APC相关息肉病

M. T. Ricci
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引用次数: 0

摘要

APC相关的息肉病是由APC基因中的组成性杂合致病性变体引起的。这些疾病包括三种主要的临床表型:家族性腺瘤性息肉病(FAP)、减毒FAP(AFAP)、胃腺癌和胃近端息肉病(GAPPS)。这种表型变异性对应于APC基因中致病性变体位置的差异,即使在具有相同APC致病性变体的个体之间和家族内可能发生变异。FAP的结直肠筛查应从10至12岁开始,AFAP的结直肠检查应从青少年晚期开始,如果有胃肠道症状,则应更早开始;手术时间和切除范围应根据患者的个人病史确定。建议20-30岁或结肠手术前进行食道胃十二指肠镜检查。支持筛查其他癌症和FAP相关表现的数据有限。目前尚不清楚筛查癌症和预防性胃切除术对GAPPS患者的疗效。
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APC-associated polyposis conditions
APC-associated polyposis conditions result from a constitutional heterozygous pathogenic variant in the APC gene. These conditions include three main clinical phenotypes: the familial adenomatous polyposis (FAP), the attenuated FAP (AFAP) and the gastric adenocarcinoma and proximal polyposis of the stomach (GAPPS). This phenotypic variability corresponds to the differences in the location of the pathogenic variant within the APC gene, even though variations among the individuals and within the families with the identical APC pathogenic variant may occur. Colorectal screening should begin from age 10 to 12 years in FAP and in late teens in AFAP, or earlier if there are gastrointestinal symptoms; the timing of surgery and the extent of resection should be determined on the basis of patient's personal history. Esophagogastroduodenoscopy is recommended by age 20-30 years or prior to colon surgery. Data to support screening for other cancers and manifestations associated with FAP are limited. The efficacy of the screening for gastric cancer and of prophylactic gastrectomy for patients with GAPPS is currently unknown.
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