Division of Pathology and Clinical Laboratories, National Cancer Center Hospital, 5-1-1, Tsukiji, Chuo-ku, Tokyo, 104-0045, Japan.
Division of Molecular Pathology, National Cancer Center Research Institute, Tokyo, Japan.
J Gastroenterol. 2020 Apr;55(4):418-427. doi: 10.1007/s00535-020-01673-z. Epub 2020 Feb 12.
Traditional serrated adenoma (TSA) is the least common type of colorectal serrated polyp, which exhibits considerable morphological and molecular diversity.
We examined the spectra of alterations in MAPK and WNT pathway genes and their relationship with clinicopathological features in 128 TSAs.
Sequencing analyses identified BRAF V600E, BRAF non-V600E, KRAS, and NRAS mutations in 77, 3, 45, and 1 lesion, respectively. Collectively, 124 lesions (97%) had mutations in MAPK pathway genes. Alterations in WNT pathway genes were identified in 107 lesions (84%), including RSPO fusions/overexpression, RNF43 mutations, ZNRF3 mutations, APC mutations, and CTNNB1 mutations in 47, 45, 2, 13, and 2 lesions, respectively. Ten lesions (8%) harbored GNAS mutations. There was significant interdependence between the altered MAPK and WNT pathway genes. RSPO fusions/overexpression was significantly associated with KRAS mutations (31/47, 66%), whereas most RNF43 mutations coexisted with the BRAF V600E mutation (40/45, 89%). Histologically, extensive slit-like serration was more common in lesions with the BRAF V600E mutation (71%) and those with RNF43 mutations (87%). Prominent ectopic crypt formation was more prevalent in lesions with RSPO fusions/overexpression (58%) and those with GNAS mutations (100%).
Our observations indicate that TSAs mostly harbor various combinations of concurrent WNT and MAPK gene alterations. The associations between genetic and morphological features suggest that the histological diversity of TSA reflects the underlying molecular heterogeneity.
传统锯齿状腺瘤(TSA)是结直肠锯齿状息肉中最不常见的类型,其表现出相当大的形态和分子多样性。
我们检查了 MAPK 和 WNT 通路基因改变的频谱及其与 128 个 TSA 的临床病理特征的关系。
测序分析分别在 77、3、45 和 1 个病变中发现了 BRAF V600E、BRAF 非-V600E、KRAS 和 NRAS 突变。共有 124 个病变(97%)存在 MAPK 通路基因的突变。在 107 个病变中发现了 WNT 通路基因的改变,包括 RSPO 融合/过表达、RNF43 突变、ZNRF3 突变、APC 突变和 CTNNB1 突变,分别在 47、45、2、13 和 2 个病变中发现。有 10 个病变(8%)携带 GNAS 突变。改变的 MAPK 和 WNT 通路基因之间存在显著的相互依存关系。RSPO 融合/过表达与 KRAS 突变显著相关(31/47,66%),而大多数 RNF43 突变与 BRAF V600E 突变共存(40/45,89%)。在组织学上,广泛的裂隙样锯齿状更常见于携带 BRAF V600E 突变的病变(71%)和携带 RNF43 突变的病变(87%)。突出的异位隐窝形成更常见于 RSPO 融合/过表达的病变(58%)和携带 GNAS 突变的病变(100%)。
我们的观察表明,TSA 主要携带各种同时存在的 WNT 和 MAPK 基因改变的组合。遗传和形态特征之间的关联表明,TSA 的组织学多样性反映了潜在的分子异质性。
