一项关于移植肾基因背景的回顾性单中心试点研究。
A retrospective single-center pilot study of the genetic background of the transplanted kidney.
作者信息
Novotna Anna, Horackova Klara, Soukupova Jana, Zemankova Petra, Nehasil Petr, Just Pavel, Voska Ludek, Kleiblova Petra, Rajnochova Bloudickova Silvie
机构信息
Department of Nephrology, Institute for Clinical and Experimental Medicine, Prague, Czech Republic.
First Faculty of Medicine, Institute of Medical Biochemistry and Laboratory Diagnostics, Charles University and General University Hospital in Prague, Prague, Czech Republic.
出版信息
PLoS One. 2025 Jan 8;20(1):e0316192. doi: 10.1371/journal.pone.0316192. eCollection 2025.
INTRODUCTION
Renal cell carcinoma (RCC) is one of the most prevalent cancers in kidney transplant recipients (KTR). The hereditary background of RCC in native kidneys has been determined, implicating its clinical importance.
MATERIALS AND METHODS
This retrospective single-center pilot study aimed to identify a potential genetic predisposition to RCC of the transplanted kidney and outcome in KTR who underwent single kidney transplantation between January 2000 and December 2020 and manifested RCC of the transplanted kidney. Next-generation sequencing (NGS) based germline genetic analysis from peripheral blood-derived genomic DNA (gDNA) was performed in both the recipient and donor using a gene panel targeting 226 cancer predisposition genes.
RESULTS
The calculated incidence of RCC of the transplanted kidney among 4146 KTR was 0.43%. In fifteen KTR and donors, NGS was performed. The mean KTR age at transplantation and the diagnosis of RCC was 50.3 years (median 54; 5-67 years) and 66 years (median 66; 24-79 years), respectively. The mean donor age at transplantation and graft age at RCC diagnosis was 39.7 years (median 42; 7-68 years) and 50.2 years (median 46; 20-83 years), respectively. The mean follow-up after RCC diagnosis was 47 months (median 39.1; 0-112 months). Papillary RCC was the most prevalent (n = 8), followed by clear cell RCC (n = 6) and unspecified RCC (n = 1). Thirteen RCCs were low-stage (pT1a/b) diseases, one was pT3, and one was of unknown stage. Most RCC was higher graded. No germline pathogenic cancer-predisposition variant was found in either KTR or donors except for several variants of uncertain significance.
CONCLUSION
RCC of the transplanted kidney is very rare. Germline cancer-predisposition testing has identified several variants of uncertain significance, but no germline genetic predisposition to graft RCC in KTR. Further research is needed to assess the clinical relevance of genetic testing for cancer risk in KTR.
引言
肾细胞癌(RCC)是肾移植受者(KTR)中最常见的癌症之一。已确定了原发性肾脏中RCC的遗传背景,这表明了其临床重要性。
材料与方法
这项回顾性单中心试点研究旨在确定接受单肾移植的KTR中移植肾发生RCC的潜在遗传易感性及其预后情况,这些KTR在2000年1月至2020年12月期间接受了单肾移植,并出现了移植肾RCC。使用针对226个癌症易感基因的基因panel,对受者和供者的外周血来源基因组DNA(gDNA)进行基于二代测序(NGS)的种系遗传分析。
结果
在4146名KTR中,移植肾RCC的计算发病率为0.43%。对15名KTR及其供者进行了NGS检测。KTR移植时的平均年龄和RCC诊断时的平均年龄分别为50.3岁(中位数54岁;范围5 - 67岁)和66岁(中位数66岁;范围24 - 79岁)。供者移植时的平均年龄和RCC诊断时移植物的平均年龄分别为39.7岁(中位数42岁;范围7 - 68岁)和50.2岁(中位数46岁;范围20 - 83岁)。RCC诊断后的平均随访时间为47个月(中位数39.1个月;范围0 - 112个月)。乳头状RCC最为常见(n = 8),其次是透明细胞RCC(n = 6)和未明确类型的RCC(n = 1)。13例RCC为低分期(pT1a/b)疾病,1例为pT3,1例分期不明。大多数RCC分级较高。除了几个意义不确定的变异外,在KTR或供者中均未发现种系致病性癌症易感变异。
结论
移植肾RCC非常罕见。种系癌症易感检测发现了几个意义不确定的变异,但未发现KTR中移植肾RCC的种系遗传易感性。需要进一步研究以评估KTR中癌症风险基因检测的临床相关性。
Zotero 插件