J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 1 Oxidative stress status in hypertensive patients on amlodipine treatment Bahaa Noor Madhloom (1), Ameena Ryhan Diajil (2) ABSTRACT Background: Oxidative stress may contribute to the etiology of hypertension in humans. Oxidative stress is an imbalance between reactive oxygen species (ROS) and antioxidant defense mechanisms, causing damage to biological macromolecules and dysregulation of normal metabolism and physiology. Amlodipine as an antihypertensive agent is a long-acting calcium channel blocker that dilates blood vessels and improves blood flow. The aim of this study was to assess the oxidative stress in hypertensive patients on Amlodipine treatment through the assessment of salivary Malondialdehyde (MDA) and superoxide dismutase (SOD) as a marker of oxidative stress. Material and method: 60 individuals were included in this study, divided into two groups; the first group composed of 30 hypertensive patients on Amlodipine antihypertensive agent. The second group, the control group, composed of 30 healthy subjects without any systemic disease and with almost healthy oral hygiene. Intraoral examination was done for each individual and salivary samples were collected with the salivary flow rate (F/R) which was calculated in ml per minute and pH was measured by pH meter. Salivary MDA and SOD were analyzed by using ELISA kit based on the principle of competitive enzyme immunoassay technique; the concentrations of markers were measured by spectrophotometer at 450nm in a microplate reader. Results: Salivary MDA was significantly higher in hypertensive patients compared to control, while salivary SOD was significantly lower in patients than control group. Salivary flow rate and pH was significantly lower in patients as compared to the control group. Conclusions: There is a relation between oxidative stress and hypertension. Salivary MDA and SOD can be used as potential marker for monitoring patients with Hypertension. Keywords: hypertension, Oxidative stress, Amlodipine, MDA and SOD. (Received: 10/1/2018; Accepted: 11/2/2018) INTRODUCTION Hypertension is defined as a systolic blood pressure (SBP) of 140 mm Hg or more, or a diastolic blood pressure (DBP) of 90 mm Hg or more.(1) Hypertension may be primary, which may be developed as a result of environmental or genetic causes, or secondary, which has multiple etiologies, including renal, vascular and endocrine causes.(2) Primary or essential hypertension accounts for 90-95% of adult cases, while secondary hypertension accounts for only 2-10% of cases.(3) Channel blocker dilates blood vessels and improves blood flow. It is a dihydropyridine calcium antagonist (calcium ion antagonist or slow-channel blocker) that inhibits the transmembrane influx of calcium ions into vascular smooth muscle and cardiac muscle.(4) Amlodipine (Norvasc), one of the antihypertension agents, is a long-acting calcium; Oxidative stress (OS) is an imbalance between the generation of reactive oxygen species (ROS) and nitrogen species (RNS) and the antioxidant defense systems in the body.(5) Under normal conditions, ROS and the byproducts of their reactions with various biomolecules are neutralized and converted into harmless molecules by the natural antioxidant system. The antioxidant defense system is a highly complex biochemical organization that consists of numerous enzymes and a large number of scavenger molecules, the body’s pool of antioxidant molecules is derived from endogenous and exogenous sources.(6,7) Superoxide dismutase (SOD) has been identified as an endogenous antioxidant enzyme.(8) Reactive O2- is converted by SOD into H2O2. In the next step, H2O2 is converted into H2O and O2 by salivary enzymes, catalase, peroxidase, and glutathione peroxidase.(9) Among the many different aldehydes which can be formed as secondary products during lipid peroxidation, malondialdehyde (MDA) propanol, hexanal, and 4-hydroxynonenal (4- HNE).(10) MDA appears to be the most mutagenic product of lipid peroxidation.