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Pathophysiology and management of monoclonal gammopathy of renal significance

机译:具有肾脏意义的单克隆丙种球蛋白病的病理生理学和处理

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摘要

Recent years have witnessed a rapid growth in our understanding of the pathogenic property of monoclonal proteins. It is evident that some of these small monoclonal proteins are capable of inducing end-organ damage as a result of their intrinsic physicochemical properties. Hence, an umbrella term, monoclonal gammopathy of clinical significance (MGCS), has been coined to include myriad conditions attributed to these pathogenic proteins. Because kidneys are the most commonly affected organ (but skin, peripheral nerves, and heart can also be involved), we discuss MGRS exclusively in this review. Mechanisms of renal damage may involve direct or indirect effects. Renal biopsy is mandatory and demonstration of monoclonal immunoglobulin in kidney, along with the corresponding immunoglobulin in serum or urine, is key to establish the diagnosis. Pitfalls exist at each diagnostic step, and a high degree of clinical suspicion is required to diagnose MGRS. Recognition of MGRS by hematologists and nephrologists is important, because timely clone-directed therapy improves renal outcomes. Autologous stem cell transplant may benefit selected patients.
机译:近年来,我们对单克隆蛋白的致病特性的了解迅速增长。显然,这些小单克隆蛋白中的一些由于其固有的物理化学性质而能够诱导终末器官损害。因此,已经创造了总括性术语,即具有临床意义的单克隆丙种球蛋白病(MGCS),以包括归因于这些致病蛋白的多种疾病。由于肾脏是最常受累的器官(但也可能涉及皮肤,周围神经和心脏),因此在本综述中我们仅讨论MGRS。肾脏损害的机制可能涉及直接或间接作用。肾脏活检是强制性的,证明肾脏中的单克隆免疫球蛋白以及血清或尿液中相应的免疫球蛋白是确定诊断的关键。在每个诊断步骤都存在陷阱,诊断MGRS需要高度的临床怀疑。血液学家和肾脏病学家对MGRS的认识很重要,因为及时的克隆指导治疗可改善肾脏结局。自体干细胞移植可能会使选定的患者受益。

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