The present study was designed to synthesis potassium dicitro bismuthate (III) complex. The complex was characterized by infrared spectra, conductivity and elemental analysis of Bi. The effect of gastro protection was investigated for the prepared complex against HCl- ethanol induced ulcer in rats. The complex was administered to rats at 50 and 100 mg\kg doses orally before one hour of receiving 0.2ml of HCl- ethanol mixture to induce gastric ulcer. Sucralfate (100mg\ kg, orally) was used as standard drug. The severity of gastro mucosal damage induced by HCl-ethanol was analyzed in term of ulcer index value. Administration of potassium dicitro bismuthate (III) one hour before HCl-ethanol had significantly decreased ulcer index value when compared to saline treated group. Sucralfate (100mg\kg, orally) also produced a significant decrease in ulcer index when compared with the saline treated group. There was no significant difference between potassium dicitro bismuthate (III) and Sucralfate in degree of protection against ulcer. Thus it can be concluded that potassium dicitro bismuthate (III) has antiulcer activity in rats.
ABSTRACT
The present study was designed to synthesis potassium dicitro bismuthate (III) complex. The complex was characterized by infrared spectra, conductivity and elemental analysis of Bi. The effect of gastro protection was investigated for the prepared complex against HCl- ethanol induced ulcer in rats. The complex was administered to rats at 50 and 100 mg\kg doses orally before one hour of receiving 0.2ml of HCl- ethanol mixture to induce gastric ulcer. Sucralfate (100mg\ kg, orally) was used as standard drug. The severity of gastro mucosal damage induced by HCl-ethanol was analyzed in term of ulcer index value. Administration of potassium dicitro bismuthate (III) one hour before HCl-ethanol had significantly decreased ulcer index value when compared to saline treated group. Sucralfate (100mg\kg, orally) also produced a significant decrease in ulcer index when compared with the saline treated group. There was no significant difference between potassium dicitro bismuthate (III) and Sucralfate in degree of protection against ulcer. Thus it can be concluded that potassium dicitro bismuthate (III) has antiulcer activity in rats. Keywords: citric acid, bismuth complex, antigastric ulcer, Sucralfate
INTRODUCTION
The importance of citric acid (CA) in abiotic and biological systems has been well established over the years (Ali et al., 2008, Carla et al., 2008, Tselesh, 2008, Maria et al., 2008). The nature of the metal-citrate complex formed depends upon the nature of the metal, the pH of the solution, type of coordination bond and the stoichiometric ratio of metal to citric acid.
Citrate is an important biological ligand for metal ions. It is present at high concentration (ca. 200 mM) in blood plasma and forms strong complexes not only with natural metal ions such as CaII, MgII and FeIII, but also with ions of toxic (e.g. AlIII), ( Petrova et al., 2008) therapeutic (e.g. BiIII) and diagnostic (e.g. 67GaIII) importance.
Peptic ulcer, one of the most widespread disease, is believed to be due to imbalance between aggressive and protective factors (Alkofahi and Atta, 1999) in the stomach such as acid-pepsin secretion, mucosal barrier, mucous secretion, blood flow, cellular regeneration, prostaglandin, epidural growth factor (Govindarajan et al., 2006, Lima et al., 2006) bacterial products (Helicobacter pylori) and drugs (Peskar and Maricic,1998). The current medical treatment of peptic ulcer is generally based on the inhibition of gastric acid secretion by H2 as Omeprazol and antimuscarinics, as well as, the acid in depended therapy provided by Sucralfate and bismuth (Bighett et al., 2005). Potassium dicitro bismuthate (III) has a topical action in the upper gastrointestinal tract (Coghill and Shepherd, 1988) and it is commonly used to treat a variety gastrointestinal disorder (Lourence and Keith, 2008). Potassium dicitro bismuthate (III) precipitate (an active metabolite) when it is reaches the acidic environment of the stomach (Wagstaff et al., 1988).