(11) It is an end-product generated by decomposition of arachidonic acid and larger polyunsaturated fatty acids.(12) Once formed, MDA can be enzymatically metabolized or react (1) Master student- Department of Oral Diagnosis, College of Dentistry, University of Baghdad. (2) Assistant Professor, Department of Oral Diagnosis, College of Dentistry, University of Baghdad. J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 2 on cellular and tissue proteins or DNA to form adducts resulting in biomolecular damages.(12) MDA is one of the most popular and reliable markers that determine oxidative stress in clinical situations(13) which is found to be contributed to the etiology of hypertension in humans.(14) Also, hypertensive patients have impaired endogenous and exogenous antioxidant defense mechanisms.(15) MATERIALS AND METHODS Sixteen individuals were included in this study, divided into two groups. The first group composed of 30 hypertensive patients on Amlodipine treatment. The second group (control) composed of 30 healthy subjects without any systemic disorder and they were almost with healthy oral hygiene. After explaining the experimental design and the purpose of the study, written informed consent was signed by each participant in this study. All patients were selected from Al-Manathera Primary Health Center in AL- Najaf city. After gathering information regarding age, sex, the dose of medication per day, family history of hypertension, oral soft tissue condition, burning mouth syndrome if existed, signs and symptoms of dry mouth, salivary samples were collected from individuals under the similar conditions. Methods: Intraoral examination was done using sterile dental mirror and probe with artificial light. The examination was performed systemically in the following sequence: • Oral mucosa, examination of oral soft tissues was done in a sequence according to WHO (1997). • Burning mouth syndrome according to (Scala, et al., 2003). • Signs and symptoms of dry mouth. The same dentist performed all examinations. A concordant diagnostic analysis was performed on 12 randomly selected patients by a second examiner. Saliva samples were collected in restful and quiet circumstances. Saliva's production during the first 2 minutes was discarded to avoid any possible contamination, spitting saliva into graduated test tubes. After the collection of adequate amounts of saliva (5 ml) according to the biological needs, the salivary F/R was calculated ml per minute. pH of salivary secretion was measured by pH meter. Salivary samples were centrifuged at 3000×rpm for 15 minutes and then the clear supernatant was taken and transported frozen in ice crushed container to the laboratory and stored at -80C until analysis. 1- Estimation of Salivary Superoxide Dismutase: 2- The level of salivary superoxide dismutase was analyzed using commercially available, BG SOD ELISA kit. It was based on the principle of competitive enzyme immunoassay technique utilizing a monoclonal anti-SOD antibody and an SOD-Horseradish Peroxidase (HRP) conjugate. The intensity of color was measured spectrophotometrically at 450nm in a microplate reader. The SOD concentration in each sample was interpolated from this standard curve. Estimation of Salivary Malondialdehyde: The level of salivary MDA was analyzed using commercially available BG MDA ELISA kit. It was based on the principle of competitive enzyme immunoassay technique utilizing a monoclonal anti-MDA antibody and an MDA-Horseradish Peroxidase (HRP) conjugate. The intensity of color was measured spectrophotometrically at 450nm in a microplate reader. The MDA concentration in each sample was interpolated from this standard curve. 