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Protein Expression in Down Syndrome Brain

Overview of attention for book
Cover of 'Protein Expression in Down Syndrome Brain'

Table of Contents

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    Book Overview
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    Chapter 1 Decreased alpha-endosulfine, an endogenous regulator of ATP-sensitive potassium channels, in brains from adult Down syndrome patients
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    Chapter 2 Developmental instability of the cerebellum and its relevance to Down syndrome
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    Chapter 3 Expression of the multidrug resistance P glycoprotein (Pgp) and multidrug resistance associated protein (MRP1) in Down syndrome brains
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    Chapter 4 Deterioration of the transcriptional, splicing and elongation machinery in brain of fetal Down Syndrome
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    Chapter 5 Fetal life in Down syndrome starts with normal neuronal density but impaired dendritic spines and synaptosomal structure.
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    Chapter 6 Antioxidant proteins in fetal brain: superoxide dismutase-1 (SOD-1) protein is not overexpressed in fetal Down syndrome
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    Chapter 7 Glial-neurotrophic mechanisms in Down syndrome
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    Chapter 8 Aberrant expression of dihydropyrimidinase related proteins-2,-3 and -4 in fetal Down Syndrome brain
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    Chapter 9 Decreased protein levels of complex I 30-kDa subunit in fetal Down syndrome brains
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    Chapter 10 Selective upregulation of the ubiquitin-proteasome proteolytic pathway proteins, proteasome zeta chain and isopeptidase T in fetal Down syndrome
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    Chapter 11 Functional genomics of Down syndrome: a multidisciplinary approach
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    Chapter 12 Unaltered expression of Fas (CD95/APO-1), Caspase-3, Bcl-2 and Annexins in brains of fetal Down syndrome: evidence against increased apoptosis
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    Chapter 13 Alteration of caspases and other apoptosis regulatory proteins in Down syndrome
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    Chapter 14 Expression of apoptosis related proteins: RAIDD, ZIP kinase, Bim/BOD, p21, Bax, Bcl-2 and NF- k B in brains of patients with Down syndrome
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    Chapter 15 Increased brain protein levels of carbonyl reductase and alcohol dehydrogenase in Down Syndrome and Alzheimer’s disease
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    Chapter 16 Carbohydrate handling enzymes in fetal Down Syndrome brain
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    Chapter 17 Changes in nicotinic acetylcholine receptor subunits expression in brain of patients with Down syndrome and Alzheimer's disease.
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    Chapter 18 Protein levels of human peroxiredoxin subtypes in brains of patients with Alzheimer's disease and Down syndrome.
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    Chapter 19 Effects of a single transdermal nicotine dose on cognitive performance in adults with Down syndrome
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    Chapter 20 The brain in Down syndrome
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    Chapter 21 Decreased levels of ARPP-19 and PKA in brains of Down syndrome and Alzheimer's disease.
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    Chapter 22 Increased protein levels of heterogeneous nuclear ribonucleoprotein A2/B1 in fetal Down syndrome brains
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    Chapter 23 Decreased protein levels of stathmin in adult brains with Down syndrome and Alzheimer’s disease
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    Chapter 24 Molecular neuropathology of transgenic mouse models of Down syndrome
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    Chapter 25 Down syndrome patients start early prenatal life with normal cholinergic, monoaminergic and serotoninergic innervation
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    Chapter 26 Expression profiles of proteins in fetal brain with Down syndrome
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    Chapter 27 Expression patterns of chaperone proteins in cerebral cortex of the fetus with Down Syndrome: dysregulation of T-complex protein 1
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    Chapter 28 β-Amyloid precursor protein, ETS-2 and collagen alpha 1 (VI) chain precursor, encoded on chromosome 21, are not overexpressed in fetal Down syndrome: further evidence against gene dosage effect
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    Chapter 29 Reduction of nucleoside diphosphate kinase B, Rab GDP-dissociation inhibitor beta and histidine triad nucleotide-binding protein in fetal Down syndrome brain.
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    Chapter 30 Alteration of gene expression in Down’s syndrome (DS) brains: its significance in neurodegeneration
Attention for Chapter 5: Fetal life in Down syndrome starts with normal neuronal density but impaired dendritic spines and synaptosomal structure.
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Chapter title
Fetal life in Down syndrome starts with normal neuronal density but impaired dendritic spines and synaptosomal structure.
Chapter number 5
Book title
Protein Expression in Down Syndrome Brain
Published in
Journal of neural transmission Supplementum, January 2001
DOI 10.1007/978-3-7091-6262-0_5
Pubmed ID
11771761
Book ISBNs
978-3-21-183704-7, 978-3-70-916262-0
Authors

