Labeling of famotidine with 99mTc and biodistribution studies on rats

Famotidine, a gastrointestinal drug was labeled with ^99mTc and its radiopharmaceutical potential was observed on male Albino Wistar rats. Labeling yield was over 95%. Average specific activity and n-octanol/water partition coefficient (lipophilicity) were approximately 74 MBq/mg-0.66 GBq/mg and 3.4, respectively. Biodistribution studies were performed on Albino Wistar rats. The activity per gram tissue was calculated and time-activity curves were generated. The majority of the activity was observed in stomach, small intestines and kidneys. Liver and kidneys showed lower uptake compared to other H₂-receptor rich tissues. Results show that ^99mTc-famotidine is H₂receptor specific. This revised version was published online in July 2006 with corrections to the Cover Date.     

Preparation and biodistribution of [<Superscript>131</Superscript>I]linezolid in animal model infection and inflammation

Linezolid is the first of new class of antibiotics, the oxazolidinones, and exhibits activity against many gram-positive organisms, including vancomycin-resistant Enterococcus faecium, methicillin-resistant Staphylococcus aureus, and penicillin-resistant Streptococcus pneumoniae. Aim of the study: Linezolid was to label with I-131 and potential of the radiolabeled antibiotic was to investigate in inflamed rats with S. aureus (S. aureus) and sterile inflamed rats with turpentine oil. Linezolid was labeled with I-131 by iodogen method. Biodistribution of [¹³¹I]linezolid was carried out in bacterial inflamed and sterile inflamed rats. Radiolabeling yield of [¹³¹I]linezolid was determined as 85 ± 1% at pH 2. After injecting of [¹³¹I]linezolid into bacterial inflamed and sterile inflamed rats, radiolabeled linezolid was rapidly removed from the circulation via the kidneys. Binding of [¹³¹I]linezolid to bacterial inflamed muscle (T/NT = 77.48 at 30 min) was five times higher than binding to sterile inflamed muscle (T/NT = 14.87 at 30 min) of rats. [¹³¹I]linezolid showed good localization in bacterial inflamed tissue. It was demonstrated that [¹³¹I]linezolid can be used to detect S. aureus inflammation in rats.     

The effect of radiolabeled antibiotics on biofilm and microorganism within biofilm

Journal of Radioanalytical and Nuclear Chemistry - The aim of this study was to investigate the 131I and 127I labeled linezolid and moxifloxacin effects of minimum inhibitory concentration, and...     

Investigation of the solid-state conductivity and the potentiometric stability constant relationships of new amino acid-Schiff bases and their complexes

Cu^II, Ni^II and Co^II complexes of new tridentate amino acid-Schiff bases derived from furfural and DL-alanine, DL-valine and DL-phenylalanine were prepared and characterized by analytical, spectroscopic, (i.r., u.v.–vis., ¹H-n.m.r and ¹³C-n.m.r) techniques, molar conductivity, magnetic and thermal measurements. Protonation constants of the Schiff bases and stability constants of the complexes have been determined potentiometrically in water. Solid-state conductivities of the synthesized substances were measured using the four-probe technique on a compressed pellet at room temperature.     

Synthesis,potentiometric and antimicrobial activity studies on 2-pyridinilidene-DL-amino acids and their complexes

To investigate the relationship between antimicrobial activities and the formation constants of Cu^II, Ni^II and Co^II complexes with three Schiff bases, which were obtained by the condensation of 2-pyridinecarboxyaldehyde with DL-alanine, DL-valine and DL-phenylalanine, have been synthesized. Schiff bases and the complexes have been characterized on the basis of elemental analyses, magnetic moments (at ca. 25 °C), molar conductivity, thermal analyses and spectral (i.r., u.v., n.m.r.) studies. The i.r. spectra show that the ligands act in a monovalent bidentate fashion, depending on the metal salt used and the reaction pH = 9, 8 and 7 medium, for Cu^II, Ni^II and Co^II, respectively. Square-planar, tetrahedral and octahedral structures are proposed for Cu^II, Ni^II and Co^II, respectively. The protonation constants of the Schiff bases and stability constants of their ML-type complexes have been calculated potentiometrically in aqueous solution at 25 ± 0.1 °C and at 0.1 M KCl ionic strength. Antimicrobial activities of the Schiff bases and the complexes were evaluated for three bacteria (Bacillus subtillis, Staphylococcus aureus, and Escherichia coli) and a yeast (Candida albicans). The structure–activity correlation in Schiff bases and their metal(II) complexes are discussed, based on the effect of their stability contants.     

