Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice.

Nevena Djogo; Igor Jakovcevski; Christian Müller; Hyun Joon Lee; Jin-Chong Xu; Mira Jakovcevski; Sebastian Kügler; Gabriele Loers; Melitta Schachner

doi:10.1016/j.nbd.2013.04.014

Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice.

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Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice. / Djogo, Nevena; Jakovcevski, Igor; Müller, Christian; Lee, Hyun Joon; Xu, Jin-Chong; Jakovcevski, Mira; Kügler, Sebastian; Loers, Gabriele; Schachner, Melitta.

in: NEUROBIOL DIS, Jahrgang 56, 08.2013, S. 104-115.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Djogo, N, Jakovcevski, I, Müller, C, Lee, HJ, Xu, J-C, Jakovcevski, M, Kügler, S, Loers, G & Schachner, M 2013, 'Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice.', NEUROBIOL DIS, Jg. 56, S. 104-115. https://doi.org/10.1016/j.nbd.2013.04.014

APA

Djogo, N., Jakovcevski, I., Müller, C., Lee, H. J., Xu, J-C., Jakovcevski, M., Kügler, S., Loers, G., & Schachner, M. (2013). Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice. NEUROBIOL DIS, 56, 104-115. https://doi.org/10.1016/j.nbd.2013.04.014

Vancouver

Djogo N, Jakovcevski I, Müller C, Lee HJ, Xu J-C, Jakovcevski M et al. Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice. NEUROBIOL DIS. 2013 Aug;56:104-115. https://doi.org/10.1016/j.nbd.2013.04.014

Bibtex

@article{6aa1514993214e8eb6616cc44c9fb6a7,

title = "Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice.",

abstract = "Alzheimer's disease (AD) is a devastating neurodegenerative disorder and the most common cause of elderly dementia. In an effort to contribute to the potential of molecular approaches to reduce degenerative processes we have tested the possibility that the neural adhesion molecule L1 ameliorates some characteristic cellular and molecular parameters associated with the disease in a mouse model of AD. Three-month-old mice overexpressing mutated forms of amyloid precursor protein and presenilin-1 under the control of a neuron-specific promoter received an injection of adeno-associated virus encoding the neuronal isoform of full-length L1 (AAV-L1) or, as negative control, green fluorescent protein (AAV-GFP) into the hippocampus and occipital cortex. Four months after virus injection, the mice were analyzed for histological and biochemical parameters of AD. AAV-L1 injection decreased the Aβ plaque load, levels of Aβ42, Aβ42/40 ratio and astrogliosis compared with AAV-GFP controls. AAV-L1 injected mice also had increased densities of inhibitory synaptic terminals on pyramidal cells in the hippocampus when compared with AAV-GFP controls. Numbers of microglial cells/macrophages were similar in both groups, but numbers of microglial cells/macrophages per plaque were increased in AAV-L1 injected mice. To probe for a molecular mechanism that may underlie these effects, we analyzed whether L1 would directly and specifically interact with Aβ. In a label-free binding assay, concentration dependent binding of the extracellular domain of L1, but not of the close homolog of L1 to Aβ40 and Aβ42 was seen, with the fibronectin type III homologous repeats 1-3 of L1 mediating this effect. Aggregation of Aβ42 in vitro was reduced in the presence of the extracellular domain of L1. The combined observations indicate that L1, when overexpressed in neurons and glia, reduces several histopathological hallmarks of AD in mice, possibly by reduction of Aβ aggregation. L1 thus appears to be a candidate molecule to ameliorate the pathology of AD, when applied in therapeutically viable treatment schemes.",

author = "Nevena Djogo and Igor Jakovcevski and Christian M{\"u}ller and Lee, {Hyun Joon} and Jin-Chong Xu and Mira Jakovcevski and Sebastian K{\"u}gler and Gabriele Loers and Melitta Schachner",

note = "Nevena Djogo and Igor Jakovcevski are equaly contributing authors ",

year = "2013",

month = aug,

doi = "10.1016/j.nbd.2013.04.014",

language = "English",

volume = "56",

pages = "104--115",

journal = "NEUROBIOL DIS",

issn = "0969-9961",

publisher = "Academic Press Inc.",

}

RIS

TY - JOUR

T1 - Adhesion molecule L1 binds to amyloid beta and reduces Alzheimer's disease pathology in mice.

