Safety, tolerability and immunogenicity of an active anti-Aβ40 vaccine (ABvac40) in patients with Alzheimer’s disease: a randomised, double-blind, placebo-controlled, phase I trial

Lacosta, Ana-María; Pascual‐Lucas, María; Pesini, Pedro; Casabona, Diego; Pérez‐Grijalba, Virginia; Marcos-Campos, Iván; Sarasa, Leticia; Canudas, Jesús; Badi, Hassnae; Monleón, Inmaculada; San-José, Itziar; Munuera, Josep; Rodríguez-Gómez, Octavio; Abdelnour, Carla; Lafuente, Asunción; Buendía, Mar; Boada, Merçé; Tárraga, Lluís; Ruiz, Agustín; Sarasa, Manuel

doi:10.1186/s13195-018-0340-8

Cited by 70 publications

(38 citation statements)

References 59 publications

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“…47,48 ADvac40 did not significantly change levels of plasma Aβ 1-40 . 40 The median concentration of plasma Aβ 1-40 in phase IIa trials of CAD106 reached a maximum of approximately two to three-fold of the baseline level (at 57 weeks, 1 week after the fourth injection), and maintained nearly that level through week 122. 41 In a phase IIb trial of CAD106, median concentration of plasma Aβ 1-40 reached a maximum of approximately 3 times the baseline level (at 38 weeks, 2 weeks after the fifth injection), and maintained a level about double the baseline through week 90, 30 weeks after the last injection.…”

Section: Vaccination For Admentioning

confidence: 98%

“…38 Median Aβ antibody titers in human trials of ADvac40 reached 810 after the third vaccination (given at week eight). 40 Median Aβ antibody titers in phase IIa trials of CAD106 reached a maximum (at 8 weeks, 2 weeks after the third injection) of about 40-50 units (in reference to rhesus monkey reference serum), and a sustained level (at 122 weeks, 30 weeks after the last injection) of 23-24 units. 41 In a phase IIb trial of CAD106, mean Aβ antibody titers reached a maximum (at 8 weeks, 2 weeks after the second injection) of about 40-90 units, and remained between about 20 and 120 units for the rest of trial.…”

Section: Vaccination For Admentioning

confidence: 98%

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Rationale for the development of an Alzheimer’s disease vaccine

Kwan

Konno

Chan

et al. 2019

Human Vaccines & Immunotherapeutics

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Vaccination traditionally has targeted infectious agents and thus has not heretofore been used to prevent neurodegenerative illness. However, amyloid β (Aβ) or tau, which can act like infectious proteins, or prions, might induce Alzheimer's disease (AD). Furthermore, evidence suggests that traditional infectious agents, including certain viruses and bacteria, may trigger AD. It is therefore worth exploring whether removing such targets could prevent AD. Although failing to treat AD patients who already display cognitive impairment, Aβ monoclonal antibodies are being tested in pre-symptomatic, at-risk individuals to prevent dementia. These antibodies might become the first AD therapeutics. However, their high cost will keep them out of the arms of the vast majority of patients, who increasingly live in developing countries. Because vaccines produce antibodies internally at much lower cost, vaccination might be the most promising approach to reducing the global burden of dementia.

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Section: Vaccination For Admentioning

confidence: 98%

Section: Vaccination For Admentioning

confidence: 98%

Rationale for the development of an Alzheimer’s disease vaccine

Kwan

Konno

Chan

et al. 2019

Human Vaccines & Immunotherapeutics

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“…Interindividual variability may prove a particularly serious problem for vaccines that focus the antibody response on a precise target, for instance, a short B cell epitope, as in the case of many second generation anti-Aβ vaccines for the prevention of Alzheimer's Disease. Since a clinical trial of immunization of Alzheimer's Disease patients with the full-length Aβ peptide 1-42 caused aseptic meningoencephalitis in some individuals [17], with evidence of a T cell infiltrate in the brain, several anti-Aβ vaccines have been generated that do not contain T cell epitopes of β-amyloid and combine a defined B cell epitope with a carrier [18][19][20][21][22][23][24].…”

Section: Discussionmentioning

confidence: 99%

Analysis of the Consolidation Phase of Immunological Memory within the IgG Response to a B Cell Epitope Displayed on a Filamentous Bacteriophage

Mantile

Capasso

Berardinis³

et al. 2020

Microorganisms

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Immunological memory can be defined as the ability to mount a response of greater magnitude and with faster kinetics upon re-encounter of the same antigen. We have previously reported that a booster dose of a protein antigen given 15 days after the first dose interferes with the development of memory, i.e., with the ability to mount an epitope-specific IgG response of greater magnitude upon re-encounter of the same antigen. We named the time-window during which memory is vulnerable to disruption a “consolidation phase in immunological memory”, by analogy with the memory consolidation processes that occur in the nervous system to stabilize memory traces. In this study, we set out to establish if a similar memory consolidation phase occurs in the IgG response to a B cell epitope displayed on a filamentous bacteriophage. To this end, we have analyzed the time-course of anti-β-amyloid IgG titers in mice immunized with prototype Alzheimer’s Disease vaccine fdAD(2-6), which consists of a fd phage that displays the B epitope AEFRH of β -amyloid at the N-terminus of the Major Capsid Protein. A booster dose of phage fdAD(2-6) given 15 days after priming significantly reduced the ratio between the magnitude of the secondary and primary IgG response to β-amyloid. This analysis confirms, in a phage vaccine, a consolidation phase in immunological memory, occurring two weeks after priming.