Reactions of iodine atoms activated by L shell photoelectric ionization in liquid benzene

Solutions of I₂ in C₆H₆ were irradiated with X-rays, in the energy range from 4.6 to 8.0 keV, thus including the characteristic X-ray of Cr /5.412 keV/, just above the L-absorption edge for iodine /5.118 keV/. Yield of iodobenzene and the organic yield of iodine were investigated as a function of I₂ concentration and of the absorbed radiation dose. It is found that the formation of iodobenzene, which was the only product detected, is due to the Auger activation of iodine atoms, and not to the radiolytic decomposition of benzene molecules from direct interaction of X-rays.     

Synthesis of <Superscript>131</Superscript>I labeled estrone derivatives and biodistribution studies on rats

Summary The aim of this study is to synthesize novel ¹³¹I labeled estrone derivatives that may have therapeutical potentials on Estrogen Receptor rich tumors. Two radiolabeled estrone derivatives, [¹³¹I]2-iodo-3-methoxy-estra-1,3,5-trien-17-one and [¹³¹I]4-iodo-3-methoxy-estra-1,3,5-trien-17-one were synthesized. Ether amino estrone derivatives were obtained from estrone in three steps by means of diazonium compounds. Tissue distribution studies exhibited receptor-mediated uptake in target organs in female Albino Wistar rats. Maximum uptakes for 2-iodo[¹³¹I]-3-methoxy-estrone are in stomach, pancreas, intestines and uterus. A similar biodistribution profile was obtained for 4-iodo[¹³¹I]-3-methoxy-estrone. However 2-iodo-3-methoxy-estra-1,3,5-trien-17-one has higher uptake in stomach, kidneys, pancreas, and intestines than 4-iodo-derivative.     

Radioiodination and biodistribution of isolated lawsone compound from Lawsonia inermis (henna) leaves extract

Lawsonia inermis (henna) is one of the most effective medicinal plants and it has been using for treatment of wounds and burns for centuries. The using of Henna leaves is very popular for cosmetic as well as medicine in many countries. Henna leaves contain lots of different compounds and lawsone (LW) is the main one. In current study, extraction with bidistillated water of henna leaves was performed and LW was isolated by using high performance liquid chromatography system. Chemical structure of LW was evaluated by nuclear magnetic resonance method. LW was radiolabeled with iodine-131 (¹³¹I) radionuclide which is well known for nuclear imaging and therapy in nuclear medicine by utilizing iodogen method. The yield of radiolabeling of LW (¹³¹I-LW) was calculated as 92.70 ± 4.312 % (n = 10) by thin layer radio chromatography. Its in vivo biological activity was investigated by biodistribution studies which were performed by using healthy female and male Balb/C mice. According to results of biodistribution, uptake of ¹³¹I labeled LW compound in uterus, breast and ovary for female mice and prostate in male mice was higher than other organs in the body.     

99mTc-glucoheptonate-guanine: Synthesis, biodistribution and imaging in animals

The aim of the current study was to design a nucleotide-based radiopharmaceutical which could be labeled with ^99mTc and to investigate its radiopharmaceutical efficiency and stability. GHA (glucoheptonate) was used as bifunctional chelate. GHA was labeled with ^99mTc by SnCl₂ reduction method first, and then G (guanine) was conjugated with ^99mTc-GHA at 90 °C. In order to determine its radiopharmaceutical stability, thin layer radio chromatography (TLRC) and electrophoresis were employed. In addition, the results were confirmed using high performance liquid radio chromatography (HPLRC). Scintigraphic imaging was performed on rats with mammary tumors, while tissue distribution was determined on Albino Wistar rats. Labeling yield was found to be over 95% and the labeled complex maintained its stability during the study period. The lipophilicity of the ^99mTc-GHG was measured and the partition coefficient (logP) of the labeled compound calculated. The results demonstrated that the uptake of ^99mTc-GHG (^99mTc-glucoheptonate-guanine) reached its maximum at 3 hours p.i. in stomach and intestines. Main way of excretion was renal. Hepatobiliary excretion was also observed. In conclusion, ^99mTc-GHG may be useful as a nucleotide-based radiopharmaceutical for in vivo applications.