Molecular Pathobiology Research Unit (UIPM), Instituto Português de Oncologia de Lisboa Francisco Gentil E.P.E. (IPOLFG, EPE), Rua Professor Lima Basto, 1099-023 Lisbon, Portugal.
Gastroenterology Department, Instituto Português de Oncologia de Lisboa Francisco Gentil E.P.E. (IPOLFG, EPE), Rua Professor Lima Basto, 1099-023 Lisbon, Portugal.
Int J Mol Sci. 2024 Nov 4;25(21):11848. doi: 10.3390/ijms252111848.
Serrated polyposis syndrome (SPS) is characterized by the development of multiple colorectal serrated polyps and increased predisposition to colorectal cancer (CRC). However, the molecular basis of SPS, especially in cases presenting family history of SPS and/or polyps and/or CRC in first-degree relatives (SPS-FHP/CRC), is still poorly understood. In a previous study, we proposed the existence of two molecular entities amongst SPS-FHP/CRC families, proximal/whole-colon and distal SPS-FHP/CRC, according to the preferential location of lesions and somatic events involved in tumor initiation. In the present study, we aimed to investigate these distinct subgroups of SPS patients in a larger cohort at the germline level and to identify the genetic defects underlying an inherited susceptibility for these two entities. Next-generation sequencing was performed using multigene analysis with a custom-designed panel in a Miseq platform in 60 SPS patients (with and without/unknown FHP/CRC). We found germline pathogenic variants in 6/60 patients (, , , , , and ). We also found variants of unknown significance (VUS), with prediction of probable damaging effect in 23/60 patients (, , , , , , , , , , , , , , , , , , , , and genes). Most variants were detected in gene coding for proteins of the Fanconi Anemia (FA) pathway involved in the DNA Interstrand-Cross Link repair (ICLR). Notably, variants in ICLR genes were significantly more frequent in the proximal/whole-colon than in the distal subgroup [15/44 (34%) vs 1/16 (6%), = 0.025], as opposed to the non-ICLR genes that were slightly more frequent in the distal group [8/44 (18%) vs. 5/16 (31%), > 0.05]. Germline defects in the DNA-ICLR genes may contribute to increased serrated colorectal polyps/carcinoma risk in SPS patients, particularly in proximal/whole-colon SPS. The inclusion of DNA-ICLR genes in the genetic diagnosis of SPS patients, mainly in those with proximal/whole-colon lesions, should be considered and validated by other studies. In addition, patients with germline defects in the DNA-ICLR genes may be more sensitive to treatment with platinum-based therapeutics, which can have implications in the clinical management of these patients.
锯齿状息肉综合征(SPS)的特征是大肠多发性锯齿状息肉的发展和结直肠癌(CRC)的易感性增加。然而,SPS 的分子基础,特别是在有 SPS 家族史和/或一级亲属结直肠息肉和/或 CRC(SPS-FHP/CRC)的情况下,仍然知之甚少。在之前的研究中,我们根据肿瘤起始涉及的病变和体细胞事件的优先位置,提出 SPS-FHP/CRC 家族中存在两种分子实体,即近端/全结肠和远端 SPS-FHP/CRC。在本研究中,我们旨在在更大的队列中在种系水平上研究这些不同的 SPS 患者亚组,并确定这两种实体遗传易感性的遗传缺陷。在 Miseq 平台上使用多基因分析的定制面板对 60 名 SPS 患者(有和无/未知 FHP/CRC)进行了下一代测序。我们在 6/60 名患者(、、、、、)中发现了种系致病性变异。我们还发现了未知意义的变异(VUS),其中 23/60 名患者(、、、、、、、、、、、、、、、、、、、)的预测可能具有破坏性影响。大多数变异发生在参与 DNA 链间交联修复(ICLR)的 Fanconi 贫血(FA)途径蛋白编码基因中。值得注意的是,ICLR 基因中的变异在近端/全结肠亚组中比在远端亚组中更为频繁[15/44(34%)比 1/16(6%),=0.025],而 ICLR 基因的非 ICLR 基因在远端组中略为频繁[8/44(18%)比 5/16(31%),>0.05]。SPS 患者中 DNA-ICLR 基因的种系缺陷可能导致锯齿状结直肠息肉/癌的风险增加,特别是在近端/全结肠 SPS 中。应考虑并通过其他研究验证将 DNA-ICLR 基因纳入 SPS 患者的遗传诊断中,特别是在有近端/全结肠病变的患者中。此外,具有 DNA-ICLR 基因突变的患者可能对基于铂的治疗更敏感,这可能对这些患者的临床管理产生影响。
