Top

Published in:

Open Access 01-07-2010 | Original Research Article

Content of Botulinum Neurotoxin in Botox®/Vistabel®, Dysport®/Azzalure®, and Xeomin®/Bocouture®

Author: Dr Jürgen Frevert

Published in: Drugs in R&D | Issue 2/2010

Abstract

Background: Botulinum neurotoxin type A (BoNT/A) is the active substance in preparations used for the highly effective treatment of neurologic disorders such as cervical dystonia, blepharospasm, or spasticity, as well as other indications such as axillary and palmar hyperhidrosis, and urologic disorders.

Objective: To determine the amount of BoNT/A protein present in pharmaceutical preparations of Botox®, Dysport®, and Xeomin®, which are identical with Vistabel®, Azzalure®, and Bocouture®, respectively.

Methods: Rabbit and guinea pig antibodies raised against the 150kD BoNT/A neurotoxin purified from Clostridium botulinum type A, strain ATCC 3502 (‘Hall strain’), were used in a sensitive sandwich ELISA to determine the overall mean concentration of the 150kD neurotoxin present in four batches of Botox® (C2344C3, C2384C3, C2419, and C2385), two batches of Dysport® (678F and 689X) and three batches of Xeomin® (61111, 70604, and 81 208). The specific neurotoxin potency, defined as the potency or biologic activity (units) per mass of neurotoxin protein (ng), was calculated based on the overall mean concentration of BoNT/A neurotoxin.

Results: Overall, the mean concentration of BoNT/A neurotoxin in Botox® was 0.73 ng per 100 unit vial (coefficient of variation [CV] = 3.5%), 3.24 ng per 500 unit vial of Dysport®, corresponding to 0.65 ng in 100 units (CV = 11.4%), and 0.44 ng per 100 unit vial of Xeomin® (CV = 1.9%). The specific potency of the 150kD BoNT/A neurotoxin was calculated as 137 units/ng for Botox®, 154 units/ng Dysport®, and 227 units/ng Xeomin®.

Conclusions: The current study has shown that of the three products, Xeomin® contains the highest specific neurotoxin activity, followed by Dysport®, with Botox® having the lowest specific activity. This result suggests that Xeomin® contains only active neurotoxin in contrast with Botox®, which is likely to contain additional denatured/inactive neurotoxin.

Jankovic J, Albanese A, Attassi MZ, et al. Botulinum toxintherapeutic clinical practice and science. Philadelphia (PA): Saunders Elsevier, 2009

Bhidayasiri R, Truong DD. Evidence for effectiveness of botulinum toxin for hyperhidrosis. J Neural Transm 2008; 115 (4): 641–5PubMedCrossRef

Smith CP. Botulinum toxin in the treatment of OAB, BPH, and IC. Toxicon 2009 Oct; 54 (5): 639–46PubMedCrossRef

Fagien S, Carruthers JD. A comprehensive review of patientreported satisfaction with botulinumtoxin typeAfor aesthetic procedures. Plast Reconstr Surg 2008 Dec; 122 (6): 1915–25PubMedCrossRef

Rossetto O, Morbiato L, Caccin P, et al. Presynaptic enzymatic neurotoxins. J Neurochem 2006 Jun; 97 (6): 1534–45PubMedCrossRef

Schantz EJ, Johnson EA. Properties and use of botulinum toxin and other microbial neurotoxins in medicine. Microbiol Rev 1992 Mar; 56 (1): 80–99PubMed

Lietzow MA, Gielow ET, Le D, et al. Subunit stoichiometry of the Clostridium botulinum type A neurotoxin complex determined using denaturing capillary electrophoresis. Protein J 2008 Dec; 27 (7–8): 420–5PubMedCrossRef

Hambleton P. Clostridium botulinum toxins: a general review of involvement in disease, structure, mode of action and preparation for clinical use. J Neurol 1992 Jan; 239 (1): 16–20PubMedCrossRef

Panjwani N, O’Keeffe R, Pickett A. Biochemical, functional and potency characteristics of type A botulinum toxin in clinical use. Botulinum J 2008; 1 (1): 153–66CrossRef

10.

Benecke R, Jost WH, Kanovsky P, et al. A new botulinum toxin type A free of complexing proteins for treatment of cervical dystonia. Neurology 2005 Jun 14; 64 (11): 1949–51PubMedCrossRef

11.

Roggenkamper P, Jost WH, Bihari K, et al. Efficacy and safety of a new botulinum toxin type A free of complexing proteins in the treatment of blepharospasm. J Neural Transm 2006 Mar; 113 (3): 303–12PubMedCrossRef

12.

