Giulia Vanessa Re Sartò, Carlo Alfieri, Laura Cosmai, Emilietta Brigati, Mariarosaria Campise, Anna Regalia, Simona Verdesca, Paolo Molinari, Anna Maria Pisacreta, Marta Pirovano, Luca Nardelli, Maurizio Gallieni, Giuseppe Castellano
{"title":"肾移植后癌症:来自意大利单个中心的真实世界回顾性分析","authors":"Giulia Vanessa Re Sartò, Carlo Alfieri, Laura Cosmai, Emilietta Brigati, Mariarosaria Campise, Anna Regalia, Simona Verdesca, Paolo Molinari, Anna Maria Pisacreta, Marta Pirovano, Luca Nardelli, Maurizio Gallieni, Giuseppe Castellano","doi":"10.3389/ti.2024.13220","DOIUrl":null,"url":null,"abstract":"<p><p>We describe the epidemiology of cancer after kidney transplantation (KTx), investigating its risk factors and impact on therapeutic management and survival in KTx recipients (KTRs). The association between modification of immunosuppressive (IS) therapy after cancer and survival outcomes was analyzed. We collected data from 930 KTRs followed for 7 [1-19] years. The majority of KTRs received KTx from a deceased donor (84%). In total, 74% of patients received induction therapy with basiliximab and 26% with ATG. Maintenance therapy included steroids, calcineurin inhibitors, and mycophenolate. Patients with at least one cancer (CA+) amounted to 19%. NMSC was the most common tumor (55%). CA+ were older and had a higher BMI. Vasculitis and ADPKD were more prevalent in CA+. ATG was independently associated with CA+ and was related to earlier cancer development in survival and competing risk analyses (<i>p</i> = 0.01 and <0.0001; basiliximab 89 ± 4 vs<i>.</i> ATG 40 ± 4 months). After cancer diagnosis, a significant prognostic impact was derived from the shift to mTOR inhibitors compared to a definitive IS drug suspension (<i>p</i> = 0.004). Our data confirm the relevance of cancer as a complication in KTRs with ATG as an independent risk factor. An individualized choice of IS to be proposed at the time of KTx is crucial in the prevention of neoplastic risk. Finally, switching to mTORi could represent an important strategy to improve patient survival.</p>","PeriodicalId":23343,"journal":{"name":"Transplant International","volume":"37 ","pages":"13220"},"PeriodicalIF":2.7000,"publicationDate":"2024-08-20","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11368674/pdf/","citationCount":"0","resultStr":"{\"title\":\"Post-Kidney Transplant Cancer: A Real-World Retrospective Analysis From a Single Italian Center.\",\"authors\":\"Giulia Vanessa Re Sartò, Carlo Alfieri, Laura Cosmai, Emilietta Brigati, Mariarosaria Campise, Anna Regalia, Simona Verdesca, Paolo Molinari, Anna Maria Pisacreta, Marta Pirovano, Luca Nardelli, Maurizio Gallieni, Giuseppe Castellano\",\"doi\":\"10.3389/ti.2024.13220\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>We describe the epidemiology of cancer after kidney transplantation (KTx), investigating its risk factors and impact on therapeutic management and survival in KTx recipients (KTRs). The association between modification of immunosuppressive (IS) therapy after cancer and survival outcomes was analyzed. We collected data from 930 KTRs followed for 7 [1-19] years. The majority of KTRs received KTx from a deceased donor (84%). In total, 74% of patients received induction therapy with basiliximab and 26% with ATG. Maintenance therapy included steroids, calcineurin inhibitors, and mycophenolate. Patients with at least one cancer (CA+) amounted to 19%. NMSC was the most common tumor (55%). CA+ were older and had a higher BMI. Vasculitis and ADPKD were more prevalent in CA+. ATG was independently associated with CA+ and was related to earlier cancer development in survival and competing risk analyses (<i>p</i> = 0.01 and <0.0001; basiliximab 89 ± 4 vs<i>.</i> ATG 40 ± 4 months). After cancer diagnosis, a significant prognostic impact was derived from the shift to mTOR inhibitors compared to a definitive IS drug suspension (<i>p</i> = 0.004). Our data confirm the relevance of cancer as a complication in KTRs with ATG as an independent risk factor. An individualized choice of IS to be proposed at the time of KTx is crucial in the prevention of neoplastic risk. 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Post-Kidney Transplant Cancer: A Real-World Retrospective Analysis From a Single Italian Center.
We describe the epidemiology of cancer after kidney transplantation (KTx), investigating its risk factors and impact on therapeutic management and survival in KTx recipients (KTRs). The association between modification of immunosuppressive (IS) therapy after cancer and survival outcomes was analyzed. We collected data from 930 KTRs followed for 7 [1-19] years. The majority of KTRs received KTx from a deceased donor (84%). In total, 74% of patients received induction therapy with basiliximab and 26% with ATG. Maintenance therapy included steroids, calcineurin inhibitors, and mycophenolate. Patients with at least one cancer (CA+) amounted to 19%. NMSC was the most common tumor (55%). CA+ were older and had a higher BMI. Vasculitis and ADPKD were more prevalent in CA+. ATG was independently associated with CA+ and was related to earlier cancer development in survival and competing risk analyses (p = 0.01 and <0.0001; basiliximab 89 ± 4 vs. ATG 40 ± 4 months). After cancer diagnosis, a significant prognostic impact was derived from the shift to mTOR inhibitors compared to a definitive IS drug suspension (p = 0.004). Our data confirm the relevance of cancer as a complication in KTRs with ATG as an independent risk factor. An individualized choice of IS to be proposed at the time of KTx is crucial in the prevention of neoplastic risk. Finally, switching to mTORi could represent an important strategy to improve patient survival.
期刊介绍:
The aim of the journal is to serve as a forum for the exchange of scientific information in the form of original and high quality papers in the field of transplantation. Clinical and experimental studies, as well as editorials, letters to the editors, and, occasionally, reviews on the biology, physiology, and immunology of transplantation of tissues and organs, are published. Publishing time for the latter is approximately six months, provided major revisions are not needed. The journal is published in yearly volumes, each volume containing twelve issues. Papers submitted to the journal are subject to peer review.