Diagnosing and Treating IgAN: Steroids, Budesonide, or Maybe Both?

Overview

Journal Diagnostics (Basel)

Specialty Radiology

Date 2024 Mar 13

PMID 38472984

Authors

Christodoulos Keskinis

Eleni Moysidou

Michalis Christodoulou

Panagiotis Pateinakis

Maria Stangou

Affiliations

Soon will be listed here.

Abstract

IgA nephropathy (IgAN), the most common primary glomerulonephritis worldwide, is characterized by a mesangial IgA deposit and a variety of histological lesions, as described by the Oxford classification system. Despite the well-described "four-hit hypothesis", there are still plenty of less or undescribed mechanisms that participate in the disease pathogenesis, such as B-cell priming, which seems to be initiated by different antigens in the intestinal microbiota. Diagnosis of the disease is currently based on kidney biopsy findings, as the sensitivity and specificity of the many serum and urinary biomarkers described so far do not seem to have diagnostic accuracy. Therapeutic strategies consist of the initial step of non-immune medication, aiming to reduce both the intraglomerular pressure and proteinuria to below 0.5 g/day, followed by systemic corticosteroid administration in patients who remain at high risk for progressive chronic kidney disease despite the maximum non-immune treatment. The 6-month systemic corticosteroid treatment reduces proteinuria levels; however, the increased possibility of adverse events and increased relapse rate after treatment raises the need for a new therapeutic approach. Targeted-release budesonide is a therapeutic modality that aims to inhibit disease pathogenetic pathways at early stages; it has minor systemic absorption and proven beneficial effects on renal function and proteinuria. In the present systemic review, the benefits and adverse events of steroids and budesonide are described, and the possibility of combined treatment is questioned in selected cases with active histologic lesions.

Citing Articles

Factors influencing early response of IgA nephropathy following targeted-release budesonide (TRB) treatment: preliminary results from a multicenter study.

Keskinis C, Moysidou E, Kapsia E, Vaios V, Bintas C, Trivyza M Clin Kidney J. 2025; 18(1):sfae364.

PMID: 39967795 PMC: 11833314. DOI: 10.1093/ckj/sfae364.

Post-transplant IgA nephropathy: a rapidly evolving field of kidney transplant medicine.

Kanbay M, Ozbek L, Guldan M, Copur S, Barratt J J Nephrol. 2024; .

PMID: 39565563 DOI: 10.1007/s40620-024-02149-6.

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