Sattler G. Comparison of the efficacy and safety of NT 201, free of complexing proteins, with a licensed botulinum toxin type A in the treatment of glabellar frown lines. IMCAS conference; 2010 Jan 8–11; Paris

13.

Dressler D, Mander G, Fink K. Equivalent potency ofXeomin® and Botox® [abstract]. Movement Disorder Society’s Twelfth International Congress of Parkinson’s Disease and Movement Disorders. Mov Disord 2008; 23 (S1): S20–1

14.

Jost WH, Blumel J, Grafe S. Botulinum neurotoxin type A free of complexing proteins (XEOMIN) in focal dystonia. Drugs 2007; 67 (5): 669–83PubMedCrossRef

15.

Marchetti A, Magar R, Findley L, et al. Retrospective evaluation of the dose of Dysport and BOTOX in the management of cervical dystonia and blepharospasm: the REAL DOSE study. Mov Disord 2005 Aug; 20 (8): 937–44PubMedCrossRef

16.

Allergan Inc. BOTOX (Botulinumtoxin type A) purified neurotoxin complex: prescribing information revised March 2010 [online]. Available from URL: http://www.allergan. com/assets/pdf/botox®pi.pdf [Accessed 2010 Jul 26]

17.

Speywood Pharmaceuticals Limited. Dysport Clostridium botulinum type A toxin-haemagglutinin complex: prescribing information revised 1994. Speywood Pharmaceuticals Limited: Maidenhead (now Ipsen, Slough, UK), 1994

18.

Schellekens H. How to predict and prevent the immunogenicity of therapeutic proteins. Biotechnol Annu Rev 2008; 14: 191–202PubMedCrossRef

19.

Ekong TA, McLellan K, Sesardic D. Immunological detection of Clostridium botulinum toxin type A in therapeutic preparations. J Immunol Methods 1995 27; 180 (2): 181–91PubMedCrossRef

20.

DasGupta BR, Sathyamoorthy V. Purification and amino acid composition of type A botulinum neurotoxin. Toxicon 1984; 22 (3): 415–24PubMedCrossRef

21.

International Conference on Harmonization Guideline Q2B validation of analytical procedures: methodology.US FDA, 1997

22.

Grein S, Mander GJ, d Harold V, et al. Xeomin® is stable without refrigeration: complexing proteins are not required for stability of botulinum neurotoxin type A preparations [abstract and poster]. Toxins conference; 2008 Jun 12–14, Baveno. Toxicon 2008; 51 Suppl. 1: 13

23.

Hunt TJ. Improved botulinum toxin composition.US Patent application 2007/0025019 [online]. Available from URL: http://www.wipo.int/pctdb/en/wo.jsp?wo=2007016018&IA= US2006028603&DISPLAY=DESC. [Accessed 2010 Jul 23]

24.

Bigalke H. Properties of pharmaceutical products of botulinum neurotoxins (chapter 32). In: Jankovic J, Albanese A, Attassi MZ, et al., editors. Botulinum toxin-therapeutic clinical practice and science. Philadelphia (PA): Saunders Elsevier, 2009

25.

Goodnough MC, Johnson EA. Stabilization of botulinum toxin type A during lyophilization. Appl Environ Microbiol 1992 Oct; 58 (10): 3426–8PubMed

26.

Shone CC, Tranter HS. Growth of clostridia and preparation of their neurotoxins. Curr Top Microbiol Immunol 1995; 195: 143–60PubMedCrossRef

27.

Data on file. Merz Pharmaceuticals GmbH, 2004

Title: Content of Botulinum Neurotoxin in Botox®/Vistabel®, Dysport®/Azzalure®, and Xeomin®/Bocouture®
Author: Dr Jürgen Frevert
Publication date: 01-07-2010
Publisher: Springer International Publishing
Published in: Drugs in R&D / Issue 2/2010
Print ISSN: 1174-5886
Electronic ISSN: 1179-6901
DOI: https://doi.org/10.2165/11584780-000000000-00000

Keynote webinar | Spotlight on medication adherence

Springer Medicine

Content of Botulinum Neurotoxin in Botox®/Vistabel®, Dysport®/Azzalure®, and Xeomin®/Bocouture®

Abstract

Keynote webinar | Spotlight on medication adherence

Springer Medicine

Abstract

Please log in to get access to this content

Other articles of this Issue 2/2010

Closed Gateways — Can Neuroprotectants Shield the Retina in Glaucoma?

Tremelimumab

Is it Possible to Accurately Determine Content of Botulinum Neurotoxin Type A in Drug Products?

Metabolism and Disposition of Tribendimidine and Its Metabolites in Healthy Chinese Volunteers

Linifanib

Visual Field Protective Effect of Erigeron breviscapus (vant.) Hand. Mazz. Extract on Glaucoma with Controlled Intraocular Pressure