Goni Katz-Greenberg, Julie M Steinbrink, Krishna Shah, Jennifer S Byrns
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The aim of this retrospective single-center study was to investigate the incidence and implications of CMV DNAemia in KTRs with prior SOTs. The study included 97 KTRs with prior SOTs and 154 KTRs with no prior transplants as a control group. In the study group, the most common SOT before the current kidney transplantation (KT), was a previous KT. Patients in the KTR group with prior SOTs were more sensitized than those in the control group [calculated panel-reactive antibody > 30%: 49 (50.5%) vs. 30 (19.45%) patients, <i>p</i> = 0.001]. There was a 39.2% incidence of CMV DNAemia in the previous SOT group compared to 48.7% in the control group [non-significant (NS)]. Patients with prior SOTs demonstrated a shorter post-transplant time to CMV DNAemia [median time 1.6 months (interquartile range, IQR 0.7-5.8) in the KTRs with prior SOTs vs. 2.6 months (IQR 1.5-8.1) in the control group (<i>p</i> = 0.001)]. Although the study highlights the need for tailored prophylaxis strategies and vigilant monitoring in KTRs with prior SOTs, its limitations, such as its retrospective nature and single-center design, call for further multicenter research to establish comprehensive guidelines for managing CMV DNAemia in this unique patient population. Despite these limitations, this study underscores the importance of recognizing the heightened risk of CMV infection or reactivation in KTRs overall and the potential benefits of proactive intervention to mitigate associated morbidity and mortality.</p>","PeriodicalId":519976,"journal":{"name":"Frontiers in transplantation","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2024-04-09","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11235366/pdf/","citationCount":"0","resultStr":"{\"title\":\"Bridging the gap: assessing CMV DNAemia in kidney transplant recipients with previous solid organ transplants.\",\"authors\":\"Goni Katz-Greenberg, Julie M Steinbrink, Krishna Shah, Jennifer S Byrns\",\"doi\":\"10.3389/frtra.2024.1280280\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Cytomegalovirus (CMV) infection poses a significant threat to solid organ transplant (SOT) recipients and can lead to various complications and adverse outcomes. In an effort to prevent CMV infection, it is common to utilize prophylactic strategies, including antiviral medications such as valganciclovir, especially for high-risk patients. Risk factors for CMV infection in kidney transplant recipients (KTRs) include CMV mismatch between donor and recipient (i.e., donor positive, recipient negative), and intensity of immunosuppression, such as the use of T-cell depleting agents. However, little attention has been given to KTRs with a history of prior SOTs, despite their prolonged exposure to immunosuppressive regimens. The aim of this retrospective single-center study was to investigate the incidence and implications of CMV DNAemia in KTRs with prior SOTs. The study included 97 KTRs with prior SOTs and 154 KTRs with no prior transplants as a control group. In the study group, the most common SOT before the current kidney transplantation (KT), was a previous KT. Patients in the KTR group with prior SOTs were more sensitized than those in the control group [calculated panel-reactive antibody > 30%: 49 (50.5%) vs. 30 (19.45%) patients, <i>p</i> = 0.001]. There was a 39.2% incidence of CMV DNAemia in the previous SOT group compared to 48.7% in the control group [non-significant (NS)]. Patients with prior SOTs demonstrated a shorter post-transplant time to CMV DNAemia [median time 1.6 months (interquartile range, IQR 0.7-5.8) in the KTRs with prior SOTs vs. 2.6 months (IQR 1.5-8.1) in the control group (<i>p</i> = 0.001)]. Although the study highlights the need for tailored prophylaxis strategies and vigilant monitoring in KTRs with prior SOTs, its limitations, such as its retrospective nature and single-center design, call for further multicenter research to establish comprehensive guidelines for managing CMV DNAemia in this unique patient population. 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引用次数: 0
