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Study of the effect of acetylsalicylic acid and a selective arginase II inhibitor KUD 975 on the correction of hemostatic disorders in experimental preeclampsia 乙酰水杨酸和精氨酸酶II选择性抑制剂KUD975对实验性先兆子痫止血障碍的影响
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-07-12 DOI: 10.3897/rrpharmacology.8.87539
A. V. Gureeva, O. Severinova, V. Gureev, I. S. Kochkarova, E. V. Avdeyeva
Introduction: The disruption of the functional state of the vascular endothelium is among the main causes of preeclampsia, which is one of the most common causes of maternal and perinatal mortality. It can be enhanced by the humoral factors secreted by the activated platelets. The use of acetylsalicylic acid is an effective way to prevent preeclampsia. However, its ability to activate eNOS is a prerequisite for researching its ability to correct the disorders in developing preeclampsia, including by reducing the platelet activity. In this case its effect can be enhanced through increasing the bioavailability of L-arginine by using a selective arginase II inhibitor KUD 975. These facts were the prerequisite for conducting this study. Materials and methods: The study was conducted on 180 female Wistar rats weighing 250–300 g. Acetylsalicylic acid was used at a dose of 7 mg/kg/day and 10 mg/kg/day, KUD 975 – at a dose of 1 mg/kg/day and 3 mg/kg/day. Adenosine diphosphate (ADP, 6.5 microns), arachidonic acid (ASPI, 0.5 mM), and collagen (3.2 mcg/ml) were used as aggregation inducers. Results and discussion: ADMA-like preeclampsia simulation led to an increase in platelet aggregation ability when using all aggregation inducers. This is evidenced by an increase in a degree, rate of aggregation, and a shortened time of thrombus formation. The use of acetylsalicylic acid and a selective arginase II inhibitor KUD 975 led to a decrease in the aggregation ability of platelets and an increase in thrombosis time, while the combined administration of the studied agents showed a more pronounced effect. Conclusion: The data obtained while performing a series of experiments strongly indicate a promising outlook for using acetylsalicylic acid and a selective arginase II inhibitor KUD 975 in order to correct emerging disorders in preeclampsia.
简介:血管内皮功能状态的破坏是子痫前期的主要原因之一,子痫前期是孕产妇和围产期死亡的最常见原因之一。活化血小板分泌的体液因子可增强其活性。使用乙酰水杨酸是预防先兆子痫的有效方法。然而,其激活eNOS的能力是研究其纠正发生子痫前期疾病的能力的先决条件,包括通过降低血小板活性。在这种情况下,可以通过使用选择性精氨酸酶II抑制剂KUD 975提高l -精氨酸的生物利用度来增强其效果。这些事实是进行这项研究的先决条件。材料与方法:选用雌性Wistar大鼠180只,体重250 ~ 300 g。乙酰水杨酸的剂量分别为7mg /kg/天和10mg /kg/天,KUD 975的剂量分别为1mg /kg/天和3mg /kg/天。二磷酸腺苷(ADP, 6.5微米)、花生四烯酸(ASPI, 0.5 mM)和胶原(3.2 mcg/ml)作为聚集诱导剂。结果和讨论:当使用所有的聚集诱导剂时,adma样子痫前期模拟导致血小板聚集能力的增加。这可以从血栓形成的程度、聚集速度和时间缩短来证明。使用乙酰水杨酸和选择性精氨酸酶II抑制剂KUD 975导致血小板聚集能力下降,血栓形成时间增加,而联合使用所研究的药物效果更明显。结论:在进行一系列实验时获得的数据强烈表明,乙酰水杨酸和选择性精氨酸酶II抑制剂KUD 975在纠正子痫前期出现的疾病方面具有良好的前景。
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引用次数: 0
Involvement of monoaminergic system in the antidepressant effect of 3-substituted thietane-1,1-dioxide derivative Involvement单胺能系统中3-取代硫烷-1,1-二氧化物衍生物的抗抑郁作用
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-30 DOI: 10.3897/rrpharmacology.8.81007
I. Nikitina, G. G. Gaisina
