Direct Observations of Amyloid beta Self-Assembly in Live Cells Provide Insights into Differences in the Kinetics of A beta(1-40) and A beta(1-42) Aggregation
Journal article, 2014
Insight into how amyloid beta (A beta) aggregation occurs in vivo is vital for understanding the molecular pathways that underlie Alzheimer's disease and requires new techniques that provide detailed kinetic and mechanistic information. Using noninvasive fluorescence lifetime recordings, we imaged the formation of A beta(1-40) and A beta(1-42) aggregates in live cells. For both peptides, the cellular uptake via endocytosis is rapid and spontaneous. They are then retained in lysosomes, where their accumulation leads to aggregation. The kinetics of A beta(1-42) aggregation are considerably faster than those of A beta(1-40) and, unlike those of the latter peptide, show no detectable lag phase. We used superresolution fluorescence imaging to examine the resulting aggregates and could observe compact amyloid structures, likely because of spatial confinement within cellular compartments. Taken together, these findings provide clues as to how A beta aggregation may occur within neurons.
FIBRILS
BRAIN
ACCUMULATION
OLIGOMERS
ALPHA-SYNUCLEIN
ALZHEIMERS-DISEASE
HUMAN
GROWTH
PROTEIN
INTRINSIC FLUORESCENCE
Biochemistry & Molecular Biology
PEPTIDE
Author
Elin Esbjörner Winters
Chemical Biology
F. Chan
University of Cambridge
E. Rees
University of Cambridge
M. Erdelyi
University of Cambridge
L. M. Luheshi
University of Cambridge
C. W. Bertoncini
IRB Barcelona - Institute for Research in Biomedicine
C. F. Kaminski
University of Cambridge
C. M. Dobson
University of Cambridge
G. S. K. Schierle
University of Cambridge
Chemistry and Biology
1074-5521 (ISSN)
Vol. 21 6 732-742Subject Categories
Medical Biotechnology (with a focus on Cell Biology (including Stem Cell Biology), Molecular Biology, Microbiology, Biochemistry or Biopharmacy)
Organic Chemistry
DOI
10.1016/j.chembiol.2014.03.014