Debulking Influenza and Herpes Simplex virus strains by a wide-spectrum anti-viral protein formulated in clinical grade chewing gum
Daniell, Henry; Guo, Yuwei; Singh, Rahul; Karki, Uddhab; Kulchar, Rachel J.; Wakade, Geetanjali; Pihlava, Juha-Matti; Khazaei, Hamid; Cohen, Gary H. (2025)
Lataukset
Daniell, Henry
Guo, Yuwei
Singh, Rahul
Karki, Uddhab
Kulchar, Rachel J.
Wakade, Geetanjali
Pihlava, Juha-Matti
Khazaei, Hamid
Cohen, Gary H.
Julkaisusarja
Molecular therapy
Volyymi
33
Numero
1
Sivut
184-200
Academic Press
2025
Julkaisun pysyvä osoite on
http://urn.fi/URN:NBN:fi-fe202501102458
http://urn.fi/URN:NBN:fi-fe202501102458
Tiivistelmä
Lack of Herpes Simplex Virus (HSV) vaccine, low vaccination rates of Influenza viruses, waning immunity and viral transmission after vaccination underscore the need to reduce viral loads at their transmission sites. Oral virus transmission is several orders of magnitude higher than nasal transmission. Therefore, in this study, we evaluated neutralization of viruses using a natural viral trap protein (FRIL) formulated in clinical-grade chewing gum. FRIL is highly stable in the lablab bean powder (683 days) and in chewing gum (790 days), and fully functional (794 days) when stored at ambient temperature. They passed the bioburden test with no aerobic bacteria, yeasts/molds, with minimal moisture content (1.28–5.9%). Bean gum extracts trapped HSV-1/HSV-2 75–94% in a dose-dependent manner through virus self-aggregation. Mastication simulator released >50% release of FRIL within 15 min of chewing the bean gum. In plaque reduction assays, >95% neutralization of H1N1 and H3N2 required ∼40 mg/mL, HSV-1 160 mg/mL, and HSV-2 74 mg/mL of bean gum for 1,000 copies/mL virus particles. Therefore, a 2000 mg bean gum tablet has more than adequate potency for clinical evaluation and is safe with no detectable levels of glycosides. These observations augur well for evaluating bean gum in human clinical studies to minimize virus infection/transmission.
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