CD36 polymorphisms and the age of disease onset in patients with pathogenic variants within the mutation cluster region of APC.

IF 2 4区 医学 Q3 ONCOLOGY Hereditary Cancer in Clinical Practice Pub Date : 2021-04-29 DOI:10.1186/s13053-021-00183-0
T Connor, M McPhillips, M Hipwell, A Ziolkowski, C Oldmeadow, M Clapham, P G Pockney, E Lis, T Banasiewicz, A Pławski, R J Scott
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引用次数: 3

Abstract

Background: Familial adenomatous polyposis (FAP) is an autosomal dominant condition that predisposes patients to colorectal cancer. FAP is the result of a loss of APC function due to germline pathogenic variants disrupting gene expression. Genotype-phenotype correlations are described for FAP. For example attenuated forms of the disease are associated with pathogenic variants at the 5' and 3' ends of APC whilst severe forms of the disease appear to be linked to variants occurring in the mutation cluster region (MCR) of the gene. Variants occurring in the MCR are phenotypically associated with hundreds to thousands of adenomas carpeting the colon and rectum and patients harbouring changes in this region have a high propensity to develop colorectal cancer. Not all patients who carry pathogenic variants in this region have severe disease which may be a result of environmental factors. Alternatively, phenotypic variation observed in these patients could be due to modifier genes that either promote or inhibit disease expression. Mouse models of FAP have provided several plausible candidate modifier genes, but very few of these have survived scrutiny. One such genetic modifier that appears to be associated with disease expression is CD36. We previously reported a weak association between a polymorphism in CD36 and a later age of disease onset on a relatively small FAP patient cohort.

Methods: In the current study, we enlarged the FAP cohort. 395 patients all carrying pathogenic variants in APC were tested against three CD36 Single Nucleotide Polymorphisms (SNP)s (rs1049673, rs1761667 rs1984112), to determine if any of them were associated with differences in the age of disease expression.

Results: Overall, there appeared to be a statistically significant difference in the age of disease onset between carriers of the variant rs1984112 and wildtype. Furthermore, test equality of survivor functions for each SNP and mutation group suggested an interaction in the Log Rank, Wilcoxon, and Tarone-Ware methods for rs1049673, rs1761667, and rs1984112, thereby supporting the notion that CD36 modifies disease expression.

Conclusions: This study supports and strengthens our previous findings concerning CD36 and an association with disease onset in FAP, AFAP and FAP-MCR affected individuals. Knowledge about the role CD36 in adenoma development may provide greater insight into the development of colorectal cancer.

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APC突变簇区致病性变异体患者的CD36多态性与发病年龄
背景:家族性腺瘤性息肉病(FAP)是一种常染色体显性遗传病,使患者易患结直肠癌。FAP是由于种系致病性变异破坏基因表达而导致APC功能丧失的结果。描述了FAP的基因型-表型相关性。例如,该病的减毒型与APC的5'和3'端致病性变异有关,而该病的严重型似乎与基因突变簇区(MCR)中发生的变异有关。MCR中发生的变异在表型上与成百上千种覆盖结肠和直肠的腺瘤相关,在该区域发生变异的患者患结直肠癌的倾向很高。并非该地区所有携带致病变异的患者都患有严重疾病,这可能是环境因素的结果。或者,在这些患者中观察到的表型变异可能是由于修饰基因促进或抑制疾病表达。FAP的小鼠模型提供了几个可能的候选修饰基因,但这些基因很少能经受住审查。其中一个与疾病表达相关的基因修饰因子是CD36。我们之前在一个相对较小的FAP患者队列中报道了CD36多态性与较晚发病年龄之间的弱关联。方法:在本研究中,我们扩大了FAP队列。对395例携带APC致病变异的患者进行了3种CD36单核苷酸多态性(SNP)s (rs1049673, rs1761667, rs1984112)检测,以确定其中是否有任何与疾病表达年龄差异相关。结果:总体而言,变异rs1984112携带者和野生型携带者在发病年龄上存在统计学上的显著差异。此外,每个SNP和突变组的存活功能测试相等性表明,在rs1049673、rs1761667和rs1984112的Log Rank、Wilcoxon和Tarone-Ware方法中存在相互作用,从而支持CD36修饰疾病表达的观点。结论:本研究支持并加强了我们之前关于CD36与FAP、AFAP和FAP- mcr患者发病相关的研究结果。了解CD36在腺瘤发展中的作用可能为了解结直肠癌的发展提供更深入的了解。
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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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