Peer-reviewed veterinary case report
Protease inhibitor TL-3 stops brain problems from feline
By Huitron-Resendiz, Salvador et al.·Published in Journal of virology·2004·Department of Neuropharmacology, United States·View original on PubMed →
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Original publication title: Resolution and prevention of feline immunodeficiency virus-induced neurological deficits by treatment with the protease inhibitor TL-3.
- Species:
- cat
Plain-English summary
A group of cats infected with feline immunodeficiency virus (FIV) showed signs of neurological problems, such as delays in brain responses. Researchers tested a medication called TL-3 to see if it could help. Cats treated with TL-3 had much lower levels of the virus and their brain response times returned to normal, while untreated cats continued to show delays. However, once the TL-3 treatment stopped, the neurological issues returned. This suggests that TL-3 can effectively help manage FIV-related neurological symptoms, but ongoing treatment is necessary to keep the cats healthy.
People also search for: cat FIV treatment · feline immunodeficiency virus symptoms · TL-3 for cat neurological issues
Abstract
In vivo tests were performed to assess the influence of the protease inhibitor TL-3 on feline immunodeficiency virus (FIV)-induced central nervous system (CNS) deficits. Twenty cats were divided into four groups of five animals each. Group 1 received no treatment, group 2 received TL-3 only, group 3 received FIV strain PPR (FIV-PPR) only, and group 4 received FIV-PPR and TL-3. Animals were monitored for immunological and virological status, along with measurements of brain stem auditory evoked potential (BAEP) changes. Groups 1 and 2 remained FIV negative, and groups 3 and 4 became virus positive and seroconverted by 3 to 5 weeks postinoculation. No adverse effects were noted with TL-3 only. The average peak viral load for the virus-only group 3 animals was 1.32 x 10(6) RNA copies/ml, compared to 6.9 x 10(4) copies/ml for TL-3-treated group 4 cats. Group 3 (virus-only) cats exhibited marked progressive delays in BAEPs starting at 2 weeks post virus exposure, which is typical of infection with FIV-PPR. In contrast, TL-3-treated cats of group 4 exhibited BAEPs similar to those of control and drug-only cats. At 97 days postinfection, treatments were switched; i.e., group 4 animals were taken off TL-3 and group 3 animals were treated with TL-3. BAEPs in group 3 animals returned to control levels, while BAEPs in group 4 animals remained at control levels. After 70 days on TL-3, group 3 was removed from the drug treatment regimen. Delays in BAEPs immediately increased to levels observed prior to TL-3 treatment. The findings show that early TL-3 treatment can effectively eliminate FIV-induced changes in the CNS. Furthermore, TL-3 can counteract FIV effects on the CNS of infected cats, although continued treatment is required to maintain unimpaired CNS function.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/15078933/