The aim of the present study is to prepare potassium dicitro bismuthate (III) complex and characterize by molar conductivity, infrared spectra, and elemental analysis and its effect as antiulcer activity in experimentally induced ulcer in rats.
MATERIALS AND METHODS
All the materials (BDH) were used without any further purification.
Preparation of Bismuth complex
The complex was prepared by adding bismuth nitrate(1mmole) in 25 ml of deionized water to an aqueous solution of citric acid (2 mmole) with continued stirring until a white precipitate was formed. The precipitate was washed with a small amount of deionized water. Bismuth citrate was suspended in (25ml) of deionized water, sodium carbonate powder was added with stirring until the solution become neutral. Absolute alcohol was added to the solution with stirring until a white precipitate was formed; the product was washed with 10 ml of dry ether and dried (yield 80%). Melting point more than 350˚C, molar conductivity (345, 125 ohm-[1] cm[2] mole-[1]) in water and ethanol, respectively.
Physical measurements: The FT-IR were measured as KBr disc by using FT-IR Spectrometer (Fourier transform infrared spectroscopy) (Bruker 27, TENSOR, Germany). Molar conductance was obtained approximately 10-[3]M in a Jenway conductivity meter model 4070. Content of Bismuth was determined by the following method (Malairajan et al., 2008). Moisten about 0.5g, accurately weighed with sulphuric acid, ignite at a temperature not exceeding 500˚C, and dissolve the product in 2ml of nitric acid and 4ml of water, add 50ml of glycerol and 0.2g of sluphuric acid, allow to stand for one minute, and add 200ml of water and 0.3ml of catechol violet solution; if a violet color is produced add dilute ammonia solution, drop wise, until a blue color is produced; titrate with M/20 sodium edentate until a yellow color is produced; each ml of M/20 sodium edentate is equivalent to 0.01045g of Bi. Pharmaceutical study Healthy rats of either sex weighing 200-250gm were selected for this study. The animals were housed and fed with standard diet and water. Animals were deprived of foot at least 24 hrs. before starting of the experiment but were allowed free access to water. The rats were divided into 4 groups, each group consist of five animals. Group 1 served as a saline control and was given normal saline 0.9% (1 ml/kg, orally), group 2 received (100 mg /Kg, orally) sucralfate (Alma company, Syria) as standard control. Group 3and 4 received (50, 100 mg /Kg, orally) potassium dicitro bismuthate (III) respectively. After one hour all the animals were treated with 0.5 ml of HCl -ethanol mixture, orally (0.3 M hydrochloric acid and ethanol 60%) to induce gastric ulcer. Animals were sacrificed by cervical dislocation, one hour after administration of HCl -ethanol mixture (Malairajan et al., 2008). The stomachs were removed, opened along the greater curvature and examined for lesion severity, lesion severity was determined by measuring ulcer index, by measuring each lesion Preparation Potassiumdicitro Bismuthate.. 41 in mm along its greater length (Singh et al., 2008, Abay and Abdulwahib, 2008). The ulcer lesions observed were scored according to the severity according to previous study (Nwafor et al., 1996).
Histological evaluation
Sections of tissue from stomach were examined histologically to study ulcerogenic and or antiulcerogenic activity of tripotassium dicitro bismuthate (III). The slides were examined microscopically (Olympic Company) for pathomorphological changes such as congestion, hemorrhage, edema and erosion using an arbitrary scale for the assessment of severity of these changes (Al-Howiriny et al., 2005).
Histopathological studies
The stomach tissues were removed from the rats and fixed in 10% normal saline for at least 48 hrs. These were then processed routinely and the tissues were embedded in paraffin wax. Histological sections were cut at 5 - 6 μm and stained with routine haematoxylin and eosin (HE). These were then examined by a histopathologist. The lesions observed were assessed for the following, mucosal atrophy, and the presence of inflammatory cells in the wall, oesinophils, lymphocytes and plasma cells. These were graded according to mild (+), moderate (++) or severe (+++). Photomicrographs of representative lesions were taken at various magnifications.
