Arterial Hypertension Clinical Trial
Official title:
Effects of Linagliptin on Endothelial- , Renal-, and Retinal Function in Comparison to Placebo in Patients With Hypertension and Albuminuria
A recent study with the DPP-IV inhibitor Linagliptin showed an improvement in the urinary
albumin creatinine ratio in patients with diabetic nephropathy. Gutzwiller et. Al. have
shown that GLP-1 increases renal Na secretion and inhibits renal H secretion, further
indicating some direct renal effects of GLP-1.
Therefore, it seems likely that treatment with the DPP-IV inhibitor Linagliptin evolves
several beneficial effects on microvascular and endothelial function beyond glucose control
which most probably have an impact on the progression of renal and retinal microvascular
disease.
The objective of this trial is to investigate the effect of Linagliptin in comparison to
placebo on the UACR in patients with high blood pressure and an increased albumin excretion.
Numerous, equivalent endothelial, renal, and retinal parameters serve as objectives of the
study. All study parameters will be handled in an exploratory sense for the generation of
models to further discuss the role of DPP-IV inhibition on renal and retinal physiology.
Renal tissue damage and an increase in the albumin excretion rate is a strong predictor for
the development and progression of endothelial dysfunction and the development of
microvascular and/or macrovascular complications. Increased blood pressure as well as
increased glucose levels were found to impair renal- and retinal function, and a close
association in the incidence and progression rate of retinopathy and nephropathy could be
observed. Endothelial dysfunction and alterations in microvascular blood flow are early
pathogenetic features in the development of renal and retinal tissue damage as found in
patients with arterial hypertension and / or diabetes mellitus. A couple of studies have
shown that urinary albumin excretion is associated with morphological and functional
alterations in retinal microvascular blood flow. In patients with arterial hypertension
blood pressure lowering treatment were shown to decrease the albumin excretion rate and to
improve endothelial function of the retinal vasculature.
Recently DPP-IV Inhibitors have been introduced in the treatment of type 2 diabetes
mellitus. Beside the metabolic effects of this drug class, several pleiotropic effects
beyond metabolic control were documented in numerous studies, and are the topic of ongoing
clinical research. Treatment with DPP-IV inhibitors was found to improve myocardial and
endothelial function, to improve blood lipids, to lower blood pressure and to improve
markers of renal function. GLP-1 receptors in vessels, kidney and the heart might account
for those glucose independent effects of GLP-1. However, it is also conceivable that DPP-IV
inhibition might exert vascular effects independent from GLP-1. In vitro studies
demonstrated that DPP-IV is expressed in endothelial cells, and the inhibition of DPP-IV
reduced the microvascular tone through direct mediation of the nitric oxide system.
Therefore, it seems conceivable that the glucose independent effects of DPP-IV inhibition
might be mediated through GLP-1 receptor signaling and /or direct inhibition of the enzyme
DPP-IV in vascular, renal, or retinal cells.
A recent study with the DPP-IV inhibitor Linagliptin showed an improvement in the urinary
albumin creatinine ratio in patients with diabetic nephropathy. Gutzwiller et. Al. have
shown that GLP-1 increases renal Na secretion and inhibits renal H secretion, further
indicating some direct renal effects of GLP-1.
Therefore, it seems likely that treatment with the DPP-IV inhibitor Linagliptin evolves
several beneficial effects on microvascular and endothelial function beyond glucose control
which most probably have an impact on the progression of renal and retinal microvascular
disease.
The objective of this trial is to investigate the effect of Linagliptin in comparison to
placebo on the UACR in patients with high blood pressure and an increased albumin excretion.
Numerous, equivalent endothelial, renal, and retinal parameters serve as objectives of the
study. All study parameters will be handled in an exploratory sense for the generation of
models to further discuss the role of DPP-IV inhibition on renal and retinal physiology.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Outcomes Assessor)
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