A Review of Focal Segmental Glomerulosclerosis Classification With a Focus on Genetic Associations

IF 3.2 Q1 UROLOGY & NEPHROLOGY
Marco Bonilla , Orhan Efe , Haresh Selvaskandan , Edgar V. Lerma , Nasim Wiegley
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Abstract

Focal segmental glomerulosclerosis (FSGS) defines a distinct histologic pattern observed in kidney tissue that is linked to several distinct underlying causes, all converging on the common factor of podocyte injury. It presents a considerable challenge in terms of classification because of its varied underlying causes and the limited correlation between histopathology and clinical outcomes. Critically, precise nomenclature is key to describe and delineate the pathogenesis, subsequently guiding the selection of suitable and precision therapies. A proposed pathomechanism-based approach has been suggested for FSGS classification. This approach differentiates among primary, secondary, genetic, and undetermined causes, aiming to provide clarity. Genetic FSGS from monogenic mutations can emerge during childhood or adulthood, and it is advisable to conduct genetic testing in cases in which there is a family history of chronic kidney disease, nephrotic syndrome, or resistance to treatment. Genome-wide association studies have identified several genetic risk variants, such as those in apolipoprotein L1 (APOL1), that play a role in the development of FSGS. Currently, no specific treatments have been approved to treat genetic FSGS; however, interventions targeting underlying cofactor deficiencies have shown potential in some cases. Furthermore, encouraging results have emerged from a phase 2 trial investigating inaxaplin, a novel small molecule APOL1 channel inhibitor, in APOL1-associated FSGS.

病灶节段性肾小球硬化症分类综述,聚焦遗传相关性
局灶节段性肾小球硬化症(FSGS)是肾脏组织中观察到的一种独特的组织学模式,它与几种不同的潜在病因有关,所有这些病因都与荚膜细胞损伤这一共同因素有关。由于其潜在病因多种多样,而且组织病理学与临床结果之间的相关性有限,因此在分类方面面临着相当大的挑战。至关重要的是,精确的命名是描述和划分发病机制的关键,从而指导选择合适的精准疗法。有人提出了一种基于病理机制的 FSGS 分类方法。这种方法区分了原发性、继发性、遗传性和未确定病因,旨在提供清晰的分类。单基因突变引起的遗传性 FSGS 可在儿童期或成年期出现,如果有慢性肾病、肾病综合征或耐药性家族史,建议进行基因检测。全基因组关联研究发现了几种遗传风险变异,如载脂蛋白 L1(APOL1)中的变异,这些变异在 FSGS 的发病中起着一定的作用。目前,治疗遗传性 FSGS 的特定疗法尚未获得批准;不过,针对潜在辅因子缺陷的干预措施已在某些病例中显示出潜力。此外,一项研究新型小分子 APOL1 通道抑制剂 inaxaplin 治疗 APOL1 相关性 FSGS 的 2 期试验也取得了令人鼓舞的结果。
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来源期刊
Kidney Medicine
Kidney Medicine Medicine-Internal Medicine
CiteScore
4.80
自引率
5.10%
发文量
176
审稿时长
12 weeks
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