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Med. J. Cairo Univ., Vol. 81, No. 1, December: 1053-1065, 2013
www.medicaljournalofcairouniversity.net
Effect of Vitamin D Supplementation and/or Physical Training on
Cigarette Smoke Induced COPD in Rats
NASHWA ELTABLAWY, M.D.; SAMAH ELATTAR, M.D. and ZIENAB ABDEL WAHAB, M.D.
The Department of Physiology, Faculty of Medicine, Cairo University
Abstract
Background: Chronic obstructive pulmonary disease (COPD) is a major health problem with increasing morbidity
and mortality. Vitamin D deficiency has been established as exceedingly prevalent in many of chronic lung disease popu-lations and exercise training in COPD patients results in
positive effects in dyspnea and exercise tolerance.
Aim of Work: The purpose of the present study was to investigate the effect of vitamin D supplementation and/or physical training on pulmonary functions, lung inflammation,
antimicrobial production and matrix degradation in a rat model of COPD.
Methodology: Forty male Albino rats were used in this study and divided into 5 groups, 8 rats each: Group1: Control
group, Group 2: (COPD group): COPD rats maintained un-treated for the experimental period, Group 3: (Vit. D+COPD):
COPD rats were treated with vitamin D injection 1, 25 (OH)
D3 was administered intraperitoneally (i.p.) at dose 0.5 µg/kg of body weight (BW), 3 times a week for 8 weeks, Group 4:
(COPD+ Exercise): COPD rats performed daily exercise
program and group 5: (COPD+Vit D+exercise) COPD rats
treated with vitamin D injection (i.p.) at a dose of 0.5 µ g/kg, 3 times a week for 8 weeks and performed daily exercise
program. After 8 weeks of treatment, pulmonary functions were tested and blood samples were withdrawn for measuring vitamin D and Ca2+ levels and the lung tissues were excised to measure interleukin 12 (IL12), tumor necrosis factor alpha
(TNF alpha), metalloproteinase-9 (MMP-9) and cathelicidin.
Results: Peak expiratory flow (PEF), forced vital capacity (FVC), vitamin D and Ca2+ were significantly reduced in COPD rats after 12 weeks of exposure to cigarette smoke.
Vitamin D supplementation and swimming training for 8 weeks improved PEF, FVC, vitamin D and Ca2+ significantly as compared to untreated COPD. Combined vitamin D treat-ment and physical training significantly improved FVC level as compared with each treatment separately. The improvement
was associated with significant reduction in inflammatory markers and MMP-9 as compared to COPD untreated rats.
The antimicrobial cathelicidin was significantly increased in
COPD rats and was further increased on vitamin D treatment
but not with exercise training.
Correspondence to: Dr. Nashwa Eltablawy, The Department of Physiology, Faculty of Medicine, Cairo University E-mail: [email protected]
Conclusion: Our results showed that COPD is an inflam-matory disease and it is associated with vitamin D deficiency. Vitamin D supplement or rehabilitation by physical training
each separately improved the pulmonary functions, reduced
inflammation, and attenuate lung parenchymal degradation.
Vitamin D in addition induced an antimicrobial protection,
however vitamin D supplement had a slightly better effects
as compared with exercise training. Combination of both vitamin D supplementation and exercise training had a syner-gistic effect and produced a significant improvement as
compared to each therapy separately. We can conclude that
vitamin D supplement has a beneficial effects as a therapy in cases of COPD and it is better added to rehabilitation training
programs for better results.
Key Words: COPD – Vitamin D – Physical training – Cathe-licidin.
Introduction
CHRONIC obstructive pulmonary disease (COPD) is a major health problem with increasing morbidity
and mortality; in 2020, COPD will be the 3 rd
leading cause of mortality worldwide and the 5 th
leading source in terms of burden of disease [1] . COPD is characterized by persistent airflow limi-tation that is usually progressive and associated
with an enhanced chronic inflammatory response in the airways and the lung to noxious particles or
gases. Exacerbations and comorbidities contribute to the overall severity in individual patients [2-4] .
Exposure to cigarette smoke is known to sig-nificantly increase the risk for the development of COPD [5,6] . The exact pathogenesis has yet to be discovered; however, numerous cellular elements
have demonstrated involvement in the pathophys-iology of COPD. These include macrophages, neutrophils and cytokines such as interleukin (IL)- 4, IL-5 and IL-13, along with interferon-gamma
[6-8] .
The alveolar wall destruction and loss of elastic
recoil that occur in COPD are believed to be the
1053
1054 Effect of Vitamin D Supplementation and/or Physical Training
result of chronic inflammation and imbalance of
antioxidants [7,9] . This oxidative stress causes a protease/antiprotease imbalance and is believed to be a contributing factor toward the pathogenesis
of COPD [9] .
