Department of Pediatrics, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15261, USA.
Clin Cancer Res. 2012 Apr 15;18(8):2382-90. doi: 10.1158/1078-0432.CCR-11-2303. Epub 2012 Feb 20.
Secondary lymphedema is a frequent complication of breast cancer associated with surgery, chemotherapy, or radiation following breast cancer treatment. The potential contribution of genetic susceptibility to risk of developing secondary lymphedema following surgical trauma, radiation, and other tissue insults has not been studied.
To determine whether women with breast cancer and secondary lymphedema had mutations in candidate lymphedema genes, we undertook a case-control study of 188 women diagnosed with breast cancer recruited from the University of Pittsburgh Breast Cancer Program (http://www.upmccancercenter.com/breast/index.cfm) between 2000 and 2010. Candidate lymphedema genes, GJC2 (encoding connexin 47 [Cx47]), FOXC2, HGF, MET, and FLT4 (encoding VEGFR3), were sequenced for mutation. Bioinformatics analysis and in vitro functional assays were used to confirm significance of novel mutations.
Cx47 mutations were identified in individuals having secondary lymphedema following breast cancer treatment but not in breast cancer controls or normal women without breast cancer. These novel mutations are dysfunctional as assessed through in vitro assays and bioinformatics analysis and provide evidence that altered gap junction function leads to lymphedema.
Our findings challenge the view that secondary lymphedema is solely due to mechanical trauma and support the hypothesis that genetic susceptibility is an important risk factor for secondary lymphedema. A priori recognition of genetic risk (i) raises the potential for early detection and intervention for a high-risk group and (ii) allows the possibility of altering surgical approach and/or chemo- and radiation therapy, or direct medical treatment of secondary lymphedema with novel connexin-modifying drugs.
继发淋巴水肿是乳腺癌术后、化疗或放疗后常见的并发症。尚未研究遗传易感性对手术创伤、放射治疗和其他组织损伤后继发淋巴水肿风险的潜在影响。
为了确定患有乳腺癌和继发性淋巴水肿的女性是否存在候选淋巴水肿基因的突变,我们对 2000 年至 2010 年间在匹兹堡大学乳腺癌项目(http://www.upmccancercenter.com/breast/index.cfm)招募的 188 名诊断为乳腺癌的女性进行了病例对照研究。对候选淋巴水肿基因 GJC2(编码间隙连接蛋白 47 [Cx47])、FOXC2、HGF、MET 和 FLT4(编码 VEGFR3)进行了突变测序。采用生物信息学分析和体外功能测定来确认新突变的意义。
在乳腺癌治疗后发生继发性淋巴水肿的个体中发现了 Cx47 突变,但在乳腺癌对照或无乳腺癌的正常女性中未发现这些突变。通过体外测定和生物信息学分析评估这些新突变是功能失调的,这为改变的间隙连接功能导致淋巴水肿提供了证据。
我们的发现对继发性淋巴水肿完全是由机械创伤引起的观点提出了挑战,并支持遗传易感性是继发性淋巴水肿的一个重要危险因素的假说。预先识别遗传风险:(i)为高风险人群的早期检测和干预提供了可能性;(ii)允许改变手术方法和/或化疗和放疗,或用新型连接蛋白修饰药物直接治疗继发性淋巴水肿。