Concomitant or Sequential Chronic Lymphocytic Leukemia (CLL) and Chronic Myeloid Leukemia (CML): A Molecular and Clinical Survey

Clinical Lymphoma and Myeloma Pub Date : 2009-12-01 DOI:10.3816/CLM.2009.n.096

Carla Said , P. Heimann , B. Dessars , Dinh Phong , B. Cantiniaux , N. Meuleman , D. Bron

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Abstract

A 75-year-old man presented with B-CLL followed by a CML. We retrospectively analyzed the frozen BM and PB lymphocytes that evidenced 2 distinct clonal proliferations: one is a B CD5⁺/CD19⁺ lymphocyte population, without BCR-ABL fusion; the other is the CD19⁺ mononuclear cell population expressing traces of BCR-ABL, 3 years before the occurrence of CML. We suggest that (1) the emergence of the Ph⁺ clone after the treatment of CLL is probably related to RFC-induced immunosuppression, and (2) the long DFS of CLL might be due to the current TK inhibitor treatment

Full Abstract

Introduction

The coexistence of B-cell chronic lymphocytic leukemia (B-CLL) and chronic myeloid leukemia (CML) is a rare event. This coexistence has led to speculation of the clonal origin of these neoplasms. In some cases, 2 independent clones were demonstrated.

Patients and Methods

A 75-year-old man presented with splenomegaly and enlarged lymph nodes. Immunophenotype (kappa, CD19⁺, CD5⁺, CD23⁺) was compatible with B-CLL. Bone marrow examination showed infiltration by small lymphocytes next to a myeloid and megakaryocytic hyperplasia. Cytogenetic analysis of the marrow showed 46XY, del(16q). Philadelphia chromosome (Ph) was negative. The patient was diagnosed with B-CLL and treated by 6 RFC (rituximab/fludarabine/cyclophosphamide). He reached a molecular remission (MCR), but 3 years after the treatment for CLL, he developed hyperleukocytosis (26000/μL), mainly myeloid cells. Bone marrow smear demonstrated a myeloid hyperplasia with predominance of immature progenitors. The Ph was clearly evidenced, and CML was confirmed. The patient thus received thus imatinib 400 mg/day orally with hematologic but only partial molecular remission at 18 months. A Y25.3H mutation was detected, and the patient was switched to dasatinib with a successful evolution. The CLL remained in MCR during this 5-year period.

Results

To know whether CML is a secondary event induced by RFC treatment or the emergence of a latent CML clone, we analyzed retrospectively the frozen BM and PBL lymphocytes. The results were consistent with the view that there are 2 distinct clonal proliferations: one is a clonal B CD5⁺/CD19⁺ lymphocyte population, without BCR-ABL fusion; the other is the CD19⁺ mononuclear cell population expressing traces of BCR-ABL, 3 years before the occurrence of CML.

Conclusion

Our data provide evidence for a separate clonal origin for each disorder, raising the hypothesis that (1) the emergence of the Ph⁺ clone after the treatment of CLL is probably related to RFC-induced immunosuppression, and (2) the long disease-free survival of CLL might be due to the current tyrosine kinase inhibitor treatment.

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伴随或顺序性慢性淋巴细胞白血病(CLL)和慢性髓性白血病(CML):分子和临床调查

一名75岁男性，以B-CLL伴CML。我们回顾性分析了冷冻的BM和PB淋巴细胞，证实了2种不同的克隆增殖:一种是B CD5+/CD19+淋巴细胞群，没有BCR-ABL融合;另一个是在CML发生前3年表达BCR-ABL痕迹的CD19+单核细胞群。我们认为(1)CLL治疗后出现Ph+克隆可能与rfc诱导的免疫抑制有关，(2)CLL的长DFS可能与目前的TK抑制剂治疗有关。b细胞慢性淋巴细胞白血病(B-CLL)和慢性髓系白血病(CML)共存是罕见的事件。这种共存导致了对这些肿瘤克隆起源的猜测。在某些情况下，2个独立克隆被证实。患者与方法男性，75岁，脾肿大，淋巴结肿大。免疫表型(kappa、CD19+、CD5+、CD23+)与B-CLL兼容。骨髓检查显示小淋巴细胞浸润，伴髓细胞和巨核细胞增生。骨髓细胞遗传学分析显示46XY, del(16q)。费城染色体(Ph)为阴性。患者被诊断为B-CLL，并接受6种RFC(利妥昔单抗/氟达拉滨/环磷酰胺)治疗。他达到了分子缓解(MCR)，但在CLL治疗3年后，他出现了白细胞增多症(26000/μL)，主要是骨髓细胞。骨髓涂片示髓系增生，以未成熟祖细胞为主。Ph值明显，CML确诊。因此，患者口服伊马替尼400mg /天，在18个月时血液学只有部分分子缓解。检测到Y25.3H突变，并通过成功的进化将患者切换到达沙替尼。在这5年期间，CLL保持在MCR。结果为了了解CML是RFC治疗引起的继发性事件还是潜伏性CML克隆的出现，我们回顾性分析了冷冻的BM和PBL淋巴细胞。结果与2种不同的克隆增殖观点一致:一种是克隆B CD5+/CD19+淋巴细胞群，没有BCR-ABL融合;另一个是在CML发生前3年表达BCR-ABL痕迹的CD19+单核细胞群。结论我们的数据为每种疾病的克隆起源提供了证据，提出了以下假设:(1)CLL治疗后Ph+克隆的出现可能与rfc诱导的免疫抑制有关;(2)CLL的长期无病生存可能与当前酪氨酸激酶抑制剂治疗有关。

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