Introduction: The aim of the study was to assess the involvement of the monoaminergic system in the antidepressant effect of a new 3-substituted thietane-1,1-dioxide derivative (N-199/1) using tests with several pharmacological antagonists and agonists. Materials and methods: We conducted 3 sets of experiments in white outbred male mice. In Experiment 1, we assessed the antidepressant effect of N-199/1 in the forced swimming test (FST) and tail suspension test (TST) when administered repeatedly for 2 weeks intraperitoneally (i.p.). In Experiment 2, we evaluated the antidepressant effect of N-199/1 in FST and TST when co-administered with 5HT1A- (WAY100635, 0.1 mg/kg), 5HT2A/2C- (ketanserin, 5 mg/kg), 5HT3- (ondansetron, 1 mg/kg) serotonergic and α2-adrenergic (yohimbine, 1 mg/kg) receptors antagonists. In Experiment 3, we assessed the effect of N-199/1 on the hypothermia induced by i.p. injection of α2-adrenergic receptors agonist clonidine (0.3 mg/kg). Results and discussion: N-199/1 reduced immobility time (IT) and index of depression (ID) in FST, and did not affect IT in TST, either when administered repeatedly in Experiment 1, or acutely in Experiment 2. In Experiment 2, ketanserin enhanced the effect of N-199/1, decreasing ID by 36%, while WAY100635 and yohimbine antagonized it, increasing ID by 27% and IT by 115%, respectively, in comparison with N-199/1. N-199/1 attenuated the effect of ondansetron, increasing IT by 36%. In Experiment, 3 N-199/1 reduced clonidine-induced hypothermia 1 h after the injection of clonidine. N-199/1 exhibited pronounced antidepressant properties in FST, an agonism to 5HT1A-receptors and an antagonism to 5HT2A/2C- and α2-receptors in tests of neuropharmacological interaction, which indicates an atypical mechanism of its antidepressant action. Conclusion: The antidepressant effect of N-199/1 is due to the stimulation of 5HT1A-receptors and blockade of 5HT2A/2C- and α2-receptors. Graphical abstract:
简介:本研究的目的是评估单胺能系统参与新的3-取代硫代烷-1,1-二氧化物衍生物(N-199/1)的抗抑郁作用,使用几种药理学拮抗剂和激动剂进行试验。材料和方法:我们在白色远交系雄性小鼠中进行了3组实验。在实验1中,我们评估了N-199/1在强迫游泳试验(FST)和悬尾试验(TST)中连续2周反复腹腔(i.p)给药的抗抑郁效果。在实验2中,我们评估了N-199/1与5HT1A- (WAY100635, 0.1 mg/kg)、5HT2A/2C-(酮色林,5 mg/kg)、5HT3-(昂丹西酮,1 mg/kg) 5 -羟色胺能和α - 2-肾上腺素能(育亨本,1 mg/kg)受体拮抗剂共同给药时对FST和TST的抗抑郁作用。实验3观察N-199/1对ig注射α2-肾上腺素能受体激动剂可乐定(0.3 mg/kg)致大鼠低温的影响。结果和讨论:N-199/1减少了FST中的静止时间(IT)和抑郁指数(ID),并且在实验1中反复给药或在实验2中急性给药时对TST中的IT没有影响。在实验2中,酮色林增强了N-199/1的作用,使ID降低了36%,而WAY100635和育亨宾对其有拮抗作用,使ID和it分别比N-199/1提高27%和115%。N-199/1减弱了昂丹司琼的作用,使IT增加36%。实验中,3 N-199/1在注射可乐定1 h后降低了可乐定引起的低温。N-199/1在FST中表现出明显的抗抑郁特性,在神经药理相互作用试验中对5ht1a受体具有激动作用,对5HT2A/2C-和α2受体具有拮抗作用,这表明其抗抑郁作用机制不典型。结论:N-199/1的抗抑郁作用可能与刺激5ht1a受体,阻断5HT2A/2C-和α2受体有关。图形化的简介:
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引用次数: 1
Combined anti-mediator therapy for severe destructive forms of acute necrotizing pancreatitis in rats 联合抗介质治疗大鼠严重破坏性急性坏死性胰腺炎
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-30 DOI: 10.3897/rrpharmacology.8.79939
T. Firsova, S. A. Alekhin, D. P. Nazarenko, L. Danilenko, Antonina G. Chub, E. Malyutina, T. Lazareva, L. V. Druzhikin
Introduction: Inflammatory mediators play a major role in pathogenesis of acute pancreatitis with TNF (tumor necrosis factor) as the most important one. Development of effective combined therapy could help to decrease tissue damage, improve results and, finally, diminish the mortality rate in this severe pathology. Materials and methods: All the studies were performed on 120 female white Wistar rats, weighing 250±25g. Acute pancreatitis reproduced by an intracanalicular injection of bile salts compound. Results and discussion: The data obtained in the course of the study on the pronounced pancreatoprotective effect of infliximab are explained by its key role in the onset of the systemic inflammatory response, and, therefore, with the blockade of tumor necrosis factor alpha in the early stages, there is no pronounced secondary damage to the pancreas, which is reflected in a significant decrease in edema from 4.87±0.03 in