Maher E R, Webster A R, Richards F M, Green J S, Crossey P A, Payne S J, Moore A T
Cambridge University Department of Pathology, UK.
J Med Genet. 1996 Apr;33(4):328-32. doi: 10.1136/jmg.33.4.328.
Von Hippel-Lindau disease is an autosomal dominantly inherited familial cancer syndrome predisposing to retinal and central nervous system haemangioblastomas, renal cell carcinoma, and phaeochromocytoma. VHL disease shows variable expression and interfamilial differences in predisposition to phaeochromocytoma. In a previous study of 65 VHL kindreds with defined VHL mutations we detected significant differences between VHL families with and without phaeochromocytoma such that missense mutations were more common and large deletions or protein truncating mutations less frequent in phaeochromocytoma positive families. To investigate the significance and cause of this association further, we studied 138 VHL kindreds for germline mutations and calculated the age related tumour risks for different classes of VHL gene mutations. Using SSCP, heteroduplex and Southern analysis we identified a germline VHL gene mutation in 101 families (73%). Direct sequencing of the VHL coding region further increased the mutation detection rate to 81%. In addition to precise presymptomatic diagnosis, identification of a VHL gene mutation can provide an indication of the likely phenotype. We found that large deletions and mutations predicted to cause a truncated protein were associated with a lower risk of phaeochromocytoma (6% and 9% at 30 and 50 years, respectively) than missense mutations (40% and 59%, respectively) and that missense mutations at codon 167 were associated with a high risk of phaeochromocytoma (53% and 82% at ages 30 and 50 years). Cumulative probabilities of renal cell carcinoma did not differ between the two groups (deletion/ truncation mutations: 8% and 60%, and missense mutations: 10% and 64% at ages 30 and 50 years, respectively). Age related risks for haemangioblastoma were similar in the two mutation groups, with the age related risks of cerebellar haemangioblastoma slightly less (35% and 64% v 38% and 75% at ages 30 and 50 years) and retinal haemangioblastoma slightly higher (45% and 72% v 37% and 64% at ages 30 and 50 years) in the missense mutation group than in the deletion/protein truncation group. These results provide valuable data for counselling VHL families and indicate that specific VHL mutations may be associated with different tumour susceptibility risks. There was no evidence of a generalised increase in age related tumour risks for missense mutations, suggesting that missense mutations predisposing to phaeochromocytoma have tissue specific effects, possibly because the VHL protein has several functions, the importance of which varies from tissue to tissue, or because the proteins which interact with VHL differ between different tissues.
冯·希佩尔-林道病是一种常染色体显性遗传的家族性癌症综合征,易患视网膜和中枢神经系统血管母细胞瘤、肾细胞癌和嗜铬细胞瘤。VHL病在嗜铬细胞瘤的易感性方面表现出可变的表达和家族间差异。在先前一项对65个具有明确VHL突变的VHL家族的研究中,我们发现有嗜铬细胞瘤和无嗜铬细胞瘤的VHL家族之间存在显著差异,即错义突变在嗜铬细胞瘤阳性家族中更常见,而大片段缺失或蛋白质截短突变则较少见。为了进一步研究这种关联的意义和原因,我们对138个VHL家族进行了种系突变研究,并计算了不同类型VHL基因突变的年龄相关肿瘤风险。通过单链构象多态性(SSCP)、异源双链分析和Southern分析,我们在101个家族(73%)中鉴定出种系VHL基因突变。对VHL编码区进行直接测序进一步将突变检测率提高到81%。除了精确的症状前诊断外,VHL基因突变的鉴定还可以提供可能表型的指示。我们发现,预测会导致截短蛋白的大片段缺失和突变与嗜铬细胞瘤的风险较低相关(30岁和50岁时分别为6%和9%),低于错义突变(分别为40%和59%),并且密码子167处的错义突变与嗜铬细胞瘤的高风险相关(30岁和50岁时分别为53%和82%)。两组肾细胞癌的累积概率没有差异(缺失/截短突变:30岁和50岁时分别为8%和60%,错义突变:分别为10%和64%)。两个突变组中血管母细胞瘤的年龄相关风险相似,错义突变组中与年龄相关的小脑血管母细胞瘤风险略低(30岁和50岁时分别为35%和64%对38%和75%),视网膜血管母细胞瘤风险略高(30岁和50岁时分别为45%和72%对37%和64%),高于缺失/蛋白质截短组。这些结果为向VHL家族提供咨询提供了有价值的数据,并表明特定的VHL突变可能与不同的肿瘤易感性风险相关。没有证据表明错义突变导致年龄相关肿瘤风险普遍增加,这表明易患嗜铬细胞瘤的错义突变具有组织特异性效应,可能是因为VHL蛋白具有多种功能,其重要性因组织而异,或者是因为与VHL相互作用的蛋白质在不同组织之间存在差异。
