Sasi Ramakrishnan, Spruill Michelle, Perrotta Peter L
Department of Pathology, Anatomy and Laboratory Medicine, West Virginia University, Morgantown, WV 26506, USA.
Case Rep Hematol. 2024 Mar 20;2024:2127657. doi: 10.1155/2024/2127657. eCollection 2024.
Evidence suggests that the earliest genetic events in the evolution of a cancer can predate diagnosis by several years or decades. In chronic myeloid leukemia (CML), the BCR::ABL1 fusion driver mutation can be present for an extended period before clinical disease manifests. The time between the BCR::ABL1 occurrence and symptom onset is referred to as the latency period. Though modeling studies predict this latency period is no more than ten years, it is still unclear how long it can be. We present a case of a patient referred for suspected CML. Both karyotype and FISH analysis identified the (9;22)(34;11.2) translocation resulting in the Philadelphia chromosome formation in 98.5% of cells analyzed. The patient responded to imatinib and achieved a sustained complete hematologic and cytogenetic remission. Clinical history revealed that the same patient presented eight years previously with anemia. Various non-neoplastic conditions were excluded, and a bone marrow biopsy was performed to rule out MDS. Cytogenetic analysis at that time revealed del(20) as the sole abnormality in all 20 cells analyzed. No treatment was given since the presence of isolated del(20) is not considered evidence of MDS in the absence of diagnostic morphologic criteria. Retrospective FISH analysis of archived bone marrow pellets from this previous specimen revealed the presence of BCR::ABL1 in 1.8% of cells. A clonal population of cells harboring the BCR::ABL1 fusion was unambiguously detected in this patient's archived bone marrow pellet obtained eight years before the current CML diagnosis. This case demonstrates that Carnoy's fixed nuclear pellets stored in cytogenetic laboratories are suitable for detecting driver mutations years before disease presentation. Such archived material may be useful for the retrospective studies needed to better understand the initiation and subsequent development of hematological malignancies. By identifying individuals who are at increased risk, it may be possible to initiate preventive measures or begin treatment at an earlier stage before disease progression.
有证据表明,癌症进化过程中最早的基因事件可能比诊断提前数年或数十年。在慢性髓性白血病(CML)中,BCR::ABL1融合驱动突变在临床疾病表现之前可能存在很长一段时间。BCR::ABL1出现与症状发作之间的时间称为潜伏期。尽管模型研究预测这个潜伏期不超过十年,但它究竟能有多长仍不清楚。我们报告一例疑似CML患者的病例。核型分析和荧光原位杂交(FISH)分析均发现(9;22)(34;11.2)易位,在98.5%的分析细胞中形成了费城染色体。该患者对伊马替尼有反应,实现了持续的完全血液学和细胞遗传学缓解。临床病史显示,该患者八年前曾出现贫血。排除了各种非肿瘤性疾病,并进行了骨髓活检以排除骨髓增生异常综合征(MDS)。当时的细胞遗传学分析显示,在所有20个分析细胞中,del(20)是唯一的异常。由于在缺乏诊断形态学标准的情况下,孤立的del(20)的存在不被视为MDS的证据,因此未给予治疗。对该先前标本存档的骨髓细胞团进行回顾性FISH分析,发现1.8% 的细胞中存在BCR::ABL1。在该患者当前CML诊断前八年获得的存档骨髓细胞团中,明确检测到了携带BCR::ABL1融合的克隆细胞群。该病例表明,储存在细胞遗传学实验室的卡诺氏固定核细胞团适合在疾病出现前数年检测驱动突变。这种存档材料可能有助于进行回顾性研究,以更好地了解血液系统恶性肿瘤的起始和后续发展。通过识别风险增加的个体,有可能在疾病进展之前更早地采取预防措施或开始治疗。
