Cerebroprotective properties of recombinant interleukin-1 receptor – an experimental study
Authors:
Katherine Shchokina; Vira Ulanova; Svitlana Drogovoz
Published in:
Čes. slov. Farm., 2022; 71, 34-40
Category:
Original Article
doi:
https://doi.org/https://doi.org/10.5817/CSF2022-1-34
Overview
Optimization of therapy of cerebrovascular disorders (CVD) is one of the most critical health problems. The current treatment regimen of CVD turns out to be often insufficient. Search for new drugs with cerebroprotective and antihypoxic properties is an essential task of modern medicine and pharmacy. Attention to cytokine mechanisms of ischemic brain damage in clinics and experimental research has been increased recently. Interleukin-1 (IL-1) receptor blockade is a perspective way of cerebroprotection that requires a more profound study of its mechanisms. The article contains the results of a study of cerebroprotective and antihypoxic properties of the recombinant IL-1 antagonist raleukin on a model of bilateral carotid occlusion in rats. Recombinant receptor antagonist IL-1 raleukin (15 mg/kg) did not affect basal blood flow in the internal carotid artery of intact group animals. Still, it prevented its decrease approximately three times in case of occlusion of both common carotid arteries followed by reperfusion. Indicators of the cerebroprotective effect of studied medication were reducing the acidotic blood shift flowing from the brain of animals with irreversible bilateral carotid occlusion, neuronal degradation, and weakening.
Keywords:
Cerebral ischemia – interleukin-1 – raleukin – bilateral carotid occlusion – neuron-specific enolase
Introduction
Optimization of therapy of cerebrovascular disorders (CVD) is one of the most important health problems1). The current treatment regimen of CVD turns out to be often insufficient2). Search for new drugs with cerebroprotective and anti-hypoxic properties is an essential task of modern medicine and pharmacy.
Attention to cytokine mechanisms of ischemic brain damage in the clinic and experiment has recently increased. Interleukin-1 (IL-1) exhibits a rapid manifestation which causes leukocytic infiltration and neurotoxicity (apoptosis)3, 4). There is strong evidence of interrelation between receptor antagonists IL-1 and correction of cerebrovascular disorders5, 6).
Early research findings showed that raleukin, the original recombinant antagonist of IL-1 receptors of Highly Pure Biochemicals (St. Petersburg, Russia), increases survival rate in rats with bilateral carotid occlusion (BCO), reduces symptoms of cerebrocardial syndrome, strengthens resistance to hypoxia, and decreases the level of toxic and traumatic brain injury7–9). Thus, IL-1 receptor blockade is a perspective way of cerebroprotection that requires a more profound study of its mechanisms. According to the data shown, it is supposed not to be limited to improving energy metabolism in the brain10, 11). Raleukin effect on cerebral blood flow in normal and CVD at cerebral ischemia that induces acid-base shift and level of neuron destruction have not been investigated thoroughly.
Experimental part
The experiments were performed on white male rats of the Wistar line, 200–220 grams of weight each. Experimental animals were kept under sanitary and hygienic standards in compliance with the principles of Directive 2010/63/EU of the European Parliament and of the Council «On the protection of animals used for scientific purposes» (Brussels, 2010), the Law of Ukraine «On Animal Protection» from brutal driving № 3477-IV of 21.02.2006 (as amended) and the Order of the Ministry of Education and Science of Ukraine About the statement of the Order of carrying out by scientific institutions of experiments, experiments on animals № 249 from 01.03.2012, as evidenced by the conclusion of the commission on bioethics of the National University of Pharmacy. Procedures that caused pain or suffering of animals were performed under anesthesia (xylazine i/m 5 mg/kg, thiopental intraperitoneally 40–70 mg/kg.
Raleukin (St. Petersburg Research Institute OCHBP) used in a conventionally-effective dose of 15 mg/kg2, 12), administered daily subcutaneously for three days, last 30–40 minutes before CVD modeling. Cardiovascular disorder of ischemic type in the forebrain was reproduced by BCO13).