摘要
巨细胞病毒(CMV)感染对实体器官移植(SOT)受者构成重大威胁,可导致各种并发症和不良后果。为了预防 CMV 感染,通常会采取预防性策略,包括使用缬更昔洛韦等抗病毒药物,尤其是针对高危患者。肾移植受者(KTR)感染 CMV 的风险因素包括供体和受体之间的 CMV 不匹配(即供体阳性,受体阴性)以及免疫抑制的强度,如使用 T 细胞消耗剂。然而,对于曾有过 SOT 病史的 KTR,尽管他们长期暴露于免疫抑制方案中,却很少有人关注。这项回顾性单中心研究旨在调查曾接受过 SOT 的 KTR 中 CMV DNA 血症的发生率及其影响。研究对象包括 97 名既往接受过 SOT 的 KTR 和 154 名既往未接受过移植的 KTR 作为对照组。在研究组中,当前肾移植(KT)前最常见的 SOT 是之前的 KT。与对照组相比,既往接受过 SOT 的 KTR 组患者的致敏程度更高[计算得出的小组反应抗体 > 30%:49(50.5%)对 30(19.45%)名患者,P = 0.001]。既往 SOT 组 CMV DNA 血症发生率为 39.2%,而对照组为 48.7% [无显著性 (NS)]。既往接受过 SOT 的患者在移植后出现 CMV DNA 血症的时间更短[既往接受过 SOT 的 KTR 中位时间为 1.6 个月(四分位距间,IQR 0.7-5.8),对照组为 2.6 个月(IQR 1.5-8.1)(P = 0.001)]。尽管该研究强调了对既往有 SOT 的 KTR 进行有针对性的预防策略和警惕性监测的必要性,但其局限性(如其回顾性和单中心设计)要求进一步开展多中心研究,以建立管理这一特殊患者群体中 CMV DNA 血症的综合指南。尽管存在这些局限性,但这项研究强调了认识到 KTR 中 CMV 感染或再激活风险增加的重要性,以及积极干预对降低相关发病率和死亡率的潜在益处。
Bridging the gap: assessing CMV DNAemia in kidney transplant recipients with previous solid organ transplants.
Cytomegalovirus (CMV) infection poses a significant threat to solid organ transplant (SOT) recipients and can lead to various complications and adverse outcomes. In an effort to prevent CMV infection, it is common to utilize prophylactic strategies, including antiviral medications such as valganciclovir, especially for high-risk patients. Risk factors for CMV infection in kidney transplant recipients (KTRs) include CMV mismatch between donor and recipient (i.e., donor positive, recipient negative), and intensity of immunosuppression, such as the use of T-cell depleting agents. However, little attention has been given to KTRs with a history of prior SOTs, despite their prolonged exposure to immunosuppressive regimens. The aim of this retrospective single-center study was to investigate the incidence and implications of CMV DNAemia in KTRs with prior SOTs. The study included 97 KTRs with prior SOTs and 154 KTRs with no prior transplants as a control group. In the study group, the most common SOT before the current kidney transplantation (KT), was a previous KT. Patients in the KTR group with prior SOTs were more sensitized than those in the control group [calculated panel-reactive antibody > 30%: 49 (50.5%) vs. 30 (19.45%) patients, p = 0.001]. There was a 39.2% incidence of CMV DNAemia in the previous SOT group compared to 48.7% in the control group [non-significant (NS)]. Patients with prior SOTs demonstrated a shorter post-transplant time to CMV DNAemia [median time 1.6 months (interquartile range, IQR 0.7-5.8) in the KTRs with prior SOTs vs. 2.6 months (IQR 1.5-8.1) in the control group (p = 0.001)]. Although the study highlights the need for tailored prophylaxis strategies and vigilant monitoring in KTRs with prior SOTs, its limitations, such as its retrospective nature and single-center design, call for further multicenter research to establish comprehensive guidelines for managing CMV DNAemia in this unique patient population. Despite these limitations, this study underscores the importance of recognizing the heightened risk of CMV infection or reactivation in KTRs overall and the potential benefits of proactive intervention to mitigate associated morbidity and mortality.
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