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Long-term effects of Abeta(42) immunisation in Alzheimer's disease: follow-up of a randomised, placebo-controlled phase I trial

Long-term effects of Abeta(42) immunisation in Alzheimer's disease: follow-up of a randomised, placebo-controlled phase I trial
Long-term effects of Abeta(42) immunisation in Alzheimer's disease: follow-up of a randomised, placebo-controlled phase I trial
Background: Immunisation of patients with Alzheimer's disease with full-length amyloid-? peptide (A?42) can clear amyloid plaques from the brain. Our aim was to assess the relation between A?42 immune response, degree of plaque removal, and long-term clinical outcomes.

Methods: In June, 2003, consent for long-term clinical follow-up, post-mortem neuropathological examination, or both, was sought from 80 patients (or their carers) who had entered a phase I randomised, placebo-controlled trial of immunisation with A?42 (AN1792, Elan Pharmaceuticals) in September, 2000. The follow-up study was completed in September, 2006. Plaques were assessed in terms of the percentage area of the cortex with A? immunostaining (A?42 load) and in terms of characteristic histological features reflecting plaque removal. Survival of all 80 individuals until severe dementia or death was assessed with a Cox proportional hazard model.

Findings: 20 participants-15 in the AN1792 group, five in the placebo group-died before follow-up started. A further 22 patients-19 in the AN1792 group, three in the placebo group-died during follow-up. Nine of the deceased patients, all in the AN1792 group, had given consent for post-mortem analysis; one of these who did not die with Alzheimer's disease was excluded. in the remaining eight participants who received immunisation and who were examined neuropathologically, mean A? load was lower than in an unimmunised control group that was matched for age at death (2.1% [SE 0.7] in treated participants vs 5.1% [0.9] in controls; mean difference 3.0%, 95% CI 0.6-5.4; p=0.02). Although there was considerable variation in A beta load and degree of plaque removal among immunised participants, the degree of plaque removal varied significantly with mean antibody response attained during the treatment study period (Kruskal-Wallis p=0.02). Seven of the eight immunised patients who underwent post-mortem assessment, including those with virtually complete plaque removal, had severe end stage dementia before death. In the whole cohort, there was no evidence of improved survival (hazard ratio 0.93, 95% CI 0.43-3.11; p=0.86) or of an improvement in the time to severe dementia (1.18, 0.45-3.11; p=0.73) in the AN1792 group versus the placebo group.

Interpretation: Although immunisation with A?42 resulted in clearance of amyloid plaques in patients with Alzheimer's disease, this clearance did not prevent progressive neurodegeneration.
treatment, placebo, follow-up, vaccination, antibodies, placebo-controlled trial, ad, disease, care, peptide, memory, amyloid-beta protein, immunotherapy, a?42 immunization, dementia, an1792, trial, model
0140-6736
216-223
Holmes, Clive
ada5abf3-8459-4cf7-be40-3f4e9391cc96
Boche, Delphine
bdcca10e-6302-4dd0-919f-67218f7e0d61
Wilkinson, David
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Yadegarfar, Ghasem
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Hopkins, Vivienne
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Bayer, Anthony
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Jones, Roy W.
c05b5bc5-836c-4bba-b5e8-b3bbe68715dd
Bullock, Roger
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Love, Seth
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Neal, James W.
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Zotova, Elina
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Nicoll, James A.R.
88c0685f-000e-4eb7-8f72-f36b4985e8ed
Holmes, Clive
ada5abf3-8459-4cf7-be40-3f4e9391cc96
Boche, Delphine
bdcca10e-6302-4dd0-919f-67218f7e0d61
Wilkinson, David
4ad8aeac-5d43-4404-be01-85cf314f5aad
Yadegarfar, Ghasem
032b05c6-84d0-49b4-ac8c-626279a5824d
Hopkins, Vivienne
20f9cb08-6c50-4c73-902f-707934ffdc43
Bayer, Anthony
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Jones, Roy W.
c05b5bc5-836c-4bba-b5e8-b3bbe68715dd
Bullock, Roger
60e07513-ab0c-4b75-b6b1-633af699ead0
Love, Seth
c8c00a86-ecf8-4f61-8377-254305bdbc02
Neal, James W.
12d0ba0f-b29d-43ca-8e61-af46a430367b
Zotova, Elina
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Nicoll, James A.R.
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Holmes, Clive, Boche, Delphine, Wilkinson, David, Yadegarfar, Ghasem, Hopkins, Vivienne, Bayer, Anthony, Jones, Roy W., Bullock, Roger, Love, Seth, Neal, James W., Zotova, Elina and Nicoll, James A.R. (2008) Long-term effects of Abeta(42) immunisation in Alzheimer's disease: follow-up of a randomised, placebo-controlled phase I trial. The Lancet, 372 (9634), 216-223. (doi:10.1016/S0140-6736(08)61075-2). (PMID:18640458)