the model up to 2.75±0.04, and as a consequence, an improvement in the blood supply of the acinar tissue from 182.38±15.92 PU up to 287.92±14.64 PU, which is expressed in a decrease in the zones of necrosis and in a decrease in mortality and, finally, efficiency coefficient from 13480.000 to 4283.348. A selective blocker of cysteinyl leukotrienes has a less pronounced protective reaction against damage to pancreatocytes, but to a much greater extent than octreotide. That is expressed by changes in the efficiency coefficient to the level of 8621.18 in montelukast group and 12767.30 in octreotide group, respectively. On the other hand, the effect of the use of infliximab does not surpass that of montelukast, and their combined use has a pronounced additive effect, which is proved by the efficiency coefficient at the level of 2390.33. This reaction is explained by the fact that TNF alpha-mediated pathway of activation of leukotriene biosynthesis is the main, but not the only one. Conclusion: The combined anti-mediator therapy provides a great opportunity to improve the standard therapy of acute pancreatitis.
简介:炎症介质在急性胰腺炎发病中起重要作用,其中肿瘤坏死因子(TNF)是最重要的炎症介质。开发有效的联合疗法可以帮助减少组织损伤,改善结果,并最终降低这种严重病理的死亡率。材料与方法:实验选用雌性Wistar大鼠120只,体重250±25g。急性胰腺炎由胆盐化合物静脉注射引起。结果与讨论:在研究过程中所获得的关于英夫利昔单抗明显的胰腺保护作用的数据可以通过其在全身炎症反应发生中的关键作用来解释,因此,在早期阻断肿瘤坏死因子α的情况下,胰腺没有明显的继发性损伤,这体现在水肿从模型中的4.87±0.03显著降低到2.75±0.04,因此,腺泡组织血供从182.38±15.92 PU提高到287.92±14.64 PU,表现为坏死区域的减少和死亡率的降低,最后,效率系数从13480.000提高到4283.348。选择性半胱氨酸白三烯阻滞剂对胰腺细胞损伤的保护作用不那么明显,但比奥曲肽的保护作用要大得多。孟鲁司特组的效率系数为8621.18,奥曲肽组的效率系数为12767.30。另一方面,英夫利昔单抗的使用效果并没有超过孟鲁司特,两者联合使用具有明显的加性效应,效率系数在2390.33水平证明了这一点。这一反应可以解释为TNF α介导的白三烯生物合成激活途径是主要的,但不是唯一的。结论:联合抗介质治疗为提高急性胰腺炎的标准治疗提供了良好的契机。
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引用次数: 0
Current view on the problem of treating fibrocystic breast disease in terms of herbal medicine Current中药治疗纤维囊性乳腺疾病问题的看法
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-22 DOI: 10.3897/rrpharmacology.8.79286
O. P. Sokolik, G. Prozorova
Introduction: Fibrocystic breast disease, commonly called fibrocystic breasts or fibrocystic change, is a benign (noncancerous) condition, which is the most common pathology in women of reproductive age. Treatment of fibrocystic breast disease and concomitant pathologies can involve using herbs. Materials and Methods: To make an analysis of literary sources on the development of fibrocystic breast disease in the pathogenesis of diseases of the female reproductive system (clinical human (75%) and animal studies (25%)) were published in the period of 2017–2021. Results and discussion: The diversity of plants in the world is a promising ground for therapeutic improvisation, allowing for an individual approach to each patient, but, most importantly, creates possibilities for maneuvering in the event of ineffectiveness of any means. In some situations, herbal medicine is not only possible or permissible, but strictly mandatory, and is essentially the only effective therapeutic method, which is relatively safe provided the correct selection of combinations and control by a doctor who applies a certain method of phytotherapy, especially given a duration of treatment. The need for a deeper study is long overdue for the pharmacological capabilities of various plant raw materials in the treatment of not only this pathology, but others as well. Conclusion: The development of phytotherapy should be based primarily on scientific developments, but this area can not be considered the prerogative of only phytotherapists, as herbal medicines should be in the arsenal of doctors of all specialties.
