Journal of Veterinary Internal Medicine (Mar 2024)

A prospective cohort study to identify clinical diagnostic and prognostic markers of primary immune thrombocytopenia in dogs

  • Marjory B. Brooks,
  • Robert Goggs,
  • Amelia H. Frye,
  • Jessica Armato,
  • Marnin Forman,
  • Julia Hertl,
  • Michael Koch,
  • John P. Loftus,
  • John Lucy,
  • Brandi Mattison,
  • Julia Merriam,
  • Sarah Shropshire,
  • Laura Van Vertloo,
  • Austin Viall,
  • Dana N. LeVine

DOI
https://doi.org/10.1111/jvim.16985
Journal volume & issue
Vol. 38, no. 2
pp. 1022 – 1034

Abstract

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Abstract Background Primary immune thrombocytopenia (pITP) in dogs presents a diagnostic challenge, and clinical markers of severity are lacking. Objectives Identify clinicopathologic features that differentiate pITP from secondary ITP (sITP) and markers related to bleeding severity, transfusion, and survival of dogs with pITP. Animals Ninety‐eight thrombocytopenic dogs (58 pITP and 40 sITP). Methods Client‐owned dogs with platelet counts <50 000/μL were enrolled in a prospective, multi‐institution cohort study. History and treatment information, through a maximum of 7 days, was recorded on standard data forms. Bleeding severity was scored daily using a bleeding assessment tool (DOGiBAT). At‐admission blood samples were collected for CBC, biochemistry, C‐reactive protein concentration, and coagulation panels, and to measure platelet surface‐associated immunoglobulin G (PSAIg) and expression of platelet membrane proteins and phospholipids. Dogs with evidence of coincident disease were classified as sITP. Results No definitive pITP diagnostic test was found. However, pITP cases were characterized by lower platelet counts, D dimer concentrations, and platelet membrane protein expression than sITP cases. Differentiation between pITP and sITP was further enhanced using logistic regression modeling combining patient sex, coagulation profile, platelet count, D dimer, and PSAIg. A second model of pITP severity indicated that low hematocrit and high BUN concentration were associated with non‐survival. Low hematocrit at admission, but not platelet count or DOGiBAT score, was associated with transfusion. Conclusions and Clinical Importance Pending validation studies, models constructed from at‐admission clinicopathologic findings may improve differentiation of pITP from sITP and identify the most severe pITP cases at the time of presentation.

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