Cefepime and diclofenac sodium combined treatment‐ potentiated multiple organ injury: Role of oxidative damage and disrupted lipid metabolism
J Biochem Mol Toxicol. • 2021
معلومات البحث
المؤلفون
Mohamed Aboubakr1 | Afaf Abdelkader2,3 | Ola A. Habotta4 | Nisreen Adel1 |
Mahmoud A. Emam5 | Ehab Y. Abdelhiee6 | Obeid Shanab7 | Khaled Shoghy8 |
Heba Elnoury9 | Mohamed M. Soliman10 | Samah F. Ibrahim11,12 |
Ahmed Abdeen
الكلمات المفتاحية
caspase 3, combined toxicity, hepato‐renal toxicity, oxidative stress, testicular damage,
testosterone
المجلة العلمية
J Biochem Mol Toxicol.
الناشر
Not Available
المجلد
e22929
العدد
Not Available
الصفحات
1:13.
publication.type
International
رابط البحث
Not Available
المواد المرفقة
Not Available
الملخص
Concurrent exposure to antimicrobial and nonsteroidal anti‐inflammatory drugs
(NSAIDs) is usually inevitable in most infections and postsurgery. Consequently, the
present study was designed to assess the intertwining impact of coadministration of
cefepime (CP, a wide spectrum antibiotic) and diclofenac sodium (DF, an NSAID) on
rat's liver, kidney, and testes. Rats received saline, CP (180 mg/kg/day, IM), DF
(10 mg/kg/day, IM), or a combination of CP and DF. After 14 days, CP or DF induced
tissue damage expressed by marked biochemical alterations in hepatic and renal
function tests. Besides this, disrupted lipid metabolism and testosterone levels along
with significant histological changes in hepatic, renal, and testicular tissues were
noticed. A significant increase in malondialdehyde and decreases in superoxide
dismutase and catalase activities alongside significant upregulated caspase 3 expression in tissues following CP or DF treatment suggested a bearable influence of
oxidative stress, lipid peroxidation, and cell death. Accordingly, the simultaneous
therapy of CP and DF evoked more obvious tissue damage than their individual
treatment. Overall, data concluded that concurrent use of CP and DF in medical
practice is a worrisome matter, so it should be done cautiously to avoid synergistic
deleterious outcomes.
(NSAIDs) is usually inevitable in most infections and postsurgery. Consequently, the
present study was designed to assess the intertwining impact of coadministration of
cefepime (CP, a wide spectrum antibiotic) and diclofenac sodium (DF, an NSAID) on
rat's liver, kidney, and testes. Rats received saline, CP (180 mg/kg/day, IM), DF
(10 mg/kg/day, IM), or a combination of CP and DF. After 14 days, CP or DF induced
tissue damage expressed by marked biochemical alterations in hepatic and renal
function tests. Besides this, disrupted lipid metabolism and testosterone levels along
with significant histological changes in hepatic, renal, and testicular tissues were
noticed. A significant increase in malondialdehyde and decreases in superoxide
dismutase and catalase activities alongside significant upregulated caspase 3 expression in tissues following CP or DF treatment suggested a bearable influence of
oxidative stress, lipid peroxidation, and cell death. Accordingly, the simultaneous
therapy of CP and DF evoked more obvious tissue damage than their individual
treatment. Overall, data concluded that concurrent use of CP and DF in medical
practice is a worrisome matter, so it should be done cautiously to avoid synergistic
deleterious outcomes.
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