Incidence and risk factors for hypoadrenocorticism in dogs treated with trilostane

• Published in: The veterinary journal (1997) Vol. 230; pp. 24 - 29
• Main Authors: King, J.B., Morton, J.M.
• Format: Journal Article
• Language: English
• Published: England Elsevier Ltd 01.12.2017
• Subjects: Canine; Hyperadrenocorticism; Hypoadrenocorticism; Trilostane; Hyperadrenocorticism; Trilostane; Hypoadrenocorticism; Canine
• ISSN: 1090-0233; 1532-2971
• DOI: 10.1016/j.tvjl.2017.10.018

•Anecdotally, dogs with hyperadrenocorticism treated with trilostane have increased risk of developing hypoadrenocorticism.•In 156 dogs, the incidence of hypoadrenocorticism following 2 years of treatment with trilostane was 15%.•In dogs treated with trilostane, dose rate was not associated with risk of hypoadrenocorticism.•This incidence is higher than expected and comparable to some previous studies. The aim of this study was to describe the incidence and permanence of hypoadrenocorticism associated with trilostane treatment and to assess potential risk factors for hypoadrenocorticism. A retrospective cohort study was conducted using case records for 156 dogs treated with trilostane after a diagnosis of hyperadrenocorticism. Occurrences of hypoadrenocorticism were categorised as either transient or permanent. After initiation of treatment with trilostane, the estimated cumulative incidence of hypoadrenocorticism was 15% by 2 years and 26% by 4.3 years, respectively. Occurrences of hypoadrenocorticism were transient in 14/19 (74%) affected study dogs. The risk of hypoadrenocorticism was not significantly associated with trilostane dose rate and other potential risk factors assessed were not significantly associated with subhazard of hypoadrenocorticism, but effect estimates for most were imprecise. In conclusion, approximately 15% of dogs being treated with trilostane developed hypoadrenocorticism within the first 2 years of treatment and about one quarter became affected by 4 years. However, first occurrences of hypoadrenocorticism were mostly transient. Over the range of dose rates studied, each 1mg/kg/day increase in trilostane dose rate resulted in, at most, only a small increase in the risk of developing hypoadrenocorticism.