R Weitzdoerfer, M Dierssen, M Fountoulakis, G Lubec, Weitzdoerfer, R., Dierssen, M., Fountoulakis, M., Lubec, G., R. Weitzdoerfer, M. Dierssen, M. Fountoulakis, G. Lubec

Abstract

Information on fetal brain in Down Syndrome (DS) is limited and there are only few histological, mainly anecdotal reports and no systematic study on the wiring of the brain in early prenatal life exists. Histological methods are also hampered by inherent problems of morphometry of neuronal structures. It was therefore the aim of the study to evaluate neuronal loss, synaptic structures and dendritic spines in the fetus with Down Syndrome as compared to controls by biochemical measurements. 2 dimensional electrophoresis with subsequent mass spectroscopical identification of spots and their quantification with specific software was selected. This technique identifies proteins unambiguously and concomitantly on the same gel. Fetal cortex samples were taken at autopsy with low post-mortem time, homogenized and neuron specific enolase (NSE) determined as a marker for neuronal density, the synaptosomal associated proteins alpha SNAP [soluble N-ethylmaleimide-sensitive fusion (NSF) attachment protein], beta SNAP, SNAP 25 and the channel associated protein of synapse 110 (chapsyn 110) as markers for synaptosomal structures and drebrin (DRB) as marker for dendritic spines. NSE, chapsyn 110 and beta SNAP were comparable in the control fetus panel and in Down Syndrome fetuses. Drebrin was significantly and remarkably reduced and not even detectable in several Down Syndrome brain samples. Quantification of SNAP 25 revealed significantly reduced values in DS cortex and alpha SNAP was only present in half of the DS individuals. We conclude that at the time point of about 19 weeks of gestation (early second trimester) no neuronal loss can be detected but drebrin, a marker for dendritic spines and synaptosomal associated proteins alpha SNAP and SNAP 25 were significantly reduced indicating impaired synaptogenesis. Early dendritic deterioration maybe leading to the degeneration of the dendritic tree and arborization, which is a hallmark of Down Syndrome from infancy.

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Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 50 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
United Kingdom 2 4%
Unknown 48 96%

Demographic breakdown

Readers by professional status Count As %
Student > Master 12 24%
Student > Ph. D. Student 10 20%
Researcher 9 18%
Student > Bachelor 4 8%
Student > Doctoral Student 1 2%
Other 6 12%
Unknown 8 16%
Readers by discipline Count As %
Agricultural and Biological Sciences 13 26%
Medicine and Dentistry 8 16%
Neuroscience 6 12%
Biochemistry, Genetics and Molecular Biology 4 8%
Psychology 3 6%
Other 5 10%
Unknown 11 22%
Attention Score in Context

Attention Score in Context

This research output has an Altmetric Attention Score of 3. This is our high-level measure of the quality and quantity of online attention that it has received. This Attention Score, as well as the ranking and number of research outputs shown below, was calculated when the research output was last mentioned on 15 December 2021.
All research outputs
#7,425,026
of 22,699,621 outputs
Outputs from Journal of neural transmission Supplementum
#21
of 99 outputs
Outputs of similar age
#26,380
of 114,017 outputs
Outputs of similar age from Journal of neural transmission Supplementum
#3
of 10 outputs
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So far Altmetric has tracked 99 research outputs from this source. They receive a mean Attention Score of 4.1. This one is in the 26th percentile – i.e., 26% of its peers scored the same or lower than it.
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