3- Statistical analysis: Data were translated into a computerized database structure. An expert statistical advice was sought for study. Statistical analysis was computer assisted using SPSS version 24 (Statistical Package for Social Sciences) association with Excel version 5. The results were expressed as mean, standard deviation (SD). The differences between the groups were analyzed by using the Student’s t-test and one-way ANOVA with the post hoc Tukey test and Pearson’s correlation was applied to determine the relationships between the variables. The statistical significance was defined at a p value of <0.05. RESULTS Age & Gender Hypertensive patients on Amlodipine were with a mean age of 56.53 year (±2.161 SD); 16 were males (53%) and 14 were females (47%). The age range was (52-60) years. Regarding control group, the mean age was 54.77 year (±3.339 SD); 15 were males and 15 were females. The age range was (50-63) years, Table 1. J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 3 Table (1): Age range, mean and standard deviation of the study and control group Groups N Age Range (years) Mean age (year) ±SD P- value Control 30 50-63 54.77 3.339 >0.01 Amlodipine 30 52-60 56.53 2.161 As shown in Table 1, no statistically significant differences in mean age were found between patient and control group (P>0.01). Salivary flow rate (F/R) & pH: Both salivary flow rate & pH of hypertensive patients were found to be significantly lower than that of the control group, as shown in table 3. Table (3): Salivary flow-rate and pH of the study and control group. Variables N Mean ±SD Std. Error P- value Salivary flow rate (ml/min) Control= 30 0.37 0.14 0.02 <0.01 Patient= 60 0.21 0.10 0.01 Salivary pH Control= 30 6.71 0.13 0.02 <0.01 Patient= 60 6.51 0.18 0.03 Salivary Malondialdehyde (MDA) level: As shown in Table 4, the mean salivary MDA was significantly higher in hypertensive patients compared to the healthy individuals (P<0.01). Mean salivary MDA of the study group was (0.67µmol/m ±0.13 SD), while that of control group was (0.23 µmol/m ±0.06 SD). Table (4): Salivary malondialdehyde level of hypertensive patients & control. Salivary Malondialdehyde (µmol/m) N Mean ±SD Std. Error P- value Control 30 0.23 0.06 0.012 <0.01 Amlodipine patients 30 0.67 0.13 0.024 Salivary Superoxide Dismutase (SOD) level: As shown in Table 5, the mean salivary SOD was significantly lower in hypertensive patients compared to the healthy individuals (P<0.01). Mean SOD in the hypertensive patients was 0.55 µg/ml (±0.16 SD), while that of control group was 1.14 µg/ml (±0.07 SD). Table (5): Salivary superoxide dismutase level of hypertensive patients & control. Salivary Superoxide Dismutase (µg/ml) N Mean ±SD Std. Error P-value Control 30 1.14 0.07 0.01 <0.01 Amlodipine patients 30 0.55 0.16 0.03 Regarding patients treated with Amlodipine SOD was significantly lower compared with control group (0.55, 1.14) (P<0.01) (Table 5). In this study, a significant negative correlation was found between age of patients and saliva F/R (R= -0.61, P<0.01) (Figure 1). Also, a negative significant correlation was found between age of patients and salivary pH (R= - 0.556, P<0.01) (Figure 2). 6.2 0 6.4 0 6.6 0 6.8 0 7.0 0 40. 00 50. 00 60. 00 70. 00 80. 00 Age (years) p H Y=7.17-0.01*x R2 Linear =0.310 Figure (1): Negative Correlation between Age and Saliva F/R in Hypertensive Patients Figure (2): Negative Correlation between Age and Salivary pH in Hypertensive Patients. 0. 10 0. 20 0. 30 0. 40 0. 40. 00 50. 00 60. 70. 80. 00 Age (years) S a li v a F lo w R a te ( m l/ m in ) Y=0.66-7.39 E–3*x R2 Linear =0.372 J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 4 Considering salivary markers, a significant positive correlation was found between age of patients and salivary MDA level in hypertensive patients (R= 0.591, P<0.01), Figure 3. The age of patients showed a significant negative correlation with salivary SOD (R= -0.570 P<0.01) (Figure 3). History of Hypertension and Study Parameters The age range was 2-12 (years) and the mean was (6.3 years). There was a significant positive correlation between MDA and history of hypertension (r=0.70, P<0.01). But a significant negative correlation was found between history of hypertension and SOD (r=0.65, P<0.01), salivary F/R (r=0.53, P<0.01) and pH (r=0.56, P=0.01), Table 6. Table (6): Correlation between history of hypertension and salivary parameters. Variables Pearson’s correlation (r) P-value Amlodipine patient MDA 0.70 <0.01 SOD -0.65 <0.01 F/R ml/min. -0.53 <0.01 pH -0.56 <0.01 DISCUSSION Hypertension, a serious medical problem, occurs when blood flows with force greater than normal. Amlodipine is a dihydropyridine calcium antagonist inhibits the transmembrane influx of calcium ions into vascular smooth muscle and cardiac muscle.