) and may be helpful for monitoring treatment efficacy in MPD patients. We evaluated the presence of the Jak2V617F mutation and increased PRV-1 mRNA expression along with previously established markers - erythropoietin (EPO) independent colony formation (EEC) and erythropoietin level for diagnosis of PV and assessment of treatment efficiency. Increased PRV-1 expression was found in 37 out of 46 patients diagnosed with PV (80%), in 4 out of 15 patients diagnosed with essential thrombocythemia (ET) (27%) and in 4 out of 8 patients with chronic idiopathic myelofibrosis (CIMF) (50%), and increased PRV-1 expression plus EEC formation was observed in 19 of 36 examined MPD patients indicating the superiority of PVSG and WHO bone marrow criteria for the diagnosis of ET, PV and CIMF. We could confirm a very high sensitivity, specificity and utility of the Jak2(V617F) mutation for differential diagnosis between PV and SE. Spontaneous EEC, serum EPO levels, PRV-1 expression was evaluated in 22 PV patients who carried the Jak2(V617F) mutation. A concordance of increased PRV-1 expression and presence of Jak2(V617F) mutation in 19/22 (85%); of increased PRV-1/Jak2/EEC in 14/22 (63%); and of Jak2/PRV-1/EEC/low Epo level in 10/22 (45%) patients was found indicating the superiority of the presence of Jak2(V617F) mutation for the diagnosis of PV. IFN-alpha therapy in patients with PV was more effective then hydroxyurea treatment and significantly reduced increased PRV-1 expression together with higher levels of Jak2(V617F) mutation (50-100%) in PV patients treated with hydroxy urea (HU) and lower levels of Jak2(V617F) mutation (35-90%) in PV patients treated with IFN-alpha. Normal PRV-1 expression level was observed in 44% of PV patients who achieved clinical remission and only in 3% of patient who did not. These preliminary observations indicate that the Jak2(V617F) mutation in particular and PRV-1 overexpression appear to be suitable markers for monitoring treatment efficiency in prospective randomised clinical studies comparing pegylated interferon and hydroxyurea in well defined PV patients with a clear indication for cytoreductive therapy.
外周血粒细胞中PRV-1 mRNA表达增加以及Jak2(V617F)突变的存在是慢性骨髓增殖性疾病(MPD)的特异性标志物,有助于真性红细胞增多症(PV)和继发性红细胞增多症(SE)的鉴别诊断,且可能有助于监测MPD患者的治疗效果。我们评估了Jak2V617F突变的存在、PRV-1 mRNA表达增加情况,以及先前确立的标志物——促红细胞生成素(EPO)非依赖性集落形成(EEC)和促红细胞生成素水平,用于PV的诊断及治疗效果评估。在46例诊断为PV的患者中,有37例(80%)PRV-1表达增加;在15例诊断为原发性血小板增多症(ET)的患者中,有4例(27%)PRV-1表达增加;在8例慢性特发性骨髓纤维化(CIMF)患者中,有4例(50%)PRV-1表达增加。在36例接受检查的MPD患者中,有19例观察到PRV-1表达增加加EEC形成,这表明PVSG和WHO骨髓标准在ET、PV和CIMF诊断方面具有优越性。我们可以证实Jak2(V617F)突变在PV和SE鉴别诊断中具有很高的敏感性、特异性和实用性。对22例携带Jak2(V617F)突变的PV患者评估了自发EEC、血清EPO水平、PRV-1表达。发现19/22(85%)的患者PRV-1表达增加与Jak2(V617F)突变同时存在;14/22(63%)的患者PRV-1/Jak2/EEC增加;10/22(45%)的患者Jak2/PRV-1/EEC/低Epo水平增加,这表明Jak2(V617F)突变在PV诊断中具有优越性。PV患者接受干扰素-α治疗比羟基脲治疗更有效,并且在接受羟基脲(HU)治疗的PV患者中,显著降低了增加的PRV-1表达以及更高水平的Jak2(V617F)突变(50 - 100%),在接受干扰素-α治疗的PV患者中Jak2(V617F)突变水平较低(35 - 90%)。在实现临床缓解的PV患者中,44%观察到PRV-1表达水平正常,而未缓解的患者中只有3%观察到PRV-1表达水平正常。这些初步观察结果表明,在比较聚乙二醇化干扰素和羟基脲对明确有细胞减灭治疗指征的PV患者疗效的前瞻性随机临床研究中,Jak2(V617F)突变尤其是PRV-1过表达似乎是监测治疗效果的合适标志物。
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