Urinary cystatin B differentiates progressive versus stable IRIS Stage 1 chronic kidney disease in dogs

Author:

Segev Gilad1ORCID,Vaden Shelly2ORCID,Ross Sheri3,Dufayet Cedric4,Cohn Leah A.5,Farace Giosi6ORCID,Szlosek Donald6,Ouyang Zenhwa6,Peterson Sarah6ORCID,Beall Melissa6,Yerramilli Murthy6,Polzin David7,Cowgill Larry D.8ORCID

Affiliation:

1. Hebrew University Jerusalem Israel

2. North Carolina State University Raleigh North Carolina USA

3. University of Prince Edward Island Charlottetown Prince Edward Island Canada

4. University of California Veterinary Medical Center‐San Diego San Diego California USA

5. University of Missouri Veterinary Health Center Columbia Missouri USA

6. IDEXX Laboratories, Inc. Westbrook Maine USA

7. University of Minnesota Minneapolis Minnesota USA

8. University of California‐Davis Davis California USA

Abstract

AbstractBackgroundEarly identification of dogs with progressive vs stable chronic kidney disease (CKD) might afford opportunity for interventions that would slow progression. However, currently no surrogate biomarker reliably predicts CKD progression.Hypothesis/ObjectivesUrinary cystatin B (uCysB), a novel kidney injury biomarker, predicts progressive disease in International Renal Interest Society (IRIS) CKD Stage 1.AnimalsSeventy‐two dogs, including 20 dogs from 4 university centers with IRIS CKD Stage 1, with IDEXX symmetric dimethylarginine (SDMA) concentration up to 17 μg/dL and no systemic comorbidities, and 52 clinically healthy staff‐owned dogs from a fifth university center.MethodsA multicenter prospective longitudinal study was conducted between 2016 and 2021 to assess uCysB concentration in IRIS CKD Stage 1 and control dogs. Dogs were followed to a maximum of 3 years (control) or 25 months (CKD). Stage 1 IRIS CKD was classified as stable or progressive using the slope of 1/SDMA, calculated from 3 timepoints during the initial 90‐day period. Dogs with slope above or below −0.0007 week × dL/μg were classified as stable or progressive, respectively. Mixed effects modeling was used to assess the association between uCysB and progression rate.ResultsEstimates of first visit uCysB results predictive of active ongoing kidney injury based on the mixed effects models were 17 ng/mL for control, 24 ng/mL for stable CKD, and 212 ng/mL for progressive CKD (P < .001).Conclusions and Clinical ImportanceUrinary cystatin B differentiated stable vs progressive IRIS CKD Stage 1. Identification of dogs with progressive CKD may provide an opportunity for clinicians to intervene early and slow progression rate.

Publisher

Wiley

Subject

General Veterinary

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