RU2488404C1 - Agent improving cardiac resistance to ischemic and following reperfusion injuries - Google Patents

Abstract

FIELD: medicine.

SUBSTANCE: what is presented is the preventive use of an opioid receptor blocker 'CTAP' as an agent improving the cardiac resistance to ischemic and following reperfusion injuries. What is shown is an ability of 'CTAP' to prevent the above injuries (to reduce a necrosis area and a risk area) when introduced 25 min before the 30-minute coronary occlusion and the following 3-hour reperfusion.

EFFECT: invention may be used for creating the new effective agent improving the cardiac resistance to ischemic and following reperfusion injuries.

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Description

The invention relates to the field of experimental medicine and can be used to create a new effective tool that increases the resistance of the heart to ischemic and subsequent reperfusion injuries.

Ischemic-reperfusion injury is the pathophysiological basis of such a socially significant disease as myocardial infarction. In addition, this type of myocardial damage occurs during heart transplantation and is a frequent complication of surgery using cardiopulmonary bypass. The pharmacological agents used in clinical practice are not able to significantly affect ischemic reperfusion damage to the heart. For example, to achieve a 25% reduction in necrosis, a 10-14-day course of mildronate is needed [Sesti C. et al., 2006; Vilskersts R. et al., 2009]. For this reason, the creation of drugs that can prevent ischemic and subsequent reperfusion damage to the heart is an urgent task of pharmacology and cardiology.

The objective of the invention is to expand the arsenal of tools that increase the resistance of the heart to ischemic and subsequent reperfusion injuries.

The presented problem is solved by the prophylactic use of the STAR opioid receptor blocker as a means of increasing myocardial resistance to ischemic and subsequent reperfusion injury.

The used STAR was synthesized by Sigma Aldrich, USA. By its nature, STAR is a cyclic penicylamine-containing octapeptide.

The chemical formula of this compound

D-Phe-Cys-Tyr-D-Trp-Arg-Thr-Pen-Thr-NH2.

STAR structure:

[Pelton J.T. et al., 1986].

The compound is able to inhibit mu-opoid receptors at a dose of 0.5 mg / kg [Abbruscato T.J. et al., 1997]. Previously, this compound has not been used as a medicine.

For the first time, its positive effect was revealed, leading to a decrease in the size of the ischemic-reperfusion necrosis zone.

The cardioprotective effect of mu-opioid receptor activators is currently known [Schultz J.E. et al., 1996]. When studying the receptor mechanisms of action of opioid receptor agonists, it is customary to investigate the effects of pharmacological agents used to block one or another type of receptor. In the course of such studies, it was found that STAR, which was supposed to be used as a pharmacological tool for blocking mu-opioid receptors, in itself has cardioprotective properties.

No information was found in the patent and medical literature that STAR increases the resistance of the heart to reperfusion injuries. This property STAR does not follow from the prior art in this field and is not obvious to a specialist.

The invention can be used in experimental studies to create a new cardioprotective drug; to reduce myocardial damage during ischemia and subsequent reperfusion in patients with acute myocardial infarction, during cardiosurgical interventions using cardiopulmonary bypass and during heart transplantation.

Based on the foregoing, the proposed invention should be considered relevant to the conditions of patentability "novelty", "inventive step", "industrial applicability".

As a comparison drug, the drug naltrexone was selected. It is known that, like STAR, naltrexone is able to block mu-opioid receptors [Takemori A.E., Portoghese P.S., 1992]. These data indicate a similar mechanism of action of the selected substances.

The invention will be clear from the following description.

The experiments were carried out on male Wistar rats weighing 250-300 g. Acute myocardial infarction was caused by occlusion of the left descending coronary artery for 30 min followed by restoration of coronary blood flow for 180 min [Neckar J. et al., 2003]. All rats were anesthetized with sodium pentobarbital (60 mg / kg, Sanofi intraperitoneally) and, for the period of coronary occlusion and subsequent reperfusion, they were connected to an artificial lung ventilation apparatus with 68 breaths / min using a modified AP-AP blood pressure (BP), which was recorded using a pressure sensor SS13L (Biopac System Inc., Goleta, California, USA), coupled with an apparatus for electrophysiological studies MP35 (Biopac System Inc., Goleta, USA). The same apparatus was used to record the ECG. Quantitative processing of the obtained data was carried out using INSTBSL-W software from Biopac System Inc., (Goleta, USA).

