locke solution
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2020 ◽  
Vol 15 (8) ◽  
pp. 1120-1127
Author(s):  
A.L. Alekseev ◽  
◽  
T.V. Alekseeva ◽  

The article presents the results of studies obtained through a comparative assessment of the infusion therapy effectiveness in treating dogs with parvovirus gastroenteritis. The problem of veterinary services for dogs in the conditions of Russian cities is becoming relevant, since in recent years in a number of cities of the Russian Federation outbreaks of natural focal and especially dangerous infections have been noted, when the source of their pathogens were domestic and synanthropic animals living near human dwellings, in economic and industrial objects and directly in urban areas. In connection with the increase in the incidence of parvovirus enteritis in dogs, the damage caused to them, in our country and abroad, the problem of studying this disease is becoming very urgent, as evidenced by numerous literary publications. The use of new drugs with a number of positive properties is limited and the issues of their use in veterinarian practice have not been sufficiently studied. The aim of the research was to carry out a comparative analysis of infusion therapy effectiveness when treating dogs with parvovirus enteritis. The studies were carried out at the “Doktor Aibolit” clinic in Rostov-on-Don. The subjects of the research were dogs with parvovirus enteritis. The initial diagnosis was made on the basis of anamnestic and clinical data, the final diagnosis was made only after laboratory tests and serological diagnostics. According to the principle of analogs, 15 dogs with parvovirus enteritis were selected for the experiment, and 3 groups were formed - 2 experimental and 1 control, 5 dogs each. Treatment of dogs with parvovirus enteritis was carried out in combination with the obligatory prescription of etiotropic and pathogenetic therapy. In 1 experimental group, Reamberin was used 100-200 ml once a day, in group 2 - RingerLocke’s solution; and in animals of the control group we used isotonic sodium chloride solution 0.9%. The effectiveness of infusion therapy in curing dogs with parvovirus gastroenteritis, using Reamberin, showed a 100% result; using a Ringer-Locke solution - 80%; using 0.9% sodium chloride - 60%. Based on the studies carried out, we recommend to use Reamberin at a dose of 100- 200 ml for intravenous infusion once a day for 4-5 days, for the treatment of dogs with parvovirus enteritis, as part of complex therapy.


2020 ◽  
Vol 20 (3) ◽  
pp. 853-869
Author(s):  
Bartosz Jarosław Przybył ◽  
Michał Szlis ◽  
Anna Wójcik-Gładysz

AbstractThe neuromodulatory effects of brain-derived neurotrophic factor (BDNF) on appetite regulation centre peptide gene activity in the sheep hypothalamus have not been examined yet. The aim of this study was to determine whether BDNF participates in modulation of neuropeptide Y (npy), agouti-related peptide (agrp), cocaine and amphetamine regulated transcript (cart), and proopiomelanocortin (pomc) mRNA expression and selected microRNAs in the sheep hypothalamic arcuate (ARC) nucleus. Animals (Polish Merino sheep, n=24) were divided into three groups. The control group received a central infusion of Ringer-Locke solution (480 µl/day) whereas the experimental groups were treated with BDNF in two doses: 10 or 60 μg/480 µl/day. All sheep received four intracerebroventricular infusions (performed from 08:40 a.m. to 01:30 p.m.; infusion scheme: 4 x 50 min infusions with 30 min intervals between them) on each of three consecutive days. Immediately after the last infusion, the sheep were slaughtered, and selected structures of the hypothalamus were frozen for further real-time qPCR analysis. Central infusion of BDNF evoked dose-dependent changes in npy, agrp, cart, pomc and peptidylglicine alpha-amidating monooxygenase (pam) mRNA expression in the sheep ARC nucleus. An increase in npy, agrp and pomc mRNA expression but also a decrease in cart mRNA expression in the ARC nucleus were detected. Moreover, a decrease in pam (gene encoding an enzyme that converts POMC into α-MSH) mRNA expression, was also noted. Furthermore, after central BDNF administration, changes in miRNA-33a-5p, miRNA-33b-5p, miRNA-377-3p, miRNA-214-3p, miRNA-485 and miRNA-488 expression were observed. Based on the presented results, it can be concluded that BDNF may affect the appetite regulating centre activity through modulation of npy, agrp, cart, pomc and pam mRNA expression in the ARC nucleus. It was also revealed that BDNF modulates miRNA expression in the sheep ARC nucleus.