In the first series of experiments, the dynamic of cerebral blood flow in ischemic conditions was followed by reperfusion determination. For this action, vessels were dissected, provisional ligatures were summed, and a superimposed ultrasonic flowmeter sensor 106 T (Transonic Systems Inc., USA) was applied on the left internal carotid artery. After hemodynamic stabilization, basal blood flow was measured, the right common carotid artery was ligated, and a miniature clamp was applied on the left common carotid artery for 40 minutes, which stopped cerebral blood flow from the carotid completely. After 40 min, the clip was removed, and blood flow in the left internal carotid artery was measured in the dynamic of reperfusion for 60 min. Vinpocetine was selected as a reference drug (Cavinton, Gedeon Richter, Hungary)14, 15) administered in a dose of 5 mg/kg i.p. in the same way as raleukin.
Raleukin was administered in rats with irreversible BCO at the above-mentioned scheme in the second series of experiments. After 1-day indices, acid-base balance was measured by an analyzer «Radiometer» (Denmark). The blood (0.2–0.3 mL) was collected from the sigmoid sinus into a heparinized syringe and stored at 3–4 °C no more than 15 minutes before analysis. The content of neuron-specific enolase (NSE) in blood was measured by ELISA using a kit NSE EIA KIT (DAI, USA) «Hipson» firm device (Czech Republic). The release of NSE (2-phospho-D glycerate hydrolyse, EC 4.2.1.11) from neurons into the spinal CSF and blood is an important marker of neural tissue damage degree16). NSE level in serum of patients with CVD correlates with the volume of cerebral infarction17).
At the end of the experiment, microscopic examinations were performed. The functional state of neurons was analyzed in 3–5 layers of the cortex. In these sections, the number of neuronal and glial cells was counted on a standard area in 5 replicates (approx. 7, lens 40), and the glioneuronal index was determined. The micro-preparations were examined under a Mikros 400 microscope, and the images were microphotographed with a Nikon Cool Pix 4500 digital camera. The photographs were processed on a computer using Nikon View 5 software.
The obtained data of inner group differences were evaluated by pairwise Wilcoxon test, inner group differences by the Student t-criterion, absence of a normal distribution by White Browse, evaluation in an alternative form by angular Fischer transformation.
Results and discussion
Neither raleukin nor vinpocetine affected basal blood flow in the internal carotid artery. Indicators in corresponding groups had no significant differences from those in the control one with a 6–7% (Table 1). Brain reperfusion in test groups after 40 min of ischemia varied considerably. In the control group, the flow rate in the internal carotid artery decreased on average by more than 50% relative to the basal level. After raleukin and vinpocetine administration, blood flow was restored significantly, reduction of ischemia was 18–19% and 9–11%, respectively (p < 0,001 compared to the control group). The decrease in the vinpocetine group was minimal, but the absolute blood flow in raleukin and vinpocetine groups had no significant differences (Table 1).
Statistically significant differences (p < 0.05).
n – the number of animals in the group
* with the initial state within the group (for pairwise Wilcoxon test)
# with simultaneous indication of the control group
^ with a synchronous indicator of the group receiving raleukin
Thus, blockade of IL-1 receptors in CVD influences the state of blood vessels, enhancing blood supply to the brain after removing the vascular occlusion approximately at the vinpocetine level. This cerebroprotection mechanism in cerebral ischemia can be considered to be a primary one because violation of energy metabolism is caused by ischemia. Along with this, raleukin increases resistance to brain hypoxia of nonischemic origin18, 19).
Blockade of IL-1 receptors as evidenced by measurement of cerebral blood flow (Table 1) significantly reduced the degree of cerebral ischemia in the acute phase.
Cerebral ischemia provoked severe metabolic acidosis. In the control pathology group, after 1 day of BCO pH decreased and CO2 partial pressure increased in venous blood flowing from the brain (Table 2). A decrease in hemoglobin and oxygen saturation of blood, a significant shortage of buffer base deficiency catches attention in this case. These results do not align with the data of moderate respiratory alkalosis due to hyperventilation in rats with BCO (15, 20). Reasons for differences are likely to be that in the mentioned study, the acid-base balance was measured in arterial blood 35 minutes after BCO, while we defined it in the venous blood of the sigmoid sinus in 1 day after BCO when the mechanism of compensatory hyperventilation was exhausted.
Statistically significant differences (p < 0.05).
n – the number of animals in the group, that pCO2 pO2 – partial pressure of CO2 and O2, Hb – hemoglobin, AB – actual
bicarbonate, BE – buffer base deficiency, BBS – the sum of the of buffer bases, SB – standard bicarbonate.
* with a group of control.