A left thoracotomy was performed, the pericardium was removed to gain access to the left descending coronary artery. A ligature was placed on the left descending coronary artery 1-2 mm below the ear of the left atrium. Coronary occlusion was verified by the appearance of epicardial cyanosis and ST segment elevation. After 20 minutes of ischemia, the ligature weakened, while the restoration of blood flow was confirmed by the appearance of epicardial hyperemia. The reperfusion duration was 3 hours. After reperfusion, the hearts were removed and washed with saline through the cannulated aorta, after which the left coronary artery was reocclosed. To determine the risk zone (SR), the myocardium was stained with potassium permanganate through the aorta. To determine the zone of necrosis (ZN), heart sections were made perpendicular to the longitudinal axis with a thickness of 1 mm and stained with a 1% solution of 2,3,5-triphenyl tetrazolium chloride for 30 minutes at 37 ° C. After staining, sections were placed in a 10% solution of neutral formaldehyde for 1 day. After 24 hours, the right ventricle was removed and sections were scanned from both sides using a HP ScanJet G2710 precision scanner. The risk area and the necrosis zone in the images of the slices were determined by a computerized planimetric method. The parameters of planimetric measurements were recalculated into weight and the size of the infarct zone was expressed as a percentage of the size of the hypoperfusion zone.

STAR was dissolved ex tempore in physiological saline and administered intravenously at a dose of 0.5 mg / kg 25 minutes before coronary occlusion (experimental group).

The control was a group of animals that were injected with saline before reperfusion.

The comparison group included 14 rats, which, 25 minutes before the start of coronary occlusion, were injected intravenously with naltexone at a dose of 5 mg / kg. This dosage of naltrexone is used by researchers to block opioid receptors [Takemori A.E., 1992].

The results were processed statistically using the Student t-test for values satisfying the normal distribution, the Wilcoxon-Mann-Whitney U-test for values that do not correspond to the normal distribution, and the x ² criterion to test the average equality hypothesis for frequency tests.

Example. The study of cardioprotective activity of STAR was carried out according to the following scheme. In the group of experimental animals, we took 14 rats, which 25 minutes before coronary occlusion were injected with a solution of the studied drug. As a control group, 20 animals were taken, which, 25 minutes before the start of reperfusion, were administered intravenously a solvent that did not contain STAR (physiological saline). The comparison group consisted of 14 rats, which 25 minutes before the reperfusion started, naltrexone was administered intravenously.

Measurement of blood pressure in rats in the experimental groups did not reveal statistically significant changes in this parameter against the background of administration of STAR or naltrexone both before the onset of coronary occlusion and during coronary occlusion (table 1).

These data indicate that STAR does not worsen the state of hemodynamics during coronary occlusion and subsequent reperfusion.

Study of the cardioprotective effect of STAR. In all the studied groups, after 30-minute coronary occlusion and subsequent 3-hour reperfusion, 38-45% of the total mass of the left ventricle was in a state of hypoperfusion (see table 2), not stained with potassium permanganate. This parameter was taken as the size of the risk zone.

The size of the necrosis zone in the control group of animals was 149.1 ± 23.2 mg, which amounted to 48.1 ± 3.3% of the risk zone.

In the experimental group (STAR administration 25 minutes before coronary occlusion), the size of the necrosis zone was 125.9 ± 19.4 mg (29.5 ± 5.2% of the hypoperfusion zone), which was 16% less than the size of the necrosis zone of the control group in absolute value (with the level of statistical significance p <0.001) and by 39% (p <0.001) by the percentage of the necrosis zone to the risk zone (see table 2).

In the comparison group (administration of naltrexone 25 minutes before coronary occlusion), the size of the necrosis zone was 177.9 ± 25.3 mg (49.7 ± 4.2% of the hypoperfusion zone), which was not statistically significantly different from the values of the control group either in absolute size, nor the percentage of the necrosis zone to the risk zone (see table 2).

Our results indicate that STAR helps to limit the size of the necrosis zone with 30-minute coronary occlusion and subsequent 3-hour reperfusion, that is, it has a cardioprotective effect, significantly greater than the comparison drug, and does not worsen the hemodynamics during ischemia and subsequent reperfusion.

The application of the invention will expand the arsenal of agents that increase the resistance of the heart to ischemic and subsequent reperfusion injuries.

