Phenotype standardization for drug-induced kidney disease

Mehta, Ravindra L.; Awdishu, Linda; Davenport, Andrew; Murray, Patrick; Macedo, Etienne; Cerdá, Jorge; Chakaravarthi, Raj; Holden, Arthur L.; Goldstein, Stuart L.

doi:10.1038/ki.2015.115

Cited by 139 publications

(103 citation statements)

References 8 publications

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“…Drug‐induced hepatotoxicity was diagnosed according to the criteria of drug‐induced liver disorders in which aspartate aminotransferase (AST) and/or alanine aminotransferase (ALT) levels more than three times the upper limit of normal were considered to have hepatotoxicity . Chronic kidney injury was diagnosed as persistence of hematuria, proteinuria, or/and casts for more than 90 days . As you can see in Figure , the diagram of study enrollment is shown.…”

Section: Methodsmentioning

confidence: 99%

Genetic polymorphisms of long noncoding RNA RP11‐37B2.1 associate with susceptibility of tuberculosis and adverse events of antituberculosis drugs in west China

Song

Liu

Zhao

et al. 2019

Clinical Laboratory Analysis

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BackgroundLittle knowledge about the biological functions of RP11‐37B2.1, a newly defined long noncoding RNA (lncRNA) molecule, is currently available. Previous studies have shown rs160441, located in the RP11‐37B2.1 gene, is significantly associated with tuberculosis (TB) in a Ghanaian and the Gambian populations.MethodsWe investigated the influence of single‐nucleotide polymorphisms (SNPs) within lncRNA RP11‐37B2.1 on the risk of TB and the possible correlation with adverse drug reactions (ADRs) from TB treatment in a Western Chinese population. Four SNPs within lncRNA RP11‐37B2.1 were genotyped in 554 TB cases and 561 healthy subjects using the improved multiplex ligation detection reaction method, and the patients were followed up monthly to monitor the development of ADRs.ResultsNo significant association between the SNPs of lncRNA RP11‐37B2.1 and TB susceptibility was observed (all P > 0.05). Surprisingly, significant association was observed between two SNPs (rs218916 and rs160441) and thrombocytopenia development during anti‐TB therapy under the dominant model (P = 0.003 and 0.014, respectively).ConclusionsOur findings firstly exhibit that rs218916 and rs160441 within lncRNA RP11‐37B2.1 significantly associate with the occurrence of thrombocytopenia and suggest RP11‐37B2.1 genetic variants are potential biosignatures for thrombocytopenia during anti‐TB treatment.

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Section: Methodsmentioning

confidence: 99%

Genetic polymorphisms of long noncoding RNA RP11‐37B2.1 associate with susceptibility of tuberculosis and adverse events of antituberculosis drugs in west China

Song

Liu

Zhao

et al. 2019

Clinical Laboratory Analysis

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“…Because NGAL and tobramycin use a similar transport receptor (megalin), these results suggest that other biomarkers may also be predictive of disordered pharmacokinetics for other medications depending on their respective transport physiologies. Finally, a recent combined adult and pediatric international multicenter initiative has been aimed at assessing genetic predisposition to medication-associated AKI by using genome-wide association studies 22 .…”

Section: What Does the Future Hold?mentioning

confidence: 99%

Nephrotoxicities

Goldstein

2017

F1000Res

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Nephrotoxic medication exposure is nearly ubiquitous in hospitalized patients and represents one of the most common causes of acute kidney injury (AKI) in the hospitalized setting. Although provision of medications that are nephrotoxic has led to improved outcomes in terms of treatment of underlying illness, unnecessary nephrotoxic medication exposure can be viewed as a potentially modifiable adverse safety event if AKI can be prevented. The advancements in electronic health record development, standardization of AKI definitions, and the ability to identify AKI risk and development in near real time provide opportunities to reduce harm from nephrotoxicity.

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“…A panel of international pediatric and adult nephrologists and pharmacists developed a standardized description of the phenotype for drug-associated kidney disease in hospitalized patients [36]. The four general categories include AKI, glomerular disorders, nephrolithiasis and tubular dysfunction, and underlying mechanisms can either be dose-dependent or dose-independent (as in acute interstitial nephritis) [36].…”

Section: Who Develops Aki?mentioning

confidence: 99%

“…The four general categories include AKI, glomerular disorders, nephrolithiasis and tubular dysfunction, and underlying mechanisms can either be dose-dependent or dose-independent (as in acute interstitial nephritis) [36]. The authors concede that multi-drug exposures and concurrent AKI risk factors make the use of these criteria challenging.…”

Section: Who Develops Aki?mentioning

confidence: 99%

Drug-associated acute kidney injury: who’s at risk?

et al. 2016

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The contribution of nephrotoxic medications to the development of acute kidney injury (AKI) is becoming better understood with the rise in incidence of AKI in children. Treatment of AKI is not yet available, so prevention continues to be the most effective approach. There is an opportunity to mitigate severity and prevent the occurrence of AKI if children at increased risk are identified early and nephrotoxins are used judiciously. Early detection of AKI is limited by the dependence on serum creatinine as an indicator. Promising new biomarkers may offer early detection of AKI prior to the rise in serum creatinine. Early detection of AKI is evolving and offers opportunities for better management of nephrotoxins. However, identification of patients at increased risk will remain an important first step both to focus the use of biomarker testing and to aid in its interpretation.

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Phenotype standardization for drug-induced kidney disease

Cited by 139 publications

References 8 publications

Genetic polymorphisms of long noncoding RNA RP11‐37B2.1 associate with susceptibility of tuberculosis and adverse events of antituberculosis drugs in west China

Genetic polymorphisms of long noncoding RNA RP11‐37B2.1 associate with susceptibility of tuberculosis and adverse events of antituberculosis drugs in west China

Nephrotoxicities

Drug-associated acute kidney injury: who’s at risk?

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