2018 ◽  
Vol 21 (05) ◽  
pp. 933-935
Author(s):  
Naseer Khan Baloch ◽  
Nusrat Jafri ◽  
Ahmed Danyal

… Histamine can stimulate the heart by directly interacting with cardiac histaminereceptors. In the present study we have investigated the H2 receptor activity in isolated rabbitheart. Cimetidine, a specific H2 receptor antagonist was used. The isolated heart was mountedin langendroff apparatus. The heart was perfused at a constant pressure with oxygenatedRinger‘s Locke solution. H2 receptor antagonist produces negative inotropic effect in thepresence of histamine. This indicates that H2 receptors are present in rabbit heart, and plays arole in mediation of positive inotropic effect produced through CAMP by histamine.


2016 ◽  
Vol 36 (3) ◽  
pp. 276-286 ◽  
Author(s):  
VK Saroj ◽  
UP Nakade ◽  
A Sharma ◽  
RS Yadav ◽  
SW Hajare ◽  
...  

Modulation of myometrial spontaneity by cadmium (Cd) and its regulatory pathways was studied in rat uterus in the absence and presence of blockers of different signaling pathways. Isometric tension in myometrial strips, under a resting tension of 1 g, mounted in organ bath containing Ringer–Locke solution (RLS) continuously aerated with carbogen, was measured using data acquisition system-based physiograph and Lab Chart Pro V7.3.7 software. Mean integral tension was measured for 8 min. Cd (1 nM–0.1 mM) not only produced concentration-dependent inhibitory effect on rat myometrium but it (10 µM) also significantly ( p < 0.05) inhibited calcium chloride and BAY K-8644-induced myometrial contraction. Glybenclamide (10 µM), 4-aminopyridine (1 mM), and propranolol (10 µM) failed to significantly attenuate Cd-induced inhibitory responses, while L-NAME (0.1 mM), 1H-[1,2,4]Oxadiazolo[4,3-a]quinoxalin-1-one (ODQ; 25 µM), and 9-(tetrahydro-2-furanyl)-9H-purin-6-amine (SQ 22536; 1 µM) significantly ( p < 0.05) produced inhibitory effects on Cd-induced myometrial relaxation. Phenylephrine (1 nM–10 µM) and salbutamol (0.01 nM–0.1 µM)-induced relaxant effects on rat myometrium were significantly potentiated by 10 µM Cd. Thus based on the results of present functional study, it may be inferred that inhibitory effects of Cd on rat myometrium are mediated through blockade of L-type calcium channels and activation of NOS-NO-sGC and/or AC-cAMP pathways.


1998 ◽  
Vol 88 (1) ◽  
pp. 165-171 ◽  
Author(s):  
Yoshikazu Sai ◽  
Kazuhide Ayajiki ◽  
Tomio Okamura ◽  
Shuichi Nosaka ◽  
Noboru Toda

