Cystatin C: A Primer for Pharmacists

Teaford, Hilary R.; Barreto, Jason N.; Vollmer, Kathryn J; Rule, Andrew D.; Barreto, Erin F.

doi:10.3390/pharmacy8010035

Cited by 36 publications

(40 citation statements)

References 107 publications

(156 reference statements)

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“…38 Production of S cys is dependent on cell turnover, which is disrupted in hypothyroidism and hyperthyroidism, which can lead to overestimation and underestimation of eGFR, respectively. 38 Despite these limitations, the international federation for clinical chemistry working group has established human serum certified reference materials and are advancing global standardization. 39 The next generation of eGFR based on endogenous biomarkers will require prospective evaluation of S cys and the combination of S cys with S cr .…”

Section: Alternate Endogenous Biomarkers For Estimated Glomerular Filmentioning

confidence: 99%

“…Simulations demonstrate that the eGFR based on the combination of these biomarkers better predicts ceftriaxone exposures and doses than body weight 36 . Limitations do exist with use of S cys due to underestimation of eGFR in patients with obesity, malignancy, high‐dose corticosteroid use, kidney transplant recipients, and in patients that smoke 38 . Production of S cys is dependent on cell turnover, which is disrupted in hypothyroidism and hyperthyroidism, which can lead to overestimation and underestimation of eGFR, respectively 38 .…”

Section: Alternate Endogenous Biomarkers For Estimated Glomerular Filmentioning

confidence: 99%

“…Limitations do exist with use of S cys due to underestimation of eGFR in patients with obesity, malignancy, high‐dose corticosteroid use, kidney transplant recipients, and in patients that smoke 38 . Production of S cys is dependent on cell turnover, which is disrupted in hypothyroidism and hyperthyroidism, which can lead to overestimation and underestimation of eGFR, respectively 38 . Despite these limitations, the international federation for clinical chemistry working group has established human serum certified reference materials and are advancing global standardization 39 .…”

Section: Alternate Endogenous Biomarkers For Estimated Glomerular Filmentioning

confidence: 99%

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Antimicrobial Dosing in Specific Populations and Novel Clinical Methodologies: Kidney Function

Pai

2021

Clin Pharma and Therapeutics

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Kidney function is a common parameter used to define antimicrobial drug dosage and frequency of administration. Several methods exist to measure kidney function but for pragmatic reasons rely on estimated kidney function equations based on the endogenous biomarker serum creatinine and common clinical variables. Current regulatory guidance on the design of studies in patients with abnormal kidney function in the United States also recommend consideration of estimated kidney function for this reason. Over the past few decades, alternate endogenous biomarkers, administration of exogenous biomarkers for noninvasive measurement, use of probe substrates to characterize individual kidney drug clearance pathways, modifications to conventional equations to account for time‐varying clearance, and improved clinical trial modeling and simulation to factor in these uncertainties have occurred. Furthermore, major changes to kidney replacement therapy delivery in the outpatient, inpatient, and at‐home setting are occurring. Antimicrobial drug dose adjustment in this diverse population is complex and in a state of flux due to technical innovations. Over‐reliance on kidney function estimates to guide drug dosing in patients with infectious diseases can bias underdosing especially among the acutely ill. A holistic approach to drug dose adjustment in patients with abnormal kidney function is necessary to optimize clinical outcomes.

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Section: Alternate Endogenous Biomarkers For Estimated Glomerular Filmentioning

confidence: 99%

Section: Alternate Endogenous Biomarkers For Estimated Glomerular Filmentioning

confidence: 99%

Section: Alternate Endogenous Biomarkers For Estimated Glomerular Filmentioning

confidence: 99%

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Antimicrobial Dosing in Specific Populations and Novel Clinical Methodologies: Kidney Function

Pai

2021

Clin Pharma and Therapeutics

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“…Cystatin C is particularly important in assessing kidney functions and is recommended by regulatory agencies for the evaluation of the glomerular filtration rate [ 51 ]. Serum levels of cystatin C in association with serum creatinine, serve as a prognosis and/or diagnostic biomarker for assessing kidney function [ 52 ]. Type-2 cystatins are shown to take part in several immune-regulatory activities [ 42 ].…”

