Type 2 Diabetes Clinical Trial
Official title:
The Production of Reactive Oxygen Species in Response to Glutathione Supplementation and Acute Exercise in Patients With Type 2 Diabetes
Objectives: The research focus of the study is the production of reactive oxygen species
(ROS) in patients with type 2 diabetes (T2D) in response to glutathione (GSH) supplementation
and in response to acute exercise.
Oxidative stress is suggested as a possible causative factor in the pathophysiology of
skeletal muscle insulin resistance. GSH is the most abundant endogenous antioxidant in the
cell and thus, a crucial protector against oxidative stress and insulin resistance. It has
been found that patients with T2D have a decreased level of GSH in plasma and that 1 h GSH
infusion improves skeletal muscle glucose uptake by ~25% and the redox environment in
patients with T2D. Therefore, we want to investigate the effect of 3 months of GSH
supplementation on skeletal muscle insulin sensitivity and mitochondrial ROS production in
patients with T2D and healthy controls.
Hypothesis: Oral GSH supplementation will improve skeletal muscle insulin sensitivity in
patients with T2D and this effect will be linked to a reduced mitochondrial ROS production in
the skeletal muscle.
In contrast to the link between oxidative stress and insulin resistance, ROS produced in
response to exercise is an important physiological stimulus as it is suggested to play a key
role in the beneficial mitochondrial biogenesis observed in response to training. It has been
reported that some patients with T2D have a diminished mitochondrial biogenesis in response
to training, but the reason for this defect is not known. We want to investigate the link
between exercise-stimulated ROS production and the mitochondrial biogenesis response in
patients with T2D and healthy controls in response to acute exercise at two different
intensities.
Hypothesis: Considering the pathological condition of T2D skeletal muscle (i.e. high chronic
ROS level), we speculate that a lower exercise intensity, leading to a lower
exercise-stimulated ROS production is a more optimal stimulus (i.e. not to high) for
mitochondrial biogenesis in patients with T2D.
ROS production in response to glutathione supplementation:
Today, 387 million people worldwide suffer from T2D and this number is expected to increase
to 592 million in 2035. Skeletal muscle is responsible for ~75% of the total glucose uptake,
making skeletal muscle the quantitatively most important tissue when it comes to insulin
resistance (1). It has been suggested that oxidative stress may represent a possible
causative factor in the pathophysiology of skeletal muscle insulin resistance. The link
between ROS and skeletal muscle insulin resistance has been established both in vitro and in
vivo (2, 3), but few studies have actually measured ROS production in skeletal muscle of T2D
patients (4-6). Mitochondria are a source of ROS, and also a major target of oxidative damage
(7). The mitochondrial defense system against oxidative stress relies on endogenous
antioxidants. Glutathione (GSH) is the most abundant endogenous antioxidant in the cell and
thus, a crucial protector against oxidative stress and insulin resistance (8). Supporting
this, patients with T2D have a decreased level of GSH and an increased level of oxidized GSH
(GSSG) in plasma (9) and insulin resistant subjects are reported to have an increased
mitochondrial ROS production as well as a reduced GSH/GSSG ratio in skeletal muscle compared
to healthy controls (3). In addition, 1 h glutathione infusion has been found to increase
glucose uptake in patients with T2D by ~25% and to improve the redox environment, as
reflected by an increased GSH/GSSG ratio in plasma; effects that were not seen in the healthy
controls (10). The effect of prolonged oral GSH supplementation on skeletal muscle insulin
sensitivity and mitochondrial ROS production in patients with T2D has, to our knowledge,
never been investigated.
Research questions 1: Does oral GSH supplementation improve skeletal muscle insulin
sensitivity in patients with T2D and healthy controls? And if so, can this effect be linked
to a more beneficial redox state in the muscle cell? Hypothesis: Oral GSH supplementation
will improve skeletal muscle insulin sensitivity in patients with T2D and this effect will be
linked to a reduced mitochondrial ROS production in the skeletal muscle.
