家族性腺瘤性息肉病的APC基因突变与肠外表型
APC gene mutations and extraintestinal phenotype of familial adenomatous polyposis.
作者信息
Giardiello F M, Petersen G M, Piantadosi S, Gruber S B, Traboulsi E I, Offerhaus G J, Muro K, Krush A J, Booker S V, Luce M C, Laken S J, Kinzler K W, Vogelstein B, Hamilton S R
机构信息
Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, USA.
出版信息
Gut. 1997 Apr;40(4):521-5. doi: 10.1136/gut.40.4.521.
BACKGROUND
Familial adenomatous polyposis (FAP) is caused by germline mutation of the adenomatous polyposis coli (APC) gene on chromosome 5q.
AIMS
This study assessed genotype-phenotype correlations for extraintestinal lesions in FAP.
METHODS
Mutations of the APC gene were compared with the occurrence of seven extraintestinal manifestations in 475 FAP patients from 51 families. The frequency of manifestations was adjusted for different ages of patients using person years of exposure. In pedigrees without identified APC gene mutation, analysis of linkage to chromosome 5q and/or assessment of neoplasms for replication errors characteristic of mutation in mismatch repair genes were performed.
RESULTS
FAP patients from the 42 families (82%) with identified mutations of the APC gene had more frequent expression of extraintestinal manifestations than affected individuals without identified mutations (risk ratio 1.2-4.0; significant difference for cutaneous cysts). The presence of a cutaneous cyst or extraintestinal cancer significantly increased the likelihood of detection of a mutation in the APC gene (94% and 92% respectively; p < 0.05). In patients without identified APC gene mutation, linkage to the APC gene was found in one large family (lod = 5.1, theta 0.01), and replication error phenotype was absent in all 24 neoplasms from 16 members of these nine pedigrees. Expression of pigmented ocular fundus lesions was strongly associated with mutations in codons 541-1309, but no other extraintestinal manifestations were related to mutation position. Multiplicity of extraintestinal manifestations was high with mutation in codons 1465, 1546, and 2621.
CONCLUSIONS
Patients with the colorectal phenotype of FAP but no extraintestinal manifestations may have non-truncating mutations of the APC gene or mutation in a gene other than APC or mismatch repair genes. The site of APC gene mutation is associated with pigmented ocular fundus lesions (codons 542-1309) and predisposition to multiplicity of extraintestinal manifestations (codons 1465, 1546, and 2621).
背景
家族性腺瘤性息肉病(FAP)由5号染色体上腺瘤性息肉病 coli(APC)基因的种系突变引起。
目的
本研究评估FAP肠外病变的基因型-表型相关性。
方法
将51个家族的475例FAP患者的APC基因突变与7种肠外表现的发生情况进行比较。使用暴露人年对不同年龄患者的表现频率进行调整。在未鉴定出APC基因突变的家系中,进行5号染色体q臂的连锁分析和/或评估肿瘤中错配修复基因突变特征性的复制错误。
结果
42个家族(82%)中鉴定出APC基因突变的FAP患者比未鉴定出突变的受累个体肠外表现的表达更频繁(风险比1.2 - 4.0;皮肤囊肿有显著差异)。皮肤囊肿或肠外癌症的存在显著增加了检测到APC基因突变的可能性(分别为94%和92%;p < 0.05)。在未鉴定出APC基因突变的患者中,在一个大家系中发现与APC基因连锁(对数优势比 = 5.1,重组率 = 0.01),这9个家系16名成员的所有24个肿瘤均无复制错误表型。眼底色素沉着病变的表达与密码子541 - 1309处的突变密切相关,但没有其他肠外表现与突变位置相关。密码子1465、1546和2621处发生突变时,肠外表现的多样性较高。
结论
具有FAP结直肠表型但无肠外表现的患者可能有APC基因的非截短突变或APC基因、错配修复基因以外的基因发生突变。APC基因突变位点与眼底色素沉着病变(密码子542 - 1309)以及肠外表现多样性的易感性(密码子1465、1546和2621)相关。
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