# a group of control pathology
Raleukin took away acid-base balance disorders at vinpocetine level (Table 2). It agrees with its property to reduce lactate accumulation in experimental cerebral ischemia1, 20).
According to Table 3, in rats of the control pathology group after 1 day, BCO NSE activity increased by 11.2 times on average –from 0.61 ng/ml to 6.86 ng/ml (p < 0.001), strongly indicating neurons destruction. After raleukin administration this index increased only by 3.43 ng/ml (p < 0.001). Thus, raleukin reduced the destruction of neurons with slight concession to Vinpocetine l (producing an effect close to Vinpocetine with the average activity of 2.34 ng/mL).
The morphological features of the sensorimotor cortex (SMC) of the large hemispheres of the rat brain were studied a day after BCO. As shown by microscopy, in intact (pseudo-operated) animals, the cytoarchitectonics of the cerebral cortex was typical (Fig. 1, 2). Different layers of nerve cells were quite clearly traced: molecular, outer granular, outer pyramidal, inner granular, inner pyramidal, and polymorphic. The neuropil had an unstructured appearance. The cells in the layers varied in size, shape, volume of the neuroplasm, and density.
Vessels of the pia mater of the usual type, capillaries penetrating the brain tissue, mostly with good turgor, plethoric, pericapillary spaces are insignificant. The cell body had a fairly clear, even contour. Neuroplasm does not have signs of vacuolization. The nucleus of neurons is rounded, predominantly centrally located; the chromatin is uncondensed. The nucleolus is one localized in the center of the nucleus. The glioneuronal index corresponds to the norm for this animal species21).
One day after the modeling of ischemic brain injury, pathological changes were observed in the cerebral hemispheres. The vessels of the pia mater are plethoric; in some places, small hemorrhages are visible. Venous vessels are dilated full-blooded (Fig. 3). In the neuropil, there are signs of impaired synaptic patency (the appearance of rarefaction); there are areas with ganglion cell emptying. Some of the capillaries are also full-blooded (sometimes diapedesis of erythrocytes is seen pericapillary); others are in a state of spasm. They pronounced perivascular and pericellular edema. Glioneuronal index significantly increased by 1.3 times.
Prophylactic administration of raleukin to a certain extent prevented the development and severity of pathological changes in rat brains during cerebral ischemia modeling. Hemorrhages into the pia mater or brain tissue were not observed, although the pia mater vessels themselves were plethoric. There were no areas of rarefaction in the neuropil, fewer areas with ganglion cell desolation. Perivascular and pericellular edema were less pronounced (Fig. 4). Perineuronal glial satelliteosis was less pronounced, especially the accumulation of glial cells around one neuron. There were no multicellular accumulations of glial cells. The glioneuronal index was significantly lower relative to the control pathology.
In rats that were prophylactically injected with the compared drug vinpocetine, the pia mater was fullblooded in places with hemorrhages; in addition, single small hemorrhages were observed in the brain tissue. There were no disturbances in the state of the neuropil. Signs of vasogenic edema varied (Fig. 5). In satelitosis, the accumulation of glial cells around one neuron quite often took place. The severity of the homotypic arrangement of cells decreased compared to the control pathology. Multicellular accumulations of glial cells were absent. The glioneuronal index decreased compared to the control pathology.
According to morphological features, it can be stated that BCO of the common carotid arteries causes significant reactive changes in the cerebral hemispheres of the rat. A day after the simulation of cerebral ischemia, vasogenic edema of the brain tissue, destruction of varying severity neurons, decreased functional activity, reduced reserve energy and plastic resources of nerve cells, and signs of impaired synaptic conduction were noted. In addition, there was a proliferation of glial elements activation of satelitosis, which, together with an increase in cases of damage and death of nerve cells, also refers to pronounced reactive processes.
Prophylactic administration of raleukin reduces the degree of reactive changes in the SMS of the cerebral hemispheres of rats. It has been established that the number of cells with focal chromatolysis, cytoplasm vacuolization, shadow cells, and neuronophagia signs slightly decrease, and the number of functionally active cells increases. Proliferative manifestations of glial elements and manifestations of vasogenic edema are also reduced. All of the above indicates that raleukin has cerebroprotective properties. Vinpocetine also moderately reduces the manifestations of reactive processes in the SMC of the cerebral hemispheres of rats after modeling ischemic disorders.