(4) In this study, 30 patients who were previously diagnosed with hypertension were enrolled. Those patients were under either Amlodipine (1- 6) years. Generally, the age of hypertensive patients showed no statically significant difference from normotensive individuals (56.53, 54.77 years). However, hypertensive patients were older than normotensive control subject, which comes with the fact that hypertension is systemic disease mostly of old age.(16) Salivary Flow Rate and pH In the present study, salivary F/R of hypertensive patients was significantly lower than normal control subjects (0.21, 0.37 ml/min). These findings are in agreement with Böhm, et al., (1985)(17) who found that salivary F/R is lower in borderline hypertensives than in normotensives. The data support the assumption that in subjects with hypertension the parasympathetic influence on the salivary glands is reduced. However, Amlodipine results in a decrease in renal vascular resistance and an increase in glomerular filtration rate.(19) Also, as the salivary F/R decreases, the concentrations of total protein, sodium, calcium, chloride, and bicarbonate as well as the pH decrease to various levels, whereas the concentrations of inorganic phosphate and magnesium raise.(20,21) This disagrees with Nimma, et al. (2016) (22) who found that there was no significant relation between hypertension and unstimulated salivary F/R. Also, kagawa, et al., (2013) (23) found no significant correlation between either hypertension or intake of antihypertensive medication and unstimulated salivary F/R, which also disagrees with the current study. Considering salivary pH, hypertensive patients significantly showed lower pH than normal control subjects (6.51, 6.71). This finding is similar to kagawa, et al., (2013)(23) who found a Figure (3): Positive Correlation between Age and MDA of Hypertensive Patients. Figure (4): Negative Correlation between Age and SOD of Hypertensive Patients. 0.30 0.40 0.7 0 0.90 40.0 0 50.0 0 60.0 0 70.0 80.0 Age (years) M D A ( µ m o l/ m l) Y=0.05+0.01* x R2 Linear =0.349 0.50 0.60 0.80 0.20 0.40 1.00 40. 00 50. 00 60. 00 70. 00 80. 00 Age (years) S O D ( µ g /m l) Y=0.05+0.01*x R2 Linear =0.349 0.60 0.8 0 1.20 https://www.ncbi.nlm.nih.gov/pubmed/?term=B%C3%B6hm%20R%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 5 significant correlation between either hypertension or intake of antihypertensive medication and pH of unstimulated saliva. Several studies have reported that the reduction in salivary F/R is also the cause of reduction in salivary pH/salivary buffering capacity in individuals (Andrei, et al., 2015)(24) and the electrolytic concentration and tonicity of saliva decrease with decreasing salivary flow rates.(25) Salivary markers Salivary Malondialdehyde level Malondialdehyde is one of the most reliable markers that determine oxidative stress in clinical situations.(13) The mean salivary malondialdehyde was significantly higher in hypertensive patients compared to the apparently healthy individuals. This agrees with Al-Rawi, et al., (2008)(26) who found that MDA level was significantly higher in hypertensive patients than that in healthy individual. Also, Ahmad et al., (2013)(27) found that the MDA levels was significantly increased in the hypertension groups as compared to those of the control group. Further, Nwanjo et al., (2007)(28) and Mahdi et al., (2002)(29) demonstrated an increase in the MDA levels in the essential hypertension cases. This can be attributed to ROS which contributes to the etiology of hypertension in humans.(14) Superoxide anion is produced by stimulation of the angiotensin II/angiotensin II type I receptor and nicotinamide adenine dinucleotide phosphate-oxidase (NADPH) oxidase by angiotensin II which in turn contribute in oxidation process products.