Record type: Article

Abstract

Background: Immunisation of patients with Alzheimer's disease with full-length amyloid-? peptide (A?42) can clear amyloid plaques from the brain. Our aim was to assess the relation between A?42 immune response, degree of plaque removal, and long-term clinical outcomes.

Methods: In June, 2003, consent for long-term clinical follow-up, post-mortem neuropathological examination, or both, was sought from 80 patients (or their carers) who had entered a phase I randomised, placebo-controlled trial of immunisation with A?42 (AN1792, Elan Pharmaceuticals) in September, 2000. The follow-up study was completed in September, 2006. Plaques were assessed in terms of the percentage area of the cortex with A? immunostaining (A?42 load) and in terms of characteristic histological features reflecting plaque removal. Survival of all 80 individuals until severe dementia or death was assessed with a Cox proportional hazard model.

Findings: 20 participants-15 in the AN1792 group, five in the placebo group-died before follow-up started. A further 22 patients-19 in the AN1792 group, three in the placebo group-died during follow-up. Nine of the deceased patients, all in the AN1792 group, had given consent for post-mortem analysis; one of these who did not die with Alzheimer's disease was excluded. in the remaining eight participants who received immunisation and who were examined neuropathologically, mean A? load was lower than in an unimmunised control group that was matched for age at death (2.1% [SE 0.7] in treated participants vs 5.1% [0.9] in controls; mean difference 3.0%, 95% CI 0.6-5.4; p=0.02). Although there was considerable variation in A beta load and degree of plaque removal among immunised participants, the degree of plaque removal varied significantly with mean antibody response attained during the treatment study period (Kruskal-Wallis p=0.02). Seven of the eight immunised patients who underwent post-mortem assessment, including those with virtually complete plaque removal, had severe end stage dementia before death. In the whole cohort, there was no evidence of improved survival (hazard ratio 0.93, 95% CI 0.43-3.11; p=0.86) or of an improvement in the time to severe dementia (1.18, 0.45-3.11; p=0.73) in the AN1792 group versus the placebo group.

Interpretation: Although immunisation with A?42 resulted in clearance of amyloid plaques in patients with Alzheimer's disease, this clearance did not prevent progressive neurodegeneration.

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More information

Published date: 19 July 2008
Keywords: treatment, placebo, follow-up, vaccination, antibodies, placebo-controlled trial, ad, disease, care, peptide, memory, amyloid-beta protein, immunotherapy, a?42 immunization, dementia, an1792, trial, model
Organisations: Medicine

Identifiers

Local EPrints ID: 62408
URI: http://eprints.soton.ac.uk/id/eprint/62408
ISSN: 0140-6736
PURE UUID: 07fa48de-bb11-4def-a4cb-50b04f63b2ff
ORCID for Clive Holmes: ORCID iD orcid.org/0000-0003-1999-6912
ORCID for Delphine Boche: ORCID iD orcid.org/0000-0002-5884-130X
ORCID for James A.R. Nicoll: ORCID iD orcid.org/0000-0002-9444-7246

Catalogue record

Date deposited: 05 Sep 2008
Last modified: 16 Mar 2024 03:26

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Contributors

Author: Clive Holmes ORCID iD
Author: Delphine Boche ORCID iD
Author: David Wilkinson
Author: Ghasem Yadegarfar
Author: Vivienne Hopkins
Author: Anthony Bayer
Author: Roy W. Jones
Author: Roger Bullock
Author: Seth Love
Author: James W. Neal
Author: Elina Zotova

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