简介:纤维囊性乳腺疾病,通常称为纤维囊性乳房或纤维囊性改变,是一种良性(非癌症)疾病,是育龄妇女最常见的病理。乳腺纤维囊性疾病和伴随病变的治疗可以使用草药。材料和方法:分析2017-2021年期间发表的关于乳腺纤维囊性疾病在女性生殖系统疾病发病机制中的发展的文献来源(临床人类研究(75%)和动物研究(25%))。结果和讨论:世界上植物的多样性是即兴治疗的一个很有前景的基础,允许对每个患者采取单独的方法,但最重要的是,在任何方法无效的情况下,都创造了操纵的可能性。在某些情况下,草药不仅是可能的或允许的,而且是严格强制性的,而且基本上是唯一有效的治疗方法,如果医生采用某种植物治疗方法,特别是在治疗持续时间内,正确选择组合和控制,草药是相对安全的。早就应该对各种植物原料的药理能力进行更深入的研究,不仅可以治疗这种病理,还可以治疗其他病理。结论:植物疗法的发展应该主要基于科学发展,但这一领域不能被视为只有植物治疗师的特权,因为草药应该在所有专业的医生手中。
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引用次数: 0
Searching for novel antagonists of adenosine A1 receptors among azolo[1,5-a]pyrimidine nitro derivatives 偶氮[1,5-a]嘧啶硝基衍生物中腺苷A1受体的新型拮抗剂Searching
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-15 DOI: 10.3897/rrpharmacology.8.77854
D. Yakovlev, P. Vassiliev, Ya. V. Agatsarskaya, A. A. Brigadirova, K. T. Sultanova, M. Skripka, A. Spasov, K. Savateev, V. Rusinov, D. Maltsev
Introduction: Ligands of adenosine A1Rs are potential candidates for the development of drugs for the treatment of paroxysmal supraventricular tachycardia, angina pectoris, hypertriglyceridemia, type 2 diabetes mellitus, neuropathic pain, and heart failure. At the same time, there is a deficiency of drugs that can regulate the functions of A1 receptors. A number of A1-antagonists are at the various stages of clinical trials; other drugs are not very selective or are characterized by an insufficient breadth of their therapeutic action. Therefore, the search for new medicinal compounds for the prevention and treatment of A1-depended diseases among nitro derivatives of tetrazolo[1,5-a]pyrimidine and 1,2,4-triazolo[1,5-a]pyrimidine is of scientific interest. Materials and methods: The search for active compounds was carried out by in silico and in vitro methods. At the first stage, a computer forecast of A1-antagonistic activity was carried out using the Microcosm BioS software. At the second stage, the prediction results were verified in vitro in a model of isolated mouse atria. Results and discussion: Based on the results of the prediction by the method of maximum similarity to standards, the most active compounds III, VIII, and XVII were selected. After testing the prediction results by the isolated atria method, the compound VIII was characterized by A1-blocking effect in vitro at a concentration of 10 μmol/L. Conclusion: The most promising compound with A1-blocking effect in vitro was identified; it is a derivative of tetrazolo[1,5-a]pyrimidine under the code of VIII. It is of interest for us for further in-depth study of its pharmacological properties.