Table 1 Blood pressure parameters in experimental animals with a 20-minute coronary occlusion BEFORE CORONAROCCLUSION CORONAROCLUSION 20 min Heart rate GARDEN DBP Wed HELL RPP Heart rate GARDEN DBP Wed HELL RPP Control (n = 20) 335.9 ± 8 115.8 ± 2.7 98.6 ± 2.9 107.2 ± 2.8 36.0 ± 0.02 329.3 ± 8.8 112.8 ± 3.2 96.8 ± 3.9 104.8 ± 3.55 34.5 ± 0.03 STAR (n = 14) 325.1 ± 10.1 115 ± 2.8 97.9 ± 3.3 106.5 ± 3.05 34.6 ÷ 0.03 326 ± 11 113.8 ± 2.9 99.6 ± 2.6 106.7 ± 2.75 34.8 ± 0.03 Naltrexone (n = 14) 329.1 ± 10.1 119 ± 2.8 99.7 ± 3.3 109.35 ± 3.05 35.9 ÷ 0.03 326 ± 11 113.8 ± 2.9 89.6 ± 2.6 98.95 ± 2.75 32.3 ± 0.03 Heart rate - heart rate; GARDEN - systolic blood pressure; DBP - diastolic blood pressure; Avg BP - mean arterial pressure; RPP - productive heart rate index * Avg.AD / 1000.

table 2 The size of the necrosis zone with a 30-minute coronary occlusion and subsequent 180-minute reperfusion in rats. The effects of STAR and naltrexone Series n LV, mg ZR, mg ZR / LV,% ZN, mg ZN / ZR,% The control twenty 867.6 ± 50.1 331.7 ± 29.9 38.23 ± 3.25 159.5 ± 23.2 48.1 ± 3.3 STAR 0.5 mg / kg fourteen 947.8 ± 64.6 427.0 ± 46.4 45.05 ± 4.32 125.9 ± 19.4 29.5 ± 5.2 p1 <0.001 P2 <0.001 Naltrexone 5 mg / kg fourteen 895.3 ± 46.4 358.1 ± 30.2 40.0 ± 2.56 177.9 ± 25.3 49.7 ± 4.2 Note: LV - the mass of the left ventricle; ЗР - weight of the risk zone; ZR / LV - the ratio of the mass of the risk zone and the mass of the left ventricle, expressed in%; ZN - the mass of the necrosis zone; ZN / ZR - the ratio of the mass of the necrosis zone and the mass of the risk zone, expressed in%. p1 is the level of statistical significance of differences relative to the control group; P2 is the level of statistical significance of differences relative to the comparison group.

LITERATURE

Abbruscato, T.J. Blood-brain barrier permeability and bioavailability of a highly potent and mu-selective opioid receptor antagonist STAR: comparison with morphine. / T.J. Abbruscato, S.A. Thomas, V.J. Hruby, T.P. Davis // J. Pharmacol. Exp. Ther. - 1997. - V.280. - P.402.

Neckar, J. Cardioprotective effect of chronic hypoxia is blunted by concomitant hypercapnia / J. Neckar, O. Szarszoi, J. Herget, B. Ostadal, F. Kolar. // Physiol. Res. - 2003. - V. 52. - P.171-175.

Pelton, J.T. Design and synthesis of conformationally constrained somatostatin analogues with high potency and specificity for mu opioid receptors. / J.T. Pelton, W. Kazmierski, K. Gulya, H.I. Yamamura, V.J. Hruby // J Med Chem. - 1986. - V.29; N No. 11. - P.2370-2375.

Schultz, J.E.J. Morphine mimics the cardioprotective effect of ischemic preconditioning via a glibenclamide-sensitive mechanism in the rat heart. / J.E.J. Schultz, A.K. Hsu, G.J. Gross // Circ Res. - 1996. - V.78; N6. - 1100-1104.

Sesti, C, Simkhovich BZ, Kalvinsh I, Kloner RA. Mildronate, a novel fatty acid oxidation inhibitor and antianginal agent, reduces myocardial infarct size without affecting hemodynamics. / B.Z. Simkhovich, I. Kalvinsh, R.A. Kloner // J Cardiovasc Pharmacol .. - 2006. - Mar; V.47; Number 3). - P.:493-499.

Takemori, A.E. Selective naltrexone-derived opioid receptor antagonists / A.E. Takemori, P.S. Portoghese // Annu. Rev. Pharmacol Toxicol. Annual Reviews Inc. -1992.-V. 32. -P. 239-269.

Vilskersts, R., Liepinsh E, Kuka J, Cirule H, Veveris M, Kalvinsh I, Dambrova M. Myocardial infarct size-limiting and anti-arrhythmic effects of mildronate orotate in the rat heart. / R. Vilskersts, E. Liepinsh, J. Kuka, H. Cirule, M. Veveris, I. Kalvinsh, M. Dambrova // Cardiovasc Drugs Ther. -. 2009. - Aug; V.23; No. (4.-) P.:281-288.

Claims (1)

Prophylactic use of the STAR opioid receptor blocker as a means of increasing the resistance of the heart to ischemic and subsequent reperfusion injuries.