Radiation toxicity grading after chemoradiotherapy of canine urinary tract carcinomas: Comparing VRTOG to VRTOG_v2.0

Author:

Ahrens Carlotta1ORCID,Beatrice Laura1,Meier Valeria1ORCID,Rohrer Bley Carla1ORCID

Affiliation:

1. Division of Radiation Oncology, Vetsuisse Faculty University of Zurich Zürich Switzerland

Abstract

AbstractRadiation toxicities may be underestimated after treatment of transitional cell carcinoma in dogs' lower urinary tract. Assessing acute and late toxicities and differentiating them from progressive disease (PD) impacts further therapeutic approach. We retrospectively assessed dogs treated with definitive‐intent chemoradiotherapy (12 × 3.8 Gy, various first‐line chemotherapeutics). Local tumour control, radiation toxicities and survival were evaluated. We classified radiation toxicities according to the previously published radiation toxicity scheme “VRTOG” as well as the updated version, “VRTOG_v2.0”. Fourteen dogs with transitional cell carcinoma of bladder ± urethra (n = 8), +prostate (n = 3) or solely urethra (n = 3), were included. Median follow‐up was 298 days (range 185–1798 days), median overall survival 305 days (95%CI = 209;402) and 28.6% deaths were tumour‐progression‐related. Acute radiation toxicity was mild and self‐limiting with both classification systems: In VRTOG, 5 dogs showed grade 1, and 1 dog grade 2 toxicity. In VRTOG_v2.0, 2 dogs showed grade 1, 3 dogs grade 2, and 3 dogs grade 3 toxicity. Late toxicity was noted in 14.2% of dogs (2/14) with the VRTOG, both with grade 3 toxicity. With VRTOG_v2.0, a larger proportion of 42.9% of dogs (6/14) showed late toxicities: Four dogs grade 3 (persistent incontinence), 2 dogs grade 5 (urethral obstructions without PD resulting in euthanasia). At time of death, 5 dogs underwent further workup and only 3 were confirmed to have PD. With the updated VRTOG_v2.0 classification system, more dogs with probable late toxicity are registered, but it is ultimately difficult to distinguish these from disease progression as restaging remains to be the most robust determinant.

Publisher

Wiley

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