引言:腺苷A1Rs配体是开发治疗阵发性室上性心动过速、心绞痛、高甘油三酯血症、2型糖尿病、神经性疼痛和心力衰竭的药物的潜在候选者。同时,缺乏能够调节A1受体功能的药物。许多A1拮抗剂处于临床试验的不同阶段;其他药物的选择性不是很强,或者其治疗作用的广度不够。因此,在四唑并[1,5-a]嘧啶的硝基衍生物和1,2,4-三唑并[1,5-a]嘧啶 具有科学意义。材料与方法:采用体外和体外两种方法对活性化合物进行了筛选。在第一阶段,使用Microcosm BioS软件对A1拮抗活性进行计算机预测。在第二阶段,在离体小鼠心房模型中验证了预测结果。结果和讨论:基于与标准物最大相似性方法的预测结果,选择了最具活性的化合物III、VIII和XVII。通过离体心房法检测预测结果,化合物VIII在10μmol/L浓度下具有A1阻断作用。结论:筛选出最有前景的A1阻断化合物;它是四唑并[1,5-a]嘧啶的衍生物,代码为VIII。对其药理性质的进一步深入研究具有重要意义。
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引用次数: 1
Genetically modified animal models of hereditary diseases for testing of gene-directed therapy Genetically改良遗传性疾病动物模型用于基因导向治疗试验
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-14 DOI: 10.3897/rrpharmacology.8.82618
A. Polikarpova, T. Egorova, M. Bardina
Disease-causing genes have been identified for many severe muscular and neurological genetic disorders. Advances in the gene therapy field offer promising solutions for drug development to treat these life-threatening conditions. Depending on how the mutation affects the function of the gene product, different gene therapy approaches may be beneficial. Gene replacement therapy is appropriate for diseases caused by mutations that result in the deficiency of the functional protein. Gene suppression strategy is suggested for disorders caused by the toxic product of the mutant gene. Splicing modulators, genome editing, and base editing techniques can be applied to disorders with different types of underlying mutations. Testing potential drugs in animal models of human diseases is an indispensable step of development. Given the specific gene therapy approach, appropriate animal models can be generated using a variety of technologies ranging from transgenesis to precise genome editing. In this review, we discuss technologies used to generate small and large animal models of the most common muscular and neurological genetic disorders. We specifically focus on animal models that were used to test gene therapies based on adeno-associated vectors and antisense nucleotides.
致病基因已被鉴定为许多严重的肌肉和神经遗传疾病。基因治疗领域的进展为治疗这些危及生命的疾病的药物开发提供了有前景的解决方案。根据突变如何影响基因产物的功能,不同的基因治疗方法可能是有益的。基因替代疗法适用于由导致功能蛋白缺乏的突变引起的疾病。对于由突变基因的毒性产物引起的疾病,建议采用基因抑制策略。剪接调节剂、基因组编辑和碱基编辑技术可以应用于具有不同类型潜在突变的疾病。在人类疾病的动物模型中测试潜在药物是开发中不可或缺的一步。考虑到特定的基因治疗方法,可以使用从转基因到精确基因组编辑的各种技术生成合适的动物模型。在这篇综述中,我们讨论了用于生成最常见的肌肉和神经遗传疾病的小型和大型动物模型的技术。我们特别关注用于测试基于腺相关载体和反义核苷酸的基因治疗的动物模型。
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引用次数: 1
Remote ischemic preconditioning combined with atorvastatin improves memory after global cerebral ischemia-reperfusion in male rats Remote缺血预处理联合阿托伐他汀可改善雄性大鼠全脑缺血再灌注后的记忆
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-14 DOI: 10.3897/rrpharmacology.8.75753
A. Hedayatpour, M. Shiasi, Peyman Modarresi, Alieh Bashghareh
Introduction: Damage to hippocampus can occur through ischemia. Memory problems are among the most significant disabilities after stroke. Therefore, improving memory is of great interest in helping post-stroke patients. This study demonstrated that intraperitoneally injection of atorvastatin with a short cycle of ischemia-reperfusion in the left femoral artery improved hippocampal CA1 neurons injury and memory problems after global cerebral ischemia. Materials and methods: In this article survey, we used 64 animals. Rats were divided into 8 groups, (n=8). Group 1: control; group 2: sham; group 3: global cerebral ischemia (GCI) only; group 4: remote ischemic preconditioning (RIP) + GCI; group 5: GCI + atorvastatin (ATO); group 6: GCI + vehicle; group 7: RIP + GCI + ATO; group 8: RIP + GCI + vehicle. We created global cerebral ischemia (GCI) with 20 min occlusion of the Common carotid artery. Results and discussion: Remote ischemic preconditioning could improve rats performance in water maze tests along