IgA nephropathy (IgAN) is the most common primary glomerulonephritis in the world and it represents an important cause of end-stage kidney failure. This disease was described as a distinct entity in 1968 by J Berger and N Hinglais. The aetiology and the pathogenesis remain still obscure. Clinical observations and immunisation studies indicate that IgAN represents a dysregulation of the immune system, rather than an intrinsic renal abnormality. Twenty years ago, some authors proposed the mucosa-bone marrow axis to explain the pathogenesis of the disease. Mucosal IgA plasmocytes are displaced and take up residence in systemic sites. The unusual characteristics featured by the IgA produced by these cells (charge, size, glycosylation) drive their accumulation, deposition and mesangial activation characteristic of IgAN. Evidence is emerging that altered lymphocyte homing may ultimately explain this aberrant localization.
Study Type
INTERVENTIONAL
Allocation
NA
Masking
NONE
Enrollment
72
University Hospital, Limoges
Limoges, France
The Primary Outcome Measure of this study is the level of expression of the molecules of intestinal localization.
Time frame: 30 minutes
The secondary outcome measure is the level of expression of the homing molecules in lymphocytes B IgA memory
Time frame: 30 minutes
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