Background Pancuronium has sympathomimetic actions but does not change or lowers systemic blood pressure in some studies of anesthetized humans and dogs. The present study was done to determine the actions and mechanisms of action of pancuronium on coronary and renal arteries other than those as a sympathomimetic agent. Methods Helical strips of coronary and renal arteries from mongrel dogs were suspended in oxygenated, warmed Ringer-Locke solution, and changes in the isometric tension were recorded. In some strips, transmural electrical stimulation (5 Hz for 40 s) was applied to activate perivascular adrenergic nerves. Results Pancuronium (10[-7] to 10[-5] M) caused dose-dependent relaxation in coronary and renal arteries contracted with prostaglandin (PG) F2alpha, whereas no significant response was induced with vecuronium. The relaxation was endothelium independent and abolished by indomethacin or tranylcypromine, a PGI2 synthase inhibitor. Transmural electrical stimulation caused coronary arterial relaxation, which was augmented by pancuronium and vecuronium. Desipramine also increased the response, and additional potentiation of the response was not elicited by pancuronium and vecuronium. In renal arteries, electrical stimulation caused contraction, which was also augmented by pancuronium and vecuronium. With desipramine treatment, these muscle relaxants did not potentiate the response. Endothelium-dependent coronary arterial relaxation caused by bradykinin was not affected by pancuronium. Conclusions Pancuronium-induced relaxations in canine coronary and renal arteries appear to be mediated by PGI2 released from subendothelial tissues. Potentiations by pancuronium and vecuronium of the response to adrenergic nerve stimulation are expected to be due to an inhibition of the norepinephrine uptake but not to facilitated release of the amine.


1991 ◽  
Vol 98 (1) ◽  
pp. 95-130 ◽  
Author(s):  
T Tamura ◽  
K Nakatani ◽  
K W Yau

Membrane current was recorded from a single primate rod with a suction pipette while the cell was bath perfused with solutions maintained at a temperature of approximately 38 degrees C. A transient inward current was observed at the onset of bright illumination after briefly exposing the outer segment in darkness to Ringer's (Locke) solution containing 3-isobutyl-1-methylxanthine (IBMX), an inhibitor of cGMP phosphodiesterase. After briefly removing external Na+ from around the outer segment in darkness, a similar current was observed upon Na+ restoration in bright light. By analogy to amphibian rods, this inward current was interpreted to represent the activity of an electrogenic Na(+)-dependent Ca2+ efflux, which under physiological conditions in the light is expected to reduce the free Ca2+ in the outer segment and provide negative feedback (the "Ca2+ feedback") to the phototransduction process. The exchange current had a saturated amplitude of up to approximately 5 pA and a decline time course that appeared to have more than one exponential component. In the absence of the Ca2+ feedback, made possible by removing the Ca2+ influx and efflux at the outer segment using a 0 Na(+)-0 Ca2+ external solution, the response of a rod to a dim flash was two to three times larger and had a longer time to peak than in physiological solution. These changes can be approximately accounted for by a simple model describing the Ca2+ feedback in primate rods. The dark hydrolytic rate for cGMP was estimated to be 1.2 s-1. The incremental hydrolytic rate, beta*(t), activated by one photoisomerization was approximately 0.09 s-1 at its peak, with a time-integrated activity, integral of beta*(t)dt, of approximately 0.033, both numbers being derived assuming spatial homogeneity in the outer segment. Finally, we have found that primate rods adapt to light in much the same way as amphibian and other mammalian rods, such as showing a Weber-Fechner relation between flash sensitivity and background light. The Ca2+ feedback model we have constructed can also explain this feature reasonably well.


1980 ◽  
Vol 76 (2) ◽  
pp. 213-231 ◽  
Author(s):  
J E Zengel ◽  
K L Magleby ◽  
J P Horn ◽  
D A McAfee ◽  
P J Yarowsky

The effect of repetitive stimulation on synaptic transmission was studied in the isolated superior cervical ganglion of the rabbit under conditions of reduced quantal content. Excitatory postsynaptic potentials (EPSP) were recorded with the sucrose gap technique to obtain estimates of transmitter release. Four components of increased transmitter release, with time constants of decay similar to those observed at the frog neuromuscular junction at 20 degrees C, were found in the ganglion at 34 degrees C: a first component of facilitation, which decayed with a time constant of 59 +/- 14 ms (mean +/- SD); a second component of facilitation, which decayed with a time constant of 388 +/- 97 ms; augmentation, which decayed with a time constant of 7.2 +/- 1 s; and potentiation, which decayed with a time constant of 88 +/- 25 s. The addition of 0.1-0.2 mM Ba2+ to the Locke solution increased the magnitude but not the time constant of decay of augmentation. Ba2+ had little effect on potentiation. The addition of 0.2-0.8 mM Sr2+ to the Locke solution appeared to increase the magnitude of the second component of facilitation. Sr2+ had little effect on augmentation or potentiation. These selective effects of Ba2+ and Sr2+ on the components of increased transmitter release in the rabbit ganglion are similar to the effects of these ions at the frog neuromuscular junction. Although the effects of Ba2+ and Sr2+ are similar in the two preparations, the magnitudes of augmentation and the second component of facilitation after a single impulse were about 6-10 times greater in the rabbit ganglion than at the frog neuromuscular junction. These results suggest that the underlying mechanisms in the nerve terminal that give rise to the components of increased transmitter release in the rabbit ganglion and frog neuromuscular junction are similar but not identical.