with a decrease in neuronal death. Also, atorvastatin combined with remote ischemic preconditioning was more effective for memory improvement and reduction of neuronal death. Inconsistent with our result, the function of the animals in the ischemia group was impaired. CA1 hippocampal neurons have an important role in memory and learning, and they can be damaged after cerebral ischemia. Therefore, ischemia can create memory problems. Remote ischemic preconditioning and atorvastatin had a neuroprotective effect and could improve rat performance in water maze test. Conclusion: This study showed that remote ischemic preconditioning with atorvastatin could improve CA1 neuronal injury and memory. Graphical abstract:
海马损伤可通过缺血发生。记忆问题是中风后最严重的残疾之一。因此,改善记忆对帮助中风后患者有很大的意义。本研究表明,左股动脉短周期缺血再灌注注射atorvastatin可改善全脑缺血后海马CA1神经元损伤和记忆问题。材料与方法:本研究选用动物64只。将大鼠分为8组(n=8)。第一组:对照组;第二组:假手术;3组:全脑缺血(GCI);4组:远端缺血预处理(RIP) + GCI;第五组:GCI + atorvastatin (ATO);第六组:GCI +车辆;第七组:RIP + GCI + ATO;第八组:RIP + GCI +车辆。我们制造了全脑缺血(GCI),闭塞颈总动脉20分钟。结果与讨论:远端缺血预处理能提高大鼠水迷宫实验的表现,减少神经元死亡。此外,atorvastatin联合远端缺血预处理对改善记忆和减少神经元死亡更有效。与我们的结果不一致的是,缺血组动物的功能受损。CA1海马神经元在记忆和学习中起着重要作用,在脑缺血后会受到损伤。因此,缺血会造成记忆问题。远端缺血预处理和atorvastatin具有神经保护作用,可提高水迷宫实验大鼠的表现。结论:atorvastatin远程缺血预处理可改善CA1神经元损伤及记忆功能。图形化的简介:
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引用次数: 0
Antiproliferative activity of a new derivative from the class of N-glycoside of indolo[2,3-a]pyrrolo[3,4-c]carbazoles 吲哚[2,3-a]吡咯[3,4-c]咔唑n -糖苷类新衍生物的Antiproliferative活性
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-14 DOI: 10.3897/rrpharmacology.8.79424
Marina P. Kiseleva, L. Borisova, G. Smirnova, Yu. A. Borisova, A. Lantsova, E. Sanarova, L. Nikolaeva, Lydia V. Ektova, M. V. Komarova
Introduction: The creation of highly effective original anticancer drugs remains an urgent direction of scientific research in tumor therapy. One of the promising groups in this regard is indolocarbazoles and their derivatives, which are capable of initiating various pathways of tumor cell death. The aim of the study was to evaluate an antiproliferative activity of a new, Russian derivative of N-glycoside substituted indolocarbazole 6-amino-12-(α-L-arabinopyranosyl)indolo[2,3-a]pyrrolo[3,4-c]carbazole-5,7-dione (LCS-1208) on models of transplantable tumors of mice and on human tumors in Balb/c nude mice. Materials and methods: Indolocarbazole sensitivity to LCS-1208 was assessed on transplantable tumors of mice – lymphatic leukemia L-1210, cervical carcinoma (CC-5), and colon adenocarcinoma (CAC) by five-fold intraperitoneal administration (ip) of the LCS-1208 substance in single doses of 50, 75, 100 mg/kg. Investigation into the effectiveness of the LCS-1208 lyo dosage form was performed on subcutaneous xenografts of human colon cancer SW620 by an intravenous administration (iv). The antitumor effect was evaluated by the tumor growth inhibition (TGI) and an increase in life span (ILS) of the treated animals as compared with the control ones. Evaluation of specific antitumor activity on xenografts was performed according to the tumor/control (T/C%) criterion (maximum criterion T/C≤42%). Results and discussion: According to the results of the study, the most sensitive to the action of the LCS-1208 substance in the case of an ip administration of a total dose of 375 mg/kg were CAC with TGI=97–62%, p≤0.001 up to 16 days after the treatment, and ILS=36% (criteria for TGI≥70% and ILS≥25%). On xenografts of a human colon cancer SW620, the effectiveness of the LCS-1208 lyo drug dosage form within the range of total doses from 50 to 150 mg/kg in case of iv to Balb/c nude mice was set at T/C = 35–2% (criterion T/C<42%). Conclusion: The presented results suggest possible effectiveness of LCS-1208 in treatment of colon malignant tumors of humans.
