Pharmaceuticals (Jun 2022)

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

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

DOI
https://doi.org/10.3390/ph15060736
Journal volume & issue
Vol. 15, no. 6
p. 736

Abstract

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Although the combination of antibiotics is generally well-tolerated, they may have nephrotoxic effects. This study investigated whether tigecycline (TG) and gentamicin (GM) co-administration could accelerate renal damage. Male Wistar rats were randomly divided into six experimental groups: the control, TG7 (tigecycline, 7 mg/kg), TG14 (tigecycline, 14 mg/kg), GM (gentamicin, 80 mg/kg), TG7+GM, and TG14+GM groups. The combination of TG and GM evoked renal damage seen by the disruption of kidney function tests. The perturbation of renal tissue was mainly confounded to the TG and GM-induced oxidative damage, which was exhibited by marked increases in renal MDA (malondialdehyde) along with a drastic reduction in GSH (reduced-glutathione) content and CAT (catalase) activity compared to their individual treatments. More obvious apoptotic events and inflammation were also revealed by elevating the annexin-V and interleukin-6 (IL-6) levels, aside from the upregulation of renal PCNA (proliferating cell nuclear antigen) expression in the TG and GM concurrent treatment. The principal component analysis indicated that creatinine, urea, annexin-V, IL-6, and MDA all played a role in discriminating the TG and GM combined toxicity. Oxidative stress, inflammatory response, and apoptosis were the key mechanisms involved in this potentiated toxicity.

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