1978 ◽  
Vol 77 (3) ◽  
pp. 427-428
Author(s):  
ANGELA DUTTON ◽  
R. G. DYER ◽  
J. O. YATES

A.R.C. Institute of Animal Physiology, Babraham, Cambridge, CB2 4AT (Received 19 January 1978) Vasopressin is present in nerve terminals of the median eminence (e.g. Silverman & Zimmerman, 1975) and the hormone may possess corticotrophin releasing activity (Pearlmutter, Rapino & Saffran, 1974, 1975). Thus, in experiments designed to investigate the release of peptides from nerve terminals of the median eminence by application of electric stimuli to synaptosomes prepared from mediobasal hypothalamic tissue, we also hoped to establish that vasopressin was secreted from these nerve-endings. Synaptosomes were prepared from tissue obtained from groups of 40 female rats (Gray & Whittaker, 1962) and incubated for 40 min in aerated Locke solution containing 2 mm-bacitracin to minimize peptidase activity. The incubation chamber consisted of an oxygen electrode (Rank Bros, Bottisham, Cambridge) modified to enclose the incubation medium between two silver electrodes. Pulsed stimuli were delivered between these electrodes (5–50 Hz; 1 ms duration; monopolar;


1977 ◽  
Vol 74 (2) ◽  
pp. 193-204
Author(s):  
J. T. BAKER ◽  
S. SOLOMON

A comparison of the renal response to extracellular fluid volume expansion (5% body weight) was made between 25 normal and 25 chronically hypophysectomized rats. The extracellular fluid compartments averaged 25 ± 1% of body weight in both groups during control, fasted conditions. Extracellular fluid volume increased to 33 ± 1% in hypophysectomized and 34 ± 2% in normal rats during expansion, based on body weight. In addition, filtration fraction was similar in both normal and hypophysectomized rats during control (0·29 ± 0·03 and 0·26 ± 0·02 respectively) and infusion of Ringer–Locke solution (0·24 ± 0·05 and 0·27 ± 0·05 respectively). Thus our results cannot be explained by differences in the degree of expansion or failure to increase filtration in proportion to plasma flow. During infusion of isotonic Ringer–Locke solution, fractional water and sodium excretion both averaged 5·1% in normal rats and only 1·3% and 0·82% respectively in hypophysectomized rats. The ratio of single nephron to whole kidney filtration rate failed to increase as much in hypophysectomized compared with normal rats. Significant increases of fractional volume excretion occurred in both groups by the end of the accessible portion of the proximal tubule. However, fractional water reabsorption was depressed significantly more in normal (mean = 37%) than in hypophysectomized rats (mean = 19%). Fractional water reabsorption in distal tubules was similar in both groups during expansion. Arterial pressure was lower in hypophysectomized rats under control conditions, but showed similar changes during expansion compared with normal rats. Passage time decreased significantly in all groups after Ringer–Locke infusion, but remained prolonged in hypophysectomized rats in proximal and distal tubules. It is concluded that chronic hypophysectomy results in a less efficient renal excretion of volume and sodium chloride load. This inefficiency appears to be related in part to (1) failure of the proximal tubule to depress water reabsorption to a level equivalent to normal rats, and (2) failure to re-distribute flow to outer cortical glomeruli following extracellular fluid volume expansion in hypophysectomized rats.


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