Synthesis and primary evaluation of the hepatoprotective properties of novel pyrimidine derivatives

A. B. Vyshtakalyuk; V. E. Semenov; V. V. Zobov; I. V. Galyametdinova; L. F. Gumarova; A. A. Parfenov; N. G. Nazarov; O. A. Lenina; S. A. Kondrashova; Sh. K. Latypov; G. V. Cherepnev; M. S. Shashyn; V. S. Reznic

doi:10.1134/S106816201704015X

Synthesis and primary evaluation of the hepatoprotective properties of novel pyrimidine derivatives

Авторы: Vyshtakalyuk A.B.¹, Semenov V.E.¹, Zobov V.V.¹^,2, Galyametdinova I.V.¹, Gumarova L.F.¹, Parfenov A.A.¹, Nazarov N.G.¹^,2, Lenina O.A.¹, Kondrashova S.A.¹, Latypov S.K.¹, Cherepnev G.V.¹^,2, Shashyn M.S.¹, Reznic V.S.¹
Учреждения:
1. Arbuzov Institute of Organic and Physical Chemistry, Kazan Research Center
2. Kazan (Volga region) Federal University
Выпуск: Том 43, № 5 (2017)
Страницы: 604-611
Раздел: Article
URL: https://journals.rcsi.science/1068-1620/article/view/228701
DOI: https://doi.org/10.1134/S106816201704015X
ID: 228701

Цитировать

Полный текст

Открытый доступ
Доступ закрыт

Доступ предоставлен
Доступ закрыт

Только для подписчиков

Аннотация
Об авторах
Список литературы
Дополнительные файлы
Статистика

Аннотация

Based on the active ingredient of the drug Ximedon (1,2-dihydro-4,6-dimethyl-1-N-(2-hydroxyethyl)pyrimidone-2, referred below to as pyrimidine (I), novel derivatives containing biogenic acids: succinic, L-ascorbic, para-aminobenzoic, nicotinic, and L-2-amino-4-(methylthio)butanoic (L-methionine) acids have been synthesized. The parameters of acute toxicity (LD₅₀) have been studied. The antitoxic effect of the compounds upon the injury by the hepatotropic poison carbon tetrachloride has been examined as the primary evaluation of their hepatoprotective properties. It has been found that, according to toxicological safety, the compounds synthesized belong to classes III and IV (moderately and little toxic compounds). The conjugates of pyrimidine (I) with ascorbic acid and methionine (LD₅₀ more than 5400 mg/kg) are least toxic. Pyrimidine (I) and its derivatives possess the antitoxic activity upon acute poisoning with carbon tetrachloride; the combined injection of carbon tetrachloride with pyrimidine (I) or its derivatives leads to an increase in the survival of animals and the normalization of the integral functional parameters, weight and body temperature, which decrease upon toxic injury. In addition, pyrimidine (I) and some of its derivatives (conjugates with L-ascorbic, succinic, para-aminobenzoic, and nicotinic acids) decrease the weight coefficients of the liver and kidneys (the organ-to-body-weight ratio) and the activity of transaminases, the markers of hepatic cytolysis, which increase upon toxic injury with carbon tetrachloride. The area of the pathological injury of the liver by steatosis and necrosis decreases by the action of pyrimidine (I) and its novel derivatives (conjugates with L-ascorbic, succinic, and nicotinic acids) two to three times. Advantages of pyrimidine (I) and its novel derivatives over the hepatoprotective drug Thiotriazolin have been revealed.

Ключевые слова

pyrimidines, Ximedon, hepatoprotectors, liver diseases, toxic hepatitis

Дополнительные файлы

Доп. файлы

Действие

1. JATS XML

Скачать

Имя пользователя
Пароль
Запомнить меня

Забыли пароль?	Регистрация

Имя пользователя
Пароль
Запомнить меня

Забыли пароль?	Регистрация

Synthesis and primary evaluation of the hepatoprotective properties of novel pyrimidine derivatives

Полный текст

Аннотация

Ключевые слова

Об авторах

A. Vyshtakalyuk

V. Semenov

V. Zobov

I. Galyametdinova

L. Gumarova

A. Parfenov

N. Nazarov

O. Lenina

S. Kondrashova

Sh. Latypov

G. Cherepnev

M. Shashyn

V. Reznic

Дополнительные файлы