Correlation of Serum Cystatin C with Glomerular Filtration Rate in Patients Receiving Platinum-Based Chemotherapy

Cavalcanti, Ernesta; Barchiesi, Vittoria; Cerasuolo, Dionigio; Paola, Flaviano Di; Cantile, Monica; Cecere, Sabrina Chiara; Pignata, Sandro; Morabito, Alessandro; Costanzo, Raffaele; Maïo, Massimo Di; Perrone, Francesco

doi:10.1155/2016/4918325

Cited by 8 publications

(7 citation statements)

References 15 publications

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“…Early studies compared raw serum cystatin c and serum creatinine levels, without the use of estimation equations and determined that serum cystatin c was superior to serum creatinine in predicting 24‐h CrCl in a small sample of individuals with cancer 55 . However, serum cystatin c alone was also shown to have a much lower area under the curve than the CG for predicting renal failure in those receiving platinum‐based chemotherapy 56 . Cystatin c was subsequently introduced into GFR estimating equations.…”

Section: Estimated Gfr In Oncologymentioning

confidence: 99%

“…Cystatin c is increased by corticosteroid exposure, hyperthyroidism (decreases with hypothyroidism), and inflammation, all of which are prevalent in patients with cancer and may bias GFR estimations 57–59 . Some authors have proposed that chemotherapeutic agents may also influence cystatin c, though the data are limited and emerging evidence suggests that cystatin c is a reliable marker of kidney function in patients being treated with chemotherapy 55,56,60–63 . Furthermore, cystatin c levels may be susceptible to the presence of malignancy independent of renal function.…”

Section: Estimated Gfr In Oncologymentioning

confidence: 99%

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Estimating kidney function in patients with cancer: A narrative review

et al. 2023

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Aim Accurate evaluation of glomerular filtration rate (GFR) is crucial in Oncology as drug eligibility and dosing depend on estimates of GFR. However, there are no clear guidelines on the optimal method of determining kidney function in patients with cancer. We aimed to summarize the evidence on estimation of kidney function in patients with cancer. Methods We searched PubMed for literature discussing the performance of GFR estimating equations in patients with malignancy to create a table of the evidence for creatinine‐ and cystatin c‐based equations. We further reviewed novel estimation techniques such as panel eGFR, real‐time measured GFR, and functional magnetic resonance imaging. Results The commonly used GFR estimating equations were derived from populations of patients without cancer. These equations may be less applicable in Oncology due to severe sarcopenia, inflammation, and other physiologic changes in patients with cancer. The Cockcroft‐Gault equation currently dominates in clinical Oncology despite significant limitations and accumulating evidence for use of the CKD‐EPICr formula. Additional considerations in the practice of Oncology include a recently developed equation (CamGFRv2, also called the Janowitz formula) and the use of cystatin c‐based equations to overcome some of the barriers to accurate GFR estimation based on creatinine alone. Conclusion Overall, we suggest using the CKD‐EPI equations (either cystatin c or creatinine‐based) among patients with cancer in routine clinical practice and measured GFR for patients at a critical threshold for treatment decisions.

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Section: Estimated Gfr In Oncologymentioning

confidence: 99%

Section: Estimated Gfr In Oncologymentioning

confidence: 99%

Estimating kidney function in patients with cancer: A narrative review

et al. 2023

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“…Thus the serum level of cystatin C depends on the GFR, and it can be used as a measure of kidney function 24 . Within oncology, the use of isolated cystatin C measurements for the determination of GFR and detection of nephrotoxicity has been questioned, as there appear to be independent effects of both the malignancy and chemotherapy on cystatin C levels that confound its utility 25,26 …”

Section: Assessment Of Kidney Function In Patients With Cancermentioning

confidence: 99%

Onconephrology: The intersections between the kidney and cancer

Rosner

Jhaveri

McMahon

et al. 2020

CA A Cancer J Clinicians

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Onconephrology is a new subspecialty of nephrology that recognizes the important intersections of kidney disease with cancer. This intersection takes many forms and includes drug-induced nephrotoxicity, electrolyte disorders, paraneoplastic glomerulonephritis, and the interactions of chronic kidney disease with cancer. Data clearly demonstrate that, when patients with cancer develop acute or chronic kidney disease, outcomes are inferior, and the promise of curative therapeutic regimens is lessened. This highlights the imperative for collaborative care between oncologists and nephrologists in recognizing and treating kidney disease in patients with cancer. In response to this need, specific training programs in onconephrology as well as dedicated onconephrology clinics have appeared. This comprehensive review covers many of the critical topics in onconephrology, with a focus on acute kidney injury, chronic kidney disease, drug-induced nephrotoxicity, kidney disease in stem cell transplantation, and electrolyte disorders in patients with cancer.

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“…The narrow therapeutic indices of chemotherapeutics are one area where accurate kidney assessment is essential for medication safety and effectiveness. Studies with platinum-agents, particularly carboplatin, which are renally-eliminated and nephrotoxic, demonstrated that cysC predicted carboplatin area under the curve and clearance at least as well as SCr (R 2 for drug clearance 0.71 with SCr and 0.8 with cysC) [61,[70][71][72]. Use of cysC to more accurately predict drug clearance could spare patients dose-dependent adverse drug reactions such as carboplatin-induced thrombocytopenia [73].…”

Section: Malignancymentioning

confidence: 99%

Cystatin C: A Primer for Pharmacists

et al. 2020

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Pharmacists are at the forefront of dosing and monitoring medications eliminated by or toxic to the kidney. To evaluate the effectiveness and safety of these medications, accurate measurement of kidney function is paramount. The mainstay of kidney assessment for drug dosing and monitoring is serum creatinine (SCr)-based estimation equations. Yet, SCr has known limitations including its insensitivity to underlying changes in kidney function and the numerous non-kidney factors that are incompletely accounted for in equations to estimate glomerular filtration rate (eGFR). Serum cystatin C (cysC) is a biomarker that can serve as an adjunct or alternative to SCr to evaluate kidney function for drug dosing. Pharmacists must be educated about the strengths and limitations of cysC prior to applying it to medication management. Not all patient populations have been studied and some evaluations demonstrated large variations in the relationship between cysC and GFR. Use of eGFR equations incorporating cysC should be reserved for drug management in scenarios with demonstrated outcomes, including to improve pharmacodynamic target attainment for antibiotics or reduce drug toxicity. This article provides an overview of cysC, discusses evidence around its use in medication dosing and in special populations, and describes practical considerations for application and implementation.

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Correlation of Serum Cystatin C with Glomerular Filtration Rate in Patients Receiving Platinum-Based Chemotherapy

Cited by 8 publications

References 15 publications

Estimating kidney function in patients with cancer: A narrative review

Estimating kidney function in patients with cancer: A narrative review

Onconephrology: The intersections between the kidney and cancer

Cystatin C: A Primer for Pharmacists

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