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Double-Binding Botulinum Molecule with Reduced Muscle Paralysis: Evaluation in In Vitro and In Vivo Models of Migraine

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dc.contributor.author Andreou A.P.
dc.contributor.author Leese C.
dc.contributor.author Greco R.
dc.contributor.author Demartini C.
dc.contributor.author Corrie E.
dc.contributor.author Simsek D.
dc.contributor.author Zanaboni A.
dc.contributor.author Koroleva K.
dc.contributor.author Lloyd J.O.
dc.contributor.author Lambru G.
dc.contributor.author Doran C.
dc.contributor.author Gafurov O.
dc.contributor.author Seward E.
dc.contributor.author Giniatullin R.
dc.contributor.author Tassorelli C.
dc.contributor.author Davletov B.
dc.date.accessioned 2021-02-25T20:50:19Z
dc.date.available 2021-02-25T20:50:19Z
dc.date.issued 2020
dc.identifier.issn 1933-7213
dc.identifier.uri https://dspace.kpfu.ru/xmlui/handle/net/162505
dc.description.abstract © 2020, The Author(s). With a prevalence of 15%, migraine is the most common neurological disorder and among the most disabling diseases, taking into account years lived with disability. Current oral medications for migraine show variable effects and are frequently associated with intolerable side effects, leading to the dissatisfaction of both patients and doctors. Injectable therapeutics, which include calcitonin gene–related peptide–targeting monoclonal antibodies and botulinum neurotoxin A (BoNT/A), provide a new paradigm for treatment of chronic migraine but are effective only in approximately 50% of subjects. Here, we investigated a novel engineered botulinum molecule with markedly reduced muscle paralyzing properties which could be beneficial for the treatment of migraine. This stapled botulinum molecule with duplicated binding domain—binary toxin-AA (BiTox/AA)—cleaves synaptosomal-associated protein 25 with a similar efficacy to BoNT/A in neurons; however, the paralyzing effect of BiTox/AA was 100 times less when compared to native BoNT/A following muscle injection. The performance of BiTox/AA was evaluated in cellular and animal models of migraine. BiTox/AA inhibited electrical nerve fiber activity in rat meningeal preparations while, in the trigeminovascular model, BiTox/AA raised electrical and mechanical stimulation thresholds in Aδ- and C-fiber nociceptors. In the rat glyceryl trinitrate (GTN) model, BiTox/AA proved effective in inhibiting GTN-induced hyperalgesia in the orofacial formalin test. We conclude that the engineered botulinum molecule provides a useful prototype for designing advanced future therapeutics for an improved efficacy in the treatment of migraine.
dc.relation.ispartofseries Neurotherapeutics
dc.subject botulinum
dc.subject glyceryl trinitrate model
dc.subject Migraine
dc.subject multivalent
dc.subject neuronal delivery
dc.subject trigeminal
dc.subject trigeminovascular
dc.title Double-Binding Botulinum Molecule with Reduced Muscle Paralysis: Evaluation in In Vitro and In Vivo Models of Migraine
dc.type Article
dc.collection Публикации сотрудников КФУ
dc.source.id SCOPUS19337213-2020-SID85096117664


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  • Публикации сотрудников КФУ Scopus [24551]
    Коллекция содержит публикации сотрудников Казанского федерального (до 2010 года Казанского государственного) университета, проиндексированные в БД Scopus, начиная с 1970г.

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