Tigecycline and Gentamicin-Combined Treatment Enhances Renal Damage: Oxidative Stress, Inflammatory Reaction, and Apoptosis Interplay

Elgazzar, Dina; Aboubakr, Mohamed; Bayoumi, Heba; Ibrahim, Amany N.; Sorour, Safwa M.; El-Hewaity, Mohamed; Elsayed, Abulmaaty M.; Shehata, Shaimaa A.; Bayoumi, Khaled A.; Alsieni, Mohammed; Behery, Maged; Abdelrahaman, Doaa; Ibrahim, Samah F.; Abdeen, Ahmed

doi:10.3390/ph15060736

Cited by 11 publications

(6 citation statements)

References 50 publications

(81 reference statements)

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“…In tigecycline-treated cells, oxidative damage to DNA, protein, and lipid was observed, which is consistent with oxidative stress (Tan et al, 2017). Previous research demonstrated the existence of DNA damage and repair processes brought on by TIG and/or GEN therapy (Elgazzar et al, 2022). Pathological research on rabbits demonstrated that longterm GEN administration causes myocardial muscle cell congestion and necrosis, which would be linked to inadequate systemic circulation (Saleh, 2018).…”

Section: Discussionsupporting

confidence: 61%

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Gentamicin potentiate tigecycline induced cardiotoxicity in rats: the cardiac susceptibility to oxidative stress

Elgazzar

Abdeen²,

Aboubakr³

2022

Benha Veterinary Medical Journal

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Tigecycline (TIG) toxicity is a threat to health because of the mortality risk attributed to its overdose. Large doses result in fatal cardiomyopathy and acute cardiotoxicity. Gentamicin (GEN) is an aminoglycoside antibacterial agent that affects kidney function, causing nephrotoxicity. Six groups of rats (n=5) were used. Control (DW), TIG 7 (TIG 7 mg/kg IP), TIG14 (TIG 14 mg/kg IP), gentamicin (GEN), TIG 7+ GEN, and TIG 14+ GEN groups. Cardiac catalase (CAT) activity, glutathione (GSH), and malondialdehyde (MDA) levels in the heart, as well as histopathological changes were recorded. Myocardium from TIG 14+ GEN group exhibited typical changes for myocardial apoptosis and degeneration, as well as an increase in interleukin-6 (IL-6) and annexin-V levels, were recorded specially in the TIG 14+ GEN group. GEN, in addition to its nephrotoxicity, increases TIG-induced cardiotoxicity. GEN may increase the cardiotoxicity of high dose TIG. Particularly large doses of GEN have a negative impact on the cardiac oxidative stress caused by TIG.

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Section: Discussionsupporting

confidence: 61%

“…These data corroborate and broaden previous research indicating a link among oxidative stress and TIGinduced cardiotoxicity. It was demonstrated that TIG causes increased ROS creation as well as protein damage measurements (Elgazzar et al, 2022). Tigecycline raises levels of mitochondrial superoxide, hydrogen peroxide, and (ROS).…”

Section: Discussionmentioning

confidence: 99%

Gentamicin potentiate tigecycline induced cardiotoxicity in rats: the cardiac susceptibility to oxidative stress

Elgazzar

Abdeen²,

Aboubakr³

2022

Benha Veterinary Medical Journal

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“…Cd promotes mitochondrial deterioration leading to reduction in ATP synthesis and incremented reactive oxygen species (ROS) generation ( Mirkov et al, 2021 ). As a result, mitochondrial dysfunction, peroxidation of membrane lipid (LPO), protein misfolding, DNA oxidation, and ultimately, overture of apoptotic pathways are instigated ( Abdeen et al, 2019 ; Mirkov et al, 2021 ; Elgazzar et al, 2022 ).…”