引言:高效原创抗癌药物的研制仍然是肿瘤治疗科学研究的迫切方向。在这方面有希望的团体之一是吲哚类 以及它们的衍生物,它们能够启动肿瘤细胞死亡的各种途径。本研究的目的是评估一种新的N-糖苷取代的俄罗斯衍生物的抗增殖活性吲哚卡巴唑 6-氨基-12-(α-L-阿拉伯吡喃酰基)吲哚并[2,3-a]吡咯并[3,4-c]咔唑-5,7-二酮(LCS-1208)在小鼠可移植肿瘤模型和Balb/c裸鼠中的人类肿瘤上的作用。材料和方法:吲哚卡巴唑 在小鼠的可移植肿瘤——淋巴白血病L-1210、宫颈癌(CC-5)和结肠腺癌(CAC)——上,通过50、75、100mg/kg单剂量的5倍腹膜内给药(ip)LCS-1208物质来评估对LCS-1208的敏感性。通过静脉内给药对人结肠癌癌症SW620的皮下异种移植物进行LCS-1208lyo剂型的有效性的研究(iv)。通过与对照动物相比,治疗动物的肿瘤生长抑制(TGI)和寿命延长(ILS)来评估抗肿瘤效果。根据肿瘤/对照(T/C%)标准(最大标准T/C≤42%)对异种移植物的特异性抗肿瘤活性进行评估。结果和讨论:根据研究结果,在总剂量375 mg/kg的ip给药情况下,对LCS-1208物质的作用最敏感的是CAC,TGI=97–62%,治疗后16天p≤0.001,ILS=36%(TGI≥70%和ILS≥25%的标准)。在人类癌症SW620的异种移植物上,在静脉注射至Balb/c裸鼠的情况下,LCS-1208 lyo药物剂型在50至150 mg/kg的总剂量范围内的有效性设定为T/c=35–2%(标准T/c<42%)。结论:本研究结果提示LCS-1208治疗人类结肠恶性肿瘤可能有效。
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引用次数: 2
Evaluation of methods of modeling and formation of experimental allergic encephalomyelitis 实验性过敏性脑脊髓炎的建模和形成方法Evaluation
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-14 DOI: 10.3897/rrpharmacology.8.77361
O. Nefodov, I. Belenichev, M. Fedchenko, O. Popazova, V. Ryzhenko, O. Morozova
Introduction: Experimental autoimmune (allergic) encephalomyelitis (EAE) induced by intradermal injection of homogenate of the brain, spinal cord and peripheral nerve with Freund’s stimulator, refers to a true autoimmune disease of the nervous system. Materials and methods: Experimental studies were conducted on white nonlinear rats. To induce experimental allergic encephalomyelitis (EAE), homologous brain homogenates was used, which leads among other drugs (homologous, heterogeneous brain and spinal cord homogenates) by encephalitogenity. The connective tissue of the animal’s tail base was injected with a mixture of encephalitogenic suspension of 0.1 ml per 100 g of the body weight. Results and discussion: According to the results, in the rats, there was weight loss, and the abnormal neurological symptoms were found on an average of 10–12th days. Our experimental studies on the formation of EAE were confirmed morphologically by electron microscopy. Conclusion: Thus, the use of this technique allowed us to obtain a simulated pathologic condition of multiple sclerosis in the form of experimental allergic encephalomyelitis and can be used in future studies to identify appropriate laws, the extent and nature of changes in the immune and nervous systems of the body when inducing experimental pathological conditions.
