Diabetes Mellitus, Type 1 Clinical Trial
Official title:
Studies on the Adaptive Responses (Cardiovascular, Respiratory and Angiogenetic) to Hypoxia in Patients With Type 1 Diabetes Compared to Controls
The general aim of this study is to define the response to hypoxic challenge in patients
with diabetes. The investigation will provide response for different questions that are
central for explaining the development of complications in diabetes
- have patients with diabetes an impaired reaction to adapt to hypoxia
- what consequence has hypoxia challenge on respiratory and on cardiovascular regulation
in patients with diabetes
- what consequence has diabetes on the angiogenetic response to hypoxia
Complications of diabetes represent the main concern for modern diabetes therapy, and it has
become a priority to further characterise the pathophysiological mechanisms of these
complications to ensure the development of novel rational therapeutic strategies.
Although the prolonged exposure of tissues to hyperglycaemia is the primary causative factor
for chronic diabetes complications, it has recently become increasingly evident that hypoxia
also plays an important role in all diabetes complications . A low tissue concentration of
oxygen in diabetes is the consequence of several mechanisms (e.g., deficient blood supply
because of micro- and macro-vascular disease , poor local oxygen diffusion because of local
oedema, or as the result of increased oxygen consumption).
Adaptive responses of cells to hypoxia are mediated by Hypoxia-Inducible Factor 1 (HIF),
which is a heterodimeric transcription factor that is composed of and subunits, which are
both constitutively expressed in mammalian cells. The regulation of HIF activity is
critically dependent on subunit degradation in normoxia. Under hypoxic conditions, HIF-1 is
stabilised, binds to HRE (hypoxic responsive elements) and up-regulates a gene series that
is involved in angiogenesis, glycolytic energy metabolism, cell proliferation, and survival,
which enables cells to adapt to reduced oxygen availability. It is estimated that that more
than 800 genes are direct HIF targets . HIF-1 is central for expression of multiple
angiogenic growth factors (reviewed by[6]), endothelial progenitor cells (EPC) recruitment .
Recently, it has been proposed that microRNAs (ex. mir210) also mediate some HIF-1 functions
.
Several pieces of evidence point to a defective response of diabetic tissues to hypoxia. An
impaired hypoxia response is present in all tissues investigated in diabetic animal and
diabetic patients. Hyperglycaemia directly represses HIF stability and function at multiple
levels, a mechanism that is not completely understood.
An impaired reaction to hypoxia in diabetes might have important consequences in acute
hypoxic challenges as acute heart infarction, stroke, limb ischemia but also in subtle
regulation of cardiovascular and respiratory system as a consequence of autonomic neuropathy
with potential severe prognostic effect on late cardiovascular events . Interventional
studies have addressed the cardiovascular responses to intermittent hypoxia (IH) compared
with normoxia exposure in patients with diabetes . However in order to establish the
appropriateness of the cardiovascular reaction to hypoxia in diabetes it is a need to
investigate the cardiorespiratory responses towards IH in patients with diabetes compared
with matched non diabetic control subjects. Moreover it is essentially to establish the
angiogenetic response in the same experimental design. The hypothesis for this study is that
both the cardiorespiratory reaction mediated through autonomic nervous system and
angiogenetic response are impaired in patients with diabetes as a consequence of an impaired
HIF reaction as seen in other tissues .
The investigators plan to study the effect of intermittent hypoxia (IH) that will consists
of five hypoxic periods (13% O2 inspired fraction of oxygen) each lasting 6 min, with five
normoxic intervals of same duration in 15 patients with type 1 diabetes without clinical
signs of neuropathy and in 15 non diabetic controls matched for sex, BMI, age. The study
will be performed during one day.
Methods:
Baseline data will be obtained in the morning of each testing day at least 2 h after
breakfast. Subjects are advised to abstain from caffeinated beverages for 12 h and from
alcohol for 36 h prior to testing.
