Inhibition by tetanus and botulinum A toxin of the release of [3H]noradrenaline and [3H]GABA from rat brain homogenate

Rat brain homogenate was preloaded with [3H]noradrenaline or [3H]GABA and stimulated with high K+. Tetanus toxin and botulinum A neurotoxin partially prevent the evoked [3H]noradrenaline release in the same range of toxin concentrations starting below 10(-10) M. In contrast, release of gamma-amino butyric acid (GABA) is much more sensitive to tetanus than to botulinum A toxin.     

Binding of [3H]GABA and [3H]muscimol to subcellular particles of a neurone-enriched culture of mouse brain

Summary Binding of [³H]GABA and [³H]muscimol, indicative of GABA-receptors, has been demonstrated in a neurone-enriched culture of embryonic mouse brain using a ligand-binding technique. Evidence is provided for the existence of different populations of GABA-receptors.This study was supported by C.N.R.S., ATP N^o 3356 and by Commissariat à l'Energie Atomique, Departement of Biologie. Thanks are due to Mlle Marie-Anne Frenkel for her excellent technical assistance.     

Presence of specific binding sites for [3H]sarcophytol-A in cultured human skin fibroblasts

Summary The presence of specific binding sites for [³H]sarcophytol-A in human skin fibroblasts was examined using biochemical and morphological methods. The displacement studies clearly revealed that high (K_D=31.0 nM) and low (K_D=6.05 M) affinity sites were present in the intact cells. Moreover, autoradiographic studies using light microscopy revealed that the specific binding sites may exist in boththe cytoplasm and the nuclei.     

Multiple daily amphetamine administration decreases both [3H]agoinst and [3]antagonist dopamine receptor binding

Summary Multiple daily amphetamine injections in rats decreased both [³H]agonist as well as [³H]antagonist striatal dopamine receptor binding. Concurrently, these animals exhibited a decrease in striatal dopamine concentration and, paradoxically, an enhancement of behavioral responsivity.This study was supported by PHS grant MH32990 to I.C. and DA0156805 to D.S.I. Creese and D. Segal are the recipients of the RSDA grants MH00316-01 and RSDA MH70183-08, respectively.     

Effects of a new cholecystokinin antagonist (GE 410) on the smooth muscle of the guinea pig ileum

Summary Suc-Tyr-(SE)-Met-Gly-Trp-Met-Asp--phenethylamide (GE 410) competitively antagonized the contractions of smooth muscle strips from guinea pig ileum (pA₂=7.6, n=0.95) induced by cholecystokinin-octapeptide (CCK8). GE 410 inhibited the electrically-induced cholinergically mediated contractile responses and the [³H]ACh release in the ileum, as well as the CCK-stimulated electrical contractile responses and the [³H]ACh release in the cholinergic nerve terminals. The results suggest the existence of CCK-receptors not only in the smooth muscles but also on the neurons.     

Synthesis and some characteristics of [13C]-specially enriched tetragastrin and the related compound

Summary [¹³C]-enriched tetragastrin and the related compound were synthesized in solution. Conversion of S-[¹³C]-methylated tetragastrin to the enriched tetragastrin gave 10.5 ppm upfield chemical shift of C resonance. The potency of the synthetic tetragastrin to stimulate gastric acid secretion was virtually identical with that of pentagastrin (ICI).Acknowledgment. A part of this research was supported by scientific research funds (No. 944059, 048253) from the Japanese Ministry of Education.     

Effect of local anaesthetics on the accumulation of [3H]-Metaraminol by rabbit atria and vasa deferentia

Zusammenfassung Es wurde die Wirkung von Lokalanästhetika auf die Anhäufung von [³H]-Metaraminol im Vorhofmuskel und Vas deferens des Kaninchens untersucht. Die von Kokain hervorgerufene Hemmung der [³H]-Metaraminol-Akkumulation ist mindestens hundertmal stärker als diejenige nach Procain, Prilocain und Lidocain.

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Supported by a grant-in-aid from the Medical Research Council of Canada. The author is indebted to Astra Pharmaceuticals (Canada) Ltd. for supplies of lidocaine hydrochloride and prilocaine hydrochloride.     