Thus, cerebroprotective raleukin action followed by reperfusion on model BCO starts with cerebral circulation intensification, weakening the ischemic cascade. On condition of irreversible BCO, raleukin contributes to the normalization of cerebral metabolism and performs antiacidotic action, proved by the state of the acid-base balance in blood flowing from the brain. The integral protective effect of raleukin on the ischemic brain shows a decrease in the activity of marker enzyme destruction of neurons by two times – NSE. It extends the concept of neuroprotective action mechanism of IL-1 receptor antagonists.
Conclusion
Recombinant receptor antagonist IL-1 raleukin 15 mg/kg did not affect basal blood flow in the internal carotid artery of intact group animals. Still, it prevents its decrease approximately by three times in case of occlusion of both common carotid arteries followed by reperfusion. Indicators of the cerebroprotective effect of studied medication reduce the acidotic blood shift flowing from the brain of animals with irreversible bilateral carotid occlusion, neuronal degradation, and weakening. Thus interleukin-1 receptor antagonist has cerebroprotective properties. These were obtained by other authors as well7, 15, 22), and they are based on the first proved marker neuronal degradation – neuron enolase. The cerebroprotective properties of raleukin are also confirmed by the data of histopathological studies. It has been proved that the cerebroprotective effect of raleukin is not inferior to the comparison drug vinpocetine in terms of the severity of morphological features.
Conflict of interest: none.
Katherine Shchokina, V. Ulanova, S Drogovoz
National University of Pharmacy, Kharkiv, Ukraine Department of Pharmacology and Pharmacotherapy of the National University of Pharmacy Pushkinska St. 53, 61002 Kharkiv, Ukraine
e-mail: acya@ukr.net
Received November 18, 2021 / Accepted February 4, 2021
Sources
1. Shchokіna K. G, Simbirtsev A. S., Ishenko A. M. Shtrygol S., Drogovoz S. Cerebroprotective properties of interleukin 1 receptor antagonist in models of brain lesions of different genesis. Cytokines and inflammation 2012; 1, 52–58.
2. Helmy A., Guilfoyle M. R., Carpenter K. L., Pickard J. D., Menon D. K., Hutchinson P. J. Recombinant human interleukin-1 receptor antagonist in severe traumatic brain injury: a phase II randomized control trial. J. Cereb. Blood. Flow Metab. 2014; 34(5), 845–851. https://doi. org/10.1038/jcbfm.2014.23
3. Fahey E., Doyle S. L. IL-1 family cytokine regulation of vascular permeability and angiogenesis. Front. Immunol. 2019; 10, 1423. https://doi.org/10.3389/fimmu. 2019.01426.
4. Simi A., Tsakiri N., Wang P., Rothwell N. J. Interleukin-1 and inflammatory neurodegeneration. Biochem. Soc. Trans. 2007; 35 (5), 1122–1126. https://doi.org/10.1042/ BST0351122
5. Patent UA 96037 (51) IPC (2011) А61K 38/20. The use of recombinant antagonist of interleukin-1 receptors (ARIL-1) as an antialcoholic agent / K. G. Shchokіna, S. Y. Shtrigol, O. M. Іschenko, No u 200912496; appl. 03.12.2009; publ. 26.09.2011.
6. Greenhalgh A. D., Galea J., Dénes A., Tyrrell P. J., Rothwell N. J. Rapid brain penetration of interleukin-1 receptor antagonist in rat cerebral ischaemia: pharmacokinetics, distribution, protection. Br. J. Pharmacol. 2010; 160, 153–159. https://doi.org/10.1111/j.1476- 5381.2010.00684.x
7. Patent UA 31373 on utility model IPC (2006) A61K 35/66 The use of an antagonist of interleukin-1 receptors as a means of cerebroprotective action / Suprun E. V., Shtrigol S. Y., Іschenko O. M., Suprun O. S. – No u200711672; appl. 22.10.2007; publ. 10.04.2008; Bull. No 7.
8. Patent UA 33402 on utility model IPC (2006) A61K 38/20 The use of an antagonist of interleukin-1 receptors as a means of antihypoxic action / Suprun E. V., Shtrigol S. Y., Іschenko O. M., Suprun O. S. – No u200800473; appl. 14.01.2008; publ. 25.06.2008; Bull. No 12.
