Action of diclofenac on kidney mitochondria and cells

The mitochondrial membrane potential measured in isolated rat kidney mitochondria and in digitonin-permeabilized MDCK type II cells pre-energized with succinate, glutamate, and/or malate was reduced by micromolar diclofenac dose-dependently. However, ATP biosynthesis from glutamate/malate was significantly more compromised compared to that from succinate. Inhibition of the malate-aspartate shuttle by diclofenac with a resultant decrease in the ability of mitochondria to generate NAD(P)H was demonstrated. Diclofenac however had no effect on the activities of NADH dehydrogenase, glutamate dehydrogenase, and malate dehydrogenase. In conclusion, decreased NAD(P)H production due to an inhibition of the entry of malate and glutamate via the malate-aspartate shuttle explained the more pronounced decreased rate of ATP biosynthesis from glutamate and malate by diclofenac. This drug, therefore affects the bioavailability of two major respiratory complex I substrates which would normally contribute substantially to supplying the reducing equivalents for mitochondrial electron transport for generation of ATP in the renal cell.     

The effect of pressure and cooling rate on spermatoza, kidney tissue, and the whole kidney

Application of high hydrostatic pressure as a cryoprotective was evaluated for the bovine sperm cell, kidney tissue, and the whole kidney. Spermatozoa samples were pressurized between 172 and 1724 bar for various lengths of time. The effect of pressure and cooling at 5 °C/min, 35 °C/min, and 55 °C/min to ?60 °C was investigated. Application of pressure to sperm cells resulted in extensive damage, as shown by a decrease in motility, an increase in morphological a bnormalities, and the release of enzymes. Freezing of sperm cells, kidney tissue, and the whole kidney under high pressure was significantly more damaging than freezing at the same rates at atmospheric pressure. Pressure did not act as a cryoprotective agent but instead led to gross cellular damage, either when applied at 4 °C or during freeze-thaw procedures.     

Effect of ethmozine on kidney function

Injection of ethmozine to rats (50 mg/kg subcutaneously) and to dogs (0,5 mg/kg intravenously) produced a substantial rise in diuresis, natriuresis and kaliuresis at the expense of the increased glomerular filtration rate and renal circulation. Injection of ethmozine (0.25-1.0 mg/min for 20 min) to the renal artery of dogs had no effect on the ipsilateral side. It is assumed that alterations in renal function induced by ethmozine injection are extrarenal in nature.     

Studies on esterase histochemistry of amphibian kidney

Summary In the hope that the histochemical picture of the kidney may help to understand its role in excretion and osmoregulation, an effort is here made to study the distribution of esterases in amphibian kidney.The kidneys of adults and tadpoles of the frog, Rana tigrina and the toad, Bufo melanostictus were used for this study. Some of these animals were subjected to dehydration for 3–4 days and to the effect of 150 mM NaCl for 8–12 days before their kidneys were used. The esterases were visualised using tweens, naphthol esters and 5-bromoindoxyl acetate as substrates. These were accompanied by activator/inhibitor studies.Very interesting results were obtained in the distribution of the esterases. Tween esterase and -naphthyl acetate esterase were found in the proximal tubules of the adult frog kidney only while 5-bromoindoxyl acetate esterase was found to be present in all the animals tested. On the other hand, naphthol AS acetate esterase was absent in the tadpole stages of the frog and toad. Further 5-bromoindoxyl acetate esterase and naphthol AS acetate esterase were demonstrated in the glomeruli of frogs and toads subjected to NaCl solution. Activator/ inhibitor studies helped in characteristically differentiating these different esterases.There seems to be a relationship between the distribution of the different esterases and the excretory and osmoregulatory adaptations of these animals which differ in the adult and tadpole stages and in the experimental conditions mentioned. The possible implications of the esterase distribution is discussed in considerable details.U.G.C. Research Scholar.     

Effects of aging on the kidney.

A host of abnormalities of renal structure and function accompany advancing age. This presentation briefly surveys the renal anatomical and functional changes associated with senescence. Four areas of renal functional change have been selected for in-depth discussion: a) renal blood flow; b) glomerular filtration rate; c) renal sodium handling; and d) renal concentrating ability. The methodologic considerations including population selection which confound the assessment of the effects of aging on renal function are discussed. In addition, the functional changes associated with senescence are discussed in the context of longitudinal studies and studies utilizing appropriate patient cohorts, including potential kidney transplant donors. The clinical implications of senescent changes with regard to adjusting "normative" standards to fit the age of the patient are addressed. Furthermore, the implications of age-related renal functional alterations in predisposing the elderly patient to a number of fluid and electrolyte derangements are considered.--Epstein, M. Effects of aging on the kidney.     

安南龟肝脏和肾脏的组织学观察

采用常规石蜡切片对安南龟的肝脏和肾脏进行了组织学观察。研究结果发现,肝脏分为3叶,肝实质内结缔组织少。肝脏由无数肝小叶构成,肝小叶分界不清。肝细胞为多角形的腺上皮细胞,细胞核圆球形,位于中央。胆小管沿着肝细胞索向肝小叶四周放射并连成细长的微细管道。肾脏由肾小体、颈段、近曲小管、中间段、远曲小管和收集管6部分构成,肾小体由肾小球和肾小囊组成,在肾小体附近可见致密斑样结构,未见髓袢结构。肾小球由盘曲的毛细血管构成。肾小囊是肾小管的起始端,由内、外两层壁层构成,内层与肾小球的毛细血管紧贴,外层为单层扁平上皮细胞。     

Effects of testosterone on renal ornithine decarboxylase and kidney function

Testosterone injection caused a 2,000% increase in renal ornithine decarboxylase activity in intact male mice. A single injection of testosterone produced the same effect as repeated injections. The response was dose-dependent and could be blocked by actinomycin, diaminopropane, and cadaverine. Cycloheximide and putrescine had no inhibitory effect. Renal ODC response to arginine vasopressin was altered after castration; however, urine specific gravity and serum osmolality were unaffected by changes in renal ornithine decarboxylase activity.