THE PROGNOSTIC IMPACT OF ERYTHROID DYSPLASIA IN APLASTIC ANEMIA AND MYELODYSPLASTIC NEOPLASMS WITH SINGLE-LINEAGE DYSPLASIA

IF 0.7 Q4 HEMATOLOGY
T. Maeda , A. Matsuda , J. Kanda , H. Kawabata , T. Ishikawa , K. Tohyama , A. Kitanaka , K. Araseki , K. Shimbo , T. Hata , T. Suzuki , H. Kayano , K. Usuki , M. Shindo-Ueda , N. Arima , M. Nohgawa , A. Ohta , S. Chiba , Y. Miyazaki , S. Nakao , K. Mitani
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引用次数: 0

Abstract

Introduction

While genetic aberrations are becoming increasingly critical in disease classification, morphological abnormalities defined by a 10% threshold in each lineage continue to play a significant role as a diagnostic tool for myelodysplastic neoplasms (MDS). However, erythroid lineage dysplasia has been reported in some cases of aplastic anemia (AA), a phenomenon noted as common in the UK guidelines.

Methods

We assessed the impact of erythroid dysplasia on the survival in AA patients enrolled in an ongoing prospective registry, central morphological review (blinded), and follow-up study of AA and MDS conducted by the Japanese National Research Group on Idiopathic Bone Marrow Failure Syndromes. Furthermore, we compared the prognosis of AA patients with erythroid dysplasia with that of patients diagnosed in the same study with MDS presenting with single-lineage erythroid dysplasia (“MDS-SLED”). According to this study's definition, the criteria for excluding MDS are stringent, considering both bone marrow cellularity and megakaryocyte counts. Therefore, AA is not diagnosed when a decrease is not observed in the megakaryocyte count.

Results

The study included a total of 32 cases of AA with erythroid dysplasia, 56 cases of AA without dysplasia, and 47 cases of MDS-SLED. The overall survival or leukemia-free survival showed no significant difference between AA patients with and without erythroid dysplasia (both p=0.14). Nevertheless, distinct differences were seen between AA with erythroid dysplasia and those diagnosed with MDS-SLED (both p<0.0001).

Conclusions

Erythroid dysplasia should not exclude an AA diagnosis. In particular, megakaryocyte count plays an important role in differentiating between MDS from AA.

红细胞发育不良对再生障碍性贫血和骨髓增生异常性肿瘤单系发育不良的预后影响
导言虽然基因畸变在疾病分类中变得越来越重要,但作为骨髓增生异常性肿瘤(MDS)的诊断工具,各系10%阈值定义的形态学异常仍发挥着重要作用。我们评估了红系发育不良对参加日本全国特发性骨髓衰竭综合征研究小组正在进行的前瞻性登记、中央形态学审查(盲法)以及 AA 和 MDS 随访研究的 AA 患者生存率的影响。此外,我们还将患有红细胞发育不良的 AA 患者的预后与同一研究中确诊的患有单系红细胞发育不良的 MDS("MDS-SLED")患者的预后进行了比较。根据该研究的定义,排除 MDS 的标准非常严格,既要考虑骨髓细胞性,又要考虑巨核细胞计数。因此,如果未观察到巨核细胞计数减少,则不能诊断为 AA。结果该研究共纳入 32 例伴红细胞发育不良的 AA 患者、56 例无发育不良的 AA 患者和 47 例 MDS-SLED 患者。有红细胞发育不良和无红细胞发育不良的AA患者的总生存率和无白血病生存率无明显差异(P均=0.14)。结论红细胞发育不良不应排除 AA 的诊断。结论红细胞发育不良不应排除 AA 的诊断,尤其是巨核细胞计数在区分 MDS 和 AA 方面起着重要作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Leukemia Research Reports
Leukemia Research Reports Medicine-Oncology
CiteScore
1.70
自引率
0.00%
发文量
70
审稿时长
23 weeks
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