LPS receptor (CD14): a receptor for phagocytosis of Alzheimer's amyloid peptide

doi:10.1093/brain/awh531

Brain Advance Access first published online on April 27, 2005
This version published online on May 31, 2005
Brain, doi:10.1093/brain/awh531

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Article

LPS receptor (CD14): a receptor for phagocytosis of Alzheimer's amyloid peptide

Yang Liu ¹^*, Silke Walter ¹, Massimiliano Stagi ², Dmitry Cherny ³, Maryse Letiembre ¹, Walter Schulz-Schaeffer ⁴, Holger Heine ⁵, Botond Penke ⁶, Harald Neumann ², and Klaus Fassbender ¹

¹ Department of Neurology, University of Göttingen, Göttingen, Germany
² European Neuroscience Institute, University of Göttingen and Hertie-Foundation, Göttingen, Germany; Institute of Multiple Sclerosis Research, University of Göttingen and Hertie-Foundation, Göttingen, Germany
³ Department of Biochemistry, University of Leicester, Leicester, UK; Institute of Molecular Genetics, Russian Academy of Sciences, Moscow, Russia
⁴ Department of Neuropathology, University of Göttingen, Göttingen, Germany
⁵ Borstel Research Centre, Centre for Medicine and Biosciences, Borstel, Germany
⁶ Department of Medical Chemistry, Albert Szent Gyorgyi Medical University, Szeged, Hungary

^* To whom correspondence should be addressed.
Yang Liu, E-mail: alexliu{at}med.uni-goettingen.de

Abstract

The amyloid ${beta}$ peptide 42 (A ${beta}$ ₄₂) plays a key role in neurotoxicityin Alzheimer's disease. Mononuclear phagocytes, i.e. microglia,have the potential to clear A ${beta}$ by phagocytosis. Recently, thelipopolysaccharide (LPS) receptor CD14 was shown to mediatephagocytosis of bacterial components and furthermore to contributeto neuroinflammation in Alzheimer's disease. Here, we investigatedwhether this key innate immunity receptor can interact withA ${beta}$ ₄₂ and mediate phagocytosis of this peptide. Using flow cytometry,confocal microscopy and two-photon fluorescence lifetime imaging(FLIM) combined with fluorescence resonance energy transfer(FRET), we demonstrated a direct molecular interaction in therange of a few nanometers between A ${beta}$ ₄₂ and CD14 in human CD14-transfectedChinese hamster ovary cells. Investigations using cells thatwere genetically deficient for this receptor showed that in<30 minutes exogenous A ${beta}$ ₄₂ added to cultured primary microglialcells was phagocytosed into the cytoplasmic compartment in aCD14-dependent manner. This phagocytosis occurred at A ${beta}$ ₄₂ concentrationranges that were considerably lower than the threshold to activatea cellular inflammatory reaction. In contrast, there was noassociation of CD14 to microglial internalization of microbeads.In complementary clinical experiments, we detected a pronouncedCD14 immunoreactivity on parenchymal microglia spatially correlatedto characteristic Alzheimer's disease lesion sites in brainsections of Alzheimer's disease patients but not in brain sectionsof control subjects. By showing a close interaction betweenCD14 and A ${beta}$ ₄₂, demonstrating a direct role of CD14 in A ${beta}$ ₄₂ phagocytosis,and detecting CD14-specific staining in brains of Alzheimer'sdisease patients, our results indicate a role of the LPS receptorin the pathophysiology of Alzheimer's disease, which could beof therapeutic relevance.

Keywords: Alzheimer's disease; amyloid ${beta}$ protein; CD14; microglia; phagocytosis.

On page 4, line 9 under the title ‘Molecular interaction between ...’ the word ‘photons’ has been changed to the word ‘energy’

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