Decrease in [3H]ouabain binding sites in heart and brain from spontaneously hypertensive rats

Summary A decrease in the number of binding sites (B_max) for [³H]ouabain was observed in the heart (37%) and the brain (22%) of spontaneously hypertensive rats (SHR) when compared with age-matched control Wistar Kyoto rats. No variation was detected in the affinity constant (K_D).     

7a-Aza-B-homo[7a, 7-d]tetrazole analogues of progesterone and testosterone

Summary The tetrazole analogues of progesterone and testosterone, namely, 7a-aza-B-homo-4-pregneno[7a, 7-d]tetrazole-3,20-dione (5) and 3-oxo-7a-aza-B-homo-4-androsteno[7a, 7-d]tetrazol-17-yl acetate (8), have been prepared which are worthy of biological testing.Part XLIII in the series Steroids and Related Studies. For Part XLII see H. Singh and K.K. Bhutani, Indian J. Chem. in press.     

The biliary excretion of [3H] lysergic acid diethylamide in Wistar and gunn rats

Summary The biliary excretion of [³H] LSD was studied in Wistar and homozygous Gunn rats. In Wistar rats approximately 46% of the given dose was recovered from bile in 2.5 h whilst in the homozygous Gunn rat 26% was recovered in the same time period. In both strains the main metabolites were glucuronides.     

LSD: The distribution of [3H]LSD in the reproductive system of the male rat and placental transfer in the female rat

Summary After administration of [³H]LSD to male rats, radioactivity was present in all tissues of the reproductive system, notably associated with spermatozoa in the epididymis. In addition, in pregnant rats LSD and/or metabolites readily crossed the placental barrier.     

Zinc antagonizes the effect of botulinum type A toxin at the mouse neuromuscular junction

Summary Zn²⁺ (10–100 M) elevated the frequency of miniature end-plate potentials (MEPPs) in the mouse diaphragm. The effect did not depend on external Ca²⁺. Botulinum type A toxin (BTX_A, 50 ng/ml) abolished MEPPs almost completely within 30 min. Zn²⁺ (100 M) restored MEPPs and increased their frequency after they had been abolished by BTX_A in Ca²⁺-free solutions. The antagonistic effect of Zn²⁺ in the Ca²⁺-free solution was reduced by exposing the diaphragm to the toxin in the Ca²⁺-free solutions containing high K⁺. Thus, the action of BTX_A is probably enhanced by depolarization of the motor nerve terminals.     

Labelling of steroids in axillary sweat after administration of3H-Δ5-pregnenolone and14C-progesterone to a healthy man

Résumé L'administration intraveineuse du prégnène-3-ol-20-one[7-³H]- ⁵ avec le progestérone[4-¹⁴C] à un homme sain amena la sécrétion d'autant de radioactivité dans la sueur des aiselles que dans la plupart du reste du corps. Le prégnénolone- ⁵, l'androstène-3,17-dione- ⁴ et le déhydroépiandrostérone furent les principaux stéroïdes marqués identifiés comme partant des deux sources de sueur.

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Acknowledgments. The author expresses grateful thanks to the subject (A.C.) who subjected himself to this experiment, and to Mr. D. A. A.Wilson for his technical assistance.     

The localization of [3H]-desipramine in central nerve terminals studied with electron microscope autoradiography and subcellular fractionation

Summary The cellular and subcellular distribution of [³H]-desipramine (DMI) in rat brain was studied by electron microscope (EM) autoradiography and by subcellular fractionation. A considerable proportion of label was found to be bound to the membranes of presynaptic nerve terminals, as well as to sites inside those terminals.Acknowledgment. The authors are most grateful to Mr and Mrs Gudelsky for their generous support.     

