Immune Dysfunction Clinical Trial
Official title:
Observational Study on T Regulatory Cells in Hemodialysis Patients
In this observational study, the investigators evaluated the Treg number and function in a
population of patients undergoing hemodialysis (HD).
In particular, the investigators considered the relationship of Treg cell status with the
different HD modalities and clinical parameters.
Patients on hemodialysis (HD) present an elevated risk of cardiovascular disease, cancer and
infectious events that may lead to the high morbidity and mortality rate characteristic of
this population. Many causes can explain this increased risk, including inflammation that,
in turn, might be secondary to dialysis-specific factors, such as contaminated water,
dialysis modality and dialysis membranes used for treatment.
In addition to chronic inflammatory, in HD patients is also present a significant alteration
of the immune system resulting in chronic lymphocytic infiltration, alteration of T-helper
balance (Th1/Th2) etc. The immune response is controlled by very complex mechanisms; it is
mediated by interaction between antigen-presenting cells (APC), CD4+ T helper (Th) and T
cells CD4+ CD25+ regulatory (Treg), a cell subpopulation of T CD4+ expressing the IL-2
receptor (CD25) and forkhead factor (foxp 3). Treg cells contribute to the maintenance of
peripheral tolerance by suppressing the immune response to self-normal or tumor antigens.
Treg cells control population's expansion of peripheral cells and suppress the proliferation
of Th activated cells. Accessory molecules such as CTLA-4 receptors, CD28 and IL-2 cytokines
and IL-6, contribute to the activation and proliferation of Treg cells.
The characterization by flow cytometry of Treg suffered for a lack of specific surface
markers. These cells are generally identified on the basis of contemporary expression of
molecules CD4 and CD25, but the specificity of these markers is limited, given that the CD25
is also expressed on activated lymphocytes. Recently it has been showed that the expression
of Foxp3 gene is a phenomenon strictly linked to the development of regulatory activity of
Treg, and so, the extent of the expression of this gene by Real Time PCR is currently
considered the most specific Treg marker. There is very poor data on Treg cells function in
HD. A recent study shows that in patients on chronic HD, the number of Treg is lower if
compared to healthy subjects. Moreover, the Treg cells of patients on HD would present a
significant impairment of their function, assessed as the ability to inhibit lymphocyte
proliferation.
Those results, however, are affected by the lack of data on the characteristics of the
studied patients and the type of dialysis treatment applied. In contrast, a recent study by
our group showed that patients on hemodialysis with poor biocompatible membranes have a
greater number of circulating Treg compared with healthy controls matched for age and sex.
Given the absence of other data, it still remains to investigate the actual significance and
function of Treg in HD, considering that Treg status might potentially affect the immune
response.
Therefore, the purpose of this study was to evaluate the structure and function of Treg
cells in patients undergoing HD, also considering their relationship with the different HD
modalities and clinical parameters.
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Observational Model: Cohort, Time Perspective: Prospective
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