PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE

Yi, Keonwoo

Psychiatria Danubina, Vol. 26 No. suppl 1, 2014.

Conference paper

PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE

Keonwoo Yi ; Downing College Cambridge, School of Clinical Medicine, University of Cambridge, Cambridge, UK

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cite

APA 6th Edition

Yi, K. (2014). PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE. Psychiatria Danubina, 26 (suppl 1), 256-265. Retrieved from https://hrcak.srce.hr/index.php/265728

MLA 8th Edition

Yi, Keonwoo. "PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE." Psychiatria Danubina, vol. 26, no. suppl 1, 2014, pp. 256-265. https://hrcak.srce.hr/index.php/265728. Accessed 17 May 2024.

Chicago 17th Edition

Yi, Keonwoo. "PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE." Psychiatria Danubina 26, no. suppl 1 (2014): 256-265. https://hrcak.srce.hr/index.php/265728

Harvard

Yi, K. (2014). 'PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE', Psychiatria Danubina, 26(suppl 1), pp. 256-265. Available at: https://hrcak.srce.hr/index.php/265728 (Accessed 17 May 2024)

Vancouver

Yi K. PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE. Psychiatria Danubina [Internet]. 2014 [cited 2024 May 17];26(suppl 1):256-265. Available from: https://hrcak.srce.hr/index.php/265728

IEEE

K. Yi, "PASSIVE IMMUNOTHERAPY - A VIABLE TREATMENT FOR ALZHEIMER'S DISEASE", Psychiatria Danubina, vol.26, no. suppl 1, pp. 256-265, 2014. [Online]. Available: https://hrcak.srce.hr/index.php/265728. [Accessed: 17 May 2024]

Abstract

Passive immunotherapy is one of the most exciting and extensively researched areas in the field of Alzheimer’s disease (AD)
today, harbouring the potential to become the first disease-modifying treatment for the disease. The interest in immunotherapy as a
treatment stemmed from the significant dangers of toxic side-effects and major obstacles in selectivity for currently pursued therapies
against amyloid beta (Aβ) proteins and neurofibrillary tangles. Passive immunotherapy especially, has received much limelight, seen
as having the potential to be the safer alternative to active immunisation which encountered a significant setback with the notorious
AN-1972 trial in which 6% of the vaccinated patients developed meningoencephalitis. At present, passive immunisation research in
animal models have exclusively focused on targeting Aβ proteins, a widely accepted pathology of AD.Following on from this, the
preliminary results of phase II trials of three distinct passive immunisation strategies were demonstrated at the 2008 International
Conference on Alzheimer’s Disease (ICAD). The three therapeutic strategies each targeted the N-terminal of Aβ, the central epitope
or utilised a polyclonal approach. The results demonstrated potential as well as caution. Efficacy was undoubtedly present but not to
the extent that was hoped and side-effects, most notably vasogenic oedema occurred in the N-terminal targeting antibody,
bapineuzimab. Lessons have been learnt by identifying the possible cause of the problems and have been taken on board to nurture
the proven efficacious results. Key points to be addressed currently are dosage of the agent to ensure that high enough
concentrations enter the central nervous system to be available to cause effect and early enough time of administration to cause
effect. The results of the efficacy and safety phase III trials and the development of newer passive immunotherapeutic agents
addressing the problems are eagerly awaited in the hope of finally yielding a disease modifying therapy of AD.

Keywords

passive immunotherapy; Alzheimer’s disease

Hrčak ID:

265728

URI

https://hrcak.srce.hr/265728

Publication date:

5.11.2014.

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Psychiatria Danubina, Vol. 26 No. suppl 1, 2014.

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