Molecular Profiling of Low-Grade Appendiceal Mucinous Neoplasms (LAMN)

IF 3.1 2区医学 Q2 GENETICS & HEREDITY

Genes, Chromosomes & Cancer Pub Date : 2024-10-14 DOI:10.1002/gcc.23270

Julia Doll, Katja Maurus, Franziska Köhler, Niels Matthes, Johan F. Lock, Christoph-Thomas Germer, Andreas Rosenwald, Armin Wiegering

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Abstract

Low-grade appendiceal mucinous neoplasia (LAMN) represents a relatively rare tumor of the appendix typically diagnosed incidentally through appendectomy for acute appendicitis. In cases where perforation occurs, mucinous content may disseminate into the abdominal cavity, leading to the development of pseudomyxoma peritonei (PMP). The primary objective of this study was to elucidate the molecular characteristics associated with various stages of LAMN and PMP. DNA was extracted from LAMN, primary PMPs, recurrent PMPs, and adenocarcinomas originating from LAMN. The subsequent analysis involved the examination of mutational hotspot regions within 50 cancer-related genes, covering over 2800 COSMIC mutations, utilizing amplicon-based next-generation sequencing (NGS). Our findings revealed activating somatic mutations within the MAPK-signaling pathway across all tumors examined. Specifically, 98.1% of cases showed mutations in KRAS, while one tumor harbored a BRAF mutation. Additionally, GNAS mutations were identified in 55.8% of tumors, with no significant difference observed between LAMN and PMP. While LAMN rarely displayed additional mutations, 42% of primary PMPs and 60% of recurrent PMPs showed additional mutations. Notably, both adenocarcinomas originating from LAMN showed mutations within TP53. Furthermore, 7.7% (4/52) of cases exhibited a potentially targetable KRAS G12C mutation. In four patients, NGS analysis was performed on both primary PMP and recurrent PMP/adenocarcinoma samples. While mutations in KRAS and GNAS were detected in almost all samples, 50% of recurrent cases displayed an additional SMAD4 mutation, suggesting a notable alteration during disease progression. Our findings indicate two key points: First, mutations within the MAPK pathway, particularly in KRAS, are evident across all tumors, along with a high frequency of GNAS mutations. Second, progression toward PMP or adenocarcinoma is associated with an accumulation of additional mutations within common oncogenic pathways.

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低级别阑尾粘液性肿瘤（LAMN）的分子谱分析

低级别阑尾粘液瘤（LAMN）是一种相对罕见的阑尾肿瘤，通常是通过急性阑尾炎阑尾切除术偶然诊断出来的。在发生穿孔的情况下，粘液内容物可能会扩散到腹腔，导致腹膜假性肌瘤（PMP）的发生。本研究的主要目的是阐明与 LAMN 和 PMP 不同阶段相关的分子特征。研究人员从 LAMN、原发性 PMP、复发性 PMP 和源自 LAMN 的腺癌中提取了 DNA。随后的分析包括利用基于扩增子的下一代测序技术（NGS）检查 50 个癌症相关基因中的突变热点区域，涵盖 2800 多个 COSMIC 突变。我们的研究结果表明，在所有受检肿瘤中，MAPK 信号通路中存在激活性体细胞突变。具体来说，98.1%的病例出现了KRAS突变，还有一个肿瘤出现了BRAF突变。此外，在55.8%的肿瘤中发现了GNAS突变，LAMN和PMP之间无明显差异。虽然 LAMN 很少出现额外的突变，但 42% 的原发性 PMP 和 60% 的复发性 PMP 出现了额外的突变。值得注意的是，源自LAMN的两种腺癌都出现了TP53突变。此外，7.7%（4/52）的病例表现出潜在的靶向性 KRAS G12C 突变。有 4 例患者的原发性 PMP 和复发性 PMP/腺癌样本都进行了 NGS 分析。虽然几乎所有样本中都检测到了 KRAS 和 GNAS 突变，但 50% 的复发病例显示了额外的 SMAD4 突变，这表明在疾病进展过程中发生了显著的改变。我们的研究结果表明了两个关键点：首先，MAPK 通路中的突变，尤其是 KRAS 中的突变，在所有肿瘤中都很明显，同时 GNAS 突变的频率也很高。其次，PMP 或腺癌的进展与常见致癌通路中其他突变的积累有关。

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来源期刊

Genes, Chromosomes & Cancer 医学-遗传学

CiteScore

7.00

自引率

8.10%

发文量

审稿时长

4-8 weeks

期刊介绍： Genes, Chromosomes & Cancer will offer rapid publication of original full-length research articles, perspectives, reviews and letters to the editors on genetic analysis as related to the study of neoplasia. The main scope of the journal is to communicate new insights into the etiology and/or pathogenesis of neoplasia, as well as molecular and cellular findings of relevance for the management of cancer patients. While preference will be given to research utilizing analytical and functional approaches, descriptive studies and case reports will also be welcomed when they offer insights regarding basic biological mechanisms or the clinical management of neoplastic disorders.