(30) In human with hypertension, ROS may increase due to a diminution of the activity of antioxidant enzymes(31) which could lead to increase oxidation process and in turn increasing lipid peroxidation process and its products (MDA). Salivary Superoxide Dismutase level The mean salivary SOD was significantly lower in hypertensive patients compared to the apparently healthy individuals. This agrees with Ahmad, et al., (2013)(27) who found that the activities of SOD was significantly lower in the hypertensive patients as compared to those in normotensive subjects. The data support the assumption that subjects with hypertension have impaired endogenous and exogenous antioxidant defense mechanisms.(15) Also, hypertensive patients have reduced activity and decreased content of antioxidant enzymes, including super oxide dismutase, glutathione peroxidase, and catalase.(32) This disagrees with Al-Rawi, et al., (2008)(26) who found that SOD level was significantly higher in hypertensive patient than that of normotensive one. Considering the correlation between age and salivary F/R, a significant negative correlation was found between age of patients and salivary F/R and this agrees with Heintze , et al., (1983);(33) Pendersen, et al., (1985);(34) Cowman, et al., (1994);(35) Michael, (1998)(36) who found that a reduction in salivary F/R with aging, but disagrees with Heft., et al., (1984)(37) who found that there was no significant correlation between age and salivary F/R. This could be due to the effect of antihypertensive medications.(19) Also, this may be attributed to the effect of aging process on physiological homeostasis which can be separated in to two different major pathways, primary and secondary aging as proposed by Busse, (1997).(38) According to Narhi, et al., (1992)(39) the concept of primary aging (chronological) is an alteration in physiological function with advancing age and is independent of extrinsic of physical and psychological disturbances such as stress, trauma and disease. Yet, secondary aging implies the result of external influences including systemic diseases and therapeutic treatment. It is well- recognized that alteration of salivary function in the elderly are commonly associated with age related diseases (secondary aging). Since the reduction in salivary F/R could be a cause of reduction in salivary pH/salivary buffering capacity in individuals.(24) So, a negative significant correlation was found between age of patients and salivary pH. A significant positive correlation was found between age of patients and salivary MDA level in hypertensive patients. However, the age of patients showed a significant negative correlation with salivary SOD. These findings suggested that increased lipid peroxidation in patients may be caused by increased free radical production and/or decreased antioxidant defense, which agrees with the previous studies Gonca Akbulut, et al., (1999);(40) Mine Erdenİnal, et al., (2001);(41) Ramazan Ozcankaya, et al., (2002);(42) Ümit Mutlu Türkoğlua, et al., (2003)(43) which hypothesized that increased oxidative stress may play an important role in the aging process or versa verse. Furthermore, Ramazan et al., (2002)(42) concluded that increased MOD level is a result of aging so that lipid peroxidation increases due to aging. Gonca, et al., (1999)(40) suggested that increased levels of lipid peroxidation products may play a role in aging. Mine Erdenİnal et al., (2001)(41) and Ümit, et al.,(2003)(43), hypothesized that higher http://europepmc.org/search;jsessionid=CFE3F69AF426695100CBB1FC683CA6B3?query=AUTH:%22Heintze+U%22&page=1 http://www.sciencedirect.com/science/article/pii/S0009898100004228#! http://www.sciencedirect.com/science/article/pii/S0009912003000353#! http://www.sciencedirect.com/science/article/pii/S0009912003000353#! http://www.sciencedirect.com/science/article/pii/S0009898100004228#! http://www.sciencedirect.com/science/article/pii/S0009912003000353#! J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 