Maeyama H, Hidaka E, Ota H, Minami S, Kajiyama M, Kuraishi A, Mori H, Matsuda Y, Wada S, Sodeyama H, Nakata S, Kawamura N, Hata S, Watanabe M, Iijima Y, Katsuyama T
Department of Gastroenterology, Nagano Red Cross Hospital, Nagano, Japan.
Gastroenterology. 2001 Jan;120(1):210-5. doi: 10.1053/gast.2001.20880.
We describe 2 siblings with multiple gastrointestinal stromal tumors (GISTs) and cutaneous hyperpigmentation. Both had a point mutation of the c-kit gene. The patients were sisters who had exhibited cutaneous hyperpigmentation since their late teens, but the diagnosis of multiple gastrointestinal submucosal tumors was not made until they were 41 and 45 years old. Histologic examination showed that these tumors were GISTs expressing CD34 and Kit protein. Both patients died of GISTs. Single-strand conformation polymorphism analysis showed a mutation of c-kit in tumor DNA extracted from paraffin-embedded specimens. Direct sequencing analysis showed that the point mutation occurred at codon 559 of exon 11 (Val-->Ala). The same single-point mutation was detected in DNA extracted from peripheral leukocytes obtained from the younger sister and her 2 children (who had similar general hyperpigmentation) as well as in DNA from a skin biopsy specimen taken from the older sister. The germline mutation at codon 559 of the c-kit gene found in the present familial GISTs differed from that in a previously reported case of familial GISTs. We propose that GISTs caused by a germline mutation of the c-kit gene should be referred to as GIST-cutaneous hyperpigmentation disease.
我们描述了2例患有多发性胃肠道间质瘤(GIST)和皮肤色素沉着的姐妹。两人均有c-kit基因的点突变。这两名患者为姐妹,自青少年晚期就出现皮肤色素沉着,但直到41岁和45岁时才诊断出多发性胃肠道黏膜下肿瘤。组织学检查显示这些肿瘤为表达CD34和Kit蛋白的GIST。两名患者均死于GIST。单链构象多态性分析显示,从石蜡包埋标本中提取的肿瘤DNA存在c-kit突变。直接测序分析表明,该点突变发生在外显子11的第559密码子(Val→Ala)。在从妹妹及其2个孩子(有类似的全身性色素沉着)获取的外周血白细胞提取的DNA以及从姐姐的皮肤活检标本提取的DNA中检测到相同的单点突变。在目前的家族性GIST中发现的c-kit基因第559密码子的种系突变与先前报道的家族性GIST病例不同。我们建议将由c-kit基因种系突变引起的GIST称为GIST-皮肤色素沉着病。
