慢性髓性白血病b淋巴母细胞期:1例报告及文献复习。

A. Ware, L. Wake, P. Brown, Jonathan A. Webster, B. Smith, A. Duffield
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引用次数: 3

摘要

慢性髓系白血病(Chronic myeloid leukemia, CML)是一种以互易位为特征的克隆性造血干细胞疾病,t(9;22) (q34.1;q11.2)。这导致BCR和ABL1基因的融合,编码一种活性酪氨酸激酶,导致髓系谱系不受调节的增殖。BCR/ABL1融合蛋白不仅存在于CML中,也存在于新发b淋巴细胞白血病(B-LL)的一个亚群中。然而,CML中的融合蛋白通常是稍长的p210变体,而在B-LL中更常见的是p190变体。如果不进行治疗,CML将进展到加速期和/或爆炸期(BP)。疾病进展通常以额外染色体异常的积累为特征。针对BCR/ABL1的酪氨酸激酶抑制剂(TKI)疗法的发展已经彻底改变了CML的治疗方法,并极大地改善了预后,尽管尽管TKI治疗,该疾病仍可能进展。胚期最常表现为髓性BP;然而,高达30%的BP表现为淋巴样BP (LBP),典型的是b细胞谱系。LBP的b淋巴母细胞具有与新生B-LL难以区分的表型。然而,LBP通常携带p210 BCR/ABL转录本,并可能表现出明显的染色体异常,包括染色体9p的缺失。CML-BP的预后很差,尽管TKI治疗和干细胞移植改善了患者的生存率,而且与髓性BP相比,LBP的生存率更高。在此,我们报告一例CML合并b淋巴样BP并回顾目前的文献。
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B-Lymphoid Blast Phase of Chronic Myeloid Leukemia: A Case Report and Review of the Literature.
Chronic myeloid leukemia (CML) is a clonal hematopoietic stem cell disorder characterized by a reciprocal translocation, t(9;22) (q34.1;q11.2). This leads to fusion of the BCR and ABL1 genes, encoding an active tyrosine kinase that causes unregulated proliferation of the myeloid lineage. The BCR/ABL1 fusion protein is found not only in CML, but also in a subset of de novo B-lymphoblastic leukemia (B-LL). However, the fusion protein in CML is characteristically the slightly longer p210 variant, whereas the p190 variant is more frequently found in B-LL. Without treatment, CML will progress to accelerated and/or blast phase (BP). Disease progression is often characterized by accumulation of additional chromosomal abnormalities. The development of tyrosine kinase inhibitor (TKI) therapy that targets BCR/ABL1 has revolutionized treatment of CML and vastly improved outcomes, although the disease can still progress despite TKI therapy. Blast phase most commonly manifests as myeloid BP; however, up to 30% of BP presents as lymphoid BP (LBP), typically of the B-cell lineage. The B-lymphoblasts of LBP have a phenotype indistinguishable from that of de novo B-LL. However, LBP typically carries the p210 BCR/ABL transcript and may show distinct chromosomal anomalies, including loss of chromosome 9p. The prognosis for CML-BP is poor, although survival has improved with TKI therapy and stem cell transplant, and LBP has been associated with superior survival compared with myeloid BP. Here we present a case of CML in B-lymphoid BP and review the current literature.
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期刊介绍: Each issue of Pathology Case Reviews examines one vital theme in the field with peer-reviewed, clinically oriented case reports that focus on diagnosis, specimen handling and reports generation. Each theme-oriented issue covers both histopathologic and cytopathologic cases, offering a comprehensive perspective that includes editorials and review articles of the newest developments in the field, differential diagnosis hints, applications of new technologies, reviews of current issues and techniques and an emphasis on new approaches.
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