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Peer-reviewed veterinary case report

Feline immunodeficiency virus load lowered by new stable peptide

By Giannecchini, Simone et al.·Published in Antiviral therapy·2005·Department of Experimental Pathology, Italy·View original on PubMed

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Original publication title: Feline immunodeficiency virus plasma load reduction by a retroinverso octapeptide reproducing the Trp-rich motif of the transmembrane glycoprotein.

Species:
cat

Plain-English summary

A group of chronically infected cats with feline immunodeficiency virus (FIV) received a new treatment called riC8, which is a modified peptide designed to inhibit the virus. Over time, the cats treated with riC8 showed a significant decrease in their viral load, meaning the amount of virus in their bodies was reduced. The treatment was well tolerated, with no major side effects noted. This study suggests that riC8 could be a promising option for managing FIV in cats.

People also search for: cat FIV treatment · feline immunodeficiency virus symptoms · antiviral treatment for cats

Abstract

The Trp-rich motif (TrpM) of the transmembrane glycoprotein (TM) of lentiviruses is an attractive domain on which to design new potential cell entry peptide inhibitors. We recently demonstrated that an octapeptide reproducing the TrpM of feline immunodeficiency virus (FIV), designated C8, broadly inhibited this virus in vitro and that the retroinverso analogue of this peptide (riC8) was almost as inhibitory and exhibited features suggestive of a much increased stability. Here, we demonstrated that riC8 is indeed highly stable, maintaining its concentration unchanged for at least 24 h in cat serum in vitro. Furthermore, once inoculated into cats, riC8 produced no major acute toxic effects and exhibited satisfactory pharmacokinetic properties. Finally, we report the results of a short-term monotherapy experiment in chronically FIV-infected cats showing that riC8 is well tolerated and also has substantial antiviral activity in vivo. In particular, the mean viral load of riC8-treated animals declined progressively with increasing time of treatment, whereas that of control animals given C8 or solvent alone did not. These results provide the first evidence that clinically useful inhibition of virus replication with a small peptide derived from a functional domain of the TM of a lentivirus can be achieved in vivo.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/16152761/