Diabetes Mellitus Clinical Trial
Official title:
Bone Marrow Responsiveness to Pharmacologic Mobilization of Progenitor Cells in Diabetic Versus Non-diabetic Patients
Diabetes mellitus is associated with a significant reduction of circulating progenitor cells
(CPCs). These include endothelial progenitor cells (EPCs), which are involved in
cardiovascular homeostasis and repair. A reduction of CPCs in metabolic patients is
associated with an increased risk of future adverse cardiovascular outcomes. Therefore, ways
to active stimulate an increase of CPC levels in diabetes are actively pursued.
Experimental animal studies and preliminary data in humans indicate that a bone marrow
defect is causally related to the low CPC level in diabetes.
Our previous data in rats indicate that diabetes reduces the bone marrow responsiveness to
granulocyte colony-stimulating factor (G-CSF) in terms of progenitor cell mobilization.
In the present study, we aim at investigating bone marrow responsiveness to pharmacological
mobilization of CPC in diabetic patients as compared to non-diabetic subjects.
Diabetes mellitus is associated with a significant reduction of circulating progenitor cells
(CPCs). CPCs are defined by the surface expression of the stem cell antigen CD34 and or
CD133. These cells include endothelial progenitor cells (EPCs), which are involved in
cardiovascular homeostasis and repair. EPCs are characterized by the co-expression of
endothelial antigen(s), such as KDR.
A reduction of CPCs in metabolic patients is associated with an increased risk of future
adverse cardiovascular outcomes, such as myocardial infarction, stroke, revascularization,
etc. Therefore, ways to active stimulate an increase of CPC levels in diabetes are actively
pursued. Indeed, there are several drugs that stimulate CPCs or EPCs, but it is not fully
clear if they are active also in diabetic patients.
The mechanisms that account for CPC reduction in diabetes include defective bone marrow
mobilization, reduced survival and increased homing outside the bloodstream. Experimental
animal studies and preliminary data in humans indicate that a bone marrow defect is causally
related to the low CPC level in diabetes.
Our previous data in rats indicate that diabetes reduces the bone marrow responsiveness to
G-CSF in terms of c-kit+/Sca-1+ progenitor cell mobilization.
There is also some experimental evidence in type 2 diabetic rats that a specific form of
autonomic neuropathy impairs bone marrow mobilization of progenitor cells.
In the present study, we aim at investigating bone marrow responsiveness to pharmacological
mobilization of CPC in diabetic patients as compared to non-diabetic subjects.
Diabetic subjects and control subjects will be administered with a single dose of
granulocyte colony stimulating factor (G-CSF) and progenitor cells will be quantified before
and 24 hours after G-CSF administration. Progenitor cells will be analyzed by flow cytometry
on the basis of the expression of CD34, CD133 and KDR.
Mean percentage variation of CPCs and EPCs will be compared in diabetic versus non diabetic
patients to understand whether or not diabetes is associated with a significant defective
mobilization of progenitor cells.
As a secondary aim, diabetic patients will be divided in those with and without diabetic
autonomic neuropathy (DAN) to understand if DAN modulates bone marrow responsiveness to
G-CSF.
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Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Diagnostic
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