[Synthesis of a cyclic enkephalin analog with prolonged action]. / Sintez tsiklicheskogo analoga énkefalina prolongirovannogo deistviia.

A cyclic analog of enkephalin, cyclo(Lys-Tyr-DMet-Gly-Phe-Pro-) and two corresponding linear hexapeptides with lysine residue on the N- and C-termini of the pentapeptide sequence, Lys-Tyr-DMet-Gly-Phe-Pro and Tyr-DMet-Gly-Phe-Pro-Lys were synthesized by classical and solid phase methods of peptide chemistry. The cyclic analog exhibited significantly prolonged analgesic effect, evaluated by the "tail pinch" method after intracysternal injection to mice. The cycloanalog also had a weak influence on the peripheral opiate receptors of the isolated segment of guinea pig iliac intestine. Addition of the lysine residue to the N-terminus of the pentapeptide sequence enhanced by an order of magnitude the selectivity of binding of the analog with opiate receptors of mu-type.

[Antagonistic properties of tetra-substituted analog of vasopressin with selective antidiuretic effects]. / Antagonisticheskie svoistva chetyrekhzameshchennogo analoga vazopressina s selektivnym antidiureticheskim deistviem.

Biological properties of a novel vasopressin analogue were investigated. It was found that this analogue has no vasopressor and oxytocic activities but it exhibits a selective antidiuretic effect which is weaker than that of adiuretin (DDAVP). Novel analogue inhibits vasopressor, oxytocic and antidiuretic effects caused by arginine--vasopressin. The usefulness of novel compound as a pharmacological tool--vasopressin antagonist is suggested.

[The slowing of the extinction of a conditioned reaction and the antiamnesic action of arginine vasopressin and des-glycine-(8-arginine) vasopressin]. / Zamedlenie ugasheniia uslovnoi reaktsii i antiamnezicheskoe deistvie arginin-vazopressina i dez-glitsin-(8-arginin)-vazopressina.

In the experiments on mice there were analysed the effects of arginine-vasopressin (AVP) and its analogue des-glycine-arginine-vasopressin (DG-AVP) on the extinction of the conditioned reaction of passive avoidance and the reproduction of memory trace in amnesia caused by detaining the animal in the dangerous section of the unit after electrocutaneous stimulation. An increase of resistance of the conditioned reaction to a sharp extinction at systemic administration of AVP and DG-AVP was shown.

Tritiation of [8-L-arginine, 9-desglycineamide] vasopressin.

Tritiated vasopressin analogue, [8-L-arginine, 9-desglycineamide]-vasopressin was prepared from its diiodo-derivative by means of catalytic reductive dehalogenation. The reaction products were purified by reversed-phase HPLC resulting in a labelled peptide with high specific radioactivity (629 TBq/mmol).

[Synthesis and pharmacological properties of des-9-glycine analogs of [Orn8]vasopressin]. / Sintez i farmakologicheskie svoistva dez-9-glitsinovykh analogov [Orn8]vazopressina.

Three new analogues of vasopressin, viz. des-Gly9-[Phe2, Orn8]vasopressin, diglycyl-des-Gly9-[Phe2, Orn8]vasopressin, and diglycyl-des-Gly9-[Val4, Orn8]vasopressin, were synthesized to investigate the structure-function relationship. Hormonal (vasopressor, antidiuretic, uterotonic, galactogogic) activities of the new compounds were determined, their effect on elaboration and retention of the active avoidance behaviour in rats was studied.

[Study of the spatial structure of des-Gly9-[Arg8]vasopressin by two-dimensional NMR spectroscopy and theoretical conformation analysis]. / Issledovanie prostranstvennoi struktury des-Gly9-[Arg8]vazopressina metodami dvumernoi spektroskopii IaMR i teoreticheskogo konformatsionnogo analiza.

