Assessing adverse effects of intra-articular botulinum toxin A in healthy Beagle dogs: A placebo-controlled, blinded, randomized trial

Heikkilä, Helka; Jokinen, Tarja S.; Syrjä, Pernilla; Junnila, Jouni; Hielm‐Björkman, Anna; Laitinen‐Vapaavuori, Outi

doi:10.1371/journal.pone.0191043

Cited by 12 publications

(5 citation statements)

References 89 publications

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“…In the present study, no serious adverse events were noted. This result supports previous studies that reported minimal adverse effects following IA BoNT-A injection in dogs [12,13,14,15].…”

Section: Discussionsupporting

confidence: 92%

Intra-articular botulinum toxin A (BoNT/A) for pain management in dogs with osteoarthritis secondary to hip dysplasia: A randomized controlled clinical trial

Nicácio

Luna

Cavaleti

et al. 2019

The Journal of Veterinary Medical Science

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The aim of this study was to evaluate the efficacy and safety of the intra-articular (IA) injection of botulinum toxin type A (BoNT/A) to the management of chronic pain in dogs. In a randomized, controlled, double-blinded study sixteen dogs with osteoarthritis secondary to hip dysplasia were distributed into two groups: 25 IU BoNT/A (BoNT) or saline solution (Control) was administered IA in each affected joint. All dogs received oral supplements (90 days) and carprofen (15 days). The dogs were assessed by a veterinarian on five occasions and the owner completed an assessment form at the same time (baseline to 90 days). The data were analyzed using unpaired-t test, Fisher’s exact test, analysis of variance and the Tukey’s test ( P <0.05). There were no differences between groups in the veterinarian and owner assessments. Lower scores were observed in both groups during 90 days after IA therapy in the owner assessments ( P <0.001). Compared with baseline, the Vet score was lower from 15–90 days after IA injection in the BoNT group, and at 15 and 30 days in the Control group ( P <0.001). Both treatments were safe and reduced the clinical signs associated with hip osteoarthritis. However, IA BoNT/A (25 IU) did not provide better pain relief than the control treatment.

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Section: Discussionsupporting

confidence: 92%

Intra-articular botulinum toxin A (BoNT/A) for pain management in dogs with osteoarthritis secondary to hip dysplasia: A randomized controlled clinical trial

Nicácio

Luna

Cavaleti

et al. 2019

The Journal of Veterinary Medical Science

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“…Murine CFA, COL IA BoNT/A vs. sham Reduced spontaneous and evoked pain behaviors in CFA arthritis, reduced spontaneous pain behavior in COL arthritis [50,51] Murine COL IA BoNT/B vs. saline or sham injection Improved visual gait analysis, improved joint tenderness [52] Dog, hip OA IA BoNT/A vs. saline BoNT did not provide better pain relief than a control [56] Dog, OA, multiple joints IA BoNT/A vs. placebo Outcome measured after 12 weeks Improved peak vertical force, improved Helsinki chronic pain index, no effect on synovial fluid SP or PGE2 levels [55,57] Healthy Beagles (safety study) IA BoNT vs. placebo No adverse clinical, cytological, or histopathological effects. Some EMG evidence for spread outside the joints to muscle [58] Rat BSA TMJ inflammatory arthritis IA BoNT/A followed by pain induction with formalin injection Significantly reduced pain behaviors, reduced SP and CGRP release, no change in glutamate release, reduced release of IL-1β but not TNFα [54] Rat CFA tibiotarsal joint IA BoNT/A (dose-ranging) compared to CFA alone and saline control All pain outcomes improved in a dose-dependent fashion.…”

Section: Arthritis Model Experiments Results Referencementioning

confidence: 99%

The Use of Botulinum Toxin for the Treatment of Chronic Joint Pain: Clinical and Experimental Evidence

