STK11基因中的一种新型种系突变(c.A527G)导致一名中国女孩患黑斑息肉综合征:病例报告。
A novel germline mutation (c.A527G) in STK11 gene causes Peutz-Jeghers syndrome in a Chinese girl: A case report.
作者信息
Zhao Zi-Ye, Jiang Yu-Liang, Li Bai-Rong, Yang Fu, Li Jing, Jin Xiao-Wei, Sun Shu-Han, Ning Shou-Bin
机构信息
Department of Medical Genetics, Naval Medical University, Shanghai 200433, China Hebei North University, Zhangjiakou, Hebei Province, China Department of Gastroenterology, Airforce General Hospital of PLA, Beijing, China.
出版信息
Medicine (Baltimore). 2017 Dec;96(49):e8591. doi: 10.1097/MD.0000000000008591.
RATIONALE
Peutz-Jeghers syndrome (PJS) is a Mendelian autosomal dominant disease caused by mutations in the tumor suppressor gene, serine/threonine kinase 11 (STK11). The features of this syndrome include gastrointestinal (GI) hamartomas, melanin spots on the lips and the extremities, and an increased risk of developing cancer. Early onset of disease is often characterized by mucocutaneous pigmentation and intussusception due to GI polyps in childhood.
PATIENT CONCERNS
A girl with a positive family history grew oral pigmentation at 1 and got intussusception by small bowel hamartomas at 5.
DIAGNOSES
She was diagnosed with PJS based on oral pigmentation and a positive family history of PJS.
INTERVENTIONS
Enteroscopy was employed to treat the GI polyps. Sanger sequencing was used to investigate STK11 mutation in this family.
OUTCOMES
A large jejunal polyp together with other smaller ones was resected, and the girl recovered uneventfully. We discovered a heterozygous substitution in STK11, c.A527G in exon 4, in the girl and her father who was also a PJS patient, and the amine acid change was an aspartic acid-glycine substitution in codon 176. This mutation was not found in other healthy family members and 50 unrelated non-PJS controls, and it is not recorded in databases, which prove it a novel mutation. Evolutionary conservation analysis of amino acid residues showed this aspartic acid is a conserved one between species, and protein structure prediction by SWISS-MODEL indicated an obvious change in local structure. In addition, PolyPhen-2 score for this mutation is 1, which indicates it probably damaging.
LESSONS
PJS can cause severe complication like intussusception in young children, and early screening for small bowel may be beneficial for these patients. The mutation of STK11 found in this girl is a novel one, which enlarges the spectrum of STK11. Our analysis supported it a causative one in PJS.
理论依据
黑斑息肉综合征(PJS)是一种孟德尔常染色体显性疾病,由肿瘤抑制基因丝氨酸/苏氨酸激酶11(STK11)突变引起。该综合征的特征包括胃肠道(GI)错构瘤、嘴唇和四肢的黑色素斑以及患癌风险增加。疾病早期通常表现为儿童期因胃肠道息肉导致的黏膜皮肤色素沉着和肠套叠。
患者情况
一名有家族病史的女孩1岁时出现口腔色素沉着,5岁时因小肠错构瘤发生肠套叠。
诊断
根据口腔色素沉着和PJS家族病史,她被诊断为PJS。
干预措施
采用小肠镜治疗胃肠道息肉。使用桑格测序法研究该家族中的STK11突变。
结果
切除了一个大的空肠息肉和其他较小的息肉,女孩恢复顺利。我们在女孩及其同为PJS患者的父亲中发现STK11基因外显子4中的杂合子替换c.A527G,氨基酸变化为密码子176处的天冬氨酸-甘氨酸替换。在其他健康家庭成员和50名无关的非PJS对照中未发现此突变,且数据库中未记录,证明这是一个新突变。氨基酸残基的进化保守性分析表明,该天冬氨酸在物种间是保守的,通过SWISS-MODEL进行的蛋白质结构预测表明局部结构有明显变化。此外,该突变的PolyPhen-2评分是1,表明它可能具有损害性。
经验教训
PJS可导致幼儿发生肠套叠等严重并发症,对小肠进行早期筛查可能对这些患者有益。在该女孩中发现的STK11突变是新的,扩大了STK11的突变谱。我们的分析支持其为PJS的致病突变。
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