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“…The free fraction in plasma (FP) of Aβ was quantified by direct analysis of plasma samples, whereas total Aβ in plasma (TP) levels were determined in diluted samples, as previously described (Perez-Grijalba et al, 2015 , 2016 ). Detection of anti-A β 40 and A β 42 antibodies in plasma (Experiment 2): Plasma anti-Aβ40 antibody levels were measured at the Araclon Biotech laboratory with ELISAs as previously reported (Lacosta et al, 2018 ). These assays yielded an estimate of the net adsorbed signal (NAS) defined as the difference between the absorbance observed without pre-adsorption and that observed in the pre-adsorbed sample with the C-terminal peptide of Aβ1-40 or Aβ1-42.…”

Section: Participants and Methodsmentioning

confidence: 99%

“…Detection of anti-A β 40 and A β 42 antibodies in plasma (Experiment 2): Plasma anti-Aβ40 antibody levels were measured at the Araclon Biotech laboratory with ELISAs as previously reported (Lacosta et al, 2018 ). These assays yielded an estimate of the net adsorbed signal (NAS) defined as the difference between the absorbance observed without pre-adsorption and that observed in the pre-adsorbed sample with the C-terminal peptide of Aβ1-40 or Aβ1-42.…”

Section: Participants and Methodsmentioning

confidence: 99%

Blood Markers in Healthy-Aged Nonagenarians: A Combination of High Telomere Length and Low Amyloidβ Are Strongly Associated With Healthy Aging in the Oldest Old

Fernández‐Eulate

Alberro

Muñoz-Culla

et al. 2018

Front. Aging Neurosci.

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Many factors may converge in healthy aging in the oldest old, but their association and predictive power on healthy or functionally impaired aging has yet to be demonstrated. By detecting healthy aging and in turn, poor aging, we could take action to prevent chronic diseases associated with age. We conducted a pilot study comparing results of a set of markers (peripheral blood mononuclear cell or PBMC telomere length, circulating Aβ peptides, anti-Aβ antibodies, and ApoE status) previously associated with poor aging or cognitive deterioration, and their combinations, in a cohort of “neurologically healthy” (both motor and cognitive) nonagenarians (n = 20) and functionally impaired, institutionalized nonagenarians (n = 38) recruited between 2014 and 2015. We recruited 58 nonagenarians (41 women, 70.7%; mean age: 92.37 years in the neurologically healthy group vs. 94.13 years in the functionally impaired group). Healthy nonagenarians had significantly higher mean PBMC telomere lengths (mean = 7, p = 0.001), this being inversely correlated with functional impairment, and lower circulating Aβ40 (total in plasma fraction or TP and free in plasma fraction or FP), Aβ42 (TP and FP) and Aβ17 (FP) levels (FP40 131.35, p = 0.004; TP40 299.10, p = 0.007; FP42 6.29, p = 0.009; TP42 22.53, p = 0.019; FP17 1.32 p = 0.001; TP17 4.47, p = 0.3), after adjusting by age. Although healthy nonagenarians had higher anti-Aβ40 antibody levels (net adsorbed signal or NAS ± SD: 0.211 ± 0.107), the number of participants that pass the threshold (NAS > 3) to be considered as positive did not show such a strong association. There was no association with ApoE status. Additionally, we propose a “Composite Neurologically Healthy Aging Score” combining TP40 and mean PBMC telomere length, the strongest correlation of measured biomarkers with neurologically healthy status in nonagenarians (AUC = 0.904).

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Safety, tolerability and immunogenicity of an active anti-Aβ40 vaccine (ABvac40) in patients with Alzheimer’s disease: a randomised, double-blind, placebo-controlled, phase I trial

Cited by 70 publications

References 59 publications

Rationale for the development of an Alzheimer’s disease vaccine

Rationale for the development of an Alzheimer’s disease vaccine

Analysis of the Consolidation Phase of Immunological Memory within the IgG Response to a B Cell Epitope Displayed on a Filamentous Bacteriophage

Blood Markers in Healthy-Aged Nonagenarians: A Combination of High Telomere Length and Low Amyloidβ Are Strongly Associated With Healthy Aging in the Oldest Old

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