Diffusible, nonfibrillar ligands derived from Aβ1-42 are potent central nervous system neurotoxins

M. P. Lambert; A. K. Barlow; B. A. Chromy; C. Edwards; R. Freed; M. Liosatos; T. E. Morgan; I. Rozovsky; B. Trommer; K. L. Viola; P. Wals; C. Zhang; C. E. Finch; G. A. Krafft; W. L. Klein

doi:10.1073/pnas.95.11.6448

Diffusible, nonfibrillar ligands derived from Aβ_1-42 are potent central nervous system neurotoxins

M. P. Lambert, A. K. Barlow, B. A. Chromy, C. Edwards, R. Freed, M. Liosatos, T. E. Morgan, I. Rozovsky, B. Trommer, K. L. Viola, P. Wals, C. Zhang, C. E. Finch, G. A. Krafft, W. L. Klein^*

^*Corresponding author for this work

Neurobiology

Research output: Contribution to journal › Article › peer-review

2901 Scopus citations

Abstract

Aβ_1-42 is a self-associating peptide whose neurotoxic derivatives are thought to play a role in Alzheinier's pathogenesis. Neurotoxicity of amyloid β protein (Aβ) has been attributed to its fibrillar forms, but experiments presented here characterize neurotoxins that assemble when fibril formation is inhibited. These neurotoxins comprise small diffusible Aβ oligomers (referred to as ADDLs, for Aβ-derived diffusible ligands), which were found to kill mature neurons in organotypic central nervous system cultures at nanomolar concentrations. At cell surfaces, ADDLs bound to trypsin-sensitive sites and surface-derived tryptic peptides blocked binding and afforded neuroprotection. Germ-line knockout of Fyn, a protein tyrosine kinase linked to apoptosis and elevated in Alzheimer's disease, also was neuroprotective. Remarkably, neurological dysfunction evoked by ADDLs occurred well in advance of cellular degeneration. Without lag, and despite retention of evoked action potentials, ADDLs inhibited hippocampal long-term potentiation, indicating an immediate impact on signal transduction. We hypothesize that impaired synaptic plasticity and associated memory dysfunction during early stage Alzheimer's disease and severe cellular degeneration and dementia during end stage could be caused by the biphasic impact of Aβ-derived diffusible ligands acting upon particular neural signal transduction pathways.

Original language	English (US)
Pages (from-to)	6448-6453
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	95
Issue number	11
DOIs	https://doi.org/10.1073/pnas.95.11.6448
State	Published - May 26 1998

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Lambert, M. P., Barlow, A. K., Chromy, B. A., Edwards, C., Freed, R., Liosatos, M., Morgan, T. E., Rozovsky, I., Trommer, B., Viola, K. L., Wals, P., Zhang, C., Finch, C. E., Krafft, G. A., & Klein, W. L. (1998). Diffusible, nonfibrillar ligands derived from Aβ_1-42 are potent central nervous system neurotoxins. Proceedings of the National Academy of Sciences of the United States of America, 95(11), 6448-6453. https://doi.org/10.1073/pnas.95.11.6448

Lambert, M. P. ; Barlow, A. K. ; Chromy, B. A. ; Edwards, C. ; Freed, R. ; Liosatos, M. ; Morgan, T. E. ; Rozovsky, I. ; Trommer, B. ; Viola, K. L. ; Wals, P. ; Zhang, C. ; Finch, C. E. ; Krafft, G. A. ; Klein, W. L. / Diffusible, nonfibrillar ligands derived from Aβ_1-42 are potent central nervous system neurotoxins. In: Proceedings of the National Academy of Sciences of the United States of America. 1998 ; Vol. 95, No. 11. pp. 6448-6453.

@article{65f39308bdf743d0a8cf036e07f194ae,

title = "Diffusible, nonfibrillar ligands derived from Aβ1-42 are potent central nervous system neurotoxins",

