Effects of 8-Week Vitamin E (α Tocopherol) Supplementation on
Reduced Insulin Resistance in Non-diabetic Obese Subjects
Erlina Marfianti
1
a
, Isnatin Miladiyah
2
b
1
Internal Medicine Department, Faculty of Medicine, Universitas Islam Indonesia, Sleman Yogyakarta, Indonesia
2
Pharmacology Department, Faculty of Medicine, Islamic Universitas Islam Indonesia, Sleman Yogyakarta, Indonesia
Keywords: Vitamin E, Obesity, Non-Diabetic, Insulin Resistance
Abstract: Obesity is a risk factor for diabetes mellitus (DM) and coronary heart disease. In obesity, oxidative stress and
adipokine hormone increase, leading to insulin resistance (IR) which can develop into DM. Vitamin E is an
antioxidant that is expected to lower IR. This study aims to determine the effects of 8-week supplementation
of vitamin E on reducing IR in non-diabetic obese subjects. The design was PROBE (Prospective Randomized
Open Blinded End-point). The subjects were ≥18 years old with ≥25 kg/m
2
body mass index and HOMA-IR
value >2.7 The exclusion criteria were DM patients and those taking metformin or antioxidants. Twenty
subjects in group A received 800 IU Vitamin E supplementation while 20 subjects in group B received
placebo, both for 8 weeks. Reduced IR was measured from the decreasing HOMA-IR value after 8 weeks.
The difference in decreasing HOMA-IR value between both groups was analyzed using independent t-test.
The mean in group A was 0.199 ± 0.336, while group B had - 0.078 ± 0.271. The between both groups was
statistically significant, with p = 0.004, 95% CI (0.096-0.457. Supplementation of 800 UI Vitamin E for 8
weeks could decrease IR in obese non-diabetic subjects.
1 INTRODUCTION
The prevalence of obesity has increased rapidly due
to lifestyle and diet changes, making it a global
problem in developed and developing countries.
Obesity is a complex, multifactorial, and mostly
preventable disease. The population with obesity and
overweight problems currently reaches more than a
third of the world's population. If secular trends
continue, it is estimated that 38% of the world's adult
population will be overweight, and another 20% will
be obese by 2030 (Chooi et al., 2019). Obesity
represents a significant health challenge because it
substantially increases the risk of diseases, such as
type-2 diabetes mellitus, fatty liver disease, and
cardiovascular disease, thereby contributing to a
decline in quality of life and life expectancy
(González-Muniesa et al., 2017). The risk of type-2
diabetes mellitus will increase significantly and
progressively in line with the increase in body mass
index and the duration of obesity (Cederberg &
Laakso, 2014).
a
https://orcid.org/0000-0001-8473-2820
b
https://orcid.org/0000-0003-1630-7130
World Health Organization (WHO) defines
overweight as BMI (body mass index) of 23-24.9
kg/m
2
and obesity as BMI of ≥25 kg/m
2
in the Asia-
Pacific population
(Purnamasari et al., 2014). In
obesity, oxidative stress and adipokines increase, and
they are responsible for the incidence of insulin
resistance (Hurrle & Hsu, 2017). A previous study
found that the prevalence of insulin resistance in
obese people was 59.6%. Insulin resistance, a process
of decreasing insulin sensitivity, is determined using
HOMA-IR (Homeostatic Model Assessment of
Insulin Resistance) values of >2.7. Insulin resistance
is a metabolic disorder with a negative impact of
underlying diabetes mellitus and cardiovascular
disorders (Reynolds & He, 2005). In obese people, an
increase in non-esterified fatty acids, glycerol,
adipokine hormones, cytokines, pro-inflammatory
markers, and other substances are associated with
insulin resistance.
Epidemiological, clinical, and animal studies have
reported the role of oxidative stress in the
pathogenesis of obesity and its associated related
104
Marfianti, E. and Miladiyah, I.
Effects of 8-Week Vitamin E ( Tocopherol) Supplementation on Reduced Insulin Resistance in Non-diabetic Obese Subjects.
