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儿童 B 细胞前体淋巴母细胞淋巴瘤的突变和转录组图谱。

Mutational and transcriptional landscape of pediatric B-cell precursor lymphoblastic lymphoma.

机构信息

Princess Máxima Center for Pediatric Oncology, Utrecht, The Netherlands.

Department of Pathology, Hematopathology Section and Lymph Node Registry, University of Kiel, Kiel, Germany.

出版信息

Blood. 2024 Jul 4;144(1):74-83. doi: 10.1182/blood.2024023938.

DOI:10.1182/blood.2024023938
PMID:38588489
Abstract

Pediatric B-cell precursor (BCP) lymphoblastic malignancies are neoplasms with manifestation either in the bone marrow or blood (BCP acute lymphoblastic leukemia [BCP-ALL]) or are less common in extramedullary tissue (BCP lymphoblastic lymphoma [BCP-LBL]). Although both presentations are similar in morphology and immunophenotype, molecular studies have been virtually restricted to BCP-ALL so far. The lack of molecular studies on BCP-LBL is due to its rarity and restriction on small, mostly formalin-fixed paraffin-embedded (FFPE) tissues. Here, to our knowledge, we present the first comprehensive mutational and transcriptional analysis of what we consider the largest BCP-LBL cohort described to date (n = 97). Whole-exome sequencing indicated a mutational spectrum of BCP-LBL, strikingly similar to that found in BCP-ALL. However, epigenetic modifiers were more frequently mutated in BCP-LBL, whereas BCP-ALL was more frequently affected by mutation in genes involved in B-cell development. Integrating copy number alterations, somatic mutations, and gene expression by RNA sequencing revealed that virtually all molecular subtypes originally defined in BCP-ALL are present in BCP-LBL, with only 7% of lymphomas that were not assigned to a subtype. Similar to BCP-ALL, the most frequent subtypes of BCP-LBL were high hyperdiploidy and ETV6::RUNX1. Tyrosine kinase/cytokine receptor rearrangements were detected in 7% of BCP-LBL. These results indicate that genetic subtypes can be identified in BCP-LBL using next-generation sequencing, even in FFPE tissue, and may be relevant to guide treatment.

摘要

儿童 B 细胞前体 (BCP) 淋母细胞恶性肿瘤是一种表现为骨髓或血液中的肿瘤(BCP 急性淋巴细胞白血病 [BCP-ALL]),或较少见于骨髓外组织的肿瘤(BCP 淋母细胞淋巴瘤 [BCP-LBL])。尽管两种表现形式在形态和免疫表型上相似,但到目前为止,分子研究实际上仅限于 BCP-ALL。BCP-LBL 缺乏分子研究是由于其罕见性和对小样本、主要是福尔马林固定石蜡包埋(FFPE)组织的限制。在这里,据我们所知,我们首次对迄今为止我们认为最大的 BCP-LBL 队列进行了全面的突变和转录分析(n=97)。全外显子组测序表明 BCP-LBL 的突变谱与在 BCP-ALL 中发现的突变谱非常相似。然而,在 BCP-LBL 中,表观遗传修饰因子更频繁发生突变,而 BCP-ALL 更频繁受到参与 B 细胞发育的基因的突变影响。通过 RNA 测序整合拷贝数改变、体细胞突变和基因表达表明,最初在 BCP-ALL 中定义的几乎所有分子亚型都存在于 BCP-LBL 中,只有 7%的淋巴瘤未被分配到一个亚型。与 BCP-ALL 相似,BCP-LBL 最常见的亚型是高倍体和 ETV6::RUNX1。在 7%的 BCP-LBL 中检测到酪氨酸激酶/细胞因子受体重排。这些结果表明,即使在 FFPE 组织中,也可以使用下一代测序在 BCP-LBL 中识别遗传亚型,这可能与指导治疗相关。

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