Bellur Shubha S, Troyanov Stéphan, Vorobyeva Olga, Coppo Rosanna, Roberts Ian S D
William Osler Health Systems Brampton & Queen's University, Kingston, Ontario, Canada.
Hôpital du Sacré-Coeur de Montréal, University of Montreal, Montreal, Quebec, Canada.
Kidney Int. 2024 Jun;105(6):1279-1290. doi: 10.1016/j.kint.2024.03.011. Epub 2024 Mar 28.
Evidence from the Oxford IgA nephropathy (IgAN) cohort supports the clinical value of subclassifying focal segmental glomerulosclerosis lesions (S1). Using the larger Validation in IgA (VALIGA) study cohort, we investigated the association between podocytopathic changes and higher proteinuria, kidney outcome and response to immunosuppressive therapy. All biopsies were evaluated for glomeruli with segmental capillary occlusion by matrix ("not otherwise specified", NOS lesion), simple capsular adhesion without capillary occlusion (Adh), tip lesions, and podocyte hypertrophy (PH). S1 required a NOS lesion and/or Adh. A Chi-Squared Automatic Interaction Detection method was used to identify subgroups of FSGS lesions associated with distinctive proteinuria at biopsy. We assessed survival from a combined event (kidney failure or 50% decline in estimated glomerular filtration rate). Finally, we evaluated within each subgroup if immunosuppression was associated with a favorable outcome using propensity analysis. In 1147 patients, S1 was found in 70% of biopsies. Subclassification found NOS lesions in 44%, Adh in 59%, PH in 13%, and tip lesions in 3%, with much overlap. Four subgroups were identified with progressively higher proteinuria: from lowest, S1 without NOS, S1 with NOS but without Adh/PH, to highest, S1 with NOS and Adh but without PH, and S1 with NOS and PH. These four subgroups showed progressively worse kidney survival. Immunosuppression was associated with a better outcome only in the two highest proteinuria subgroups. Propensity analysis in these two groups, adjusted for clinical and pathological findings, found a significantly reduced time-dependent hazard of combined outcome with corticosteroids. Podocyte hypertrophy and glomeruli with simple adhesions appeared to reflect active lesions associated with a response to corticosteroids, while other S1 lesions defined chronicity. Thus, our findings support subclassifying S1 lesions in IgAN.
来自牛津IgA肾病(IgAN)队列的证据支持对局灶节段性肾小球硬化病变(S1)进行亚分类的临床价值。利用规模更大的IgA验证(VALIGA)研究队列,我们调查了足细胞病变改变与更高蛋白尿、肾脏结局及免疫抑制治疗反应之间的关联。对所有活检标本评估有基质导致的节段性毛细血管闭塞的肾小球(“未另作说明”,NOS病变)、无毛细血管闭塞的单纯包膜粘连(Adh)、顶端病变和足细胞肥大(PH)。S1需要存在NOS病变和/或Adh。采用卡方自动相互作用检测方法来识别活检时与独特蛋白尿相关的FSGS病变亚组。我们评估了联合事件(肾衰竭或估计肾小球滤过率下降50%)的生存率。最后,我们在每个亚组内使用倾向分析评估免疫抑制是否与良好结局相关。在1147例患者中,70%的活检标本发现有S1。亚分类发现44%有NOS病变,59%有Adh,13%有PH,3%有顶端病变,存在大量重叠。识别出四个亚组,蛋白尿逐渐升高:从最低的无NOS的S1、有NOS但无Adh/PH的S1,到最高的有NOS和Adh但无PH的S1以及有NOS和PH的S1。这四个亚组的肾脏生存率逐渐变差。仅在蛋白尿最高的两个亚组中,免疫抑制与更好的结局相关。对这两组进行倾向分析,校正临床和病理结果后,发现使用皮质类固醇可显著降低联合结局的时间依赖性风险。足细胞肥大和有单纯粘连的肾小球似乎反映了与对皮质类固醇反应相关的活动性病变,而其他S1病变则定义为慢性病变。因此,我们的研究结果支持对IgAN中的S1病变进行亚分类。
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