6 level of OS plays an important role in the aging process of individual. A significant positive correlation was found between history of hypertension and salivary MDA level in hypertensive patients suggests a relation between increased oxidative stress and hypertension which is in agreement with Am et al., (2007)(44) who reported an association between increased oxidative stress and higher blood pressure. A significant negative correlation was found between history of hypertension and SOD which could be attributed to the fact that hypertensive patients have reduced activity and decreased content of antioxidant enzymes.(32) Also, the decrease in the antioxidant enzymes could be due to their inactivation as the result of a continuous exposure to hydrogen peroxide, hydrogen peroxynitrite and other free radicals.(45) Moreover, a significant negative correlation was found between history of hypertension and salivary F/R, this could be the effect of aging.(38) Also a significant negative correlation was found between history of hypertension and salivary pH, this could be due to the reduction in salivary F/R which could be due to reduction in salivary pH/salivary buffering capacity in individuals.(26) CONCLUSION 1. Over production of the free-radicals may lead to increased oxidative stress which leads to oxidative damage to the biological molecules, leading to several chronic diseases. 2. Salivary MDA increases in hypertensive patients which represent an increasing in oxidative process. 3. Salivary SOD decreases in hypertensive patients which represent a decrease in anti- oxidant enzyme system. 4. Salivary F/R & pH are negatively associated with hypertension due to the effect of antihypertensive medications or in hypertension the parasympathetic influence on the salivary glands is reduced. 5. This study recommends anti-oxidant supplements for patients with hypertension along with antihypertension medications. REFERENCES 1- Benjamin EJ., Blaha MJ, Chiuve SE. for the American Heart Association Statistics Committee and Stroke Statistics Subcommittee. Heart disease and stroke statistics-update: a report from the American Heart Association. Circulation. 2017;7:135:e146-e603. 2- Poulter NR, Prabhakaran, D, Caulfield M. (2015) Hypertension. Lancet (London, England). 386(9995): 801–12. 3- Chobanian AV, Bakris GL, Black HR, Cushman WC, Green LA, Izzo JL, et al. Seventh report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. 2003;42:1206-1252. 4- Burges RA. Amlodipine: a once daily calcium antagonist. J Hum Hypertens. 1991;5:49-54. 5- Kitiyakara C, Wilcox C. Antioxidants for hypertension. Curr Opin Nephrol Hypertens. 1998;7:531–538. 6- Briviba K, Sies H. Non enzymatic antioxidant defense systems. In: Frie B, editor. Natural antioxidants in human health and diseases. San Diego (CA): Academic press Inc.;1994; p. 119–21. 7- Jawanda MK. Antitumor activity of antioxidants – an overview. Int J Dental Clin. 2009;1:3–7. 8- Valko M, Leibfritz D, Moncol J, Cronin MTD, Mazur M, Teser J. Free radicals and antioxidants in normal physiological functions and human disease. Int J Biochem Cell Biol. 2006;39:44-84. 9- Kanehira T, Shibata K, Kashiwazaki H. Comparison of antioxidant enzymes in saliva of elderly smokers and nonsmokers. Gerodontology. 2006;23:38-42. 10- Esterbauer H, Cheeseman KH, Dianzani MU. “Separation and characterization of the aldehydic products of lipid peroxidation stimulated by ADP- Fe2+ in rat liver microsomes. Biochem J. 1987;208:129–140. 11- Esterbauer H, Cheeseman KH. Determination of aldehydic lipid peroxidation products: malonaldehyde and 4- hydroxynonenal. Methods in Enzymology. 1990;186:407-421. 12- Esterbauer H, Schaur RJ, Zollner H. Chemistry and Biochemistry of 4 hydroxynonenal, malonaldehyde and related aldehydes. Free Radical Biology and Medicine. 1991;11:81-128. 13- Giera M, Lingeman H, Niessen WMA. Recent advancements in the LC- and GC-based analysis of malondialdehyde (MDA): a brief overview. Chromatographia. 2012;75:433-440. 