Investigation of Mechanism Activity of Antitumor and Radiosensitizing Activity of Preparations К-26 and K-26w

Ибрагимов, А. А.; Enikeeva, Z. M.; Agzamova, Nigora; Salihov, Faizullo S.; Rahimov, Okiljon Abduhalilovich; Askarova, Mavluda Turapovna

doi:10.11648/j.ajbls.20200805.12

Cited by 2 publications

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“…Based on colchicine and colchamine, we created new alkaloids that are less toxic and more active than the original alkaloids, as well as other mitotic inhibitors and anticancer drugs [6][7][8][9]. The new drug colhametin was synthesized from colhamin, which was widely used in the clinic in the treatment of stage I and II skin cancer in the form of a 0.5-1% ointment [6], and the amino acid methionine [10], which gave a noticeable decrease in toxicity.…”

Section: Introductionmentioning

confidence: 99%

Studying the Acute Toxicity and Anti-Tumor Activity of the New Drug Colhametin

Javlonabduraimovich¹,

Narzikulovich²,

Shavkatovna³

et al. 2023

ijmscr

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The aim of the study was to study acute toxicity during intraperitoneal administration of a new antitumor drug "colhametin" (K-2) in mice and rats and its antitumor activity on 2 strains of tumors, including with a smaller number of injections. Material and research methods. Acute toxicity of the K-2 preparation after a single intraperitoneal injection was carried out according to the Litchfield and Wilcoxon method on 30 white outbred mice weighing 20±2g of both sexes and 30 male and female rats weighing 140±10g, 5 animals in each group. The study of antitumor activity was performed on 12 outbred mice and 16 outbred rats with transplanted tumors S-180 (Sarcoma-180) and WC (Walker's sarcoma) which were administered drugs on the 4th day after tumor inoculation 10- and 5-fold. The results were evaluated according to standard criteria: tumor growth inhibition (TGI), body weight and spleen of animals Differences were considered significant at p<0.05. Results. The following data were obtained with a single intraperitoneal injection to mice: the average lethal dose of LD50 is 890 (-150 + 172) mg/kg, LD50 with a single intraperitoneal dose of K-2 preparation in rats, LD50 is 410 (-56 + 61) mg/kg, the values are also determined LD10, LD16 and LD84. The antitumor activity of the drug K-2 on the tumor strain Sarcoma - 180 was high, 99/90%. On WC tumors the effect of K-2 reached 90/91% with 10-fold administration, and 89/89% with 5-fold administration, however, its effect was accompanied by a decrease in hematopoietic parameters. Conclusions. The study of the acute toxicity of the substance of the preparation K-2 showed that this preparation belongs to the IV class of low-toxic compounds. On 2 tumors, the effect of the new drug was high, which did not decrease with a decrease in the number of injections.

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Section: Introductionmentioning

confidence: 99%

Studying the Acute Toxicity and Anti-Tumor Activity of the New Drug Colhametin

Javlonabduraimovich¹,

Narzikulovich²,

Shavkatovna³

et al. 2023

ijmscr

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Изучение Противоопухолевой Активности Колхицинола-2 (К-26-В) На Опухолевом Штамме Солидная Опухоль Эрлиха

Enikeeva¹,

Agzamova²,

Abdirova³

et al. 2021

Евразийский Онкологический Журнал

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Цель работы. Оценка противоопухолевой активности нового препарата колхицинола-2 (К-26-в) на животных с опухолевым штаммом солидная опухоль Эрлиха (СОЭ) в разные периоды после перевивки, а также при разных путях введения.Материалы и методы. Изучение выполнено на 86 беспородных мышах с перевиваемой опухолью СОЭ. К-26-в вводили мышам на 3, 5 и 10-й день после перевивки опухоли 10- и 8-кратно в/б в разных дозах, в сравнении с К-26, а также при разных путях 10-кратного введения через 6 дней после перевивки. Оценку результатов проводили по стандартным критериям: торможение роста опухоли (ТРО), масса тела и селезенки животных. Достоверными считали различия при р<0,05.Результаты. К-26-в в дозе 32 мг/кг на опухоли СОЭ проявил активность на 3-й и 5-й дни после перевивки в 93–98%, через 10 дней после перевивки был эффективен на 95%. При разных способах введения лечение К-26-в вызвало следующий результат: при подкожном введении эффект составлял 98/97%, внутримышечном – 93/93%, внутрибрюшинном – 88/87% и внутривенном – 82/83% (по объему и массе опухоли). Во всех опытных группах не было гибели животных, депрессии массы тела и селезенки.Заключение. К-26-в оказался высокоактивным в отношении опухоли СОЭ, уровень ТРО=93– 98% как в раннем периоде, так и в отсроченном при влиянии на развившиеся опухоли (с эффектом в 95%). При изучении лучшего пути введения нового препарата показано, что наиболее предпочтительный способ введения – внутримышечное или подкожное введение с эффектом в 93–98%, которое рекомендовано для проведения клинических испытаний. Purpose. Evaluation of the antitumor activity of the new preparation colchicinol-2 (K-26-w) in animals with the tumor strain Ehrlich's solid tumor (EST) in different periods after inoculation, as well as in different routes of administration.Materials and Methods. The study was carried out on outbred mice with the transplanted EST tumor. K-26-w was injected into mice on the 3rd, 5th, and 10th days after tumor inoculation, 10 and 8 times intraperitoneally at different doses, in comparison with K-26, as well as in different routes of 10-time administration in 6 days after inoculation. The results were assessed according to the standard criteria: tumor growth inhibition (TGI), weight of the body and spleen of animals. The differences were considered significant in p<0.05.Results. K-26-w in the dose of 32 mg/kg showed the activity on the 3rd day after inoculation (the activity was 93–98%); in 10 days after inoculation, it was 95% effective. In different methods of administration, the treatment with K-26-w caused the following result: in subcutaneous administration, the effect was 98/97%, intramuscular administration – 93/93%, intraperitoneal – 88/87%, and intravenous – 82/83% (by volume and weight of tumor). In all experimental groups, there was no death of animals, depression of body weight and spleen.Conclusion. K-26-w proved to be highly active in EST tumors; TGI level=93–98% both in the early period and in the delayed period, with the effect on the developed tumors (with the effect of 95%). When studying the best route of administration of a new drug, it was showed that the best routes of administration are intramuscular or subcutaneous ones with the effect of 93–98%, which is recommended for clinical trials.

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Investigation of Mechanism Activity of Antitumor and Radiosensitizing Activity of Preparations К-26 and K-26w

Cited by 2 publications

References 5 publications

Studying the Acute Toxicity and Anti-Tumor Activity of the New Drug Colhametin

Studying the Acute Toxicity and Anti-Tumor Activity of the New Drug Colhametin

Изучение Противоопухолевой Активности Колхицинола-2 (К-26-В) На Опухолевом Штамме Солидная Опухоль Эрлиха

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