233. Efficacy and safety results from the Phase 2 clinical trial of pritelivir versus foscarnet for treatment of acyclovir-refractory and/or resistant mucocutaneous HSV infections in immunocompromised subjects
Camille N Kotton, Robin K Avery, Kimberly Workowski, Princy N Kumar, Joerg Albrecht, Pranatharthi Chandrasekar, Mayur Ramesh, Anna Wald, Alexander Birkmann, Melanie E Sumner, Bernadette Surujbally, Cynthia Wat, Roy F Chemaly

TL;DR
A new drug called pritelivir shows promise as a safer and more effective treatment for difficult-to-treat herpes infections in people with weakened immune systems.
Contribution
Pritelivir is a novel oral treatment for acyclovir-resistant herpes infections in immunocompromised patients, showing higher healing rates and fewer side effects than foscarnet.
Findings
93% of patients treated with pritelivir healed compared to 57% with foscarnet.
Pritelivir had fewer treatment-emergent adverse events leading to drug discontinuation (4%) compared to foscarnet (43%).
62.6% of patients with foscarnet-resistant/intolerant HSV infections healed with pritelivir.
Abstract
Treatment of herpes simplex viruses (HSV-1 or HSV-2) mucocutaneous infections in the immunocompromised (IC) host can be difficult due to refractory and/or acyclovir-resistant (ACV R/R) infection. Drug-resistant HSV infection occurs in up to 14% of hematopoietic cell transplant recipients and up to 7% in persons with HIV infection. Foscarnet is the only FDA-approved agent for ACV R/R HSV infection. While effective, foscarnet is associated with significant toxicity including nephrotoxicity and electrolyte disturbances necessitating hospitalization for treatment. Pritelivir is an investigational novel viral helicase primase inhibitor active against ACV and foscarnet-resistant HSV. Pritelivir showed a statistically significant reduction in viral shedding and clinical lesions in healthy persons with genital HSV-2 infection, compared to valacyclovir. We report the efficacy and safety of oral…
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Taxonomy
TopicsHerpesvirus Infections and Treatments · RNA Interference and Gene Delivery · Virus-based gene therapy research