14- Russo C, Olivieri O, Girelli D, Faccini G, Zenari ML, Lombardi S, Corrocher R. Antioxidant status and lipid peroxidation in patients with essential hypertension. J Hypertens. 1998;16:1267-1271. 15- Mansego ML, Solar Gde M, Alonso MP, Martínez F, Sáez GT, Escudero JC. Polymorphisms of antioxidant enzymes, blood pressure and risk of hypertension. J Hypertens. 2011;29:492-500. 16- Pinto E. Blood pressure and ageing. Postgraduate Medical Journal. 2017;83:109-114. 17- Böhm R, van Baak M, van Hooff M, Moy J, Rahn KH. Salivary flow in borderline hypertension. 1985;63:154-156. 18- Atkinson AB and Robertson JIS. Captopril in the treatment of clinical hypertension and cardiac failure. Lancet. 1979;2:836-839. 19- Silke B, Frais MA, Midtbo KA. Comparative hemodynamic dose-response effects of five slow calcium channel blocking agents in coronary artery disease. Clin Pharmacol Ther. 1989;42:381-387. 20- Edgar WM. Saliva: its secretion, composition and functions. Br Dent J. 1992;172:305-312. 21- Tenovuo J, Lagerlöf F. (1994). Saliva. In: Thylstrup A, Fejerskov O. Textbook of clinical cariology. 2nd ed. Copenhagen: Munksgaard. 22- Nimma V, Talla H, Poosa M, Gopaladas M, Meesala D, Jayanth L. Influence of Hypertension on pH of https://www.ncbi.nlm.nih.gov/pubmed/?term=B%C3%B6hm%20R%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 https://www.ncbi.nlm.nih.gov/pubmed/?term=van%20Baak%20M%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 https://www.ncbi.nlm.nih.gov/pubmed/?term=van%20Hooff%20M%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 https://www.ncbi.nlm.nih.gov/pubmed/?term=Moy%20J%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 https://www.ncbi.nlm.nih.gov/pubmed/?term=Rahn%20KH%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 https://www.ncbi.nlm.nih.gov/pubmed/?term=Rahn%20KH%5BAuthor%5D&cauthor=true&cauthor_uid=3999634 J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 7 Saliva and Flow Rate in Elder Adults Correlating with Oral Health Status. J Clin Diagn Res. 2016;10:ZC34–ZC36. 23- kagawa R, ikebeb k, enoki K, murai s, okada t, matsuda k, maeda y. Influence of hypertension on pH of saliva in older adults. Oral Dis. 2013;19:525-529. 24- Prodan A, Brand HS, Ligtenberg AJ, et al. Interindividual variation, correlations, and sex- related differences in the salivary biochemistry of young healthy adults. Eur J Oral Sci. 2015;123:149- 157. 25- Bardow A, Madsen J, Nauntofte B. The bicarbonate concentration in human saliva does not exceed the plasma level under normal physiological conditions. Clin Oral Investig. 2000;4:245. 26- Al-Rawi N, Jaber F, Atiyah K. Assessment of salivary and serum oxidative stress and antioxidants as plausible parameters in prediction of ischemic stroke among Iraqi Samples. The Internet Journal of Third World Medicine. 2008;7. 27- Ahmad A, Singhal U, Hossain MM, Islam N, Rizvi I. The Role of the Endogenous Antioxidant Enzymes and Malondialdehyde in Essential Hypertension. J Clin Diagn Res. 2013;7987-990. 28- Nwanjo HU, Oze G, Okafor MC, Nwasu D, Nwankpa P. Oxidative stress and non enzymic antioxidant status in hypertensive patients in Nigeria. Afr. J. Biotechnol. 2007;6:1681–1684. 29- Mahdi AA. A, (2002). textbook of Biochemistry by S.P Singh. 3rd edn. New Delhi: CBs publishers and distributors. Free radicals and other antioxidant; pp. 545–55. 30- Bonomini F, Rodella LF, Rezzani R. Metabolic Syndrome, Aging and Involvement of Oxidative Stress. Aging Dis. 2015;6:109-120. 31- Pedro-Botet J, Covas MI, Martin S, Rubies-Prat J. Decreased endogenous antioxidant enzymatic status in essential hypertension. J Hum Hypertens. 2000;14:343–345. 32- Saez GT, Tormos C, Giner V, Chaves J, Lozano JV, Iradi A, Redon J. Factors related to the impact of antihypertensive treatment in antioxidant activities and oxidative stress by-products in human hypertension. Am J Hypertens. 2004;17:809–816. 33- Heintze U , Birkhed D , Björn H. Secretion rate and buffer effect of resting and stimulated whole saliva as a function of age and sex. Swed Dent J. 1983;7:227-238. 