Genotype-phenotype correlation of BMPR1a disease causing variants in juvenile polyposis syndrome.

IF 2 4区 医学 Q3 ONCOLOGY Hereditary Cancer in Clinical Practice Pub Date : 2023-07-03 DOI:10.1186/s13053-023-00255-3
M E Papadopulos, J P Plazzer, F A Macrae
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引用次数: 2

Abstract

Background: Juvenile Polyposis Syndrome (JPS) is an autosomal dominant condition with hamartomatous polyps in the gastrointestinal tract, associated with an increased risk of gastrointestinal malignancy. Disease causing variants (DCVs) in BMPR1a or SMAD4 account for 45-60% of JPS cases, with BMPR1a DCVs accounting for 17-38% of JPS cases. Within those with either a BMPR1a or SMAD4 DCV, there is phenotypic variability in location of polyps, risk of malignancy and extra-intestinal manifestations with limited published reports of gene-phenotype association or genotype-phenotype correlation. We aimed to identify any gene-phenotype association or genotype-phenotype correlation in BMPR1a to inform surveillance recommendations, and gene-specific modification to the ACMG classification of pathogenicity of DCVs.

Methods: A literature search was performed through EMBASE, MEDLINE and PubMed. Studies that were included explored BMPR1a DCV-related JPS or contiguous deletion of PTEN and BMPR1a. Data was also drawn from the BMPR1a specific databases on LOVD and ClinVar.

Results: There were 211 DCVs in BMPR1a identified, 82 from patients with JPS in the literature, and 17 from LOVD and 112 from ClinVar classified as pathogenic or likely pathogenic. These included missense, nonsense and frameshift variants and large deletions, occurring across all functional domains of the gene. Unlike in SMAD4 carriers, gastric polyposis and malignancy were not identified in our review in BMPR1a carriers, but colonic polyposis and malignancy occurred in carriers of either BMPR1a or SMAD4 DCVs. Those with contiguous deletion of PTEN and BMPR1a can present with JPS of infancy, with a severe phenotype of GI bleeding, diarrhoea, exudative enteropathy and rectal prolapse. No specific BMPR1a genotype-phenotype correlation could be ascertained including by variant type or functional domain.

Conclusion: Phenotypic characteristics cannot be used to inform variant location in BMPR1a. However, the phenotypic characteristics of BMPR1a DCV carriers, being almost exclusively related to the colon and rectum, can assist in pathogenicity assessment of BMPR1a variants. Given these findings, we propose that carriers of BMPR1a DCVs should only require surveillance for colorectal polyps and malignancy, and that surveillance for gastric polyps and malignancy may be unnecessary. However variant location within BMPR1a does not support differential surveillance recommendations.

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青少年息肉病综合征中BMPR1a致病变异的基因型-表型相关性
背景:青少年息肉病综合征(JPS)是一种常染色体显性遗传病,伴有胃肠道错构瘤性息肉,与胃肠道恶性肿瘤的风险增加有关。BMPR1a或SMAD4的致病变异(DCVs)占JPS病例的45-60%,其中BMPR1a DCVs占JPS病例的17-38%。在BMPR1a或SMAD4 DCV患者中,息肉的位置、恶性肿瘤的风险和肠外表现存在表型变异,基因-表型关联或基因-表型相关性的已发表报道有限。我们的目的是确定BMPR1a中任何基因-表型关联或基因型-表型相关性,以提供监测建议,并对dcv致病性的ACMG分类进行基因特异性修改。方法:通过EMBASE、MEDLINE和PubMed进行文献检索。纳入的研究探讨了BMPR1a dcv相关的JPS或PTEN和BMPR1a的连续缺失。数据也来自BMPR1a关于LOVD和ClinVar的特定数据库。结果:BMPR1a共鉴定出211例DCVs,其中82例来自文献报道的JPS患者,17例来自LOVD, 112例来自ClinVar,被分类为致病性或可能致病性。这些包括错义、无义、移码变异和大缺失,发生在基因的所有功能区域。与SMAD4携带者不同,在我们的综述中,BMPR1a携带者未发现胃息肉病和恶性肿瘤,但BMPR1a或SMAD4 DCVs携带者均发生结肠息肉病和恶性肿瘤。PTEN和BMPR1a连续缺失者可出现婴儿期JPS,并伴有严重的胃肠道出血、腹泻、渗出性肠病和直肠脱垂。没有明确的BMPR1a基因型与表型的相关性,包括变异类型或功能域。结论:表型特征不能用于BMPR1a的变异位置。然而,BMPR1a DCV携带者的表型特征几乎完全与结肠和直肠相关,可以帮助评估BMPR1a变异的致病性。鉴于这些发现,我们建议BMPR1a DCVs携带者只需要监测结直肠息肉和恶性肿瘤,而对胃息肉和恶性肿瘤的监测可能是不必要的。然而,BMPR1a内的变异位置不支持差别监测建议。
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来源期刊
CiteScore
3.10
自引率
5.90%
发文量
38
审稿时长
>12 weeks
期刊介绍: Hereditary Cancer in Clinical Practice is an open access journal that publishes articles of interest for the cancer genetics community and serves as a discussion forum for the development appropriate healthcare strategies. Cancer genetics encompasses a wide variety of disciplines and knowledge in the field is rapidly growing, especially as the amount of information linking genetic differences to inherited cancer predispositions continues expanding. With the increased knowledge of genetic variability and how this relates to cancer risk there is a growing demand not only to disseminate this information into clinical practice but also to enable competent debate concerning how such information is managed and what it implies for patient care. Topics covered by the journal include but are not limited to: Original research articles on any aspect of inherited predispositions to cancer. Reviews of inherited cancer predispositions. Application of molecular and cytogenetic analysis to clinical decision making. Clinical aspects of the management of hereditary cancers. Genetic counselling issues associated with cancer genetics. The role of registries in improving health care of patients with an inherited predisposition to cancer.
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