DOI: 10.5220/0010488501040108
In Proceedings of the 1st Jenderal Soedirman International Medical Conference in conjunction with the 5th Annual Scientific Meeting (Temilnas) Consortium of Biomedical Science Indonesia
(JIMC 2020), pages 104-108
ISBN: 978-989-758-499-2
Copyright
c
2021 by SCITEPRESS – Science and Technology Publications, Lda. All rights reserved
conditions, including insulin resistance. Obesity can
also induce systemic oxidative stress through
multiple biochemical mechanisms, such as
superoxide generation from NADPH oxidases
(NOX), oxidative phosphorylation, glyceraldehyde
auto-oxidation, and protein kinase C (PKC) activation
(Savini et al., 2013). Other factors contributing to
oxidative stress due to obesity include increased free
fatty acid, hyperleptinemia,
tissue dysfunction,
low
antioxidant defence, and chronic inflammation
(Serra
et al., 2013). In obesity, free fatty acids that enter the
target organs are stored as triglycerides or used as a
substrate for the oxidation of mitochondrial cells to
produce ROS (Reactive Oxygen Species). Reactive
Oxygen Species causes oxidative stress which has the
potential to damage cellular functions. To prevent
these damaging effects, the cells create a complex
antioxidant system to eliminate ROS (Serra et al.,
2013). In obese people, however, antioxidants'
concentration decreases, causing an imbalance in
ROS production and antioxidants that prevent
oxidative stress (Manna & Jain, 2015). Deficiencies
in vitamins and minerals can also contribute to the
development of an impaired antioxidant defence in
obesity. Increased BMI is found to be correlated with
lower levels of carotenoids, vitamin C, and vitamin
E. In obesity, oxidative stress is thought to be one of
the factors causing insulin resistance and developing
diabetes mellitus (McMurray et al., 2016).
Vitamin E is a major fat-soluble component in the
cell's antioxidant defence system and is obtained
exclusively from food. It has many essential roles in
the metabolic system due to its antioxidant activity.
Vitamin E is also a potent chain-breaking antioxidant
that inhibits molecules of reactive oxygen species'
production when fat is oxidized
(Rizvi et al., 2014).
Such antioxidant is known to have the effect of
preventing free radicals that can adversely affect and
damage cells (Han, 2016)
Previous studies of vitamin E's effects to reduce
insulin resistance have been controversial as the
results were inconsistent. A study by Manning et al.
(2004) showed that the effects of high doses of
vitamin E are associated with decreased insulin
resistance and several inflammatory parameters,
including FFA, in the overweight population
(Manning et al., 2004). Another study by Balbi et al.
(2018) found that Vitamin E correlates with a
significant reduction in blood glucose and glycated
hemoglobin compared to placebo in Type-2 DM
patients (Balbi et al., 2018). A previous study
indicated that the combination of vitamins C, E, and
β-carotene during an 8-week supplementation
moderately reduces HOMA-IR values in overweight
young adults. Oxidative stress also decreases and may
become a potential mechanism underlying such
favorable changes in cardiovascular disease and
precursors of diabetes
(Vincent et al., 2009). Several
studies, however, do not support the role of vitamin E
in improving insulin sensitivity. An animal study
found that vitamin E supplementation in obese
rodents does not improve insulin sensitivity but
changes mitochondrial biogenesis and mitochondrial
protein expression (Picklo & Thyfault, 2015). Since
vitamin E's role in insulin resistance remains unclear,
this study aims to determine the effects of vitamin E
on reduced insulin resistance in the obese population
without diabetes mellitus.
2 MATERIAL AND METHODS
2.1 Research Design
This study was conducted with a clinical trial design
of prospective randomized open and blinded endpoint
evaluation (PROBE). In PROBE, the researcher
knows the patients' medication but not the patients'
final evaluation (laboratory results).
2.2 Subjects and Methods
Forty subjects aged 18-65 with a BMI of ≥25 kg/m2
and HOMA-IR of >2.7 (insulin resistance) were
recruited from community populations using an open
recruitment method. The exclusion criteria were
diabetes mellitus patients and candidates using
metformin or TZD drugs and antioxidant
supplements during the last one month. The
independent variable was the vitamin E therapy, and
the dependent variable was HOMA-IR. The required
number of subjects was calculated using the formula
for unpaired numerical analytic research (Dahlan,
2010).
The subjects received a clinical examination,
and the anthropometric, health, and lifestyle
information was collected. The participants agreed
and signed informed consent, and they were
randomized into two groups, namely group A that
received 800 IU Vitamin E supplementation, and
group B, that received placebo.