Vitamin D is a steroid hormone that is synthe-sized in the epidermal keratinocytes under influence
of UV-B light (290-315nm) or acquired in the diet. Dietary sources include supplemented dairy prod-ucts, fish oil, fish liver and eggs. It is estimated
that approximately 3 percent of the human genome
is regulated directly or indirectly by the vitamin D endocrine system [10,11] .
Recent research has revealed new sites of action
that may force the re-examination of vitamin D and its role in human physiology. Vitamin D recep-tors (VDRs) have been found in organs not typically
believed to be involved with bone metabolism, including the pancreas, gonads, liver, heart, brain
and breast, as well as the hematopoietic and im-mune systems [10] .
Vitamin D deficiency has been established as exceedingly prevalent in many of chronic lung
disease populations [12] . COPD patients without any glucocorticoid use had significantly decreased
25-hydroxyvitamin D levels when compared with age-matched controls [13] . Children with a diagnosis of wheezy bronchitis had more than two-and-a-half times the incidence of rickets than the age-matched controls. Also it was noted a 10 times
higher incidence of wheezy bronchitis when severe rickets was present [14] . Limited studies [15,16] in patients with chronic lung disease suggest that
bone mineral density is correlated with lung func-tion, whereas another study [17] was unable to confirm this.
Recent studies have shown that vitamin D has
pleiotropic protective effects [18,19] . 1,25 (OH)2D3 (1,25-dihydroxyvitamin D 3), an active metabolite of vitamin D is also a potent regulator of the
immune response in Th1 cell-directed diseases
[20,21] . Sunder and colleagues [22] have recently shown that VDR deficiency invokes lung inflam-mation and alterations in lung function. Hence,
understanding the molecular mechanisms of dietary vitamin D for the treatment of lung disease and
their exacerbations are an emerging area of research
[23] .
Skeletal muscle dysfunction is common in patients with advanced COPD and it contributes
importantly to limiting their functional capacity
and quality of life [24] . The role of exercise training in pulmonary rehabilitation of patients with severe
COPD has been studied [25] . Exercise training in
COPD patients results in positive effects in dyspnea
and exercise tolerance [25,26] , however, the mech-anisms by which exercise affect the pulmonary
functions in COPD have not been determined.
Aim of work: Accordingly, the purpose of the present study was to investigate the effect of vita-min D supplementation and/or physical training on pulmonary functions (peak expiratory flow rates
(PEF) and forced vital capacity (FVC) in a rat
model of COPD induced by 3 months exposure to
cigarette smoke. The effect of vitamin D supple-mentation and physical training on vitamin D level
and calcaemic state, lung inflammation as deter-mined by lung expression of TNF-α and IL-12 was measured. The effect of vitamin D and physical
training on the antimicrobial protein cathelicidin
and tissue breakdown as indicated by measuring lung metalloproteinase 9 (MMP-9) was also inves-tigated.
Material and Methods
Experimental animals and groups: Forty male Albino rats, weighing 100-120g,
were used in this study. This work was conducted in the Physiology department, Cairo University from May 2013 – October 2013. The rats were
kept under standard conditions. Placed in cages,
at 20±5° C, average humidity, and normal light/dark
cycles. Standard chow and water were available
ad libitum.
Rats were divided into 5 groups: Group 1: Control group (8 rats): These are
normal rats serving as control rats for the different
values measured in the other groups.
Remaining rats were exposed to passive ciga-rette smoke for 3 months in order to develop COPD
and then tested by pulmonary function tests to
examine the development of COPD.
32 male rats were daily exposed to the smoke
resulted from burning of 12-15 cigarettes. COPD
was induced by cigarette smoking exposure tech-nique: Cigarette smoke (CS) exposure was achieved by same procedure which had been used in a pre-vious study [27] with some modification in periods of exposure and number of cigarettes. Popular
Egyptian filter-tipped cigarette were used contain-ing (25mg) tar and (1.8mg) nicotine.
The exposure to the CS was initial progressive concerning the burned material mass and the ex-posure time in order to permit the biological adap-tation of the animals and to avoid accidents such
as smoke intoxication that could determine death
of rats.
Nashwa Eltablawy, et al. 1055
The cigarette smoke exposure lasts for 3 months.
The rats were randomly divided into 4 groups after
developing COPD:
Group 2: (COPD group): Eight rats were in-cluded in this group and maintained untreated for
the experiment period.
