Focal and segmental glomerulosclerosis induced in mice lacking decay-accelerating factor in T cells
Lihua Bao, … , Stuart J. Shankland, Richard J. Quigg
Lihua Bao, … , Stuart J. Shankland, Richard J. Quigg
Published April 1, 2009
Citation Information: J Clin Invest. 2009;119(5):1264-1274. https://doi.org/10.1172/JCI36000.
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Research Article Nephrology

Focal and segmental glomerulosclerosis induced in mice lacking decay-accelerating factor in T cells

Abstract

Heritable and acquired diseases of podocytes can result in focal and segmental glomerulosclerosis (FSGS). We modeled FSGS by passively transferring mouse podocyte–specific sheep Abs into BALB/c mice. BALB/c mice deficient in the key complement regulator, decay-accelerating factor (DAF), but not WT or CD59-deficient BALB/c mice developed histological and ultrastructural features of FSGS, marked albuminuria, periglomerular monocytic and T cell inflammation, and enhanced T cell reactivity to sheep IgG. All of these findings, which are characteristic of FSGS, were substantially reduced by depleting CD4+ T cells from Daf–/– mice. Furthermore, WT kidneys transplanted into Daf–/– recipients and kidneys of DAF-sufficient but T cell–deficient Balb/cnu/nu mice reconstituted with Daf–/– T cells developed FSGS. In contrast, DAF-deficient kidneys in WT hosts and Balb/cnu/nu mice reconstituted with DAF-sufficient T cells did not develop FSGS. Thus, we have described what we believe to be a novel mouse model of FSGS attributable to DAF-deficient T cell immune responses. These findings add to growing evidence that complement-derived signals shape T cell responses, since T cells that recognize sheep Abs bound to podocytes can lead to cellular injury and development of FSGS.

Authors

Lihua Bao, Mark Haas, Jeffrey Pippin, Ying Wang, Takashi Miwa, Anthony Chang, Andrew W. Minto, Miglena Petkova, Guilin Qiao, Wen-Chao Song, Charles E. Alpers, Jian Zhang, Stuart J. Shankland, Richard J. Quigg

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Figure 2

Immunological events induced by anti-podo Abs in DAF-deficient mice.

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Immunological events induced by anti-podo Abs in DAF-deficient mice. (A)...
(A) In the kidneys of all mice, there was little neutrophil (brown) or B cell (purple) infiltration, while in DAF-deficient mice, there was marked infiltration with Thy-1.2+ T cells (brown) and F4/80+ monocytic cells (purple). Original magnification, ×400. (B) Flow cytometric analysis of cells isolated from kidneys of DAF-deficient mice 30 days after anti-podo Ab administration showing relative proportions of F4/80+ and CD3+ cells (left panel). The majority of F4/80+ cells were also CD11c+ (right panel). Numbers shown are the percentage of total cells in individual quadrants. (C) Splenic CD4+ cells from WT and DAF-deficient mice were assessed for CD62L (upper panels) and CD44 expression (lower panels) at baseline (d0) and 10 (d10) and 20 days (d20) after passive administration of anti-podo IgG. The CD62Llo and CD44hi populations are denoted by horizontal lines.