Section: Introductionmentioning

confidence: 99%

The Combination of Tamarindus indica and Coenzyme Q10 can be a Potential Therapy Preference to Attenuate Cadmium-Induced Hepatorenal Injury

et al. 2022

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Cadmium (Cd) is a hazardous environmental pollutant that menaces human and animal health and induces serious adverse effects in various organs, particularly the liver and kidneys. Thus, the current study was designed to look into the possible mechanisms behind the ameliorative activities of Tamarindus indica (TM) and coenzyme Q10 (CoQ) combined therapy toward Cd-inflicted tissue injury. Male Wistar rats were categorized into seven groups: Control (received saline only); TM (50 mg/kg); CoQ (40 mg/kg); Cd (2 mg/kg); (Cd + TM); (Cd + CoQ); and (Cd + TM + CoQ). All the treatments were employed once daily via oral gavage for 28 consecutive days. The results revealed that Cd exposure considerably induced liver and kidney damage, evidenced by enhancement of liver and kidney function tests. In addition, Cd intoxication could provoke oxidative stress evidenced by markedly decreased glutathione (GSH) content and catalase (CAT) activity alongside a substantial increase in malondialdehyde (MDA) concentrations in the hepatic and renal tissues. Besides, disrupted protein and lipid metabolism were noticed. Unambiguously, TM or CoQ supplementation alleviated Cd-induced hepatorenal damage, which is most likely attributed to their antioxidant and anti-inflammatory contents. Interestingly, when TM and CoQ were given in combination, a better restoration of Cd-induced liver and kidney damage was noticed than was during their individual treatments.

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“…There is ample proof indicating the embroilment of oxidative stress, inflammatory responses, and apoptotic pathway in AFT-induced nephrotoxicity ( Owumi et al, 2020 ; Wang et al, 2022 ). Thus, excess generation of reactive oxygen species (ROS), with consumption of antioxidant enzymes after AFT intoxication, provokes tissue injuries such as DNA mutations, mitochondrial disruption, improper folding of protein, and ultimately necroptosis ( Dlamini et al, 2021 ; Elgazzar et al, 2022 ; Li et al, 2022 ). Moreover, the stability of AFTs and their metabolites highlights the necessity for developing secure, feasible, and efficient strategies for reducing their damaging impacts ( Kolosova and Stroka, 2012 ).…”

Section: Introductionmentioning

confidence: 99%

Microalgae (Chlorella vulgaris) attenuates aflatoxin-associated renal injury

Abdeen,

Elsabagh,

Elbasuni

et al. 2023

Front. Pharmacol.

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Introduction: Aflatoxins (AFT) are ubiquitous environmental pollutants that are extremely dangerous for both human beings as well as animals. A safe, effective, and considerate strategy is therefore credited with controlling AFT intoxication. Therefore, our study aimed to evaluate the mitigating properties of Chlorella vulgaris (ChV) against AFT-induced nephrotoxicity and altered egg quality.Methods: Quails were randomized into Control group (receiving a normal diet); ChV group (1 g/kg diet); AFT group (receiving an AFT-containing diet); and the AFT-ChV group were given both treatments.Results and discussion: AFT provoked kidney injury, exhibited by increased renal biochemical parameters and reduced protein levels. Malondialdehyde (MDA) levels dramatically increased as a consequence of AFT exposure, and glutathione (GSH) levels, superoxide dismutase (SOD), and glutathione peroxidase (GPx) activities were also decreased. Substantial up-modulation of the mRNA expression of the inflammatory cytokines (TNF-α, IL-1β, and IL-6) was additionally reported. Furthermore, AFT residues were detected in the egg compromising its quality and nutritional value. Contrarily, ChV supplemented diet suppressed the AFT-prompted oxidative stress and inflammation, together with enhancing the nutritional value and quality of eggs and decreasing AFT residues. These beneficial impacts are proposed to be attributed to its antioxidant and nutritional ingredients. The molecular docking dynamics confirmed the inflammatory and apoptotic protein targets for ChV. Our findings recommend that adding ChV supplements to foods might guard against nephrotoxicity brought on by AFT exposure.

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Tigecycline and Gentamicin-Combined Treatment Enhances Renal Damage: Oxidative Stress, Inflammatory Reaction, and Apoptosis Interplay

Cited by 11 publications

References 50 publications

Gentamicin potentiate tigecycline induced cardiotoxicity in rats: the cardiac susceptibility to oxidative stress

Gentamicin potentiate tigecycline induced cardiotoxicity in rats: the cardiac susceptibility to oxidative stress

The Combination of Tamarindus indica and Coenzyme Q10 can be a Potential Therapy Preference to Attenuate Cadmium-Induced Hepatorenal Injury

Microalgae (Chlorella vulgaris) attenuates aflatoxin-associated renal injury

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