De novo Glomerular Disease and the Significance of Electron Microscopy in Renal Transplantation.

Surya V Seshan, Steven P Salvatore
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Abstract

Background: De novo glomerular diseases comprising those both common and unique to transplant may develop in the renal allograft leading to posttransplant proteinuria, hematuria, or allograft failure. Electron microscopy (EM) is a useful adjunct to the standard light and immunofluorescence microscopy for accurately diagnosing these diseases and subsequently aiding the clinician in initiating appropriate treatments.

Summary: De novo diseases are those new-onset diseases in renal transplantation that are unrelated to the original kidney disease in the recipient. They include virtually any primary or secondary glomerular, tubulointerstitial, or vascular diseases, ranging from subclinical to clinically overt, having acute, subacute, or chronic clinical presentations. This review focuses on common or significant, mainly glomerular, entities, with particular attention to the EM findings. The time of onset, stage, and severity of these diseases may often be modified by the current immunosuppressive protocols and other donor and recipient predisposing characteristics.

Key messages: A renal allograft biopsy not only improves our understanding of the pathophysiology but also provides diagnostic accuracy prognostic information, and potential for reversibility. In some cases, the biopsy leads to detection of unsuspected or clinically asymptomatic de novo diseases in the setting of other concomitant rejection processes, infection, or toxicity, which can dictate appropriate therapy. Routine EM in transplant kidney biopsies is a valuable modality in recognizing fully developed or early/subtle features of evolving de novo diseases, often during the subclinical phases, in "for cause" or surveillance/protocol allograft biopsies.

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新生肾小球疾病及电子显微镜在肾移植中的意义。
背景:新生肾小球疾病包括移植常见和独特的肾小球疾病,可在移植肾中发生,导致移植后蛋白尿、血尿或移植失败。电子显微镜(EM)是标准光镜和免疫荧光显微镜的有用辅助手段,可以准确诊断这些疾病,并随后帮助临床医生开始适当的治疗。摘要:新生疾病是指肾移植术后新发的与受者原有肾脏疾病无关的疾病。它们包括几乎所有原发性或继发性肾小球、小管间质或血管疾病,从亚临床到临床显性,具有急性、亚急性或慢性临床表现。本综述的重点是常见或重要的实体,主要是肾小球,特别关注EM的发现。这些疾病的发病时间、分期和严重程度可能经常被当前的免疫抑制方案和其他供体和受体易感特征所改变。关键信息:肾移植活检不仅提高了我们对病理生理学的理解,而且提供了诊断准确性、预后信息和潜在的可逆性。在某些情况下,活检可在其他伴随排斥反应、感染或毒性的情况下发现未怀疑的或临床无症状的新生疾病,这可以指示适当的治疗。在“病因”或监测/协议同种异体移植活检中,移植肾活检常规EM是一种有价值的方式,可以识别完全发展或早期/微妙的发展中的新发疾病特征,通常在亚临床阶段。
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