Do Foxp3+ Regulatory T Cells (Treg Cells) Play a Role in the Immunopathogenesis of Primary/Idiopathic Minimal Change Disease?

Author:

Hue Susan Swee-Shan1,Suhail Sufi Muhammad2,Choo Jason Chon Jun2,Yusof Nurhashikin3ORCID,Loh Alwin Hwai-Liang4,Salcido-Ochoa Francisco3ORCID

Affiliation:

1. Tregs and HLA Research Force and Department of Pathology, Singapore General Hospital, The Academia, 20 College Road, Singapore 169856

2. Renal Medicine Department, Singapore General Hospital, The Academia, 20 College Road, Singapore 169856

3. Tregs and HLA Research Force and Renal Medicine Department, Singapore General Hospital, The Academia, Level 3, 20 College Road, Singapore 169856

4. Department of Pathology, Singapore General Hospital, The Academia, 20 College Road, Singapore 169856

Abstract

Minimal change disease constitutes a major cause of nephrotic syndrome. It is regarded as a non-immune-complex mediated primary glomerulopathy and pathogenetically is characterised by podocyte injury and effacement of foot processes; therefore, it is also classified as a type of podocytopathy. T cell dysfunction with increased levels of a soluble glomerular permeability factor has been proposed to play a major role in the pathogenesis of minimal change disease. It has been therefore suggested that a dysfunction of regulatory T cells, the orchestrators of immune homeostasis, could be implicated in perpetuating T cell activation in this condition. However, the actual contribution of regulatory T cell dysfunction in the immunopathogenesis of primary minimal change disease is still largely unclear. We here propose a theoretical model based on the available evidence.

Publisher

Hindawi Limited

Subject

General Earth and Planetary Sciences,General Environmental Science

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