First human study of follow-on fusion inhibitor

This article is more than 24 years old.

Delegates at the 8th Retroviruses Conference currently underway in Chicago have heard new data this morning on T-1249, a fusion inhibitor. Interest in this new class of antiretrovirals, has so far focussed on T-20 (pentafuside), which has been studied in drug-experienced individuals. At present, drugs in this class are administered by subcutaneous injection, a method which does not favour its use beyond the ‘salvage’ setting.

T-1249 is a second generation fusion inhibitor, which like T-20, is under development from Trimeris with Roche Products. Findings from study T-1249-101, the first study to administer this drug to humans, were presented this morning.

72 people were recruited to this dose-ranging, monotherapy pilot study. All were treatment experienced with viral load over 5,000 copies. Following a two week antiretroviral wash-out period, volunteers were randomised to one of six dosing arms: 6.25mg once or twice daily; 12.5 mg once or twice daily; or 25mg once or twice daily.

Glossary

pilot study

Small-scale, preliminary study, conducted to evaluate feasibility, time, cost, adverse events, and improve upon the design of a future full-scale research project.

 

fusion inhibitor

Anti-HIV drug targeting the point where HIV locks on to an immune cell.

hypersensitivity

An allergic reaction.

diarrhoea

Abnormal bowel movements, characterised by loose, watery or frequent stools, three or more times a day.

dose-ranging trial

A clinical trial where two or more doses of a drug are compared to see which works best and is least harmful, usually done at an early stage of drug development.

Of 72 individuals enrolled, 63 received at least one dose, and 61 completed the 14 day study period. Mean viral load was in the range of 4.95-5.54 log, mean CD4 from 84-146 cells, and the prior number of antiretrovirals which participants had been exposed to was 10. Of 194 treated-related adverse events, just two were considered serious: one case of hypersensitivity and one neutropenia. Aside from these, common side-effects were injection site reactions (40%); headache (11%); dizziness (8%); fever (8%); and diarrhoea (6%).

Viral load responses, and average trough concentrations were dose dependent, though at the 6.25mg dose there was no measurable virological effect. At the other end of the spectrum, those who received the twice daily high dose exhibited an average viral load fall of 1.3 logs between 10 and 14 days after treatment begun.

T-1249 is a so-called ‘rationally designed’ compound, meaning its structure is intended to allow efficacy against HIV mutants which are resistant to T-20; and indeed test tube studies support this possibility. An alternative proposed by a delegate here in Chicago would be for Trimeris/Roche to investigate the combined use of T-20 and T-1249, given the shortage of new drug options with activity against multiply resistant virus.

References

Eron J et al. A 14-day assessment of the safety, pharmacokinetics, and antiviral activity of T-1249, a peptide inhibitor of membrane fusion. 8th Conference on Retroviruses and Opportunistic Infections, abstract 14, Chicago, February 4-8th, 2001.