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Home: Papers of the Week
Annotation


Fiala M, Liu QN, Sayre J, Pop V, Brahmandam V, Graves MC, Vinters HV. Cyclooxygenase-2-positive macrophages infiltrate the Alzheimer's disease brain and damage the blood-brain barrier. Eur J Clin Invest. 2002 May;32(5):360-71. PubMed Abstract

Comments on Related News
  Related News: Exchange of Letters Asks if Silver Lining in Vaccine Trial Was Real

Comment by:  Milan Fiala (Disclosure)
Submitted 8 February 2004  |  Permalink Posted 8 February 2004

Akiyama and McGeer describe focal clearance of senile plaques in the cortex of a patient with Alzheimer’s disease in an advanced stage. They interpret this as a result of “microglia and macrophage invasion of the affected area.” Their data are remarkable for showing localized areas of clearing related to a hemorrhagic ischemic infarction, which necessarily implies disrupted blood-brain barrier. Although their Fig. 1C shows intensely concentrated typical microglia, an inset in the top part of Fig. 1C shows large cells resembling macrophages. We previously described in Alzheimer’s disease brains large macrophages infiltrating and partially clearing senile plaques (Fiala et al., 2002). One answer to Akiyama's and McGeer's findings is that disrupted blood-brain barrier allowed immigration of blood-borne macrophages and phagocytosis of Aβ by macrophages. Our Fig. 6 shows that infiltrating macrophages can phagocytose and partially clear senile plaques.

Why are brain phagocytic cells of Alzheimer’s disease...  Read more


  Related News: Exchange of Letters Asks if Silver Lining in Vaccine Trial Was Real

Comment by:  Neelima Chauhan
Submitted 8 February 2004  |  Permalink Posted 8 February 2004

There has been considerable interest in using immunization strategies for clearing pre-existing Aβ. Studies in AD-models showed that active or systemic passive immunizations with Aβ peptide reduced cerebral plaques and improved behavior. However, clinical translation of active immunization failed miserably due to inflammation and hemorrhage produced in patients that received Aβ-vaccine (Nicoll et al., 2002). Follow-up studies confirmed that weekly intraperitoneal injections of anti-Aβ for five months resulted in microhemorrhage in APP23 mice with cerebral amyloid angiopathy (CAA) (Pfeifer et al., 2002), and that immunization of C57 mice with Aβ-42 and pertussin toxin developed inflammation in brain and spinal cord (Furlan et al., 2003). I have put forward the idea of immuno-neutralization and intracerebroventricular passive immunization in Tg2576 back in late 90s. Our laboratory has established an effective method of intracerebroventricular (icv) passive immunization that circumvented problems associated with active and systemic passive immunization (Chauhan and Siegel, 2002,...  Read more

  Related News: Exchange of Letters Asks if Silver Lining in Vaccine Trial Was Real

Comment by:  Michael D'Andrea, Robert Nagele
Submitted 17 February 2004  |  Permalink Posted 17 February 2004

Recently, a highly publicized clinical trial of patients vaccinated with the amyloid-β (Aβ) protein was terminated when several patients receiving the vaccine displayed CNS complications that included extensive encephalitis and macrophage infiltration into the brain parenchyma; they also had a reduction in amyloid plaques. In this report, Akiyama and McGeer report a reduction in senile plaques in a region of the cortex of a 79-year-old Alzheimer’s patient showing incomplete ischemia. They suggest that the observed plaque reduction is due to the activity of microglia and macrophages, which immigrated into the affected region, and further propose that encephalitis, regardless of cause, may promote the removal of amyloid plaques through enhanced phagocytosis.

The idea that local ischemia and the resulting inflammatory response may create conditions that favor removal of existing plaques through the action of local phagocytic cells is provocative. Since this work deals with a single case, the results of further confirmatory work will be eagerly awaited to see if this phenomenon...  Read more

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