Induction of cerebral β-amyloidosis: Intracerebral versus systemic Aβ inoculation

  1. Yvonne S. Eiselea,b,
  2. Tristan Bolmonta,
  3. Mathias Heikenwalderc,
  4. Franziska Langera,b,
  5. Laura H. Jacobsond,
  6. Zheng-Xin Yane,
  7. Klaus Rothe,
  8. Adriano Aguzzic,
  9. Matthias Staufenbield,
  10. Lary C. Walkerf and
  11. Mathias Juckera,g,1
  1. aDepartment of Cellular Neurology, Hertie Institute for Clinical Brain Research, University of Tübingen, D-72076 Tübingen, Germany;
  2. bGraduate School for Cellular and Molecular Neuroscience, University of Tübingen, D-72074 Tübingen, Germany;
  3. cDepartment of Pathology, Institute for Neuropathology, University Hospital, Zürich, CH-8091 Switzerland;
  4. dNervous System Research, Novartis Institutes for Biomedical Research, CH-4002 Basel, Switzerland;
  5. eSMP GmbH, D-72072 Tübingen, Germany;
  6. fYerkes National Primate Research Center and Department of Neurology, Emory University, Atlanta, GA 30322; and
  7. gGerman Center for Neurodegenerative Diseases, 72076 Tübingen, Germany

Abstract

Despite the importance of the aberrant polymerization of Aβ in the early pathogenic cascade of Alzheimer's disease, little is known about the induction of Aβ aggregation in vivo. Here we show that induction of cerebral β-amyloidosis can be achieved in many different brain areas of APP23 transgenic mice through the injection of dilute Aβ-containing brain extracts. Once the amyloidogenic process has been exogenously induced, the nature of the induced Aβ-deposition is determined by the brain region of the host. Because these observations are reminiscent of a prion-like mechanism, we then investigated whether cerebral β-amyloidosis also can be induced by peripheral and systemic inoculations or by the intracerebral implantation of stainless steel wires previously coated with minute amounts of Aβ-containing brain extract. Results reveal that oral, intravenous, intraocular, and intranasal inoculations yielded no detectable induction of cerebral β-amyloidosis in APP23 transgenic mice. In contrast, transmission of cerebral β-amyloidosis through the Aβ-contaminated steel wires was demonstrated. Notably, plasma sterilization, but not boiling of the wires before implantation, prevented the induction of β-amyloidosis. Our results suggest that minute amounts of Aβ-containing brain material in direct contact with the CNS can induce cerebral β-amyloidosis, but that systemic cellular mechanisms of prion uptake and transport to the CNS may not apply to Aβ.

Footnotes

  • 1To whom correspondence should be addressed. E-mail: mathias.jucker{at}uni-tuebingen.de

  • Edited by Stanley B. Prusiner, University of California, San Francisco, CA, and approved June 4, 2009

  • Author contributions: Y.S.E., M.H., L.C.W., and M.J. designed research; Y.S.E., T.B., M.H., F.L., and L.H.J. performed research; Z.-X.Y., K.R., A.A., and M.S. contributed new reagents/analytic tools; Y.S.E. and M.J. analyzed data; and Y.S.E., M.H., M.S., L.C.W., and M.J. wrote the paper.

  • The authors declare no conflict of interest.

  • This article is a PNAS Direct Submission.

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  1. Published online before print July 21, 2009, doi: 10.1073/pnas.0903200106 PNAS August 4, 2009 vol. 106 no. 31 12926-12931
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