2D 1H-NMR spectra of des-Gly9-[Arg8]vasopressin in dimethylsulfoxide have been taken and the 1H resonances have been assigned. The coupling constants and amide proton temperature coefficients (delta delta/delta T) have been measured and the NOE cross-peaks in the NOESY spectrum have been analyzed. The most essential information on the spatial structure of des-Gly9-[Arg8]vasopressin is extracted from the low delta delta/delta T value for Asn5 amide proton and from the NOE between the Cys1 and Cys6 alpha-protons. A diminished accessibility of the Asn5 NH proton for the solvent is ascribed to the presence of a beta-turn in the fragment 2-5. The distance between the Cys1 and Cys6 C alpha H protons seems to be less than 4 A. These constraints were taken into account in the conformational analysis of the title peptide. The derived set of the low-energy backbone conformations was analyzed against the background of the all available NMR data. The most probable conformation of the cyclic moiety in des-Gly9-[Arg8]vasopressin was found to be the type III beta-turn. The corner positions are occupied by the residues 3, 4, while the residues 1-2 and 5-6 are at the extended sites. Some NMR data indicate that this structure is in a dynamic equilibrium with other minor conformers.

[Non-classic effects of luliberin confirming the pleiotropy of neuropeptides]. / "Neklassicheskie" éffekty liuliberina, podtverzhdaiushchie mnogoadresnost' neiropeptidov.

The effects of synthetic neuropeptide LH-RH and its analogues were studied in experiments on 174 white male rats. The influence of the substances was shown on instrumental avoidance learning in Y-shaped maze. Convulsive and anticonvulsive effects of the preparations were studied on experimental model of corasol seizures. The analgetic effect of the substances was evaluated by behavioural pain reaction to electrical stimulation of the tail root. Analgetic, anticonvulsive, and psychostimulating LH-RH properties confirm polyfunctionality and "pleiotropy" of neuropeptides as a class of new endogenous informational compounds.

[Effect of desglycine-arginine vasopressin on the excitability of the command neurons of the defensive reflex in the edible snail]. / Vliianie dezglitsinarginin-vazopressina na vozbudimost' komandnykh neironov oboronitel'nogo refleksa vinogradnoi ulitki.

Perfusion of the snail (Helix lucorum L.) CNS with DG-AVP (concentration 10(-6) M) in the course of low frequency intracellular stimulation (2-4-minute interval) of the defensive reflex command neurons led to an increase in the excitability. It was expressed both in the reduction of the spike generation latency, in the increased number of spikes in response to fixed stimuli, and in the activation of pacemaker potentials. If DG-AVP was added to the medium during endoneuronal habituation, there was no increase in the excitability. It is supposed that modification of the neuronal excitability may be caused by the DG-AVP effect on the pacemaker mechanism.

[Use of vasopressin the treatment of the paranoid form of schizophrenia]. / Primenenie vazopressina v terapii bol'nykh paranoidnoi formoi shizofrenii.

Forty-seven males suffering from paranoid schizophrenia running a paroxysm-like progressive course were treated with the synthetic neuropeptide arginine-vasopressin, a hormone of the posterior lobe of the hypophysis. The therapeutic effect of the hormone was confirmed by a complex of clinical, laboratory and pathopsychological techniques. Both objective methods of investigation and subjective assessment of the patients demonstrated a high efficacy of the drug which was expressed in a marked psychoenergizing action, a beneficial effect on emotional disorders, a memory improvement and a favourable influence on the apatho-abulic manifestations.

[Relation between the effects of the memory neuromodulator arginine-vasopressin and the levels of activity of the serotonin-, dopamine- and noradrenergic systems of the brain]. / Zavisimost' éffektov neiromoduliatora pamiati arginin-vazopressina ot urovnia aktivnosti serotonin-, dofamin- i noradrenergicheskoi sistem mozga.

The effect of vasopressin on learning, habituation and habit recovery in rat before and after electrolytic ablation of locus coeruleus, nuclei dorsalis et medialis raphe and pars compacta substantiae nigrae was studied by behavioural methods. The rats were learned with positive reinforcement in a T-shaped maze and with negative reinforcement in a U-shaped maze. It was found that improvement of trace consolidation and acceleration of learning were in many cases dependent on the activity level of the dophaminergic, noradrenergic and to a lesser degree on that of serotoninergic brain systems.