引言:实验性自身免疫性(变态反应性)脑脊髓炎(EAE)是指用弗氏刺激器皮内注射大脑、脊髓和外周神经匀浆诱发的一种真正的神经系统自身免疫性疾病。材料与方法:采用白色非线性大鼠进行实验研究。为了诱导实验性变态反应性脑脊髓炎(EAE),使用同源脑匀浆,这在其他药物(同源、异质性脑和脊髓匀浆)中领先于脑炎。将每100g体重0.1ml的致脑炎悬浮液的混合物注射到动物尾部基底的结缔组织中。结果与讨论:根据结果,大鼠体重减轻,平均10-12天出现神经系统异常症状。我们对EAE形成的实验研究通过电子显微镜在形态学上得到了证实。结论:因此,该技术的使用使我们能够获得实验性变态反应性脑脊髓炎形式的多发性硬化症的模拟病理状况,并可用于未来的研究,以确定在诱导实验性病理状况时身体免疫和神经系统变化的适当规律、程度和性质。
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引用次数: 0
Neuroprotective effects of a 40% ethanol extract of the black walnut bark (Juglans nigra L.) 黑胡桃皮40%乙醇提取物的神经保护作用
Q3 Pharmacology, Toxicology and Pharmaceutics Pub Date : 2022-06-14 DOI: 10.3897/rrpharmacology.8.77172
D. Pozdnyakov, Z. Dayronas, D. S. Zolotych, Anastasya D. Geraschenko, N. B. Shabanova
Introduction: Neuroprotection is a promising area of adjuvant therapy of ischemic brain lesions. At the same time, among potentially effective neuroprotectors, herbal remedies are distinguished due to their high efficiency and safety of use. In this work, some aspects of the neuroprotective effect of 40% ethanol extract of black walnut bark were investigated in comparison with its major component juglone. Materials and methods: The work was performed on male Wistar rats, which were simulated with cerebral ischemia by irreversible occlusion of the middle cerebral artery. The acute toxicity of the extract was preliminarily evaluated. During the work, the following parameters were determined: changes in the behavior of animals in the Morris water maze, cerebral blood flow, brain necrosis zone area, the activity of mitochondrial complexes, citrate synthase activity, lactic, pyruvic, and ATP concentrations. The activity of the studied extract was compared with juglone in a concentration of 1 mg/kg (per os). Discussion: The study showed that the use of black walnut bark extract in conditions of cerebral ischemia contributed to an increase in the activity of mitochondrial complexes I-V, citrate synthase, which in turn led to the normalization of aerobic-anaerobic metabolism reactions. The increase in the activity of respiratory complexes is probably mediated by the antioxidant properties of juglone, which is a major component of the test extract of black walnut bark. Conclusion: Thus, the test extract can be a potentially effective neuroprotective agent and requires further study.
引言:神经保护是缺血性脑损伤辅助治疗的一个很有前途的领域。同时,在潜在有效的神经保护剂中,草药疗法因其高效和安全的使用而与众不同。在这项工作中,某些方面的神经保护作用达到40%乙醇 对黑胡桃皮提取物及其主要成分进行了比较研究朱古龙. 材料和方法:以雄性Wistar大鼠为实验对象,采用不可逆性脑中动脉闭塞法模拟脑缺血。初步评价了提取物的急性毒性。在工作过程中,确定了以下参数:动物在Morris水迷宫中的行为变化、脑血流量、脑坏死区面积、线粒体复合物的活性、柠檬酸合成酶活性、乳酸、丙酮酸和ATP浓度。研究提取物的活性与朱古龙 浓度为1mg/kg(每os)。讨论:研究表明,在脑缺血条件下使用黑胡桃皮提取物有助于提高线粒体复合物I-V、柠檬酸合成酶的活性,从而使有氧厌氧代谢反应正常化。呼吸复合物活性的增加可能是由朱古龙, 它是黑胡桃皮试验提取物的主要成分。结论:因此,试验提取物可能是一种潜在有效的神经保护剂,需要进一步研究。
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引用次数: 0
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Research Results in Pharmacology
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