Group 3: (Vit.D+COPD): Eight COPD rats were treated with vitamin D injection1, 25(OH)
D3 was administered intraperitoneally (i.p.) at dose
0.5µg/kg BW, 3 times a week for 8 weeks [28] .
Group 4: (COPD+Exercise): Eight COPD rats performed daily exercise program.
The exercise protocol consisted of swimming exercise (1hr/day, 5 days/week) [29] for 8 weeks in a swimming tank filled with water at a temper-ature of 36ºc. Daily swimming period was divided into 2 sessions each formed of 30 minutes separated
by 1 hour rest. At the completion of each period
of swimming exercise, the rats were removed from
the water, carefully dried and returned to their cages. The exercised rats underwent a swimming
programme consisting of gradually increasing
periods of swimming in the first 4 days the duration of exercise was gradual increased from an initial
period of 15min to the maximum permissible per-iod of 30min.
Group 5: (COPD+Vit.D+Exercise) eight COPD
rats treated with vitamin D injection (i.p.) at dose
0.5µgm/kg, 3 times a week for 8 weeks and per-formed daily exercise program similar to the pro-tocol tried by group 4.
After 8 weeks, the animals were transferred to
National Research Centre, Cairo, Egypt where
pulmonary functions were assessed and blood samples were withdrawn by capillary tubes and
left to clot to get the serum for measurement of vitamin D and Ca2+. The animals were then sacri-ficed and their chests were opened and the lungs
were excised for measurement of IL12, TNF alpha,
cathelicidin and MMP-9.
Measurement of pulmonary function:
Rats were placed in a specific body plethysmo-graph made of plexi glass. Rats head protruded
through a neck collar made of a dental latex dam into a head exposure chamber that ends with a
flow head connected to spirometer (AD Instruments spirometer, ML 140) which is a precision differential pressure transducer for measuring respiratory vari-ables. It measures differential pressure across fine
gauze mounted in a flow head [30] .
Estimation of vitamin D and calcium:
Blood samples were withdrawn and left to clot for 20min then centrifuged at 12,000rpm for 1o
min then the separated serum was kept frozen at
-80c till analysis. Serum samples were examined for 25(OH) D levels by Enzyme-linked immun-osorbent assay (ELISA) by kit supplied by (Im-mundiagnostic USA) briefly, monoclonal antibody identify 25, OH vitamin D was used in the assay. The samples were incubated with the detection antibody after the extraction step. Then Peroxidase-conjugated antibody was then added into microplate well, forming a complex of 25-hydroxy vitamin D-detection antibody-peroxidase conjugate. Tet-ramethylbenzidine (TMB) was used as a substrate, the colour density developed is proportional to
vitamin d concentration. Finally, to terminate the
reaction stop solution was added and the microplate
were read by elisa reader at 520nm [31] . Serum calcium concentrations were measured by standard
laboratory methods.
Measurement of TNF- α and IL-12: TNF-α and IL-12 in lung tissues were measured
by using ELISA (quantikine R&D system USA) according to the manufacturer`s instructions [32,33] .
Detection of MMP-9 & cathelcidin gene ex-pression using real time:
PCR (RT-PCR):
RNA extraction:
Total RNA was isolated from lung tissue homo-genates using RNeasy Purification Reagent (Qiagen, Valencia, CA) according to manufacturer's instruction. The purity (A260/A280 ratio) and the concentration of RNA were obtained using spec-trophotometry (GeneQuant 1300, Uppsala, Swe-den). RNA quality was confirmed by gel electro-phoresis.
cDNA synthesis:
First-strand cDNA was synthesized from 4µg of total RNA using an Oligo (dT) 12-18 primer
and SuperscriptTM II RNase Reverse Transcriptase,
This mixture was incubated at 42 ° C for 1h, the kit was supplied by Super Script Choice System (Life
Technologies, Breda, the Netherlands).
Real-time quantitative polymerase chain reac-tion (PCR):
Real-time PCR (RT-PCR) amplification was
carried out using 10µL amplification mixtures containing Power SYBR Green PCR Master Mix (Applied Biosystems, Foster City, CA USA), equiv-
1056 Effect of Vitamin D Supplementation and/or Physical Training
Abstract
Background: Chronic obstructive pulmonary disease (COPD) is a major health problem with increasing morbidity
and mortality. Vitamin D deficiency has been established as exceedingly prevalent in many of chronic lung disease popu-lations and exercise training in COPD patients results in
positive effects in dyspnea and exercise tolerance.
Aim of Work: The purpose of the present study was to investigate the effect of vitamin D supplementation and/or
physical training on pulmonary functions, lung inflammation,
antimicrobial production and matrix degradation in a rat model
of COPD.