Statistical analysis
The data were expressed as mean ± SD , difference between three experimental groups were statistically analyzed by one way analysis of variance ( ANOVA) followed by the least significant difference test. The level of significance was at p < 0.05.
RESULTS AND DISCUSSION
A- Structure assignment
Fourier transform-infrared spectroscopy (FTIR)
The following factors affect metal-ligand stretching vibrations: i) oxidation state of the metal atom, ii) coordination number and symmetry, iii) coordination bond strength, iv) the base strength of the ligand, and, v) bridging ligands.
Citric acid
The structure consists of two methylenic carbons (CH2), three carboxylic acid (COOH) groups, and a tertiary alcohol group (C3C−OH). The sharp peak at 3500 cm−[1] is due to α - hydroxyl O−H stretching, reflecting intermolecular hydrogen bonding. A broad group of bands between 3300 and 2500 cm−[1] is due to O−H stretching vibrations resulting from hydrogen bonding indicating a dimeric structure. The C−O stretching vibrations for the alcoholic group occur at 1140, 1175, 1210, and 1240 cm−[1]. Carboxylic acid dimer peaks are indicated at 1350 to 1290 cm−[1] and at 940 cm−[1] due to C−O stretching vibrations. The primary C=O stretching vibration for COOH groups is seen as a doublet peak at 1740 cm−[1] and 1710 cm−[1]. The split structure signifies the non-equivalence between the two terminal carboxylates and the central carboxylate group. The sharp peak at 1430 cm−[1] manifests the tertiary alcohol in-plane O−H stretching vibrations, while the moderately broad peak at 935 cm−[1] is due to the dimeric carboxylic acid O−H out-of plane stretching vibration.
potassiumdicitro bismuthate (III) complex
The association of a hydroxid group in metal bonding is indicated by the absorption peak at 3610 (O−H) and the C α −OH stretch is reflected in the peaks at 910, 850, and 830 cm−[1]. Complexation of the α -hydroxyl group of citric acid is indicated by the absence of a 42 Amer A. Taqa peak at 3500 cm−[1] compared to citric acid. Additional evidence for the association of the α - hydroxyl group is indicated by the shift in the C−O bending vibrations of the hydroxyl group to higher energies (1190, 1230, 1260, 1300 cm−[1]) compared to those in citric acid. Lattice water is indicated by the shoulder peak at 3380 cm−[1]. Involvement of the citric acid carboxylate groups with the metals is suggested by the asymmetric C=O stretching peaks at 1640 and 1570 cm−[1]. The position of these peaks is strong indication of unidentate as well as bidentate coordination to the metal. The shift in the symmetric C=O stretch (medium) to 1440 cm−[1] signifies bidentate or bridging carboxylate coordination, while unidentate coordination is confirmed by the peak at 1360 cm−[1]. The presence of a sharp peak at 1790 cm−[1] is due to the C=O stretch of the free carboxylate group.
The molar conductivity measurement: A high value of molar conductivity for the reflects complex has a 1:3 ratio of metal to ligand in both solvents. These results suggested a structure of complex Fig.1, the suggested structure was further confirmed by metal content analysis of bismuth (calculated;29.665, found 30.01%)
illustration not visible in this excerpt
Fig. 1: The suggested structure for tripotasium dicitro bismuthate (III) complex.
B- Antiulcer activity of the complex
In the present study, the potassiumdicitro bismuthate (III) was evaluated for its antiulcer activity against HCl -ethanol induced gastric ulcer in rat. Oral administration of HCl - ethanol produces sever ulceration, potassium dicitro bismuthate (III) at (50,100 mg/Kg, orally ) as well as standard drug Sucralfate at (100 mg /Kg , orally) significantly reduce lesion score of ulcer in compare to saline treated group (Fig. 2,3,4).
[...]
- Quote paper
- Amer Taqa (Author), 2011, Preparation of PotassiumDicitro Bismuthate Complex as Antigastric Ulcer, Munich, GRIN Verlag, https://www.hausarbeiten.de/document/209691