ROS production in response to acute exercise:
Acute exercise induces a marked increase in the transcription of peroxisome
proliferator-activated receptor-γ coactivator-1α (PGC-1α) (11), and therefore, PGC-1α is
believed to play a key role in training-induced mitochondrial biogenesis (12). Contraction of
rat skeletal muscle cells increases ROS production and PGC-1α mRNA expression, but in the
presence of antioxidants, ROS production is reduced and the increase in PGC-1α mRNA is
abolished (13). Also, exercise combined with allopurinol (an inhibitor of ROS production)
severely attenuates the magnitude of the exercise-induced increased PGC-1α mRNA in rats,
compared to exercise alone (14). These findings suggest that PGC-1α, at least in part, is
regulated through a mechanism that involves ROS. Furthermore, it has been suggested that ROS
regulates PGC-1α via activation of AMP-activated protein kinase (AMPK) (15). Interestingly,
subjects with insulin resistance have a decreased exercise-stimulated AMPK activity, compared
to lean controls (16, 17), which might explain the attenuated training-induced mitochondrial
biogenesis observed in some patients with T2D (5, 17, 18), but not all (19). Whether ROS
production is implicated in an abnormal training response is not known. Our current knowledge
of ROS in response to acute exercise is derived from studies in animals and cells, and no
study has, to our knowledge, investigated the link between ROS and mitochondrial biogenesis
in patients with T2D in response to acute exercise.
Research questions 2: Does the exercise-induced increased ROS production required for a
mitochondrial biogenesis response differ between patients with T2D and healthy controls? If
so, does low intensity exercise reduce the transient ROS production and thus, result in a
higher mitochondrial biogenesis response in patients with T2D, compared to exercise at high
intensity? Hypothesis: Considering the pathological condition of T2D skeletal muscle (i.e.
high chronic ROS level), it is hypothesized that a lower exercise intensity, leading to a
lower exercise-stimulated ROS production is a more optimal stimulus (i.e. not to high) for
mitochondrial biogenesis in patients with T2D.
Material and methodology:
20 patients with T2D (non-insulin dependent) and 20 healthy controls will be recruited to the
study. The two groups will be matched on age, weight and maximal oxygen consumption (VO2
max).
Approach for the study: The study is a double blinded randomized placebo controlled trial.
At each attendance to the laboratory (except for the day of screening), the subjects are
asked to:
- Report to the laboratory in an overnight fasted state
- Abstain from alcohol and physical activity 24 hours prior to each study day.
- Repeat the same diet as the enclosed 24-hour recall questionnaire prescribes (the
subjects are also asked to complete a 24-hour dietary recall questionnaire on their
first attendance to the laboratory)
Screening: Before the subjects are included in the study, a standard clinical examination
will be conducted, including medical history, glycated hemoglobin (HbA1c) and ECG.
If included in the study, the subjects undergoes 3 experimental days before and after the
intervention.
Test day 1:
- Dual Energy X-ray Absorptiometry-scan to measure body composition,
- Incremental exercise test to determine the exercise intensity that elicits maximal fat
oxidation (Fatmax test)
- Incremental exercise test to exhaustion to determine VO2 max.
Test day 2:
- Muscle biopsies from vastus lateralis (basal, immediately after exercise cessation and
after 90 min of recovery)
- Acute exercise tests on bicycle ergometers at 70% of VO2 max (moderate intensity) or at
50% of VO2 max (low intensity). The two exercise tests will be matched for total amount
of work (kJ).
10 subjects with T2D and 10 control subjects are randomized to each exercise test.
Test day 3:
- Measurement of resting metabolic rate by canopy hood (basal and during the clamp)
- Intravenous glucose tolerance test
- Hyperinsulinaemic euglycaemic clamp
After the experimental days, the subjects are randomized into placebo or GSH supplementation
and instructed to consume either 1000 mg GSH/day or placebo daily (2 tablets in the morning
and 2 tablets in the evening) for 4 weeks.
Statistical considerations:
The comparison of the groups or the interventions will be performed using a one-way or a
two-way ANOVA test with repeated measures, as appropriate. Based on the variation shown in
previous studies an expected 80% power and a significance level of P<0.05, power calculations
have shown that 12 subjects in each group is sufficient in regards to mitochondrial
functionality measurements and insulin sensitivity. Data from a previous study investigating
GSH in healthy subjects indicates that 15 subjects are needed in order to find a difference
in this parameter (3).
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