Clinical, Immunologic, and Genetic Characteristics of T-lymphoblastic Leukemia with STIL-TAL1 Fusion.

IF 0.7 4区医学 Q4 MEDICAL LABORATORY TECHNOLOGY

Clinical laboratory Pub Date : 2025-03-01 DOI:10.7754/Clin.Lab.2024.241025

Sang Mook Kim, Soong Ki Roh, Ji Yeon Ham, Yu Kyung Kim, Soon Hee Chang

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引用次数: 0

Abstract

Background: T-lymphoblastic leukemia (T-ALL) is an aggressive hematologic malignancy with a less favorable prognosis. The genetic background of T-ALL is widely heterogeneous, with the co-occurrence of multiple genetic abnormalities. The STIL-TAL1 rearrangement results from a submicroscopic deletion on chromosome 1p33 and is present in 15 - 25% of T-ALL cases. Submicroscopic deletions are not detected by conventional cytogenetic ana-lyses but can be identified through array comparative genomic hybridization and/or high-throughput RNA sequencing. Patients with the STIL-TAL1 fusion exhibit distinct characteristics, such as a young age, high white blood cell count, typical immunophenotype, and specific genetic abnormalities. However, the clinical, laboratory, and prognostic significance of this rearrangement remains unclear. This study was performed to identify STIL-TAL1 rearrangement resulting from submicroscopic 1p33 deletion in T-ALL and to investigate the clinical, immunologic, and genetic characteristics of T-ALL patients with STIL-TAL1 fusion.

Methods: A total of 15 T-ALL patients were enrolled over a 6-year period (2018 - 2023). We evaluated clinical features and laboratory findings, including immunophenotyping, multiplex reverse transcriptase-polymerase chain reaction (RT-PCR), karyotype analysis, next-generation sequencing (NGS), and chromosomal microarray analysis (CMA), on bone marrow or peripheral blood specimens at the diagnostic stage.

Results: Multiplex RT-PCR was performed on 15 cases of T-ALL, and STIL-TAL1 fusion was detected in 3 cases (20.0%, 3/15). STIL-TAL1-positive patients were all male, under 40 years of age, and presented with lymph node enlargement, hepatosplenomegaly, and mediastinal mass. They showed relatively higher leukocyte counts and hemoglobin levels, but lower platelet counts compared to STIL-TAL1 negative cases. Immunophenotyping analysis revealed higher sCD3 and lower CD34 expression with no aberrant myeloid lineage expression. CMA demonstrated a 63-kb heterozygous deletion at 1p33, along with additional copy number abnormalities such as TCR rearrangements and a biallelic CDKN2A deletion.

Conclusions: The T-ALL with STIL-TAL1 fusion exhibits unique clinical, immunologic, and genetic characteristics. Further multi-center studies, incorporating cytogenetic and molecular analyses, are needed to elucidate the detailed pathophysiology, characteristics, and clinical significance of this gene rearrangement.

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t淋巴细胞白血病STIL-TAL1融合的临床、免疫学和遗传学特征。

背景：t淋巴细胞白血病（T-ALL）是一种侵袭性血液系统恶性肿瘤，预后较差。T-ALL的遗传背景具有广泛的异质性，可同时发生多种遗传异常。STIL-TAL1重排源于染色体1p33的亚显微缺失，在15 - 25%的T-ALL病例中存在。亚显微缺失不能通过常规的细胞遗传学分析检测到，但可以通过阵列比较基因组杂交和/或高通量RNA测序来鉴定。STIL-TAL1融合的患者表现出明显的特征，如年轻、白细胞计数高、典型的免疫表型和特定的遗传异常。然而，这种重排的临床、实验室和预后意义尚不清楚。本研究旨在鉴定T-ALL中由亚显微镜下1p33缺失引起的still - tal1重排，并研究still - tal1融合T-ALL患者的临床、免疫学和遗传特征。方法：在6年（2018 - 2023年）期间，共有15例T-ALL患者入组。我们评估了诊断阶段骨髓或外周血标本的临床特征和实验室结果，包括免疫表型、多重逆转录聚合酶链反应（RT-PCR）、核型分析、下一代测序（NGS）和染色体微阵列分析（CMA）。结果：对15例T-ALL进行多重RT-PCR检测，3例（20.0%,3/15）检测到still - tal1融合。still - tal1阳性患者均为男性，年龄在40岁以下，表现为淋巴结肿大、肝脾肿大、纵隔肿块。与still - tal1阴性病例相比，他们的白细胞计数和血红蛋白水平相对较高，但血小板计数较低。免疫表型分析显示高sCD3和低CD34表达，无异常髓系表达。CMA显示在1p33位点有63kb的杂合缺失，以及额外的拷贝数异常，如TCR重排和双等位基因CDKN2A缺失。结论：T-ALL与still - tal1融合表现出独特的临床、免疫学和遗传学特征。需要进一步的多中心研究，结合细胞遗传学和分子分析，来阐明这种基因重排的详细病理生理、特征和临床意义。

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来源期刊

Clinical laboratory 医学-医学实验技术

CiteScore

1.50

自引率

0.00%

发文量

494

审稿时长

3 months

期刊介绍： Clinical Laboratory is an international fully peer-reviewed journal covering all aspects of laboratory medicine and transfusion medicine. In addition to transfusion medicine topics Clinical Laboratory represents submissions concerning tissue transplantation and hematopoietic, cellular and gene therapies. The journal publishes original articles, review articles, posters, short reports, case studies and letters to the editor dealing with 1) the scientific background, implementation and diagnostic significance of laboratory methods employed in hospitals, blood banks and physicians'' offices and with 2) scientific, administrative and clinical aspects of transfusion medicine and 3) in addition to transfusion medicine topics Clinical Laboratory represents submissions concerning tissue transplantation and hematopoietic, cellular and gene therapies.