abstract = "Aβ1-42 is a self-associating peptide whose neurotoxic derivatives are thought to play a role in Alzheinier's pathogenesis. Neurotoxicity of amyloid β protein (Aβ) has been attributed to its fibrillar forms, but experiments presented here characterize neurotoxins that assemble when fibril formation is inhibited. These neurotoxins comprise small diffusible Aβ oligomers (referred to as ADDLs, for Aβ-derived diffusible ligands), which were found to kill mature neurons in organotypic central nervous system cultures at nanomolar concentrations. At cell surfaces, ADDLs bound to trypsin-sensitive sites and surface-derived tryptic peptides blocked binding and afforded neuroprotection. Germ-line knockout of Fyn, a protein tyrosine kinase linked to apoptosis and elevated in Alzheimer's disease, also was neuroprotective. Remarkably, neurological dysfunction evoked by ADDLs occurred well in advance of cellular degeneration. Without lag, and despite retention of evoked action potentials, ADDLs inhibited hippocampal long-term potentiation, indicating an immediate impact on signal transduction. We hypothesize that impaired synaptic plasticity and associated memory dysfunction during early stage Alzheimer's disease and severe cellular degeneration and dementia during end stage could be caused by the biphasic impact of Aβ-derived diffusible ligands acting upon particular neural signal transduction pathways.",

author = "Lambert, {M. P.} and Barlow, {A. K.} and Chromy, {B. A.} and C. Edwards and R. Freed and M. Liosatos and Morgan, {T. E.} and I. Rozovsky and B. Trommer and Viola, {K. L.} and P. Wals and C. Zhang and Finch, {C. E.} and Krafft, {G. A.} and Klein, {W. L.}",

year = "1998",

month = may,

day = "26",

doi = "10.1073/pnas.95.11.6448",

language = "English (US)",

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journal = "Proceedings of the National Academy of Sciences of the United States of America",

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Lambert, MP, Barlow, AK, Chromy, BA, Edwards, C, Freed, R, Liosatos, M, Morgan, TE, Rozovsky, I, Trommer, B, Viola, KL, Wals, P, Zhang, C, Finch, CE, Krafft, GA & Klein, WL 1998, 'Diffusible, nonfibrillar ligands derived from Aβ_1-42 are potent central nervous system neurotoxins', Proceedings of the National Academy of Sciences of the United States of America, vol. 95, no. 11, pp. 6448-6453. https://doi.org/10.1073/pnas.95.11.6448

Diffusible, nonfibrillar ligands derived from Aβ_1-42 are potent central nervous system neurotoxins. / Lambert, M. P.; Barlow, A. K.; Chromy, B. A.; Edwards, C.; Freed, R.; Liosatos, M.; Morgan, T. E.; Rozovsky, I.; Trommer, B.; Viola, K. L.; Wals, P.; Zhang, C.; Finch, C. E.; Krafft, G. A.; Klein, W. L.

In: Proceedings of the National Academy of Sciences of the United States of America, Vol. 95, No. 11, 26.05.1998, p. 6448-6453.

Research output: Contribution to journal › Article › peer-review

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T1 - Diffusible, nonfibrillar ligands derived from Aβ1-42 are potent central nervous system neurotoxins

AU - Lambert, M. P.

AU - Barlow, A. K.

AU - Chromy, B. A.

AU - Edwards, C.

AU - Freed, R.

AU - Liosatos, M.

AU - Morgan, T. E.

AU - Rozovsky, I.

AU - Trommer, B.

AU - Viola, K. L.

AU - Wals, P.

AU - Zhang, C.

AU - Finch, C. E.

AU - Krafft, G. A.

AU - Klein, W. L.

PY - 1998/5/26

Y1 - 1998/5/26

N2 - Aβ1-42 is a self-associating peptide whose neurotoxic derivatives are thought to play a role in Alzheinier's pathogenesis. Neurotoxicity of amyloid β protein (Aβ) has been attributed to its fibrillar forms, but experiments presented here characterize neurotoxins that assemble when fibril formation is inhibited. These neurotoxins comprise small diffusible Aβ oligomers (referred to as ADDLs, for Aβ-derived diffusible ligands), which were found to kill mature neurons in organotypic central nervous system cultures at nanomolar concentrations. At cell surfaces, ADDLs bound to trypsin-sensitive sites and surface-derived tryptic peptides blocked binding and afforded neuroprotection. Germ-line knockout of Fyn, a protein tyrosine kinase linked to apoptosis and elevated in Alzheimer's disease, also was neuroprotective. Remarkably, neurological dysfunction evoked by ADDLs occurred well in advance of cellular degeneration. Without lag, and despite retention of evoked action potentials, ADDLs inhibited hippocampal long-term potentiation, indicating an immediate impact on signal transduction. We hypothesize that impaired synaptic plasticity and associated memory dysfunction during early stage Alzheimer's disease and severe cellular degeneration and dementia during end stage could be caused by the biphasic impact of Aβ-derived diffusible ligands acting upon particular neural signal transduction pathways.

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