Methodology: Forty male Albino rats were used in this study and divided into 5 groups, 8 rats each: Group 1: Control
Primer sequences used for RT-PCR.
Primer Sequence
MMP-9
Cathelicidin
GAPDH
Forward:5’- CATTCGCGTGGATAAGGAGT -3´ Reverse:5´- ACCTGGTTCACCTCATGGTC -3´ according to gene bank
accession number NM-013599
Forward:5´AGGATTGTGACTTCAAGAAGGACG-3´ Reverse:5´GTTTATTTCTCAGAGCCCAGAAGC-3´. according to gene bank
accession number XM_005253678.1
Forward 5´ TGCTGGTGCTGAGTATGTCG 3´ Reverse 5´ TTGAGAGCAATGCCAGCC 3´ gene bank accession NM_017008
group, Group 2: (COPD group): COPD rats maintained un-treated for the experimental period, Group 3: (Vit. D+COPD):
COPD rats were treated with vitamin D injection 1, 25 (OH)
D3 was administered intraperitoneally (i.p.) at dose 0.5µg/kg of body weight (BW), 3 times a week for 8 weeks, Group 4:
(COPD+ Exercise): COPD rats performed daily exercise
program and group 5: (COPD+Vit D+exercise) COPD rats
treated with vitamin D injection (i.p.) at a dose of 0.5µg/kg, 3 times a week for 8 weeks and performed daily exercise
program. After 8 weeks of treatment, pulmonary functions were tested and blood samples were withdrawn for measuring vitamin D and Ca2+ levels and the lung tissues were excised to measure interleukin 12 (IL12), tumor necrosis factor alpha
(TNF alpha), metalloproteinase-9 (MMP-9) and cathelicidin.
Results: Peak expiratory flow (PEF), forced vital capacity (FVC), vitamin D and Ca2+ were significantly reduced in COPD rats after 12 weeks of exposure to cigarette smoke.
Vitamin D supplementation and swimming training for 8 weeks improved PEF, FVC, vitamin D and Ca2+ significantly
as compared to untreated COPD. Combined vitamin D treat-ment and physical training significantly improved FVC level as compared with each treatment separately. The improvement
was associated with significant reduction in inflammatory
markers and MMP-9 as compared to COPD untreated rats.
The antimicrobial cathelicidin was significantly increased in
COPD rats and was further increased on vitamin D treatment
but not with exercise training.
Conclusion: Our results showed that COPD is an inflam-matory disease and it is associated with vitamin D deficiency. Vitamin D supplement or rehabilitation by physical training
each separately improved the pulmonary functions, reduced
inflammation, and attenuate lung parenchymal degradation.
Vitamin D in addition induced an antimicrobial protection,
however vitamin D supplement had a slightly better effects
as compared with exercise training. Combination of both vitamin D supplementation and exercise training had a syner-gistic effect and produced a significant improvement as
compared to each therapy separately. We can conclude that
Table (1): Changes in pulmonary functions (PEF and FVC) in untreated COPD rats and in
COPD rats after 8 weeks of either vitamin D supplementation, exercise training
or both.
Control COPD COPD+ Vit D
COPD+ exercise
COPD+ vit D+exercise
PEF (mL/min) Mean±S.D. 13.65± 1.04a
6.78± 1.15b 10.36±0.87c
8.80±0.89d 10.45± 1.02c
FVC (mL) Mean±S.D. 9.24±0.78a
4.81±0.85b 7.90±0.54 c
6.21 ±0.56c 8.43±0.63 a
- (n=8). - Values are Mean±SD. - Values with different letters in the same row are significantly different from each other ( p<0.05). - Values with the same letters in the same row are insignificantly different from each other ( p>0.05).
c d
Copd+ vit d exercise
c
Copd+ vit d+
exercise
a
b
Control Copd Copd+
PE
F m
L/m
in
16.00
14.00
12.00
10.00
8.00
6.00
4.00
2.00
0.00 Control Copd Copd+
vit d Copd+
exercise Copd+ vit d+
exercise
a
b
c
c
a
FV
C =
mL
12.00
10.00
8.00
6.00
4.00
2.00
0.00
a
b
a a a
Control Copd Copd+ vit d
Copd+ exercise
Copd+ vit d+
exercise
0
70
60
50
40
30
20
10
Vit
D (
ng/m
l)
Control Copd Copd+
Copd+
Copd+ vit d
exercise vit d+ exercise
Ca2
+ (
mg/
di)
12
10
8
6
4
2
0
a
b
a ab a
Nashwa Eltablawy, et al. 1057
Fig. (1): Effects of vitamin D supplement and physical training
for 8 weeks on pulmonary function (PEF) in COPD rats (Mean±SD).
