Transient Facial Nerve Paralysis (Bell's Palsy) following Intranasal Delivery of a Genetically Detoxified Mutant of Escherichia coli Heat Labile Toxin |
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| Authors: | David J M Lewis Zhiming Huo Susan Barnett Ingrid Kromann Rafaela Giemza Eva Galiza Maria Woodrow Birgit Thierry-Carstensen Peter Andersen Deborah Novicki Giuseppe Del Giudice Rino Rappuoli |
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| Institution: | 1. St George''s Vaccine Institute, St George''s University of London, London, United Kingdom.; 2. Novartis Vaccines, Siena, Italy.; 3. Staten Serum Institute, Copenhagen, Denmark.;Charité-Universitätsmedizin Berlin, Germany |
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| Abstract: | BackgroundAn association was previously established between facial nerve paralysis (Bell''s palsy) and intranasal administration of an inactivated influenza virosome vaccine containing an enzymatically active Escherichia coli Heat Labile Toxin (LT) adjuvant. The individual component(s) responsible for paralysis were not identified, and the vaccine was withdrawn.Methodology/Principal FindingsSubjects participating in two contemporaneous non-randomized Phase 1 clinical trials of nasal subunit vaccines against Human Immunodeficiency Virus and tuberculosis, both of which employed an enzymatically inactive non-toxic mutant LT adjuvant (LTK63), underwent active follow-up for adverse events using diary-cards and clinical examination. Two healthy subjects experienced transient peripheral facial nerve palsies 44 and 60 days after passive nasal instillation of LTK63, possibly a result of retrograde axonal transport after neuronal ganglioside binding or an inflammatory immune response, but without exaggerated immune responses to LTK63.Conclusions/SignificanceWhile the unique anatomical predisposition of the facial nerve to compression suggests nasal delivery of neuronal-binding LT–derived adjuvants is inadvisable, their continued investigation as topical or mucosal adjuvants and antigens appears warranted on the basis of longstanding safety via oral, percutaneous, and other mucosal routes. |
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