Blanshan

Krug

2020

Toxins

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Chronic osteoarthritis pain is an increasing worldwide problem. Treatment for osteoarthritis pain is generally inadequate or fraught with potential toxicities. Botulinum toxins (BoNTs) are potent inhibitors of neuropeptide release. Paralytic toxicity is due to inhibition at the neuromuscular junction, and this effect has been utilized for treatments of painful dystonias. Pain relief following BoNT muscle injection has been noted to be more significant than muscle weakness and hypothesized to occur because of the inhibition of peripheral neuropeptide release and reduction of peripheral sensitization. Because of this observation, BoNT has been studied as an intra-articular (IA) analgesic for chronic joint pain. In clinical trials, BoNT appears to be effective for nociceptive joint pain. No toxicity has been reported. In preclinical models of joint pain, BoNT is similarly effective. Examination of the dorsal root ganglion (DRG) and the central nervous system has shown that catalytically active BoNT is retrogradely transported by neurons and then transcytosed to afferent synapses in the brain. This suggests that pain relief may also be due to the central effects of the drug. In summary, BoNT appears to be safe and effective for the treatment of chronic joint pain. The long-term effects of IA BoNT are still being determined.

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“…This study evaluated dynamic and static weight bearing, range of motion, joint tenderness, synovial fluid, neurologic function and electrophysiologic recordings, and histopathology of joint structures and adjacent muscles and nerves. Intra-articular botulinum toxin A did not produce significant clinical, cytological, or histopathological adverse effects in healthy dogs, but based on the electrophysiological recordings that found low compound muscle action potentials in 2 dogs in the botulinum toxin injected limb, the authors concluded that toxin may spread from the joint, but that its clinical impact is probably low [34]. In rats with inflammatory arthritis of the temporal mandibular joint (TMJ) produced by immunization with bovine serum albumin (BSA) and subsequent intra-articular challenge with BSA, injecting the joint with botulinum toxin A significantly reduced nociceptive behaviors that resulted from IA injection of low dose formalin into these inflamed joints.…”

Section: Botulinum Toxin Studies In Preclinical Models Of Joint Painmentioning

confidence: 99%

The Use of Neurotoxins for Palliative Treatment of Chronic Joint Pain

Krug¹

2019

From Conventional to Innovative Approaches for Pain Treatment

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Osteoarthritis is a significant public health problem and is rapidly increasing in prevalence with the aging population. Pain is the most disabling consequence of osteoarthritis. Treatment for pain is inadequate and needs to be addressed with new therapeutic modalities. Chronic pain is often the result of peripheral and central pain sensitization which reduces the pain threshold and increases the perceived pain response to noxious and even non-noxious stimuli. Neurotoxins can reduce this sensitization by various mechanisms and are a fertile area of research for the treatment of chronic pain. Botulinum toxins, vanilloids, and conotoxin have all been studied for the treatment of chronic pain. Botulinum toxins and vanilloids have the greatest potential as analgesics for chronic joint pain thus far. Monoclonal antibodies directed against nerve growth factor have also been developed for the treatment of chronic joint pain due to osteoarthritis. These antibodies are not technically neurotoxins but have significant analgesic potential. However, they may have undesirable side effects and are still being evaluated as possible therapies for chronic osteoarthritis pain.

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Assessing adverse effects of intra-articular botulinum toxin A in healthy Beagle dogs: A placebo-controlled, blinded, randomized trial

Cited by 12 publications

References 89 publications

Intra-articular botulinum toxin A (BoNT/A) for pain management in dogs with osteoarthritis secondary to hip dysplasia: A randomized controlled clinical trial

Intra-articular botulinum toxin A (BoNT/A) for pain management in dogs with osteoarthritis secondary to hip dysplasia: A randomized controlled clinical trial

The Use of Botulinum Toxin for the Treatment of Chronic Joint Pain: Clinical and Experimental Evidence

The Use of Neurotoxins for Palliative Treatment of Chronic Joint Pain

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