Effect of COPD, vitamin D supplementation,
and exercise training on vitamin D levels and serum Ca2+ level in rats:
As expected from previous researches the present results showed deficiency of vitamin D
and a hypocalcaemic state in rats with COPD and
Fig. (2): Effects of vitamin D supplement and physical training
for 8 weeks on pulmonary function (FVC) in COPD rats (Mean±SD).
the levels of vitamin D and Ca2+ were significantly reduced in COPD rats as compared to control rats.
It can be seen from Table (2) and Figs. (3,4) that
vitamin D supplementation and/or exercise correct-ed the deficiency and the values of these two parameters were back to normal control values.
Table (2): Effects of vitamin D supplement and physical training for 8 weeks on serum
levels of vitamin D and Ca2+ in COPD rats.
Control COPD COPD+ Vit D
COPD+ exercise
COPD+ vit D+exercise
Vit D (ng/ml) Mean±S.D. 52.25±8.65a
29.00±5.41 b 51.41±3.06a
53.95±5.92a 52.46±9.48a
Ca (mg/dl) Mean±S.D. 10.18±0.32a
7.40±0.57b 9.25±0.48a
8.48±0.82ab
9.75±0.43 a
- (n=8). - Values are mean±SD. - Values with different letters in the same row are significantly different from each other ( p<0.05). - Values with the same letters in the same row are insignificantly different from each other ( p>0.05).
Fig. (3): Effects of vitamin D supplement and physical training
for 8 weeks on serum level of vitamin D in COPD rats (Mean±SD).
Changes in inflammatory markers TNF alpha and IL12 in lung tissues in untreated COPD rats and in COPD rats after 8 weeks of either vitamin D supplementation, exercise training or both:
The results of the present work confirmed that
COPD is an inflammatory disease. As shown in
Fig. (4): Effects of vitamin D supplement and physical training
for 8 weeks on serum Ca2+ levels in COPD rats (Mean±SD).
Table (3) and Figs. (5,6), lung TNF alpha and IL12 were significantly increased in COPD rats as com-pared to control rats. Treatment with i.p. injection
of vitamin D, for 8 weeks reduced the inflammation
and the levels of the inflammatory markers were
significantly decreased as compared to the untreated
COPD rats. Physical training induced also an anti-
Control Copd Copd+
Copd+
Copd+ vit d
exercise vit d+ exercise
IL-1
2 (p
g/m
l)
160
140
120
100
80
60
40
20
0
a
b
c
d
e
Control Copd Copd+
Copd+
Copd+ vit d
exercise vit d+ exercise
TN
F-al
pha
(pg/
ml)
350
300
250
200
150
100
50
0
a
b
c d
e
1058 Effect of Vitamin D Supplementation and/or Physical Training
inflammatory effect and significantly reduced the
level of TNF alpha and IL 12 as compared to the untreated COPD rats but the reduction was signif-icantly less than that produced by vitamin D treat-
ment. Combined treatment with vitamin D and
physical training induced a further significant
decline in the levels of inflammatory markers as compared to each treatment alone.
Table (3): Effects of vitamin D supplement and physical training for 8weeks on lung inflammatory markers
(TNF alpha and IL10), matrix degradation (MMP-9) and antimicrobial (cathelidicine) in COPD
rats.
Control COPD COPD+ Vit D
COPD+ exercise
COPD+ vit D+exercise
IL-12 (pg/ml) Mean±S.D. 30.56±4.05a
113.66± 19.75b 56.93±7.03 c
86.86±5.09d 44.99±4.60e
TNF-alpha (pg/ml) Mean±S.D. 46.60±9.53 a
266.56±59.59b 133.24±8.96c
152.63 ± 17.78d 102.46±9.18 e
MMP-9 Mean±S.D. 1.35±0.32a 9.51± 1.85b 5.42±0.70c
6.62±0.35d 4.68±0.56e
Cathelicidin Mean±S.D. 0.14±0.03 a
0.3 8±0.06b 0.86±0.12c
0.39±0.13 b 0.84±0.10c
- (n=8). - Values are Mean±SD. - Values with different letters in the same row are significantly different from each other ( p<0.05). - Values with the same letters in the same row are insignificantly different from each other ( p>0.05).
Fig. (5): Effects of vitamin D supplement and physical training
for 8 weeks on lung inflammatory marker (IL12) in
COPD rats (Mean±SD).
