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العنوان
Teratogenic Effects of Anti- Arrhythmic Drug (Propaphenon HCl), on Albino Rat Fetuses /
المؤلف
Salma Hisham Amin Hassan,
هيئة الاعداد
باحث / Salma Hisham Amin Hassan
مشرف / Mohamed Ahmed Badawy
مشرف / Abdel-Wahab Abu-Bakr El-Ghareeb
مشرف / Entsar Rashad Abd-Allah
الموضوع
Arrhythmic
تاريخ النشر
2022.
عدد الصفحات
81 p. :
اللغة
الإنجليزية
الدرجة
ماجستير
التخصص
Chemistry (miscellaneous)
تاريخ الإجازة
1/1/2022
مكان الإجازة
جامعة القاهرة - كلية العلوم - Chemistry
الفهرس
Only 14 pages are availabe for public view

from 131

from 131

Abstract

Propafenone is a well-known class 1C antiarrhythmic agent that has sodium channel blocking properties as well as the ability to block other channels and a modest calcium antagonistic effect. Propafenone has a profound electrophysiologic effect on auxiliary atrioventricular circuits and in patients with atrioventricular nodal reentry tachycardia can obstruct conduction in the fast conducting pathway. Furthermore, propafenone is less likely than other class 1C drugs to cause proarrhythmia. However, although this medicine can pass through the placenta, the effects during pregnancy remain unknown. Here, we investigated the potential teratogenic and genotoxic effects of Rythmol during rat development. Pregnant Wistar rats received 46.25 mg/kg body weight of propafenone daily by gavage from gestation day (GD) 5 to GD 19. At GD 20, the dams were dissected, and their fetuses assessed via morphologic, skeletal, and histologic investigation. In addition, comet assay was used to measure DNA impairment of fetal skull osteocytes and hepatic cells. The study showed that propafenone treatment of pregnant rats led to a marked decrease in gravid uterine weight, number of implants/litter, number of viable fetuses and body weight of fetuses but a clear increase in placental weight and placental index in the treated group. Frequent morphologic abnormalities and severe ossification deficiency in the cranium bones were observed in the treatment group. Various histopathological changes were observed in the liver, kidney, and brain tissues of maternally treated fetuses. Similarly, propafenone induced DNA damage of examined samples. Thus, out study indicates that propafenone may be embryotoxic in humans.