The Complexities of Interpreting Reversible Elevated Serum Creatinine Levels in Drug Development: Does a Correlation with Inhibition of Renal Transporters Exist?

Chu, Xiaoyan; Bleasby, Kelly; Chan, Grace K.Y.; Nunes, Irene; Evers, Raymond

doi:10.1124/dmd.115.067694

Cited by 83 publications

(88 citation statements)

References 112 publications

(135 reference statements)

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“…Abemaciclib administration has been associated with mild and variable but consistent elevations in SCr . Increased SCr can arise from a reduction in glomerular filtration, indicating damage to the nephron and associated reduction in renal function, or from inhibition of the active tubular secretion of creatinine.…”

Section: Discussionmentioning

confidence: 99%

“…The in vitro assessment of OCT2 and/or MATE inhibition is important in evaluating potential for drug–drug interactions (DDIs) at these transporters and for many drugs recognized as having inhibitory potential . A number of marketed drugs cause elevations in SCr by inhibition of these renal transporters . Early assessment of the clinical inhibition of renal transporters may be prudent if transporter inhibition has been identified in vitro or if increases in SCr concentrations have been identified during preclinical development, or first‐in‐human clinical trials.…”

mentioning

confidence: 99%

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Abemaciclib Inhibits Renal Tubular Secretion Without Changing Glomerular Filtration Rate

Chappell

Turner

Pak

et al. 2018

Clin Pharma and Therapeutics

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Abemaciclib, an inhibitor of cyclin dependent kinases 4 and 6, is indicated for metastatic breast cancer treatment. Reversible increases in serum creatinine levels of ~15–40% over baseline have been observed following abemaciclib dosing. This study assessed the in vitro and clinical inhibition of renal transporters by abemaciclib and its metabolites using metformin (a clinically relevant transporter substrate), in a clinical study that quantified glomerular filtration and iohexol clearance. In vitro , abemaciclib inhibited metformin uptake by organic cation transporter 2, multidrug and toxin extrusion (MATE)1, and MATE2‐K transporters with a half‐maximal inhibitory concentration of 0.4–3.8 μM. Clinically, abemaciclib significantly increased metformin exposure but did not significantly affect measured glomerular filtration rate, serum neutrophil gelatinase‐associated lipocalin (NGAL), serum cystatin‐C, or the urinary markers of kidney tubular injury, NGAL and kidney injury molecule‐1.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Abemaciclib Inhibits Renal Tubular Secretion Without Changing Glomerular Filtration Rate

Chappell

Turner

Pak

et al. 2018

Clin Pharma and Therapeutics

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“…32,33 Clinically, it is important to distinguish whether serum creatinine increases are due to impairment of glomerular filtration or inhibition of renal transporters since some drugs, such as cobicistat, cause an early, mild (ß0.3 mg/dL), and transient increase in serum creatinine due to potent inhibition of renal transporters, without altering glomerular filtration rate. 32 Serum creatinine increases of ࣙ0.5 mg/dL above baseline have been observed in plazomicin-treated patients with complicated urinary tract infections in a phase 3 clinical trial. 7 The lack of a clinically significant DDI with metformin observed in the present phase 1 study suggests that inhibition of renal transporters is not likely to be the primary mechanism for serum creatinine changes following treatment with plazomicin in patients.…”

Section: Discussionmentioning

confidence: 99%

No Effect of Plazomicin on the Pharmacokinetics of Metformin in Healthy Subjects

Choi¹,

Komirenko²,

Riddle³

et al. 2019

Clinical Pharm in Drug Dev

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Plazomicin is an aminoglycoside that was engineered to overcome aminoglycoside‐modifying enzymes, which are the most common aminoglycoside resistance mechanism in Enterobacteriaceae. Because plazomicin is predominantly eliminated via renal pathways, an in vitro study was conducted to determine whether plazomicin inhibits the organic cation transporter 2 (OCT2) and the multidrug and toxin extrusion (MATE1 and MATE2‐K) transporters, using metformin as a probe substrate. Plazomicin inhibited OCT2, MATE1, and MATE2‐K transporters with half‐maximal inhibition of the transporter values of 5120, 1300, and 338 µg/mL, respectively. To determine whether this in vitro inhibition translates in vivo, an open‐label, randomized, 2‐period, 2‐treatment crossover study (NCT03270553) was carried out in healthy subjects (N = 16), who received a single oral dose of metformin 850 mg alone and in combination with a single intravenous infusion of plazomicin 15 mg/kg. Geometric least‐squares mean ratios of the test treatment (combination) vs the reference treatment (metformin alone) and 90% confidence intervals were within the equivalence interval of 80% to 125% (peak plasma concentration, 104.5 [95.1–114.9]; area under the plasma concentration–time curve from time zero to time of last quantifiable concentration, 103.7 [93.5–115.0]; area under the plasma concentration–time curve from time zero to infinity, 104.0 [94.2–114.8]). The results demonstrate that there is no clinically significant drug‐drug interaction resulting from coadministration of single doses of intravenous plazomicin 15 mg/kg and oral metformin 850 mg in healthy subjects. Coadministration of plazomicin and metformin was well tolerated in healthy subjects.

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“…Notable species differences and interlaboratory discrepancies have been found regarding the plasma membrane localization of OAT2/Oat2. In humans, OAT2 has been detected either both in the brush border (apical) and basolateral plasma membrane or in the basolateral membrane only, whereas, in rodents, localization of Oat2 has been limited to the apical membrane . The overall role of OAT2/Oat2 in creatinine transport in vivo , therefore, remains to be established.…”

Section: Creatinine and Other Biomarkers Of Renal Functionmentioning

confidence: 99%

Transporters affecting biochemical test results: Creatinine‐drug interactions

Chu

Bleasby

Chan

et al. 2016

Clin Pharma and Therapeutics

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Creatinine is eliminated by the kidneys through a combination of glomerular filtration and active transport. Drug-induced increases in serum creatinine (SCr) and/or reduced creatinine renal clearance are used as a marker for acute kidney injury. However, inhibition of active transport of creatinine can result in reversible and, therefore, benign increases in SCr levels. Herein, the transporters involved in creatinine clearance are discussed, in addition to limitations of using creatinine as a biomarker for kidney damage.

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The Complexities of Interpreting Reversible Elevated Serum Creatinine Levels in Drug Development: Does a Correlation with Inhibition of Renal Transporters Exist?

Cited by 83 publications

References 112 publications

Abemaciclib Inhibits Renal Tubular Secretion Without Changing Glomerular Filtration Rate

Abemaciclib Inhibits Renal Tubular Secretion Without Changing Glomerular Filtration Rate

No Effect of Plazomicin on the Pharmacokinetics of Metformin in Healthy Subjects

Transporters affecting biochemical test results: Creatinine‐drug interactions

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