A treatment-refractory aggressive MDS-MLD with multiple highly complex chromosome 5 intrachromosomal rearrangements: a case report.

IF 1.3 4区 生物学 Q4 GENETICS & HEREDITY Molecular Cytogenetics Pub Date : 2022-12-06 DOI:10.1186/s13039-022-00630-0
Ramakrishnan Sasi, Jamie Senft, Michelle Spruill, Subit Barua, Sam Dougaparsad, Jeffrey A Vos, Peter L Perrotta
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Abstract

Background: A patient with a myelodysplastic neoplasm exhibited a karyotype with multiple complex chromosome 5 rearrangements. This patient appeared to have a catastrophic cytogenetic event that manifested as a treatment-refractory aggressive form of disease, which lead to patient demise within one year. Both the clinical presentation and disease course were unusual based on the medical history and morphologic findings. Such cases of myelodysplastic syndrome with multilineage dysplasia (MDS-MLD) with complex abnormalities are not reported in the literature.

Case presentation: The patient was a 62-year-old female who presented with pancytopenia and dyspnea. The morphologic appearance of the peripheral blood smear and bone marrow biopsy, along with flow cytometric findings, favored the diagnosis of MDS-MLD unclassifiable. Myelodysplastic syndrome (MDS) with multilineage dysplasia (MDS-MLD), is an MDS characterized by one or more cytopenias and dysplastic changes in two or more of the myeloid lineages (i.e., erythroid, granulocytic, and megakaryocytic). The bone marrow, in particular, showed prominent dysplasia, including the presence of atypical megakaryocytes with small hypolobated morphology reminiscent of those typically seen in MDS with isolated 5q deletion. Cytogenetic analysis, including interphase and metaphase FISH, karyotype and SNP chromosomal microarray were performed, as well as DNA sequencing studies. Cytogenetic analysis showed a very complex karyotype featuring multiple 5q intrachromosomal rearrangements including a pericentric inversion with multiple interspersed deletions and monosomy 7. FISH studies showed a partial deletion of the PDGFRβ gene, and SNP chromosomal microarray and targeted panel-based sequencing identified biallelic loss of function of the TP53 gene. Based on the pathologic findings, the patient was treated for MDS but did not respond to either lenalidomide or azacitidine.

Conclusion: The genetic changes described, in particular, the complex intrachromosomal rearrangements of chromosome 5, suggest the occurrence of a sudden catastrophic event that led to an aggressive course in the patient's disease. Conventional karyotyping, metaphase and interphase FISH, SNP chromosomal microarray and NGS helped to identify the complex genetic changes seen in this case. This highlights the importance of utilizing a multimodality approach to fully characterize complex chromosomal events that may significantly impact disease progression, treatment and survival.

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难治性侵袭性MDS-MLD伴5号染色体内多重高度复杂重排1例。
背景:一个骨髓增生异常肿瘤患者表现出多重复杂5号染色体重排的核型。这名患者似乎有一个灾难性的细胞遗传学事件,表现为一种治疗难治性侵袭性疾病,导致患者在一年内死亡。根据病史和形态学发现,临床表现和病程都不寻常。此类骨髓增生异常综合征伴多系发育不良(MDS-MLD)伴复杂异常的病例在文献中未见报道。病例介绍:患者为62岁女性,表现为全血细胞减少和呼吸困难。外周血涂片和骨髓活检的形态学表现,以及流式细胞术的结果,有利于MDS-MLD的诊断。骨髓增生异常综合征(MDS)伴多系发育不良(MDS- mld)是一种MDS,其特征是两个或多个髓系(即红细胞、粒细胞和巨核细胞)的一个或多个细胞减少和发育异常改变。尤其是骨髓,表现出明显的发育不良,包括非典型巨核细胞的存在,具有小的低染色体形态,使人想起那些典型的5q缺失MDS。细胞遗传学分析,包括间期和中期FISH,核型和SNP染色体微阵列,以及DNA测序研究。细胞遗传学分析显示一个非常复杂的核型,具有多个5q染色体内重排,包括多个散布缺失和7号单体的中心反转。FISH研究显示PDGFRβ基因部分缺失,SNP染色体微阵列和基于靶向小组的测序发现TP53基因的双等位基因功能缺失。根据病理结果,患者接受了MDS治疗,但来那度胺或阿扎胞苷均无反应。结论:所描述的遗传变化,特别是5号染色体的复杂染色体内重排,提示发生了突然的灾难性事件,导致了患者疾病的侵袭过程。常规核型、中期和间期FISH、SNP染色体微阵列和NGS有助于鉴定本病例中所见的复杂遗传变化。这突出了利用多模态方法来充分表征可能显著影响疾病进展、治疗和生存的复杂染色体事件的重要性。
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来源期刊
Molecular Cytogenetics
Molecular Cytogenetics GENETICS & HEREDITY-
CiteScore
2.60
自引率
7.70%
发文量
49
审稿时长
>12 weeks
期刊介绍: Molecular Cytogenetics encompasses all aspects of chromosome biology and the application of molecular cytogenetic techniques in all areas of biology and medicine, including structural and functional organization of the chromosome and nucleus, genome variation, expression and evolution, chromosome abnormalities and genomic variations in medical genetics and tumor genetics. Molecular Cytogenetics primarily defines a large set of the techniques that operate either with the entire genome or with specific targeted DNA sequences. Topical areas include, but are not limited to: -Structural and functional organization of chromosome and nucleus- Genome variation, expression and evolution- Animal and plant molecular cytogenetics and genomics- Chromosome abnormalities and genomic variations in clinical genetics- Applications in preimplantation, pre- and post-natal diagnosis- Applications in the central nervous system, cancer and haematology research- Previously unreported applications of molecular cytogenetic techniques- Development of new techniques or significant enhancements to established techniques. This journal is a source for numerous scientists all over the world, who wish to improve or introduce molecular cytogenetic techniques into their practice.
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