Blood pressure and heart rate and arterial oxygen saturation will be continuously measured.
In case of a decrease in oxygen saturation 80% or the occurrence of symptoms, hypoxia would
have been discontinued until oxygen levels reached at least 80%. A technician will regulate
and control the breathing periods under supervision of a medical doctor in a way that the
intervention could not be observed by any patient. Thereafter, three measurement sessions
will be performed: immediately after (t2), after 3 h (t3), and after 6 h (t4). After t2,
each patient will obtaine an individual meal according to diet requirement.
Cardiovascular and respiratory testing.
Hypoxic ventilatory response (HVR) and hypercapnic ventilatory response (HCVR) will be
evaluated to determine respiratory system activity. All patients will be tested in the
supine position in a silent room at comfortable temperature. Before participants will be
connected to a rebreathing circuit through a mouthpiece with an antibacterial filter,
spontaneous breathing of room air at rest will be performed for4 min in order to obtain
baseline data.
During each condition, the investigators will perform continuous measurement of oxygen
saturation (SaO2) by a pulse oximeter and end-tidal CO2 (CO2-et) using a capnograph
connected to a mouthpiece. Recordings of electrocardiogram will be performed by chest leads,
and continuous noninvasive blood pressure will be recorded using the cuff method. A heated
Fleish pneumotachograph will be connected to a differential pressure transducer and inserted
in series to the expiratory component of the rebreathing system to measure airway flow. For
measurement of the response to hypoxia, the participants will be connected to a rebreathing
circuit inducing progressive decrease in SaO2 while maintaining CO2-et values at constant
levels, until SaO2 will reach 80%, and measuring breath-to-breath changes in minute
ventilation. The response to hypercapnia will be evaluated by ventilatory changes induced by
progressive increase in CO2-et levels (up to 13 mmHg above resting levels), while SaO2 will
be maintained 98% by oxygen at very low flow.
Cardiovascular autonomic function will be determined performing four tests according to
recent guidelines: deep-breathing, 30:15 ratio, Valsalva maneuver and systolic blood
pressure response to standing. Cardiovascular autonomic neuropathy will be defined as the
"presence of two or more abnormal tests".
Measurement of chemoreflex sensitivity: The slope of the linear regression line of minute
ventilation versus SaO2 or CO2-et indicates in each case the chemoreflex sensitivity to
hypoxia or hypercapnia. In the hypercapnic test, the point at which the ventilation start to
increase indicates as ventilator recruitment threshold to CO2 (VRT- CO2). VRT- CO2 will be
identified by interpolating the ventilation/CO2-et plot by a fourth-order polynomial
function.
Assessment of baroreflex sensitivity: The baroreflex sensitivity (BRS) will be measured
during spontaneous breathing at each measurement session. Since previous studies did not
document a better performance of one method over the others, the investigators will
calculate the average of seven different methods: positive and negative sequences, the
a-coefficient in the low- and high-frequency bands and its average, the transfer function
technique, and the ratio of SDs of R-R interval and systolic blood pressure variabilities.
Besides BRS, SD of the R-R interval (SDNN) will be applied to determine a global index of
heart rate variability. This selection is done based on the fact that normal distribution is
more pronounced in this variable compared with other indices of variability (e.g.,
variance). The Hypoxic ventilatory response (HVR) and hypercapnic ventilatory response
(HCVR), baroreflex sensitivity (BRS) will be evaluated before (t1), immediately after (t2),
3 h (t3), and 6 h (t4) after IH.
The angiogenetic potential will be evaluated at the same endpoints by measuring in serum
relevant cytokines that are gene targets for HIF-1 (i.e. VEGFA, SDF-1a, erythropoietin etc).
The direct response of HIF signaling will be evaluated by the serum levels of mir210 which
exclusively regulated by HIF.
The absolute endothelial precoursor cell account (EPC) response will be evaluated at the
same time points by FACS analysis of the number of CD34+/CD133+/KDR +
;
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