Effect of COPD, vitamin D supplementation,
and exercise training on mRNA of lung matrix
(MMP-9): Table (3) and Fig. (7) show that in rats devel-
oped COPD there is enhanced degradation of lung
parenchyma as indicated by elevated level of MMP-9 in lung tissues. Treatment of COPD rats with vitamin D for 8 weeks or exercise significantly reduced destruction of lung tissue by attenuation
of MMP-9 production as compared to the untreated
rats. It can be observed that vitamin D supplemen-tation caused a more significant reduction in MMP-9 production than did exercise training. Combining both therapy together induced a better improvement
Fig. (6): Effects of vitamin D supplement and physical training
for 8 weeks on lung inflammatory marker (TNFalpha)
in COPD rats (Mean ±SD).
and a significant reduction in MMP-9 in lung tissues as compared to each therapy alone.
Effect of COPD, vitamin D supplementation,
and exercise training on mRNA of antimicrobial cathelicidin in lung tissue:
Table (2) and Fig. (8) showed that COPD was
associated with a significant increase in the level
of antimicrobial cathelicidin. Vitamin D supple-mentation for eight weeks alone or in combination
with exercise training induced a further significant
increase in its value. Exercise alone had no effect
on the lung level of cathelicidin as compared to
COPD untreated group.
a
b
c d
e
Control Copd Copd+ vit d
Copd+ exercise
Copd+ vit d+
exercise
0
12
10
8
6
4
2
MM
P-9
a
b
c c
b
Control Copd Copd+ vit d
Copd+ exercise
Copd+ vit d+
exercise
0
Cat
helic
idin
e
1.2
1
0.8
0.6
0.4
0.2
Nashwa Eltablawy, et al. 1059
Fig. (7): Effects of vitamin D supplement and physical training
for 8 weeks on M RNA of lung matrix degradation (MMP-9) in COPD rats (Mean ±SD.
Fig. (8): Effects of vitamin D supplement and physical training
for 8 weeks on mRNA of antimicrobial (cathelicidin) in COPD rats (Mean ±SD.).
Discussion
Chronic obstructive pulmonary disease (COPD) has been defined as a preventable and treatable
pathologic condition characterized by partially reversible airflow limitation [35] . It is well known that cigarette smoke is one of the most important
risk factors for COPD, and it can accelerate the
development of COPD in humans [36] . In this study, we found that exposure to cigarette smoke caused
COPD after 12 weeks in male albino rats; it pro-duced a significant reduction in pulmonary function
as detected by a significant decrease in mean values
of PEF and FVC as compared to control group.
Short term exposure to noxious gases as ciga-rette smoke (days) [37] resulted in a pulmonary inflammatory infiltrate, increased mucus produc-tion, and pulmonary edema. Long term induction protocols (weeks or months) [38] produced, in addition to the inflammatory infiltrate, emphysema
and pulmonary remodeling characterized by fibro-sis, and thickened bronchiole and arterial walls.
In the present study, we found that vitamin D was deficient in rats with COPD and that the dose
of vitamin D supplemented in our study was enough to raise the blood vitamin D level to be comparable with the control value. Exercise protocol performed in COPD rats also was able to significantly increase
vitamin D level as compared to COPD untreated
rats. In rats with COPD treated with both vitamin
D and exercise, there was a significant increase in
vitamin D levels as compared with the COPD untreated rats but the increase was insignificant
when compared with vitamin D or exercise treated rats.
There are several factors that could account for vitamin D deficiency in COPD patients: Poor diet,
a reduced capacity of aging skin for vitamin D synthesis, reduced outdoor activity and therefore
sun exposure, an increased catabolism by gluco-corticoids, impaired activation because of renal dysfunction, and a lower storage capacity in mus-cles or fat due to wasting [38] . Many steps of the vitamin D pathway (intake, synthesis, storage,
metabolism) can potentially be disturbed in COPD patients.
In agreement with our results, Forli et al., [12] found vitamin D deficiency (in their study defined
as below 20ng/ml) in more than 50% of a cohort
waiting for lung transplantation. In an outpatient
study on patients with COPD in Denmark, 68% of the participants had osteoporosis or osteopenia
[40] . A recent study showed that vitamin D defi-ciency is highly prevalent in COPD and correlates with variants in the vitamin D binding gene [41] .
Moderate endurance exercise increases serum 1,25(OH)2D3 level [42,43] . Also, Sato et al., [44] , reported that immobilization, in contrast to endur-ance exercise, 1,25-(OH) 2D3 are suppressed. How-ever, Maimoun et al., [45] , reported that in exercise trained rats, serum 1,25-(OH) 2D3 concentration was not affected.
In this study vitamin D supplementation, exer-cise training or both significantly improved pul-monary functions compared with COPD untreated
group.