34- Pendersen W, Schuber M, Izutsu K, Mersai T, Truelove E. Age-dependent decrease in human submandibular gland flow rate as measured under resting and post-stimulation condition. J Dent Res. 1985;64.882-825. 35- Cowman RA, Frisch M, Lasseter CJ, Scarpace PJ. Effects of beta-adrenergic antagonist on salivary secretory function in individuals of different ages. J Gerontol. 1994;49:B208-B214. 36- Yeh CK, Johnson DA, Dodds MW. Impact of aging on human salivary gland function: a community- based study. Aging (Milano). 1998;10:421–428. 37- Heft MW, Baum BJ. Unstimulated and stimulated parotid salivary flow rate in individuals of different ages. J Dent Res. 1984;63:1182–1185. 38- Busse EW: Theories of aging in Busse E.W., Pfeiffer E. (1997). Behavior and Adaption in Later Life. Little, Brown and Company, Boston, pp.8-30. 39- Narhi TO, Meurman JH, Ainamo A, et al. Association between salivary flow rate and the use of systemic medication among 76-81 and 86 years old inhabitants in Helsinki, Finland. J Dent Res. 1992;71:1875-1880. 40- Gonca Akbulut K, Gönül B, Akbulut H. Differential effects of pharmacological doses of melatonin on malondialdehyde and glutathione levels in young and old rats. Gerontology. 1999;45:67-71. 41- Inal ME, Kanbak G, Sunal E. Antioxidant enzyme activities and malondialdehyde levels related to aging. Clin Chim Acta. 2001;305:75–80. 42- Ozcankaya R, Delibas N. Malondialdehyde, superoxide dismutase, melatonin, iron, copper, and zinc blood concentrations in patients with Alzheimer disease: cross-sectional study. Croat Med J. 2002;43:28–32. 43- Mutlu-Türkoğlu U, Ilhan E, Oztezcan S, Kuru A, Aykaç-Toker G, Uysal M. Age-related increases in plasma malondialdehyde and protein carbonyl levels and lymphocyte DNA damage in elderly subjects. Clin Biochem. 2003;36(5):397–400. 44- Armas-Padilla MC, Armas-Hernández MJ, Sosa- Canache B, et al. Nitric oxide and malondialdehyde in human hypertension. Am J Ther. 2007;14:172– 176. 45- Kedziora-Kornatowska K, Czuczejko J, Pawluk H, et al. The markers of oxidative stress and activity of the antioxidant system in the blood of elderly patients with essential arterial hypertension. Cell Mol Biol Lett. 2004;9:635–641. الخالصة: دضغط اوعي ادمت و عاد ي وضغ ا ت ش غم تمغ ش ادلغم اد همغمي و يم ارتفاع ضغط ادم و اد ضغا اد ي ون ه ا ارتفاع تمغ همغي ن اد فايي عأد ادمهاع ضغم االهمغمتس تمغرر ضغ ر أ ادم عيم ان يا هم ادت ي اض اووضغ عاد ا ف اد ر ت عاد از ب ن أن اع اال ينم ادنادن ادرل ي ش دييممش ادلم اد هممي ت نن ا وماوم هم اسراب ارتفاع ضط ادم و يالج ومغغغ م د تادي ارتفاع ضغغغط ادم س وت ط ه نر دلنات ادنادمغغغ د ودي ادال ت سغغغت االعي ادمت و Amlodipineات ي دب ن عو من س وا ادم ش هتالج تن Amlodipineضغال اد اغاب ن بارتفاع ضغط ادم عومغ مت االت ي دب ن تل م ادلغم اد همغمي هم اد اد مف تن ادمراسغ هم اديتابش SOD ع انزوم سر ر أعهم م دس تز MDA خالل ق اس تم ى تاد نمادمو اوم ت وض تاغاب (30( غ ي اقم ع تلمغ ن ادال تي ي ن اد ي ي االعدال ت ن تن 60و ادمراسغ تودف تن :اد اد عاد ول ( غ سغي م يغ اش تم ه ادفم دنط ه دس عاخ ن ج 30بارتفاع ضغط ادم عومغ م يالج االت ي دب نش اد ي ي ادنان ت ن تن م تن اديتاب دل اس ه اديتاب اد ف ز باد يي /دق ل ع ضغغ اديتابش تم ق اس تمغغ ى تاد نمادمو اوم ع انزوم سغغر ر أعهمغغ م دسغغ تز ه نان ت ش 450اديتاب باس ما ت ي ط اد ما عق اس ه اد ه ز باس ما تل اس اد ف ادي نم https://www.ncbi.nlm.nih.gov/pubmed/23279167 http://europepmc.org/search;jsessionid=CFE3F69AF426695100CBB1FC683CA6B3?query=AUTH:%22Heintze+U%22&page=1 http://europepmc.org/search;jsessionid=CFE3F69AF426695100CBB1FC683CA6B3?query=AUTH:%22Birkhed+D%22&page=1 http://europepmc.org/search;jsessionid=CFE3F69AF426695100CBB1FC683CA6B3?query=AUTH:%22Bj%C3%B6rn+H%22&page=1 J Bagh College Dentistry Vol. 32(1), March 2020 Oxidative Stress Status 8 اد ي ط اإل اغادم ديل اسغاض اع م انا تمغ ى تاد نمادمو اوم هم دتاب ت ضغال ادضغط اييال بنن تن اال غ اي ادمغي ن شب ن ا :ادن ي ال ادضغط تلارنا باويغ ا س ه وا اديتاب عتمغ ى اد ضغ اقط هم ت ضغال انزوم سغر ر أعهمغ م دسغ تز اقط هم دتاب ت ضغ ارتفاع ضط ادم تلارن باو اي االي ا ش االسغ ن اج وناد يالق ب ن ادلغم اد همغمي عارتفاع ضغط ادم ع تمغ ى تاد نمادمو اوم ع انزوم سغر ر أعهمغ م دسغ تز هم اديتاب و نن ا ت ابتا اد ضال اد ااب ن بارتفاع ضط ادم ش وم م هتالتا هم