9. Banwell V., Sena E. S., Macleod M. R. Systematic review and stratified meta-analysis of the efficacy of interleukin- 1 receptor antagonist in animal models of stroke. J. Stroke Cerebrovasc. Dis. 2009; 18(4), 269–276. https:// doi.org/10.1016/j.jstrokecerebrovasdis.2008.11.009
10. Xia Y. Y., Song S. W., Min Y., Zhong Y., Sheng Y. C., Li R. P. The effects of anakinra on focal cerebral ischemic injury in rats. CNS Neurosci. Ther. 2014; 20, 879–881. https:// doi.org/10.1111/cns.12310
11. Pradillo J. M., Denes A., Greenhalgh A. D. Delayed administration of interleukin-1 receptor antagonist reduces ischemic brain damage and inflammation in comorbid rats. J. Cereb. Blood Flow Metab. 2012; 32(9), 1810–1819. https://doi.org/10.1038/jcbfm.2012.101
12. Mulcahy N. J., Ross J., Rothwell N. J., Loddick S. A. Delayed administration of interleukin-1 receptor antagonist protects against transient cerebral ischaemia in the rat. Br. J. Pharmacol. 2003; 140, 471–476. https://doi. org/10.1038/sj.bjp.0705462
13. Mironov A. N. Manual on experimental (preclinical) study of new pharmacological substances. Moscow: IIA «Remedium» 2012.
14. Ghajari M., Hellyer P. J., Sharp D. J. Computational modelling of traumatic brain injury predicts the location of chronic traumatic encephalopathy pathology. Brain 2017; 140 (2), 333–343. https://doi.org/10.1093/brain/ aww317
15. Garcia J. H., Liu K. F., Relton J. K. Interleukin-1 receptor antagonist decreases the number of necrotic neurons in rats with middle cerebral artery occlusion. Am. J. Pathol. 1995; 147, 1477–1486.
16. Haupt W. F., Chopan G., Sobesky J., Liu W.C., Dohmen C. Prognostic value of somatosensory evoked potentials, neuron-specific enolase, and S100 for short-term outcome in ischemic stroke. J. Neurophysiol. 2016; 115, 1273–1278. https://doi. org/10.1152/jn.01012.2015
17. Anand N., Stead L. G. Neuron-specific enolase as a marker for acute ischemic stroke: a systematic review. Cerebrovasc. Dis. 2005; 20(4), 213–219. https://doi. org/10.1159/000087701
18. Basu A., Krady J. K., O’Malley M. The type 1 interleukin- 1 receptor is essential for the efficient activation of microglia and the induction of multiple proinflammatory mediators in response to brain injury. J. Neurosci. 2002; 22(14), 6071–6082. https://doi.org/10.1523/JNEUROSCI. 22-14-06071.2002
19. Thom J. G., Reeder E. L., Collins S. M., Gopalan P., Robson M. J. Contributions of interleukin-1 receptor signaling in traumatic brain injury. Front. Behav. Neurosci. 2020; 13, 287. https://doi.org/10.3389/fnbeh. 2019.00287
20. Loddick S. A., Rothwell N. J. Neuroprotective effects of human recombinant interleukin-1 receptor antagonist in focal cerebral ischaemia in the rat. J. Cereb. Blood Flow Metab. 1996; 16, 932–940. https://doi. org/10.1097/00004647-199609000-00017
21. Belayev L., Alonso O. F., Busto R., Zhao W., Ginsberg, M. D. Middle cerebral artery occlusion in the rat by intraluminal suture. Neurological and pathological evaluation of an improved model. Stroke 1996; 27, 1616–1622. https://doi.org/10.1161/01. str.27.9.1616
22. Lee J. H., Kam E. H., Kim J. M., Kim S. Y., Kim E. J., Cheon S. Y., Koo B. N. Intranasal Administration of Interleukin-1 Receptor Antagonist in a Transient Focal Cerebral Ischemia Rat. Model. Biomol. Ther. (Seoul) 2017; 25(2), 149–157. https://doi.org/10.4062/biomolther. 2016.050
Labels
Pharmacy Clinical pharmacologyArticle was published in
Czech and Slovak Pharmacy
2022 Issue 1
Most read in this issue
- Ethical and legal requirements for vaccination against COVID-19
- The role of individuals receiving health care – terminological notes
- Surviving of production probiotic strains in a selected application form
- Colour and antioxidant activity of honey