In agreement with our results, a strong relation-ship between serum levels of vitamin D and lung
function (FEV1 and FVC) was found [46,47] . In another study, 25(OH)D was correlated with FEV1
[48] . Ferrari et al., [49] also demonstrated that the maximal exercise capacity and carbon monoxide transfer in the single breath method were both
positively correlated with serum 25(OH)D concen-trations.
1060 Effect of Vitamin D Supplementation and/or Physical Training
A cross-sectional study found that higher plasma
levels of vitamin D are associated with increased
bone mineral density and exercise capacity in
people with COPD [50] . Evidence also showed that high dose vitamin D supplementation improved
respiratory muscle strength and exercise capacity in people with COPD [51] . Epidemiological studies revealed a dose-dependent association between
serum 25(OH)D levels and pulmonary function so
that adequate vitamin D supplementation may extend beyond its protection against osteoporotic fractures [52] .
However Shaheen et al., [53] reported that total vitamin D intake was positively associated with forced expiratory volume in 1 s (FEV1); they did not confirm a positive association between blood
25(OH)D concentrations and adult lung function.
They suggested that the apparent relationships with
dietary vitamin D are likely to be explained by
other highly correlated nutrients in the diet.
Also, Bjerk et al., [54] , reported that short-term vitamin D supplementation in patients with COPD
had no discernible effect on a simple measure of
physical performance [55] .
As regard the effects of physical exercise on
pulmonary functions, there was a controversy.
Maltais et al., [56] reported improvement of pulmo-nary functions FEV 1 and demonstrated physiologic gain following 12 weeks of exercise in persons with severe COPD. Similar improvement in phys-iologic parameters have been confirmed by several
additional studies [57,58] .
On the other hand, Flo et al., [59] , reported worsening of pulmonary emphysema induced by exercise training. Their hypothesis is that the increase in mechanical forces on the connective tissue may contribute to the worsening of pulmo-nary function. One alternative explanation for the
worsening of emphysema induced by exercise was the presence of exercise-induced oxidative stress.
It has been demonstrated that strenuous aerobic
exercise is associated with oxidative stress and
tissue damage [60,61] . However, moderate exercise training is associated with adaptive responses in
at least some antioxidant capacities [62] .
The beneficial effect of vitamin D supplemen-tation and or exercise on pulmonary functions
could depend on the calcemic effects of vitamin
D.
In the present study it was observed that the
calcium levels in the blood of COPD rats were
significantly lower than normal control. Treatment of the COPD rats for 8 weeks with vitamin D
improved the calcemic state of the rats to the normal control values. Also in the exercise trained
group or combined vitamin D and exercise group calcium levels were increased to be insignificantly
changed as compared to the control rats.
The vital capacity and total lung capacity were found to decline with an increasing number of
thoracic vertebral fractures as a direct consequence
of vitamin D deficiency and hypocalcemia [63] . Nuti et al., observed 3030 ambulatory COPD pa-tients and found a strong association between
COPD severity and fractures [64] . Kyphosis related to osteoporosis caused limitation in rib mobility and inspiratory muscle function and correlated
with a reduction in FEV 1 and FVC [65] . The altered properties of the thoracic skeleton could result in
failure of the respiratory muscles contributing to
the pathophysiology of COPD.
It was seen from the results of this study that
exercise also improved pulmonary functions in COPD rats and we can find that also exercise improved the calcemic state in COPD rats. Blood
Ca2+ levels were increased but not significantly in exercise trained groups as compared with un-treated COPD rats.
In agreement with our results, Yeh et al., report-ed that in exercise trained rats plasma ionized calcium slightly increased [42] . Previous studies suggest that moderate endurance exercise increases
serum 1,25(OH)2D3 level, decreases urinary calci-um excretion [43] . By using a flat-bed treadmill exercise, Yeh and co-workers found that the endur-ance exercise trained female Sprague-Dawley rats had higher duodenal active, but not passive, calcium absorption than the control [42] . Although exercise-enhanced intestinal calcium absorption is likely
mediated by an increase in serum 1,25-(OH) 2D3 level, exercise may also stimulate calcium absorp-tion by changing intestinal motility and epithelial permeability [66,67] .
Acute exacerbations of COPD are an important
cause of hospitalization and lead to a faster decline
in FEV 1 [68] . Exacerbations are triggered by virus-es, bacteria, atypical strains, or a combination of these [69,70] .
In the present study it was found that vitamin D treatment enhances the innate immune system
by inducing the production of antimicrobial cathe-licidin and was associated with a significant in-crease in its lung production.
