Literature DB >> 8717340

Production and increased detection of amyloid beta protein and amyloidogenic fragments in brain microvessels, meningeal vessels and choroid plexus in Alzheimer's disease.

R N Kalaria1, D R Premkumar, A B Pax, D L Cohen, I Lieberburg.   

Abstract

Recent advances indicate soluble amyloid beta (A beta) protein is produced constitutively during normal metabolism of the amyloid precursor protein (APP). This has not been directly examined in human brain vascular tissues. Using a panel of well-characterized antibodies, here we show that increased amounts of soluble A beta were found in isolated vascular tissues from AD subjects compared to age-matched controls without significant Alzheimer pathology. Immunocytochemical analyses of isolated vessel preparations showed characteristic transverse patterns of A beta deposits in large vessels with smooth muscle, however, fine A beta deposits were apparent even in capillaries. A proportion of such A beta protein and potentially amyloidogenic carboxyl terminal fragments were released by solubilization and disruption of the vascular basement membrane by collagenase treatments. We further demonstrated by in vitro metabolic labelling that soluble A beta or an A beta-like peptide is associated and produced by cerebral microvessels, meningeal vessels and the choroid plexus isolated postmortem from human as well as rat brain. Compared to those from young rats, cerebral microvessels from aging rats showed increased release of carboxyl terminal fragments of APP and A beta-like peptide. Our observations provide the first direct demonstration that human vascular tissues produce soluble A beta, a product of the secretory pathway in APP processing. Our findings also suggest that aging associated alterations in the basement membranes are a factor in A beta accumulation that results in vascular amyloid deposition, the principal feature of cerebral amyloid angiopathy.

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Year:  1996        PMID: 8717340     DOI: 10.1016/0169-328x(95)00180-z

Source DB:  PubMed          Journal:  Brain Res Mol Brain Res        ISSN: 0169-328X


  36 in total

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2.  Prominent cerebral amyloid angiopathy in transgenic mice overexpressing the london mutant of human APP in neurons.

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Review 3.  Genetic animal models of cerebral vasculopathies.

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4.  Altered clearance of beta-amyloid from the cerebrospinal fluid following subchronic lead exposure in rats: Roles of RAGE and LRP1 in the choroid plexus.

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5.  Amyloid precursor protein mediates monocyte adhesion in AD tissue and apoE(-)/(-) mice.

Authors:  Susan A Austin; Colin K Combs
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6.  Macromolecules involved in production and metabolism of beta-amyloid at the brain barriers.

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7.  Brain ventricular volume and cerebrospinal fluid biomarkers of Alzheimer's disease.

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Journal:  J Alzheimers Dis       Date:  2010       Impact factor: 4.472

8.  γ-secretase binding sites in aged and Alzheimer's disease human cerebrum: the choroid plexus as a putative origin of CSF Aβ.

Authors:  Fei Liu; Zhi-Qin Xue; Si-Hao Deng; Xiong Kun; Xue-Gang Luo; Peter R Patrylo; Gregory M Rose; Huaibin Cai; Robert G Struble; Yan Cai; Xiao-Xin Yan
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9.  Prognostic value of amyloid PET scan in normal pressure hydrocephalus.

Authors:  Hyemin Jang; Seong Beom Park; Yeshin Kim; Ko Woon Kim; Jung Il Lee; Sung Tae Kim; Kyung Han Lee; Eun-Suk Kang; Yeong Sim Choe; Sang Won Seo; Hee Jin Kim; Yeo Jin Kim; Cindy W Yoon; Duk L Na
Journal:  J Neurol       Date:  2017-11-11       Impact factor: 4.849

10.  Neuronal overexpression of mutant amyloid precursor protein results in prominent deposition of cerebrovascular amyloid.

Authors:  M E Calhoun; P Burgermeister; A L Phinney; M Stalder; M Tolnay; K H Wiederhold; D Abramowski; C Sturchler-Pierrat; B Sommer; M Staufenbiel; M Jucker
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