The subjects were instructed to take vitamin E
and placebo with meals. Vitamin E at a dose of 800
IU was given twice a day in a capsule form containing
Vitamin E (alpha-tocopherol) maleate. The placebo
used was a capsule containing flour with a shape
similar to a capsule containing Vitamin E and also
given twice a day. The supplementation was carried
Effects of 8-Week Vitamin E ( Tocopherol) Supplementation on Reduced Insulin Resistance in Non-diabetic Obese Subjects
105
out for 8 weeks, and HOMA-IR was measured before
and after 8 weeks of 800 IU Vitamin E
supplementation or placebo. The participants were
instructed not to make lifestyle changes during the
study. In the course of the supplementation, the
participants reported their conditions and complaints
to the researcher.
2.3 Blood Sampling
Fasting blood samples were collected using a catheter
from an antecubital vein into heparinized vacutainer
tubes before and after supplementation. The blood
samples were then analyzed for glucose, insulin,
cholesterol, and triglycerides of pre-supplementation
and glucose and insulin of post-supplementation. All
of the samples were batched within each subject and
run in the same assay. The homeostasis model
assessment (HOMA) was calculated from the fasting
glucose (G
0
) and insulin (I
0
) concentrations using the
following formula: (G
0
X I
0
)/ 22.5.
2.4 Statistics
All of the data were expressed in mean ± standard
error (SE) and analyzed using a Statistical Package
for Social Sciences. The differences in the mean
reduced HOMA-IR values (insulin resistance
reduction) after 8 weeks of treatment in the two
groups were analyzed using the independent t-test
with a significance level of p <0.05. and a 95%
confidence level.
2.5 Ethical Consideration
This study kept the confidentiality of the patients and
performed all procedures according to the study
ethics. The research approval was obtained from the
ethical review committee of Faculty of Medicine
Universitas Islam Indonesia for biomedical studies
involving human subjects and written informed
consent was taken from the subjects.
3 RESULTS
Forty subjects who met the inclusion and exclusion
criteria were randomized into two groups: twenty
subjects in group A (Vitamin E) and 20 subjects in
group B (placebo). The subjects consisted of 17 men
and 23 women. Table 1 shows the baseline
characteristics of the 40 subjects in this study. No
significant differences existed in the variables of age,
weight, BMI, systolic blood pressure, diastolic blood
pressure, fasting glucose levels, fasting insulin levels,
HOMA-IR, and cholesterol levels between the two
groups at the baseline.
Table 2 shows the HOMA-IR levels before and
after supplementation in the two groups. HOMA IR-
values after the supplementation of 800 IU vitamin E
for 8 weeks decreased significantly (p = 0.04).
Meanwhile, Group B had increased HOMA-IR after
receiving the placebo, although it was not significant
with p = 0.08. A decrease in HOMA-IR values
indicates insulin resistance reduction. Table 3 shows
the mean HOMA-IR reduction differences after 800
IU vitamin E and placebo supplementation for 8
weeks between the two groups.
Table 3 indicates a significant difference in the
decreased HOMA-IR values between group A
receiving vitamin E supplementation and group B
receiving placebo. In Group B, the HOMA-IR value
increased as opposed to the baseline. This significant
difference in decreased HOMA-IR values indicates
that Vitamin E supplementation can lower insulin
resistance than placebo.
4 DISCUSSION
Oxidative stress has been implicated in the
development of insulin resistance, and in some
studies, antioxidant therapy has proved to reduce
ROS and improve glycemic control in people with
type-2 diabetes. Besides, antioxidant concentrations
significantly decrease in individuals with obesity
(Manning et al., 2004)
,.
Table 2: HOMA-IR Levels before and after Supplementation Vitamin E and Placebo
Variable
Group A (Vitamin E) Group B (Plasebo)
Before Afte
r
p
* Before Afte
r
p
*
HOMA IR
3.070±0.630
2.871±0.430
0,04
3.081±0.856
3.158±0.534
0,08
* anal
y
sis of differences in the mean levels before and after thera
py
usin
g
p
aired t-test
JIMC 2020 - 1’s t Jenderal Soedirman International Medical Conference (JIMC) in conjunction with the Annual Scientific Meeting
(Temilnas) Consortium of Biomedical Science Indonesia (KIBI )
106
However, it remains unknown whether
antioxidant therapy improves insulin sensitivity in
non-diabetic obese individuals. Our results suggest
that 800 IU vitamin E supplementation for 8 weeks
can reduce insulin resistance condition in obese
people in conjunction with decreased HOMA-IR.
