47 research outputs found
Insecticide imidacloprid induces morphological and DNA damage through oxidative toxicity on the reproductive organs of developing male rats
We investigated whether treatment with imidacloprid would induce morphological changes, DNA fragmentation, antioxidant imbalance
and apoptosis in the reproductive system of developing male rats. Twenty-four male rats were included in this 90-day study, starting at 7 days of
age. The rats were divided into four groups. The first group was used as control. The second, third and fourth groups received oral 0.5-, 2- and
8-mg/kg imidacloprid, respectively. Serum, spermand testis sampleswere collected fromall groups at the end of the experimental period. Theweights
of the epididymis, vesicula seminalis, epididymal sperm concentration, body weight gain, testosterone and reduced glutathione values were lower in
the imidacloprid-treated groups than that in the controls. All treated groups had increased lipid peroxidation, fatty acid concentrations and higher rates
of abnormal sperm. Apoptosis and fragmentation of seminal DNA were higher in rats treated at the two higher doses of imidacloprid. These results
show that this compound has a negative effect on sperm and testis of rat
Effects of clothianidin exposure on sperm quality, testicular apoptosis and fatty acid composition in developing male rats
Clothianidin (CTD) is one of the latest members
of the synthetic organic insecticides, the neonicotinoids.
In the present study, it was aimed to investigate if
daily oral administration of CTD at low doses for
90 days has any deleterious effects on reproductive
functions of developing male rats. Animals were randomly
divided into four groups of six rats each, assigned
as control rats, or rats treated with 2 (CTD-2), 8 (CTD-8)
or 32 (CTD-32) mg CTD/kg body weight by oral gavage.
The significant decreases of the absolute weights
of right cauda epididymis and seminal vesicles, and
body weight were detected in the animals exposed to
CTD administration at 32 mg/kgBW/day. Epididymal
sperm concentration decreased significantly in CTD-32
group and the abnormal sperm rates increased in CTD-
8 and CTD-32 groups when compared to control group.
The testosterone level was significantly decreased in
CTD-32 group when compared to control group. The
administration of all CTD doses resulted in a significant
decrease in the level of GSH. The number of TUNELpositive
cells significantly increased in the germinal
epithelium of testis of rats exposed to CTD at
32 mg/kgBW/day. In groups CTD-8 and CTD-32,
only docosapentaenoic, arachidonic, palmitic and palmitoleic
acids were significantly elevated when compared
to control. The ratios of 20:4/18:2 and 18:1n−9/
18:0 were decreased when rats exposed to CTD. Sperm
DNA fragmentation was observed in CTD-32 group,
but not CTD-2 and CTD-8. It is concluded that low
doses of CTD exposure during critical stages of sexual maturation had moderate detrimental effects on reproductive
organ system and more severe effects are likely
to be observed at higher dose levels. In addition, the
reproductive system may be more sensitive to exposure
of CTD even earlier in development (prenatal and early
postnatal), and therefore it could be expected that more
severe effects could also be observed at the NOAEL
dose levels, if dosing had occurred in utero or early
postnatal
Requirement for the N-Terminal Coiled-Coil Domain for Expression and Function, but not Subunit Interaction of, the ADPR-Activated TRPM2 Channel
Transient receptor potential melastatin 2 (TRPM2) proteins form multiple-subunit complexes, most likely homotetramers, which operate as Ca2+-permeable, nonselective cation channels activated by intracellular ADP-ribose (ADPR) and oxidative stress. Each TRPM2 channel subunit is predicted to contain two coiled-coil (CC) domains, one in the N-terminus and the other in the C-terminus. Our recent study has shown that the C-terminal CC domain plays an important, but not exclusive, role in the TRPM2 channel assembly. This study aimed to examine the potential role of the N-terminal CC domain. Domain deletion dramatically reduced protein expression and abolished ADPR-evoked currents but did not alter the subunit interaction. Deletion of both CC domains strongly attenuated the subunit interaction, confirming that the C-terminal CC domain is critical in the subunit interaction. Glutamine substitutions into individual hydrophobic residues at positions a and d in the heptad repeats to disrupt the CC formation had no effect on protein expression, subunit interaction, or ADPR-evoked currents. Mutation of Ile658 to glutamine, which did not perturb the CC formation, decreased ADPR-evoked currents without affecting protein expression, subunit interaction, or membrane trafficking. These results collectively suggest the requirement for the N-terminal CC domain for protein expression and function, but not subunit interaction, of the TRPM2 channel
Effects of vitamin E supplementation on renal non-enzymatic antioxidants in young rats submitted to exhaustive exercise stress
<p>Abstract</p> <p>Background</p> <p>Exercise stress was shown to increase oxidative stress in rats. It lacks reports of increased protection afforded by dietary antioxidant supplements against ROS production during exercise stress. We evaluated the effects of vitamin E supplementation on renal non-enzymatic antioxidants in young rats submitted to exhaustive exercise stress.</p> <p>Methods</p> <p>Wistar rats were divided into three groups: 1) control group; 2) exercise stress group and; 3) exercise stress + Vitamin E group. Rats from the group 3 were treated with gavage administration of 1 mL of Vitamin E (5 mg/kg) for seven consecutive days. Animals from groups 2 and 3 were submitted to a bout of swimming exhaustive exercise stress. Kidney samples were analyzed for Thiobarbituric Acid Reactive Substances to (TBARS) by malondialdehyde (MDA), reduced glutathione (GSH) and vitamin-E levels.</p> <p>Results</p> <p>The group treated with vitamin E and submitted to exercise stress presented the lowest levels of renal MDA (1: 0.16+0.02 mmmol/mgprot vs. 2: 0.34+0.07 mmmol/mgprot vs. 3: 0.1+0.01 mmmol/mgprot; p < 0.0001), the highest levels of renal GSH (1: 23+4 μmol/gprot vs. 2: 23+2 μmol/gprot vs. 3: 58+9 μmol/gprot; p < 0.0001) and the highest levels of renal vitamin E (1: 24+6 μM/gtissue vs. 2: 28+2 μM/gtissue vs. 3: 43+4 μM/gtissue; p < 0.001).</p> <p>Conclusion</p> <p>Vitamin E supplementation improved non-enzymatic antioxidant activity in young rats submitted to exhaustive exercise stress.</p
Protective effects of nanostructures of hydrated C60 fullerene on reproductive function in streptozotocin-diabetic male rats
Diabetes mellitus is a well-recognized cause of male sexual dysfunction and impairments of male fertility.
