Author:
Cai Feng,Zhang Yi-Dan,Zhao Xiuli,Yang Ya-Kun,Ma Si-Hai,Dai Cong-Xin,Liu Xiao-Hai,Yao Yong,Feng Ming,Wei Jun-Ji,Xing Bing,Jiao Yong-Hui,Wei Zhen-Qing,Yin Zhen-Ming,Zhang Bo,Gu Feng,Wang Ren-Zhi
Abstract
ObjectiveThe aryl hydrocarbon receptor interacting protein gene (AIP) is associated with pituitary adenoma (PA). AIP has not been sequenced in East Asian PA populations, so we performed this study in a Han Chinese cohort.DesignOur study included six familial PA pedigrees comprising 16 patients and 27 unaffected relatives, as well as 216 sporadic PA (SPA) patients and 100 unrelated healthy controls.MethodsAIP sequencing was carried out on genomic DNA isolated from blood samples. Multiplex ligation-dependent probe amplification and microsatellite marker analyses on DNA from the paired tumor tissues were performed for loss of heterozygosity analysis.ResultsWe identified three common and four rare single nucleotide polymorphisms (SNPs), one intron insertion, one novel synonymous variant, four novel missense variants, and a reported nonsense mutation in three familial isolated PA (FIPA) cases from the same family. Large genetic deletions were not observed in the germline but were seen in the sporadic tumor DNA from three missense variant carriers. The prevalence of AIP pathogenic variants in PA patients here was low (3.88%), but was higher in somatotropinoma patients (9.30%), especially in young adults (≤30 years) and pediatric (≥18 years) paients (17.24% and 25.00% respectively). All AIP variant patients suffered from macroadenomas. However, the AIP mutation rate in FIPA families was low in this cohort (16.67%, 1/6 families).ConclusionAIP gene mutation may not be frequent in FIPA or SPA from the Han Chinese population. AIP sequencing and long-term follow-up investigations should be performed for young patients with large PAs and their families with PA predisposition.
Subject
Endocrinology,General Medicine,Endocrinology, Diabetes and Metabolism
Cited by
27 articles.
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