N‐acetylcysteine as a Novel Prophylactic Treatment for Ifosfamide‐Induced Nephrotoxicity in Children: Translational Pharmacokinetics

Hanly, Lauren; Chen, Nancy; Aleksa, Katarina; Cutler, Murray J.; Bajcetic, Milica; Palassery, Rasmi; Regueira, Osvaldo; Turner, Cortney A.; Baw, Bandar; Malkin, Becky; Freeman, David J.; Rieder, Michael J.; Vasylyeva, Tetyana L.; Koren, Gideon

doi:10.1177/0091270010391790

Cited by 29 publications

(12 citation statements)

References 46 publications

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“…Similarly, younger age has been identified as 1 of the major risk factors for valproic acid–induced hepatotoxicity . A similar pattern has been demonstrated for ifosfamide, in that young children are at increased risk for ifosfamide‐induced nephrotoxicity that we believe to be due to increased ability to produce the toxin chloroacetaldehyde by side‐chain oxidation of ifosfamide versus oxidative metabolism of ifosfamide to isophosphoramide mustard, the desired antitumor metabolite . When contemplating therapy for toddlers and early school age children—notably in the context of complex chronic care—ADR risk needs to be factored into care planning.…”

Section: The Ontogeny Of Adverse Drug Reactionssupporting

confidence: 55%

“…53,54 A similar pattern has been demonstrated for ifosfamide, in that young children are at increased risk for ifosfamideinduced nephrotoxicity that we believe to be due to increased ability to produce the toxin chloroacetaldehyde by side-chain oxidation of ifosfamide versus oxidative metabolism of ifosfamide to isophosphoramide mustard, the desired antitumor metabolite. 55 When contemplating therapy for toddlers and early school age children-notably in the context of complex chronic care-ADR risk needs to be factored into care planning. A potentially important and largely unexplored consideration germane to ontogeny is the potential impact of developmental changes in receptor and transporter expression and activity on risk for ADRs.…”

Section: S41mentioning

confidence: 99%

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Adverse Drug Reactions Across the Age Continuum: Epidemiology, Diagnostic Challenges, Prevention, and Treatments

Rieder

2018

The Journal of Clinical Pharma

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Adverse drug reactions (ADRs) are common and important complications of drug therapy for children. The risk for ADRs changes over childhood, as do the nature and types of ADRs. Importantly, the risk and nature of ADRs in children are markedly different from those of adults, and adult data cannot be relied on to guide safe drug therapy in children. There are groups of children, notably those with complex and chronic diseases, who are at substantial risk for ADRs. The evaluation of an undesired effect during therapy is ideally accomplished by an organized approach that is a skill that clinicians who care for children—especially those children at high risk for ADRs must have. Additionally, clinicians as well as drug regulatory agencies and industry need to be both vigilant and astute as well as aware that ADRs in children are often different in nature and frequency from those in adults. The increasing use of pharmacogenomics to guide drug dosing and the increasing number of biological agents will provide new sets of challenges to clinicians over the next decade.

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Section: The Ontogeny Of Adverse Drug Reactionssupporting

confidence: 55%

Section: S41mentioning

confidence: 99%

Adverse Drug Reactions Across the Age Continuum: Epidemiology, Diagnostic Challenges, Prevention, and Treatments

Rieder

2018

The Journal of Clinical Pharma

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“…At overdoses, however, APAP leads to accumulation of NAPQI 1 and critical depletion of GSH. 3 The mechanism of APAP-induced nephrotoxicity is not entirely known. It is thought to be due to oxidative stress with a critical depletion of GSH and renal inflammation.…”

Section: Introductionmentioning

confidence: 99%

The Effects of N-Acetylcysteine and Ozone Therapy on Oxidative Stress and Inflammation in Acetaminophen-Induced Nephrotoxicity Model

Uçar¹,

Taşlıpınar²,

Fırat³

et al. 2013

Renal Failure

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“…Early in vitro and in vivo animal studies have shown the effectiveness of NAC in preventing IFO toxicity, as well its lack of interference on the antineoplastic effects of IFO. These findings have been supported by three clinical experiences , although randomized controlled trials (RCTs) are required to assess the role NAC played in protection of the kidney in the published cases. Given the promise of anti‐oxidants, and in particular NAC, further research needs to be carried out to determine which potential treatments are the most clinically useful.…”

Section: Cancer Chemotherapeuticsmentioning

confidence: 80%

Drug‐induced acute kidney injury in children

Faught

Greff

Rieder

et al. 2015

Brit J Clinical Pharma

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Acute kidney injury (AKI) is a serious problem occurring in anywhere between 8 and 30% of children in the intensive care unit. Up to 25% of these cases are believed to be the result of pharmacotherapy. In this review we have focused on several relevant drugs and/or drug classes, which are known to cause AKI in children, including cancer chemotherapeutics, non-steroidal anti-inflammatory drugs and antimicrobials. AKI demonstrates a steady association with increased long term risk of poor outcomes including chronic kidney disease and death as determined by the extent of injury. For this reason it is important to understand the causality and implications of these drugs and drug classes. Children occupy a unique patient population, advocating the importance of understanding how they are affected dissimilarly compared with adults. While the kidney itself is likely more susceptible to injury than other organs, the inherent toxicity of these drugs also plays a major role in the resulting AKI. Mechanisms involved in the toxicity of these drugs include oxidative damage, hypersensitivity reactions, altered haemodynamics and tubule obstruction and may affect the glomerulus and/or the tubules. Understanding these mechanisms is critical in determining the most effective strategies for treatment and/or prevention, whether these strategies are less toxic versions of the same drugs or add-on agents to mitigate the toxic effect of the existing therapy.

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N‐acetylcysteine as a Novel Prophylactic Treatment for Ifosfamide‐Induced Nephrotoxicity in Children: Translational Pharmacokinetics

Cited by 29 publications

References 46 publications

Adverse Drug Reactions Across the Age Continuum: Epidemiology, Diagnostic Challenges, Prevention, and Treatments

Adverse Drug Reactions Across the Age Continuum: Epidemiology, Diagnostic Challenges, Prevention, and Treatments

The Effects of N-Acetylcysteine and Ozone Therapy on Oxidative Stress and Inflammation in Acetaminophen-Induced Nephrotoxicity Model

Drug‐induced acute kidney injury in children

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