Bernasconi P, Alessandrino E P, Boni M, Bonfichi M, Morra E, Lazzarino M, Campagnoli C, Astori C
Division of Hematology, Policlinico San Matteo IRCCS, Pavia, Italy.
Am J Hematol. 1994 Aug;46(4):270-7. doi: 10.1002/ajh.2830460404.
One hundred eighty-eight unselected consecutive patients with "de novo" myelodysplastic syndrome (MDS) were studied cytogenetically. They were subclassified as 4 refractory anemia with ringed sideroblasts (RARS), 67 refractory anemia (RA), 58 refractory anemia with excess of blasts (RAEB), 40 RAEB in transformation (RAEB-t), and 19 chronic myelomonocytic leukemia (CMML). The overall incidence of chromosome abnormalities was 69%. The RAEB and RAEB-t patients showed karyotypic changes, more often than RA and CMML (76% and 100% vs. 56% and 42%, respectively). The most frequent single anomaly was del(5)(q13-q22q33) (22 cases), followed by monosomy 7 or del 7q (11 cases), del(11) (q14q23) (8 cases), trisomy 8 (4 cases). Complex karyotypes (defined by the presence of three or more structural or numerical abnormalities) were detected in 33 patients. With regard to the FAB classification, del (5)(q13q33) was associated with RA, and complex rearrangements with RAEB and RAEB-t. Leukemic transformation occurred in 66 patients (46%), none with a normal karyotype or del(11)(q14q23) as single abnormality. In patients carrying 5q- alone, acute evolution correlated with proximal breakpoint localization, being found in no case with del(5)(q13q33) but in three out of four cases with del(5)(q22q33). Acute leukemia (AL) progression happened in all cases with complex rearrangements and monosomy 7 or del(7q). Two of the four trisomy eight patients evolved in AL. By using the Cox proportional hazard regression analysis it was demonstrated that the karyotype abnormality was a significant predictor of leukemic transformation (P < 0.001). Patients with abnormal karyotypes without complex abnormalities had a survival (median survival 12 months) shorter than that of cases with only normal metaphases (median 83 months) (P < 0.001); patients with a mixture of normal/abnormal metaphases had a median survival of 31 months. The median survival for complex karyotypes was 7 months. Among cases with single defects, del(5)(q13q33) showed the best survival (64 months), monosomy 7 and del(7q) the worst (7 months) (P < 0.001).
对188例未经选择的连续性“初发”骨髓增生异常综合征(MDS)患者进行了细胞遗传学研究。他们被分类为4例环形铁粒幼细胞难治性贫血(RARS)、67例难治性贫血(RA)、58例原始细胞增多的难治性贫血(RAEB)、40例转化中的RAEB(RAEB-t)和19例慢性粒单核细胞白血病(CMML)。染色体异常的总体发生率为69%。RAEB和RAEB-t患者的核型改变比RA和CMML更常见(分别为76%和100%对56%和42%)。最常见的单一异常是del(5)(q13-q22q33)(22例),其次是7号单体或del 7q(11例)、del(11)(q14q23)(8例)、8号三体(4例)。在33例患者中检测到复杂核型(由三个或更多结构或数量异常定义)。关于FAB分类,del(5)(q13q33)与RA相关,复杂重排与RAEB和RAEB-t相关。66例患者(46%)发生白血病转化,无一例核型正常或单一异常为del(11)(q14q23)。在仅携带5q-的患者中,急性进展与近端断点定位相关,在del(5)(q13q33)患者中未发现,但在del(5)(q22q33)患者中四分之三出现。所有复杂重排以及7号单体或del(7q)的患者均发生急性白血病(AL)进展。4例8号三体患者中有2例进展为AL。通过Cox比例风险回归分析表明,核型异常是白血病转化的重要预测指标(P<0.001)。核型异常但无复杂异常的患者生存期(中位生存期12个月)短于仅中期正常的患者(中位83个月)(P<0.001);正常/异常中期混合的患者中位生存期为31个月。复杂核型的中位生存期为7个月。在单一缺陷病例中,del(5)(q13q33)生存期最佳(64个月),7号单体和del(7q)最差(7个月)(P<0.001)。