AU - Djogo, Nevena

AU - Jakovcevski, Igor

AU - Müller, Christian

AU - Lee, Hyun Joon

AU - Xu, Jin-Chong

AU - Jakovcevski, Mira

AU - Kügler, Sebastian

AU - Loers, Gabriele

AU - Schachner, Melitta

N1 - Nevena Djogo and Igor Jakovcevski are equaly contributing authors

PY - 2013/8

Y1 - 2013/8

N2 - Alzheimer's disease (AD) is a devastating neurodegenerative disorder and the most common cause of elderly dementia. In an effort to contribute to the potential of molecular approaches to reduce degenerative processes we have tested the possibility that the neural adhesion molecule L1 ameliorates some characteristic cellular and molecular parameters associated with the disease in a mouse model of AD. Three-month-old mice overexpressing mutated forms of amyloid precursor protein and presenilin-1 under the control of a neuron-specific promoter received an injection of adeno-associated virus encoding the neuronal isoform of full-length L1 (AAV-L1) or, as negative control, green fluorescent protein (AAV-GFP) into the hippocampus and occipital cortex. Four months after virus injection, the mice were analyzed for histological and biochemical parameters of AD. AAV-L1 injection decreased the Aβ plaque load, levels of Aβ42, Aβ42/40 ratio and astrogliosis compared with AAV-GFP controls. AAV-L1 injected mice also had increased densities of inhibitory synaptic terminals on pyramidal cells in the hippocampus when compared with AAV-GFP controls. Numbers of microglial cells/macrophages were similar in both groups, but numbers of microglial cells/macrophages per plaque were increased in AAV-L1 injected mice. To probe for a molecular mechanism that may underlie these effects, we analyzed whether L1 would directly and specifically interact with Aβ. In a label-free binding assay, concentration dependent binding of the extracellular domain of L1, but not of the close homolog of L1 to Aβ40 and Aβ42 was seen, with the fibronectin type III homologous repeats 1-3 of L1 mediating this effect. Aggregation of Aβ42 in vitro was reduced in the presence of the extracellular domain of L1. The combined observations indicate that L1, when overexpressed in neurons and glia, reduces several histopathological hallmarks of AD in mice, possibly by reduction of Aβ aggregation. L1 thus appears to be a candidate molecule to ameliorate the pathology of AD, when applied in therapeutically viable treatment schemes.

AB - Alzheimer's disease (AD) is a devastating neurodegenerative disorder and the most common cause of elderly dementia. In an effort to contribute to the potential of molecular approaches to reduce degenerative processes we have tested the possibility that the neural adhesion molecule L1 ameliorates some characteristic cellular and molecular parameters associated with the disease in a mouse model of AD. Three-month-old mice overexpressing mutated forms of amyloid precursor protein and presenilin-1 under the control of a neuron-specific promoter received an injection of adeno-associated virus encoding the neuronal isoform of full-length L1 (AAV-L1) or, as negative control, green fluorescent protein (AAV-GFP) into the hippocampus and occipital cortex. Four months after virus injection, the mice were analyzed for histological and biochemical parameters of AD. AAV-L1 injection decreased the Aβ plaque load, levels of Aβ42, Aβ42/40 ratio and astrogliosis compared with AAV-GFP controls. AAV-L1 injected mice also had increased densities of inhibitory synaptic terminals on pyramidal cells in the hippocampus when compared with AAV-GFP controls. Numbers of microglial cells/macrophages were similar in both groups, but numbers of microglial cells/macrophages per plaque were increased in AAV-L1 injected mice. To probe for a molecular mechanism that may underlie these effects, we analyzed whether L1 would directly and specifically interact with Aβ. In a label-free binding assay, concentration dependent binding of the extracellular domain of L1, but not of the close homolog of L1 to Aβ40 and Aβ42 was seen, with the fibronectin type III homologous repeats 1-3 of L1 mediating this effect. Aggregation of Aβ42 in vitro was reduced in the presence of the extracellular domain of L1. The combined observations indicate that L1, when overexpressed in neurons and glia, reduces several histopathological hallmarks of AD in mice, possibly by reduction of Aβ aggregation. L1 thus appears to be a candidate molecule to ameliorate the pathology of AD, when applied in therapeutically viable treatment schemes.

U2 - 10.1016/j.nbd.2013.04.014

DO - 10.1016/j.nbd.2013.04.014

M3 - SCORING: Journal article

VL - 56

SP - 104

EP - 115

JO - NEUROBIOL DIS

JF - NEUROBIOL DIS

SN - 0969-9961

ER -