Immunogenicity Associated with Botulinum Toxin Treatment

Bellows, Steven T.; Jankovic, Joseph

doi:10.3390/toxins11090491

Cited by 115 publications

(148 citation statements)

References 91 publications

(216 reference statements)

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“…Many of the points raised in the commentary by Foster and Beard are echoed in our review [1]. Immunoresistance is a rare phenomenon and accounts for a small minority of patients found to be unresponsive to BoNT.…”

mentioning

confidence: 58%

“…examined NAb prevalence in patients treated with BoNT for spasticity. This indication, as discussed in our review [1], appears to have a very low rate of NAbs formation and, therefore, is not suitable for addressing immunogenicity. Likewise, the review by Lacroix-Desmazes et al [6] is not appropriate for citation as the investigators excluded data from studies on patients with SNR.…”

mentioning

confidence: 88%

“…In our review we noted that some patients desire shorter injection cycles, based on a survey which found that 45% of patients expressed preference for a treatment cycle of less than 10 weeks [11]. Although this view is frequently expressed by patients treated with BoNT, we certainly do not endorse or advocate for "booster" injections, which in the past have been associated with high frequency of immunoresistance [1]. Most studies examining the effects and safety of shorter inter-dose intervals used incobotulinumtoxinA [12][13][14], but more comparative data are needed before concluding that one product or another is associated with less immunogenicity or longer duration of action [15].…”

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confidence: 90%

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Reply to Comment on Re-Visiting Immunogenicity Associated with Botulinum Toxin Treatment. Toxins 2019, 11, 491

Bellows

Jankovic

2020

Toxins

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confidence: 58%

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confidence: 88%

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confidence: 90%

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Reply to Comment on Re-Visiting Immunogenicity Associated with Botulinum Toxin Treatment. Toxins 2019, 11, 491

Bellows

Jankovic

2020

Toxins

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“…Many investigative methods to confirm diagnosis of BTF were developed. These methods described elsewhere 4,26,27 . They can be categorized as in vitro tests and in vivo tests as summarized in Table 2.…”

Section: Investigation For Antibody‐induced Btfmentioning

confidence: 99%

Antibody‐induced botulinum toxin treatment failure: A review and novel management approach

Srinoulprasert

Wanitphakdeedecha

2020

J of Cosmetic Dermatology

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Background Botulinum neurotoxin A (BoNT/A) has been used for cosmetic indications for many decades. Consumption of BoNT/A usage has been markedly increased for a few years. Even new formulations of BoNT/A to decrease immunogenicity have been released, repeated treatment to maintain efficacy outcome is inevitable and could finally provoke immune response. In the past, prevalence of botulinum treatment failure (BTF) in cosmetic indication was rare leading to less medical concern. Current decade, case reports on BTF, especially antibody‐induced botulinum toxin treatment failure (ABTF), have been increasingly revealed and risk factors associated with ABTF have been intensively studied. Aims In this article, we will review antibody‐induced botulinum toxin treatment failure (ABTF), risk‐associated ABTF, prevalence and recent case reports of ABTF, and new approach to deal with ABTF. Methods Literature search was conducted using PubMed. The relevant literatures published between January 2000 and May 2020 concerning BTF and ABTF including investigation for ABTF were included and analyzed. Results Possible causes of BTF were summarized. ABTF could be a tip of iceberg of BTF, its prevalence, and currently, 10‐year case reports of ABTF were published evidence. Risk factors and investigation methods for ABTF were also summarized. Based on previous studies and our experience, novel approach to management of ABTF was described. Conclusion Effective management of BTF is to explore causes of treatment failure. Antibodies against BoNT/A complex could be one of many possibilities. Laboratory in vitro tests could be alternative tools to decrease adverse effect and rebooting immune responses in BTF patients.

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“…Enhancing toxin binding to nerve terminals facilitates their absorption into local neurons, thus reducing both diffusion from the injection site, which can lead to severe adverse effects [55], and the chance of triggering antibody responses, which renders future treatment ineffective [56]. For instance, BoNT/B shows lower efficacy in humans than BoNT/A, as a single residue change in human Syt II from the mouse version reduced binding affinity of BoNT/B to human Syt II [8,48].…”

Section: Introductionmentioning

confidence: 99%

Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy

et al. 2020

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Immunogenicity Associated with Botulinum Toxin Treatment

Cited by 115 publications

References 91 publications

Reply to Comment on Re-Visiting Immunogenicity Associated with Botulinum Toxin Treatment. Toxins 2019, 11, 491

Reply to Comment on Re-Visiting Immunogenicity Associated with Botulinum Toxin Treatment. Toxins 2019, 11, 491

Antibody‐induced botulinum toxin treatment failure: A review and novel management approach

Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy

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