分子显微诊断系统在真实世界移植队列中的临床实用性:迈向新范例

Andrea Fernandez Valledor, Cathrine Marie Moeller, Gal Rubinstein, Salwa Rahman, Daniel Oren, julia baranowska, Changhee Lee, Ruben Anthony Salazar, Carolyn Hennecken, Afsana Rahman, Boaz Elad, Dor Lotan, Ersilia Marie DeFilippis, Adil Yunis, Justin A Fried, Jayant Raikhelkar, Kyung T. Oh, David Bae, Edward Lin, Sun Hi Lee, Matthew Regan, Melana Yuzefpolskaya, Paolo C. Colombo, David Majure, Farhana Latif, Kevin J Clerkin, Gabriel T Sayer, Nir Uriel
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引用次数: 0

摘要

研究目的评估对疑似排斥反应的心脏移植(HT)受者活检标本进行辅助分子基因表达分析(MMDx)的临床意义。导言:组织病理学评估仍是诊断心脏移植排斥反应的标准方法。然而,由于观察者之间的差异很大,再加上 "活检阴性 "排斥反应的发生率相对较高,因此人们担心会出现假阴性结果。MMDx 利用基因表达检测排斥反应的早期征兆,是一种有望进一步完善 HT 排斥反应评估的检测方法。方法:单中心前瞻性研究对2022年11月至2024年5月期间进行的418例连续因心内膜心肌活检进行单中心前瞻性研究。根据组织学对每个活检进行分级,并使用 MMDx 评估排斥模式。如果存在边缘性或确定性排斥反应,则 MMDx 结果被视为阳性。评估了 MMDx 结果对临床管理的影响。主要结果是在 MMDx 指导下进行临床管理后的 1 年存活率和移植物功能障碍。次要结果包括供体特异性抗体、MMDx 基因转录物和供体来源无细胞 DNA(dd-cfDNA)水平的变化。结果我们分析了来自 237 名患者的 418 份分子样本。组织学鉴定出排斥反应的有 32 例(7.7%),而 MMDx 鉴定出排斥反应的有 95 例(22.7%)。值得注意的是,在 95 例 MMDx 检测出排斥反应的病例中,有 79 例组织学检测结果为阴性,其中大部分为抗体介导的排斥反应(62.1%)。与MMDx结果为边缘或阴性的样本相比,MMDx结果为排斥反应的样本更有可能出现dd-cfDNA和外周血基因表达谱的联合升高(36.7% vs 28.0% vs 10.3%;p<0.001)。20.4%的病例因MMDx结果而实施了特定的抗排斥方案或改变了免疫抑制,73.4%的病例因组织学检查阴性而MMDx结果显示存在排斥反应。以MMDx结果指导临床治疗的MMDx阳性组的1年生存率更高(87.0% vs 78.6%; log rank p=0.0017)。结论:在我们的队列中,MMDx结果比组织学结果更常显示出排斥反应,通常会导致抗排斥治疗的启动。以 MMDx 阳性结果为指导进行干预可改善预后。
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Clinical Utility of the Molecular Microscope Diagnostic System in a Real-World Transplant Cohort: Moving Towards a New Paradigm
Objectives: To evaluate the clinical implications of adjunctive molecular gene expression analysis (MMDx) of biopsy specimens in heart transplant (HT) recipients with suspected rejection. Introduction: Histopathological evaluation remains the standard method for rejection diagnosis in HT. However, the wide inter-observer variability combined with a relatively common incidence of "biopsy-negative" rejection has raised concerns about the likelihood of false-negative results. MMDx, which uses gene expression to detect early signs of rejection, is a promising test to further refine the assessment of HT rejection. Methods: Single-center prospective study of 418 consecutive for-cause endomyocardial biopsies performed between November 2022 and May 2024. Each biopsy was graded based on histology and assessed for rejection patterns using MMDx. MMDx results were deemed positive if borderline or definitive rejection was present. The impact of MMDx results on clinical management was evaluated. Primary outcomes were 1-year survival and graft dysfunction following MMDx-guided clinical management. Secondary outcomes included changes in donor-specific antibodies, MMDx gene transcripts, and donor-derived cell-free DNA (dd-cfDNA) levels. Results: We analyzed 418 molecular samples from 237 unique patients. Histology identified rejection in 32 cases (7.7%), while MMDx identified rejection in 95 cases (22.7%). Notably, in 79 of the 95 cases where MMDx identified rejection, histology results were negative, with the majority of these cases being antibody-mediated rejection (62.1%). Samples with rejection on MMDx were more likely to show a combined elevation of dd-cfDNA and peripheral blood gene expression profiling than those with borderline or negative MMDx results (36.7% vs 28.0% vs 10.3%; p<0.001). MMDx results led to the implementation of specific anti-rejection protocols or changes in immunosuppression in 20.4% of cases, and in 73.4% of cases where histology was negative and MMDx showed rejection. 1-year survival was better in the positive MMDx group where clinical management was guided by MMDx results (87.0% vs 78.6%; log rank p=0.0017). Conclusions: In our cohort, MMDx results more frequently indicated rejection than histology, often leading to the initiation of anti-rejection treatment. Intervention guided by positive MMDx results was associated with improved outcomes.
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