Department of Urology, Peking University First Hospital, Beijing, China.
Institute of Urology, Peking University, Beijing, China.
Cancer Med. 2017 Sep;6(9):2131-2141. doi: 10.1002/cam4.1134. Epub 2017 Aug 4.
Von Hippel-Lindau (VHL) disease is a rare autosomal dominant cancer syndrome caused by alterations of VHL gene. Patients are predisposed to develop pheochromocytomas and solid or cystic tumors of the central nervous system, kidney, pancreas, and retina. Remarkable phenotypic heterogeneity exits in organ involvement and tumor onset age between and within VHL families. However, no reliable markers have been found to predict the age-related tumor risks in VHL patients. A large Chinese cohort composed of 300 VHL patients and 92 healthy family controls was enrolled in our study. Blood relative telomere length was measured in 184 patients and all the controls available for genomic DNA samples. Age-related risks for the five major VHL-associated tumors were evaluated using Kaplan-Meier plots and Cox regression analysis. Differences in clinical phenotype were observed between Chinese cohort and the United Kingdom cohort. VHL patients showed significantly shorter telomere length than healthy family controls(P = 0.0183), and a positive correlation was found between telomere length and onset age of the five major tumors, respectively. Moreover, patients in the shorter telomere group (age-adjusted telomere length ≤ 0.44) suffered higher age-related risks for VHL-associated central nervous system hemangioblastomas (HR: 1.879, P = 0.004), renal cell carcinoma (HR: 2.126, P = 0.002) and pancreatic cyst and neuroendocrine tumors (HR: 2.093, P = 0.001). These results indicate that blood shorter telomere length is a new biomarker for age-related tumor risks in VHL patients, which will be crucial to genetic counseling and future research about the role of telomere shortening in the pathogenesis of VHL-associated tumors.
希佩尔-林道(VHL)病是一种罕见的常染色体显性遗传癌症综合征,由 VHL 基因突变引起。患者易发生嗜铬细胞瘤以及中枢神经系统、肾脏、胰腺和视网膜的实体或囊性肿瘤。VHL 家系内和家系间的器官受累和肿瘤发病年龄存在显著的表型异质性。然而,目前尚未发现可靠的标志物来预测 VHL 患者的年龄相关肿瘤风险。我们的研究纳入了一个由 300 名 VHL 患者和 92 名健康家族对照组成的大型中国队列。对 184 名患者和所有可获得基因组 DNA 样本的对照者进行了血液相对端粒长度测量。使用 Kaplan-Meier 图和 Cox 回归分析评估了 5 种主要 VHL 相关肿瘤的年龄相关风险。中国队列与英国队列的临床表型存在差异。VHL 患者的端粒长度明显短于健康家族对照者(P=0.0183),并且端粒长度与 5 种主要肿瘤的发病年龄呈正相关。此外,端粒较短组(校正年龄后的端粒长度≤0.44)的患者发生 VHL 相关中枢神经系统血管母细胞瘤(HR:1.879,P=0.004)、肾细胞癌(HR:2.126,P=0.002)和胰腺囊肿和神经内分泌肿瘤的年龄相关风险更高(HR:2.093,P=0.001)。这些结果表明,血液端粒较短是 VHL 患者年龄相关肿瘤风险的一个新的生物标志物,这对于遗传咨询和未来关于端粒缩短在 VHL 相关肿瘤发病机制中的作用的研究至关重要。