Streptozotocin (STZ) is used for medical treatment of neoplastic islet -cells of pancreas and producing of
animal model of diabetes mellitus type 1 that is characterized by suppression of reproductive activity due
to the hyperglycaemia-induced oxidative stress and histopathological alterations in testes. Seeking for
the agents that could alleviate diabetes-induced damage to reproductive system is yet the important area
of inquiry. The present study was designed to evaluate whether hydrated C60 fullerene (C60HyFn), which
is known to be powerful bioantioxidant, eliminate testicular dysfunction induced by STZ-diabetes in rats.
Wistar strain male albino rats were divided into four groups of six animals each: (1) control group, (2)
C60HyFn-treated nondiabetic group, (3) STZ-diabetic group and (4) C60HyFn-treated diabetic group. Once
hyperglycaemia was induced by STZ, rats in the second and fourth groups were treated with C60HyFn (in
the form of drinking water) at the dose of 4 g/kg daily for 5 weeks. In diabetic rats, relative weights of
right cauda epididymis, seminal vesicles, prostate, sperm motility and epididymal sperm concentration
were significantly less than those of control group, but which were restored in the fourth group treated
with C60HyFn (p < 0.001). In hematoxylin and eosin staining, marked histopathological changes including
degeneration, desquamation, disorganisation and reduction in germinal cells, interstitial oedema and
congestion were evident in the testis of diabetic rats, but C60HyFn treatment resulted in recovery of
histopathological changes and an increase in Johnsen’s testicular score significantly (p < 0.001). C60HyFn
treatment restores the increased apoptosis induced by STZ-diabetes. In diabetic rats, levels of serum
testosterone, testicular reduced glutathione (GSH) and alpha-tocopherol were significantly reduced and
testicular lipid peroxidation level was increased (p < 0.001). Nevertheless, treatment of diabetic rats with
C60HyFn resulted in significant corrective effects on these parameters towards the control levels. C60HyFn,
applied alone, did not exert any toxic effects in testicular tissues. Furthermore, C60HyFn treatment in
diabetic and nondiabetic rats resulted in considerable elevations of some important polyunsaturated
fatty acids. In conclusion, we have presented for the first time substantial evidence that administration
of C60HyFn significantly reduces diabetes-induced oxidative stress and associated complications such as
testicular dysfunction and spermatogenic disruptio
Assessment of imidacloprid toxicity on reproductive organ system of adult male rats
In the current study it was aimed to investigate the toxicity of low doses of imidacloprid (IMI) on the reproductive organ systems
of adult male rats. The treatment groups received 0.5 (IMI-0.5), 2 (IMI-2) or 8 mg IMI/kg body weight by oral gavage (IMI-8) for
three months. The deterioration in sperm motility in IMI-8 group and epidydimal sperm concentration in IMI-2 and IMI-8 groups
and abnormality in sperm morphology in IMI-8 were significant. The levels of testosterone (T) and GSH decreased significantly
in group IMI-8 compared to the control group. Upon treatment with IMI, apoptotic index increased significantly only in germ
cells of the seminiferous tubules of IMI-8 group when compared to control. Fragmentation was striking in the seminal DNA from
the IMI-8 group, but it was much less obvious in the IMI-2 one. IMI exposure resulted in elevation of all fatty acids analyzed,
but the increases were significant only in stearic, oleic, linoleic and arachidonic acids. The ratios of 20:4/20:3 and 20:4/18:2 were
decreased and 16:1n-9/16:0 ratio was increased. In conclusion, the present animal experiments revealed that the treatment with IMI
at NOAEL dose-levels caused deterioration in sperm parameters, decreased T level, increased apoptosis of germ cells, seminal DNA
fragmentation, the depletion of antioxidants and change in disturbance of fatty acid composition. All these changes indicate the
suppression of testicular function
Lipid Peroxidative Damage on Cisplatin Exposure and Alterations in Antioxidant Defense System in Rat Kidneys: A Possible Protective Effect of Selenium
Cisplatin (Cis-diamminedichloroplatinum II, CP) is an important chemotherapeutic agent, useful in the treatment of several cancers, but with several side effects such as nephrotoxicity. The present study investigated the possible protective effect of selenium (Se) against CP-induced oxidative stress in the rat kidneys. Male Wistar albino rats were injected with a single dose of cisplatin (7 mg CP/kg b.m., i.p.) and selenium (6 mg Se/kg b.m, as Na2SeO3, i.p.), alone or in combination. The obtained results showed that CP increased lipid peroxidation (LPO) and decreased reduced glutathione (GSH) concentrations, suggesting the CP-induced oxidative stress, while Se treatment reversed this change to control values. Acute intoxication of rats with CP was followed by statistically significant decreased activity of antioxidant defense enzymes: superoxide dismutase (SOD), catalase (CAT), glutathione peroxidase (GSH-Px), glutathione reductase (GR) and glutathione-S-transferase (GST). Treatment with Se reversed CP-induced alterations of antioxidant defense enzyme activities and significantly prevented the CP-induced kidney damage