Kidney Disease Clinical Trial
Official title:
Biological Collection in Nephrology for the Study of the Links Between Kidney Disease, Immunity System and Cardiovascular Complications
The NephoMIC project is a biological collection in patients of Nephrology, allowing the study
of the links between kidney diseases, Immunity system and Cardiovascular complications.
Its aim is to allow the development of a translational research on the theme of "Systemic
Nephrology", which concerns both renal complications of autoimmune and inflammatory diseases,
and systemic complications of patients with kidney disease, linked to both a state of
immunosuppression and an increased risk of cardiovascular complications.
It is based on the proximity between the Clinical investigation Center (CIC) of the hospital,
where the samples are received, techniqued and preserved, and the Center of Nephrology and
Renal Transplantation of the hospital.
The collection includes blood samples (whole blood, serum, plasma, total blood RNA, PBMC
cells), and urine samples (fresh urine).
Participation in the collection is particularly recommended for patients who require a
medical renal biopsy in the Nephrology Department. Other well-phenotyped patients
(well-defined renal disease diagnosis) may also participate in NephroMIC.
Kidney damage to systemic lupus erythematosus (SLE), anti-cytoplasmic neutrophil cytoplasmic
(ANCA) vasculitis or systemic amyloidosis, expose patients to:
- a risk of renal insufficiency, which depends on the severity of the attack, the delay in
the initiation of treatment, and the possible occurrence of relapses, which may leave
fibrous sequelae and lead to the development of insufficiency chronic renal disease
(CKD)
- a risk of immunosuppression and infectious complications, linked to the renal
insufficiency itself or to the toxicity of immunosuppressive treatments aimed at
controlling renal disease
- an increased risk of cardiovascular complications, linked on the one hand to the
activity of the systemic disease and to the endothelial dysfunction it may entail, and
on the other hand to the cardiovascular risk associated with the IRC .
Systemic lupus erythematosus (SLE) is a chronic autoimmune disease, evolving in relapses
interrupted by periods of remission. Renal impairment of SLE is common (20-30% of patients in
Europe) [1] and severe [2], with an impact on patient survival [3] and a risk of progression
to chronic renal insufficiency (IRC). Thus, nearly 40% of patients with severe form develop
IRC [4], and 5-10% have terminal IRC at 10 years [5,6]. The classification of renal
involvement according to the International Society of Nephrology / Renal Pathology Society
(ISN / RPS) [7] distinguishes active proliferative forms, requiring immunosuppressive therapy
[8], nonproliferative or purely chronic forms. However, renal biopsy remains an invasive
procedure [9], which can hardly be repeatedly performed, let alone pre-emptively, although
the onset of tissue damage precedes the emergence of clinically detectable proteinuria [10] .
In addition, the response of proliferative lupus nephropathy to immunosuppressive therapy is
difficult to predict. The progression in treatment is favorable in 70 to 80% of patients with
proliferative form, but 20-30% are refractory to the standard treatment, while others retain
important chronic lesions leading to chronic renal insufficiency.
There is therefore a crucial need for non-invasive biomarkers to identify lupus patients at
risk for developing renal disease and to predict the severity of histological involvement and
response to immunosuppressive therapy.
The investigators believe that the pathophysiological complexity of lupus nephropathy can not
be summarized to a single biomarker, and that a global "omic" approach could capture this
complexity or identify new pathways.
The blood transcriptome study is a non-invasive and usable approach in clinical research,
which allowed 10 years ago to identify the signature of lupus interferon (IFN) [11], which
had not been detected in serum of patients, and led to new therapeutic pathways. The
complexity and size of pan-genomic transcriptomic data may be an obstacle to their analysis
and interpretation [12]. Using a modular approach to reduce the size of transcriptomic blood
glucose data and facilitate their interpretation, the investigators were able to show the
gradation of the interferon signature during lupus [13], and describe the link between
neutrophil modular signature and renal impairment of lupus [14].
In addition, the search for noninvasive urinary biomarkers to avoid or limit biopsy
indications in the NL, or to predict the response to IS treatment to early adapt the
intensity, is of great interest. The current PeptiduLUP study is being conducted to determine
the diagnostic and prognostic value of urinary peptidoma analysis during lupus nephropathy.
The study of the urinary peptidome could make it possible to refine the indications of renal
biopsy in the renal involvement of the lupus.
In addition, there is an increased cardiovascular risk in patients with chronic renal failure
(CKD). Our team has demonstrated that the uremic toxins that accumulate in the IRC patients
are agonists of the AhR transmission factor and induce endothelial dysfunction with
development of a pro-thrombotic [15] and pro-inflammatory phenotype [16] ]. During lupus or
vasculitis at ANCA, the risk of cardiovascular complications increases as renal function
deteriorates [17,18], while in parallel the risk of immunological outbreak of the disease
decreases [19,18]. , 20]. The investigators believe that activation of AhR by uremic toxins
may be involved both in increasing the cardiovascular risk of these patients and in
inhibiting the autoimmune response.
There is therefore a strong rationale for studying the links between kidney disease, immunity
and cardiovascular complications.
The expected results are the identification of new blood (transcriptomic) and urinary
(peptidomic) biomarkers for diagnostic and prognostic purposes during renal disease.
NephroMIC will also provide research fellowships on biomarkers during renal disease,
especially during systemic diseases with renal involvement. The NephroMIC collection will
also allow participation in collaborative Nephrology research projects.
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