Section: Cystatinsmentioning

confidence: 99%

Parasite Cystatin: Immunomodulatory Molecule with Therapeutic Activity against Immune Mediated Disorders

2020

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The use of parasites or their products for treating chronic inflammation associated diseases (CIADs) has generated significant attention recently. Findings from basic and clinical research have provided valuable information on strengthening the notion that parasites’ molecules can be developed as biotherapeutic agents. Completion of the genome, secreotome, and proteome of the parasites has provided an excellent platform for screening and identifying several host immunomodulatory molecules from the parasites and evaluate their therapeutic potential for CIADs. One of the widely studied host immunomodulatory molecules of the parasites is the cysteine protease inhibitor (cystatin), which is primarily secreted by the parasites to evade host immune responses. In this review, we have attempted to summarize the findings to date on the use of helminth parasite-derived cystatin as a therapeutic agent against CIADs. Although several studies suggest a role for alternatively activated macrophages, other regulatory cells, and immunosuppressive molecules, in this immunoregulatory activity of the parasite-derived cystatin, there is still no clear demonstration as to how cystatin induces its anti-inflammatory effect in suppressing CIADs.

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“…7 Although cystatin C improves the precision of kidney function estimation with a modified CKD-EPI function, it is not a widely accessible assay and not included in any product label to guide drug dosing. 8 Translation of a single-point measurement of serum creatinine into clearance (CL) is based on the assumption of homeostasis, i.e., production or systemic input of creatinine and the rate of creatinine elimination is constant and equivalent. 9 A corollary to this estimation method occurs with continuous infusion drug dosing, where the rate of infusion (Ro) divided by the steady-state concentration (Css) equals clearance (CL).…”

Section: O R I G I N a L R E S E A R C H A R T I C L E Smentioning

confidence: 99%

Modeling Kinetic Glomerular Filtration Rate in Adults with Stable and Unstable Kidney Function: Vancomycin as the Motivating Example

Pai

DeBacker

2020

Pharmacotherapy

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Background Equations used to estimate kidney function for drug dosing rely on the assumption of homeostasis to translate a single‐point measurement of serum creatinine into clearance (CL). Our objective was to rank order the performance of alternate kidney function equations as predictors of drug CL in stable and unstable patients. Methods Data were extracted from medical records at a single center for all adult patients treated with vancomycin over a 5‐year period for population pharmacokinetic analysis. This analysis focused on comparison of nine kidney function equations as covariates of vancomycin CL. Both body surface area (BSA) indexed (ml/min/1.73 m2) and unindexed units (ml/min) of kidney function were tested, as time‐varying and time‐invariant covariates of vancomycin CL. Results The final data set consisted of 2640 patients (62% male, 81% white) with 6628 concentration measurements. The median (5th, 95th percentile) of measurements per patient, age, weight, body mass index (BMI) was 2 (1, 7) concentrations, 61.5 (28, 83) years, 90.0 (56.7, 147) kg, and 30.0 (20.7, 48.0) kg/m2. Unstable kidney function was documented in 43.6% of patients, primarily as acute kidney injury (AKI) on admission with improvement (19.4%) and AKI during the admission (17.4%). Models based on time‐varying kidney function estimates performed better than as time‐invariant. Kidney function estimated by the Chen method was ranked higher than other estimation methods. Conclusions A time‐varying kinetic estimated glomerular filtration rate method not indexed to BSA was identified as the highest ranked covariate model of vancomycin CL.

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Cystatin C: A Primer for Pharmacists

Cited by 36 publications

References 107 publications

Antimicrobial Dosing in Specific Populations and Novel Clinical Methodologies: Kidney Function

Antimicrobial Dosing in Specific Populations and Novel Clinical Methodologies: Kidney Function

Parasite Cystatin: Immunomodulatory Molecule with Therapeutic Activity against Immune Mediated Disorders

Modeling Kinetic Glomerular Filtration Rate in Adults with Stable and Unstable Kidney Function: Vancomycin as the Motivating Example

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