Effect of tingenone,a quinonoid triterpene,on growth and macromolecule biosynthesis inTrypanosoma cruzi

Summary Tingenone and horminone, two natural quinonoid substances, inhibited the in vitro growth ofTrypanosoma cruzi, 30 M drug concentration producing total inhibition of growth. Tingenone inhibited total uptake and incorporation of [³H]thymidine, [³H]uridine, L-[³H]leucine into parasite macromolecules. Other quinonoids assayed were either less effective (abruquinone A) or even quite inactive (visminone B and ferruginin B). Investigation of several mechanisms for the cytotoxic action of tingenone pointed to the interaction with DNA as the most likely factor involved. Tingenone also inhibited the growth ofCrithidia fasciculata, but the drug was significantly less active on this organism than onT. cruzi.This work was supported by grants of UNDP/World Bank/World Health Organization Special Programme for Research and Training in Tropical Diseases, Organization of American States (Multinational Programme of Biochemistry) and Programa Nacional de Enfermedades Endémicas (SECYT), República Argentina. A preliminary account was given at the Workshop on Oxidative Damage and Related Enzymes, Frascatti (Italy), 1983.     

Na*-independent binding of [3H] muscimol to a membrane fraction of the brains of normal and dwarf mice

Summary Although their body weights were decreased by about 77% and their brain weights by about 30%, high-affinity [³H] muscimol binding to a cerebral membrane fraction was not altered in hereditary pituitary dwarf mice. Marked changes in the level of pituitary growth-associated hormones do not appear to be associated with a change in cerebral GABA-receptors.Supported by a UNESCO/IBRO Fellowship. Permanent address: Semmelweis University Medical School, 1st Institute of Biochemistry, Budapest, Hungary.     

Maternal vitamin A restriction alters biochemical development of the brain in rats

Summary The biochemical development of the fetal brain in relation to maternal vitamin A restriction was studied in rats. The vitamin A status of pregnant rats was varied by supplying low, medium and adequate amounts (6, 40, and 100 g retinol/day/kg body weight, respectively) of vitamin A during pregnancy and suckling. The maternal vitamin A restriction caused an altered brain development in terms of tissue weight, DNA, RNA and protein levels, and biosynthesis of DNA and protein from [³H]-thymidine and [³H]-leucine, respectively. A dose-dependent effect of maternal vitamin A restriction on the metabolism of DNA, RNA and protein was noticed in the developing fetal brain of rats.     

Synthesis of L-[3-2H,18O]glycerol and its incorporation into the 4-methyl-5-hydroxyethyl thiazole moiety of thiamine byEscherichia coli

Summary L-[3-²H,¹⁸O]glycerol was prepared and fed toEscherichia coli in order to determine the origin of the oxygen atom in the biosynthesized thiazole moiety of thiamine. Measurement by GC-MS of the isotope incorporation into the thiazole from this substrate confirmed that the 2 hydrogens and the oxygen on the C-3 carbon of glycerol are incorporated directly into the thiazole.     

Light evoked release of radioactivity from rabbit retinas preloaded with (3H)-GABA

Summary Light flashes evoke an increased release of radioactivity in vitro from rabbit retinas preloaded with (³H)-GABA in vivo. Constant light does not affect the release. No light evoked release can be demonstrated from the glia. Pentobarbitone and AOAA depress the evoked release. The results are consistent with GABA being a retinal neurotransmitter, most likely in a class of amacrines.This work was supported by grants from the Swedish Medical Research Council (project 04X2321), The Faculty of Medicine, University of Lund, Royal Physiographic Society.     

3[H]-Sulpiride labels mesolimbic non-dopaminergic sites that bind antidepressant drugs

3[H]-(-)-Sulpiride and 3[H]-spiperone binding was compared in rat amygdala, nucleus accumbens and striatum, using (+/-)-sulpiride to define specific binding. 3[H]-(-)-Sulpiride bound to twice as many sites in amygdala and nucleus accumbens as 3[H]-spiperone. 3[H]-(-)-Sulpiride binding was directed to these additional sites by using 1 microM spiperone to mask dopaminergic binding. The binding of 3[H]-(-)-sulpiride to these sites was high affinity, reversible, Na+-dependent, but not stereospecific. Metoclopramide, tiapride and antidepressant medications, but not other neuroleptics, ADTN, or serotonin displaced 3[H]-(-)-sulpiride binding to these sites. These data suggest that 3[H]-(-)-sulpiride labels mesolimbic sites other than dopamine receptors which may mediate antidepressant effects.