Peer-reviewed veterinary case report
Treating diabetic ketoacidosis in dogs with muscle or IV insulin
By Malerba, Eleonora et al.·Published in Frontiers in veterinary science·2020·Department of Veterinary Medical Sciences, Italy·View original on PubMed →
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Original publication title: Efficacy and Safety of Intramuscular Insulin Lispro vs. Continuous Intravenous Regular Insulin for the Treatment of Dogs With Diabetic Ketoacidosis.
- Species:
- dog
Plain-English summary
A group of dogs with diabetic ketoacidosis (DKA), a serious condition caused by high blood sugar, were treated with either an injection of insulin lispro or a continuous IV drip of regular insulin. The dogs receiving the injection showed a quicker improvement, with their ketosis resolving in about 12 hours compared to 23 hours for those on the IV treatment. Both methods were found to be safe, with no significant differences in side effects like low blood sugar. This suggests that using insulin lispro injections could be an effective option for treating DKA in dogs.
People also search for: dog diabetic ketoacidosis treatment · insulin lispro for dogs · dog high blood sugar symptoms
Abstract
The use of rapid-acting insulin analogs as routes of administration other than IV has never been described for the treatment of dogs with diabetic ketoacidosis (DKA). This study aims to compare the efficacy and safety of a new protocol based on IM administration of insulin lispro with that of low-dose IV continuous rate infusion of regular insulin in the treatment of canine DKA. Client-owned dogs with naturally occurring DKA were included. Dogs treated with IM insulin lispro (Group L,= 11) received 0.25 U/kg. The goal was to achieve a drop of at least 10% in blood glucose between 1 h and the next. If this goal was not achieved, the insulin dose was repeated hourly; otherwise, the insulin dose was not repeated up to a maximum of 3 h, after which the insulin dose was repeated anyway. When blood glucose was ≤250 mg/dL, the insulin dose was reduced to 0.125 U/kg IM every 3 h. Cases receiving IV continuous rate infusion of regular insulin (Group R,= 13) were treated according to a previously published protocol. The median time to resolution of ketosis was significantly shorter in Group L (12 h; range, 4-27 h) compared to Group R (23 h; 10-46 h;= 0.04). The median times to resolution of acidemia and ketoacidosis were 13 h (4-35 h) and 17.5 h (4-35 h) in Group L, and 22 h (9-80 h) and 23.5 h (10-80 h) in Group R, respectively. These differences were not significant (= 0.06 and= 0.09, respectively). The median length of hospitalization did not differ significantly between groups (= 0.67). There were no differences in the frequency and severity of adverse events (hypoglycemia, hypokaliemia, and hypophosphatemia) between groups. The new protocol based on IM administration of insulin lispro preliminarily appears effective and safe for treatment of canine DKA.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/33195532/