非狼疮性全满贯肾病:系统评价。
Nonlupus Full House Nephropathy: A Systematic Review.
机构信息
Department of Medicine and Surgery, University of Milano-Bicocca and ASST Monza, Monza, Italy.
Department of Pathology and Medical Biology, University Medical Center, University of Groningen, Groningen, The Netherlands.
出版信息
Clin J Am Soc Nephrol. 2024 Jun 1;19(6):743-754. doi: 10.2215/CJN.0000000000000438. Epub 2024 Mar 26.
KEY POINTS
Nonlupus full house nephropathy is a rare, complex entity: confusion arises by the low-quality evidence and the lack of consensus on nomenclature. This systematic review supports that systemic lupus erythematosus and nonlupus full house nephropathy are distinct clinical entities, with comparable outcomes. The identification of three pathogenetic categories provides further clues for a shared clinical and diagnostic approach to the disease.
BACKGROUND
The presence of a full house pattern at immunofluorescence on kidney biopsy in a patient without clinical and laboratory features of systemic lupus erythematosus (SLE) has led to the descriptive term nonlupus full house nephropathy. This systematic review and meta-analysis focus on nonlupus full house nephropathy nomenclature, clinical findings, and outcomes.
METHODS
In a reiterative process, all identified terms for nonlupus full house nephropathy and other medical subject headings terms were searched in PubMed. Out of 344 results, 57 records published between 1982 and 2022 were included in the analysis. Clinical data of single patients from different reports were collected. Patients were classified into three pathogenetic categories, which were compared according to baseline characteristics, treatments, and outcomes.
RESULTS
Out of the 57 records, 61% were case reports. Nonlupus full house nephropathy was addressed with 17 different names. We identified 148 patients: 75 (51%) were men; median age 35 (23–58) years. Serum creatinine and proteinuria at onset were 1.4 (0.8–2.5) mg/dl and 5.7 (2.7–8.8) g/d. About half of patients achieved complete response. A causative agent was identified in 51 patients (44%), mainly infectious (41%). Secondary nonlupus full house nephropathy was mostly nonrelapsing with worse kidney function at onset compared with idiopathic disease ( = 0.001). Among the 57 patients (50%) with idiopathic nonlupus full house nephropathy, complete response was comparable between patients treated with immunosuppression and supportive therapy; however, proteinuria and creatinine at onset were higher in patients treated with immunosuppression ( = 0.09 and = 0.07). The remaining 7 patients (6%) developed SLE after a median follow-up of 5.0 (1.9–9.0) years.
CONCLUSIONS
Our data support that SLE and nonlupus full house nephropathy are distinct clinical entities, with comparable outcomes. A small subset of patients develops SLE during follow-up. Nonlupus full house nephropathy is addressed by many different names in the literature. The identification of three pathogenetic categories provides further clues for the management of the disease.
要点
非狼疮性满堂肾病是一种罕见且复杂的实体疾病:由于证据质量低和命名缺乏共识,导致存在混淆。本系统评价支持红斑狼疮和非狼疮性满堂肾病是两种不同的临床实体,具有可比的结局。三种发病机制类别的确定为该疾病的临床和诊断方法提供了进一步的线索。
背景
在没有系统性红斑狼疮(SLE)的临床和实验室特征的患者中,肾脏活检免疫荧光出现满堂模式,导致了非狼疮性满堂肾病的描述性术语。本系统评价和荟萃分析重点关注非狼疮性满堂肾病的命名、临床发现和结局。
方法
在反复的过程中,在 PubMed 中搜索了所有确定的非狼疮性满堂肾病和其他医学主题词术语。在 344 项结果中,纳入了 1982 年至 2022 年期间发表的 57 份记录进行分析。从不同报告的单个患者中收集临床数据。将患者分为三种发病机制类别,并根据基线特征、治疗和结局进行比较。
结果
在 57 份记录中,有 61%是病例报告。非狼疮性满堂肾病有 17 种不同的名称。共纳入 148 名患者:75 名(51%)为男性;中位年龄为 35 岁(23-58 岁)。发病时血清肌酐和蛋白尿分别为 1.4(0.8-2.5)mg/dl 和 5.7(2.7-8.8)g/d。约一半的患者获得完全缓解。在 51 名患者(44%)中确定了病因,主要是感染(41%)。继发性非狼疮性满堂肾病大多为非复发,与特发性疾病相比,发病时肾功能更差( = 0.001)。在 57 名(50%)特发性非狼疮性满堂肾病患者中,接受免疫抑制和支持治疗的患者完全缓解率相当;然而,接受免疫抑制治疗的患者蛋白尿和肌酐更高( = 0.09 和 = 0.07)。在中位随访 5.0(1.9-9.0)年后,其余 7 名(6%)患者发展为系统性红斑狼疮。
结论
我们的数据支持红斑狼疮和非狼疮性满堂肾病是两种不同的临床实体,具有可比的结局。一小部分患者在随访期间发展为系统性红斑狼疮。非狼疮性满堂肾病在文献中有许多不同的名称。三种发病机制类别的确定为该疾病的管理提供了进一步的线索。
Zotero 插件