The occurrence of exacerbations, which are very often caused by bacterial or viral infections,
increases the severity of COPD and causes a higher
Nashwa Eltablawy, et al. 1061
death rate in humans [71] . 1,25(OH)2D3 is a direct regulator of antimicrobial peptides, such as cathe-licidin (camp) and defensin ß2 (defß2) genes that are driven by vitamin D response elements
(VDRE)-containing promoters, revealing the po-tential therapeutic role of vitamin D3 analogs
against opportunistic infections, including the infections in the respiratory tracts which occurs in patients with COPD susceptible to exacerbations [72] .
In agreement with our results, Vazirnia ei al., [73] reported a beneficial effect of 1,25(OH) 2D on the innate immunity and they also found an eleva-tion of the antimicrobial cathelicidin in cases treated
with vitamin D.
Several interventional studies examining the effect of vitamin D supplementation on the risk of
influenza [74,75] and in patients with active tuber-culosis showed a significantly reduced risk for influence an improved immunity against mycobac-teria [76,77] . There was also a higher rate of tuber-culosis symptom improvement in children [78] .
Several mechanisms could explain vitamin D’s potentially beneficial effects on infectious diseases.
In addition to its antimicrobial effect, vitamin D
can affect the inflammatory response. In the present
study, the increase of lung production of inflam-matory mediators in untreated COPD rats relative to healthy controls are in agreement with those
previously reported in patients with stable COPD of similar severity and body mass index [79] . Studies have also reported increased levels of circulating
cytokines (interleukin (IL)-6 and -8 and tumour
necrosis factor-a (TNF-(x) and acute phase reactant
protein (C-reactive protein (CRP), both of which reflect systemic inflammation, in the peripheral
circulation of stable COPD patients [80,81] .
In agreement with our results, it was reported
that 1,25D (1,25-dihydroxyvitamin D) decreases
TNF-alpha [82] . Other studies showed that vitamin D can modulate the activity of various immune
cells and inhibit inflammatory responses [83,84] . It was reported that vitamin D-induced inhibition of
IL-12 release by dendritic cells has a profound
effect on T lymphocyte differentiation [85] . Vitamin D-binding protein has immunomodulatory functions pertinent to the lung, and is associated with acti-vation of macrophages and neutrophil chemotaxis
[19] .
In agreement with our results, regular exercise
was noted to protect against diseases associated
with chronic inflammation [86] . On the other hand, American Thoracic Society reported that exercise
induced oxidative stress and could, inversely,
induce abnormal exercise-induced inflammation
in COPD. Plasma inflammatory mediators TNF alpha and IL-6 were not significantly modified by
training. Pulmonary rehabilitation can induce pe-ripheral muscle adaptations without decreasing the levels of systemic or local muscle inflammation [87] .
In our study it can be observed that matrix
metalloproteinasis-9 (MMP-9) is significantly elevated in lung tissues of COPD rats and a caus-ative role has been suggested in the development
of COPD [88] . The effect of vitamin D on extracel-lular matrix homeostasis not only in bone tissue,
but also within the lung may have a role in COPD
development. In the present study, vitamin D sup-plementation significantly reduced MMP-9 pro-duction in lung tissues of treated COPD rats as compared with untreated controls.
In agreement with our results, Boyan and Schwartz [89] found vitamin D to be an autocrine regulator of extracellular matrix turnover and
growth factor release via matrix metalloproteinases.
Also Bahar-Shany et al., [90] reported that vitamin D attenuates MMP-9 production in keratinocytes
and they suggested that vitamin D deficiency may
lead to a reduced attenuation of MMP-9 activity
resulting in enhanced degradation of lung paren-chyma.
Our results showed that exercise training re-duced lung production of MMP-9, suggesting that
exercise training may be important not only in
pulmonary rehabilitation in COPD but also as an adjuvant in the prevention and progression of lung
destruction due to cigarette smoking.
Few studies investigated the effect of physical training on lung production of MMP-9 in COPD. Toledo et al., [91] found a decrease in TIMP 1 in mice exposed to cigarette smoke that was reversed by aerobic exercise.
Conclusion: We can see from the results of this work that,
COPD is an inflammatory disease and it is associ-ated with vitamin D deficiency. Vitamin D supple-ment or rehabilitation by physical training each separately improved the pulmonary functions, reduced inflammation, and attenuate lung paren-chymal degradation. Vitamin D in addition induced an antimicrobial protection, however vitamin D
supplement had a slightly better effects as compared
with exercise training. Combination of both vitamin
D supplementation and exercise training had a
1062 Effect of Vitamin D Supplementation and/or Physical Training
synergistic effect and produced a significant im-provement as compared to each therapy separately.
We can conclude that vitamin D supplement has
a beneficial effects as a therapy in cases of COPD
and it is better added to rehabilitation training
programs for better results.
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