Katz-Greenberg Goni, Ghimire Sushil, Zhan Tinging, Mallari Kashka, Whitaker-Menezes Diana, Gong Jerald, Uppal Guldeep, Martinez-Outschoorn Ubaldo, Martinez Cantarin Maria P
Department of Medicine, Division of Nephrology, Duke University Durham, NC 27710, USA.
Department of Medicine, Division of Nephrology, Sidney Kimmel Cancer Center, Thomas Jefferson University Philadelphia, PA 19107, USA.
Am J Cancer Res. 2021 Sep 15;11(9):4624-4637. eCollection 2021.
Post-transplant lymphoproliferative disorders (PTLD) are among the most serious complications after solid organ transplantation (SOT). Monomorphic diffuse large B-cell lymphoma (DLBCL) is the most common subtype of PTLD. Historically, outcomes of PTLD have been poor with high mortality rates and allograft loss, although this has improved in the last 10 years. Most of our understanding about PTLD DLBCL is extrapolated from studies in non-PTLD DLBCL, and while several clinical factors have been identified and validated for predicting non-PTLD DLBCL outcomes, the molecular profile of PTLD DLBCL has not yet been characterized. Compartment-specific metabolic reprograming has been described in non-PTLD DLBCL with a lactate uptake metabolic phenotype with high monocarboxylate transporter 1 (MCT1) expression associated with worse outcomes. The aim of our study was to compare the outcomes of PTLD in our transplant center to historic cohorts, as well as study a subgroup of our PTLD DLBCL tumors and compare metabolic profiles with non-PTLD DLBCL. We performed a retrospective single institution study of all adult patients who underwent a SOT between the years 1992-2018, who were later diagnosed with PTLD. All available clinical information was extracted from the patients' medical records. Tumor metabolic markers were studied in a subgroup of PTLD DLBCL and compared to a group of non-PTLD DLBCL. Thirty patients were diagnosed with PTLD following SOT in our center. Median time from SOT to PTLD diagnosis was 62.8 months (IQR 7.6; 134.4), with 37% of patients diagnosed with early PTLD, and 63% with late PTLD. The most common PTLD subtype was DLBCL. Most patients were treated with reduction of their immunosuppression (RIS) including a group who were switched from calcineurin inhibitor (CNI) to mTOR inhibitor based IS, in conjunction with standard anti-lymphoma chemoimmunotherapy. Progression free survival of the PTLD DLBCL cohort was calculated at 86% at 1 year, and 77% at 3 and 5-years, with overall survival of 86% at 1 and 3-years, and 75% at 5 years. Death censored allograft survival in the kidney cohort was 100% at 1 year, and 93% at 3, 5 and 10 years. MCT1 H scores were significantly higher in a subset of the non-PTLD DLBCL patients than in a PTLD DLBCL cohort. Our data is concordant with improved PTLD outcomes in the last 10 years. mTOR inhibitors could be an alternative to CNI as a RIS strategy. Finally, PTLD DLBCL may have a distinct metabolic profile with reduced MCT1 expression compared to non-PTLD DLBCL, but further studies are needed to corroborate our limited cohort findings and to determine if a specific metabolic profile is associated with outcomes.
移植后淋巴细胞增生性疾病(PTLD)是实体器官移植(SOT)后最严重的并发症之一。单形性弥漫性大B细胞淋巴瘤(DLBCL)是PTLD最常见的亚型。从历史上看,PTLD的预后很差,死亡率和移植器官丢失率都很高,不过在过去10年中这种情况有所改善。我们对PTLD DLBCL的大多数了解都是从非PTLD DLBCL的研究中推断出来的,虽然已经确定并验证了几个临床因素可用于预测非PTLD DLBCL的预后,但PTLD DLBCL的分子特征尚未得到描述。在非PTLD DLBCL中已描述了特定区域的代谢重编程,其具有乳酸摄取代谢表型,高表达单羧酸转运蛋白1(MCT1)与较差的预后相关。我们研究的目的是将我们移植中心PTLD的预后与历史队列进行比较,同时研究我们PTLD DLBCL肿瘤的一个亚组,并将其代谢谱与非PTLD DLBCL进行比较。我们对1992年至2018年间接受SOT且后来被诊断为PTLD的所有成年患者进行了一项回顾性单机构研究。从患者病历中提取了所有可用的临床信息。在PTLD DLBCL的一个亚组中研究了肿瘤代谢标志物,并与一组非PTLD DLBCL进行了比较。我们中心有30例患者在SOT后被诊断为PTLD。从SOT到PTLD诊断的中位时间为62.8个月(四分位间距7.6;134.4),37%的患者被诊断为早期PTLD,63%为晚期PTLD。最常见的PTLD亚型是DLBCL。大多数患者接受了免疫抑制降低(RIS)治疗,包括一组从钙调神经磷酸酶抑制剂(CNI)转换为基于mTOR抑制剂的免疫抑制治疗的患者,同时联合标准的抗淋巴瘤化疗免疫治疗。PTLD DLBCL队列的无进展生存率在1年时为86%,3年和5年时为77%,总生存率在1年和3年时为86%,5年时为75%。肾脏队列中死亡截尾的移植器官生存率在1年时为100%,3年、5年和10年时为93%。非PTLD DLBCL患者亚组中的MCT1 H评分显著高于PTLD DLBCL队列。我们的数据与过去10年中PTLD预后的改善一致。mTOR抑制剂可作为RIS策略替代CNI。最后,与非PTLD DLBCL相比,PTLD DLBCL可能具有独特的代谢谱,MCT1表达降低,但需要进一步研究来证实我们有限队列的发现,并确定特定的代谢谱是否与预后相关。
