Cisplatin Nephrotoxicity: A Review

TL;DR: The use of nanoparticles in cancer therapies has spawned a new field of study known as cancer nanomedicines as discussed by the authors , which is an astonishment to see the benefits and application of metal nanoparticles over traditional therapy.

TL;DR: Data suggest that α-Bisabolol exerts a protective action against CP-induced nephrotoxicity by mitigating inflammation and oxidative stress through the inhibition of NFκB activation.

TL;DR: Recent research highlights the therapeutic potential of natural compounds, particularly triterpenoids, in mitigating cisplatin-induced renal cytotoxicity through antioxidant and anti-inflammatory pathways, offering a promising approach to reduce nephrotoxicity in cancer patients.

TL;DR: This research denotes the first comprehensive analysis to identify the effects of OS extracts on cisplatin nephrotoxicity in rats and identified that OSFE had higher concentrations of the secondary metabolites such as caffeic acid, chlorogenic acid, protocatechuic acid and orthosiphol, among others, whereas, OSAE was characterized byHigher concentrations of acetate, lactate, succinic acid, valine and phosphatidylcholine.

TL;DR: The results indicate cisplatin nephrotoxicity is characterized by activation of proinflammatory cytokines and chemokines and TNF-alpha appears to play a central role in the activation of this cytokine response and also in the pathogenesis of cisPlatin renal injury.

TL;DR: The epidemiology and pathophysiology of ARF are discussed, including the vascular, tubular, and inflammatory perturbations and implications for potential future therapies to decrease the high mortality.

TL;DR: This paper reviews the existing data on the mechanism of DDP accumulation and develops the postulate that some component of transport occurs through a gated ion channel.

TL;DR: It is demonstrated that uptake of cis-platin is mediated by hOCT2 in renal proximal tubules, explaining its organ-specific toxicity.