This study is in line with some findings of
previous studies. Research by Manning et al. (2004)
showed the effects of high doses of vitamin E on
reducing insulin resistance and several inflammatory
parameters, including FFA in the overweight
population. The reduced insulin resistance after the
administration of high doses of vitamin E has an 18%
difference from placebo treatment. A meta-analysis
study by Balbi et al. (2018) indicated that Vitamin E
is associated with a significant decrease in blood
glucose as well as glycated hemoglobin compared to
placebo. Supplementation of vitamin E can be a
valuable strategy for controlling diabetes
complications and enhancing antioxidant capacity.
Supplementation of vitamin E in obesity and type-
2 diabetes mellitus can significantly impact the
parameters of antioxidant status and glycemic
control, which may positively benefit patients. The
beneficial effects of vitamin E can be explained by
the reduced damaging effects of free radicals on the
structural and functional components of cells and
vessel walls. Type-2 diabetes mellitus patients have a
high risk of experiencing microvascular and
macrovascular complications, and daily vitamin E
supplementation provides an alternative strategy for
metabolic control, in addition to the combination of
diet, exercise, and medication (Balbi et al., 2018).
A previous study also showed that a combination
of vitamins C, E, and β-carotene during an 8-week
supplementation period moderately reduces HOMA-
IR values in overweight young adults (Vincent et al.,
2009). In animal subjects studies, vitamin E
supplementation can improve adipose tissue
expansion through a reduction in the fibrotic process.
This improvement, in turn, reduces steatosis and
inflammation, thereby restoring insulin sensitivity.
The mechanism may involve, although not
exclusively, vitamin E antioxidant activity, thus
reducing ROS-mediated collagen deposition and
inflammation (Alcalá et al., 2015). A review by
Wong et al. (2017) summarized the findings in animal
and human studies of the effects of vitamin E and
articulated the contrasting potential of vitamin E in
preventing the medical conditions associated with
obesity and metabolic syndrome. It suggests that
vitamin E may be a promising agent for attenuating
obesity and metabolic syndrome (Wong et al., 2017).
These previous studies support our findings that
vitamin E has a potential mechanism in vitamin E-
induced metabolic improvement, including insulin
resistance reduction in obesity.
However, some previous research had different
results, such as a study by Picklo et al. (2015) which
showed that vitamin E and vitamin C
supplementation in obese rodents do not modify
exercise-induced insulin sensitivity improvement.
Changes in mitochondrial biogenesis and
mitochondrial protein expression may be modified by
antioxidant supplementation (Picklo & Thyfault,
2015). A study of obese adolescents by Hendarto et
al. (2019) found that vitamin E supplementation at a
dose of 400 IU/day for two months does not
significantly affect lipid profiles and adiponectin
levels (Hendarto et al., 2019).
This study has limitations in terms of a limited
number of subjects and design. In addition, the
confounding factors that could affect the level of
HOMA-IR in the study samples were not fully
controlled, thereby suggesting the importance of
performing a study with a larger number of samples
and a better study design. We strongly recommend
that further well-designed, large-scale, long-term,
head-to-head controlled trials and meta-analyses be
carried out to demonstrate the effects of vitamin E
supplementation on non-diabetes mellitus obesity.
Further studies should also be conducted to
strengthen this evidence, especially for defining the
appropriate doses and regimen of vitamin E and
supporting its use in daily practice.
5 CONCLUSION
The supplementation of 800 UI Vitamin E for 8
weeks can reduce insulin resistance in obese people
without diabetes mellitus. This finding may represent
a step forward in disease management.
ACKNOWLEDGEMENTS
We want to thank the Faculty of Medicine, the
Islamic University of Indonesia for supporting this
research.
Table 3:Mean levels of reduction in plasma HOMA-
IR after supplementation
Group A
(
Vitamin E
)
Group B
(
Plasebo
)
p*
HOMA IR 3.070±0.630 2.871±0.430 0,04
*analysis using independent t test
Effects of 8-Week Vitamin E ( Tocopherol) Supplementation on Reduced Insulin Resistance in Non-diabetic Obese Subjects
107
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