Differential regional and cellular distribution of β-amyloid precursor protein messenger RNAs containing and lacking the kunitz protease inhibitor domain in the brain of human, rat and mouse

The β-amyloid precursor protein is the precursor of the main component of senile plaques (the β-amyloid peptide or β/A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of β-amyloid precursor p...

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Published inNeuroscience Vol. 53; no. 1; pp. 267 - 295
Main Authors Sola`, C., Mengod, G., Probst, A., Palacios, J.M.
Format Journal Article
LanguageEnglish
Published Oxford Elsevier Ltd 01.03.1993
Elsevier
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Abstract The β-amyloid precursor protein is the precursor of the main component of senile plaques (the β-amyloid peptide or β/A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of β-amyloid precursor protein messenger RNAs have been described in humans and rodents: β-amyloid precursor protein 695, β-amyloid precursor protein 714, β-amyloid precursor protein 751 and β-amyloid precursor protein 770 messenger RNAs (numbers corresponding to the number of encoded amino acids). The two latter forms are characterized by containing in their sequence a region with high homology to the Kunitz family of serine protease inhibitors. We have used oligonucleotide probes to study the distribution of the different messenger RNAs encoding each of the four β-amyloid precursor proteins by in situ hybridization histochemistry in human, rat and mouse brain. We found that β-amyloid precursor protein 695, β-amyloid precursor protein 714 and β-amyloid precursor protein 751 messenger RNAs were widely distributed in the human, rat and mouse brain and that their distribution was roughly similar in most brain areas in these three species. The distribution of β-amyloid precursor protein 770 messenger RNA was not so wide and differed among the three species studied, β-amyloid precursor protein 751 and 770 messenger RNAs were the only forms present at significant levels in rodent choroid plexus and meninges, while β-amyloid precursor protein messenger RNA isoforms containing and lacking the Kunitz domain were detected in the human choroid plexus. We also observed that the relative levels of β-amyloid precursor protein 751 and 770 messenger RNAs in the rat cerebral white matter as well as in the mouse and human striatum were higher than those of the β-amyloid precursor protein messenger RNAs lacking the Kunitz domain. While the most abundant β-amyloid precursor protein messenger RNAs in the brain of all three species under study were, in descending order, β-amyloid precursor protein 695 and β-amyloid precursor protein 751 messenger RNAs, the least abundant form was not the same for all species: in human it was β-amyloid precursor protein 714 messenger RNA and in rat and mouse brain it was β-amyloid precursor protein 770 messenger RNA. Our results show differences both inter- and intraspecies of the relative abundance and distribution of four β-amyloid precursor protein messenger RNAs in rat, mouse and human brain. The non-coincidence of the distribution of β-amyloid precursor protein messenger RNA isoforms suggests different physiological functions for the β-amyloid precursor proteins. Interspecies differences should be considered when comparing results from animal and human studies.
AbstractList The beta -amyloid precursor protein is the precursor of the main component of senile plaques (the beta -amyloid peptide or beta /A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of beta -amyloid precursor protein messenger RNAs have been described in humans and rodents: beta -amyloid precursor protein 695, beta -amyloid precursor protein 714, beta -amyloid precursor protein 751 and beta -amyloid precursor protein 770 messenger RNAs (numbers corresponding to the number of encoded amino acids). The two latter forms are characterized by containing in their sequence a region with high homology to the Kunitz family of serine protease inhibitors. We have used oligonucleotide probes to study the distribution of the different messenger RNAs encoding each of the four beta -amyloid precursor proteins by in situ hybridization histochemistry in human, rat and mouse brain. Our results show differences both inter- and intraspecies of the relative abundance and distribution of four beta -amyloid precursor protein messenger RNAs in rat, mouse and human brain.
The beta-amyloid precursor protein is the precursor of the main component of senile plaques (the beta-amyloid peptide or beta/A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of beta-amyloid precursor protein messenger RNAs have been described in humans and rodents: beta-amyloid precursor protein 695, beta-amyloid precursor protein 714, beta-amyloid precursor protein 751 and beta-amyloid precursor protein 770 messenger RNAs (numbers corresponding to the number of encoded amino acids). The two latter forms are characterized by containing in their sequence a region with high homology to the Kunitz family of serine protease inhibitors. We have used oligonucleotide probes to study the distribution of the different messenger RNAs encoding each of the four beta-amyloid precursor proteins by in situ hybridization histochemistry in human, rat and mouse brain. We found that beta-amyloid precursor protein 695, beta-amyloid precursor protein 714 and beta-amyloid precursor protein 751 messenger RNAs were widely distributed in the human, rat and mouse brain and that their distribution was roughly similar in most brain areas in these three species. The distribution of beta-amyloid precursor protein 770 messenger RNA was not so wide and differed among the three species studied. beta-amyloid precursor protein 751 and 770 messenger RNAs were the only forms present at significant levels in rodent choroid plexus and meninges, while beta-amyloid precursor protein messenger RNA isoforms containing and lacking the Kunitz domain were detected in the human choroid plexus. We also observed that the relative levels of beta-amyloid precursor protein 751 and 770 messenger RNAs in the rat cerebral white matter as well as in the mouse and human striatum were higher than those of the beta-amyloid precursor protein messenger RNAs lacking the Kunitz domain. While the most abundant beta-amyloid precursor protein messenger RNAs in the brain of all three species under study were, in descending order, beta-amyloid precursor protein 695 and beta-amyloid precursor protein 751 messenger RNAs, the least abundant form was not the same for all species: in human it was beta-amyloid precursor protein 714 messenger RNA and in rat and mouse brain it was beta-amyloid precursor protein 770 messenger RNA. Our results show differences both inter- and intraspecies of the relative abundance and distribution of four beta-amyloid precursor protein messenger RNAs in rat, mouse and human brain.The beta-amyloid precursor protein is the precursor of the main component of senile plaques (the beta-amyloid peptide or beta/A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of beta-amyloid precursor protein messenger RNAs have been described in humans and rodents: beta-amyloid precursor protein 695, beta-amyloid precursor protein 714, beta-amyloid precursor protein 751 and beta-amyloid precursor protein 770 messenger RNAs (numbers corresponding to the number of encoded amino acids). The two latter forms are characterized by containing in their sequence a region with high homology to the Kunitz family of serine protease inhibitors. We have used oligonucleotide probes to study the distribution of the different messenger RNAs encoding each of the four beta-amyloid precursor proteins by in situ hybridization histochemistry in human, rat and mouse brain. We found that beta-amyloid precursor protein 695, beta-amyloid precursor protein 714 and beta-amyloid precursor protein 751 messenger RNAs were widely distributed in the human, rat and mouse brain and that their distribution was roughly similar in most brain areas in these three species. The distribution of beta-amyloid precursor protein 770 messenger RNA was not so wide and differed among the three species studied. beta-amyloid precursor protein 751 and 770 messenger RNAs were the only forms present at significant levels in rodent choroid plexus and meninges, while beta-amyloid precursor protein messenger RNA isoforms containing and lacking the Kunitz domain were detected in the human choroid plexus. We also observed that the relative levels of beta-amyloid precursor protein 751 and 770 messenger RNAs in the rat cerebral white matter as well as in the mouse and human striatum were higher than those of the beta-amyloid precursor protein messenger RNAs lacking the Kunitz domain. While the most abundant beta-amyloid precursor protein messenger RNAs in the brain of all three species under study were, in descending order, beta-amyloid precursor protein 695 and beta-amyloid precursor protein 751 messenger RNAs, the least abundant form was not the same for all species: in human it was beta-amyloid precursor protein 714 messenger RNA and in rat and mouse brain it was beta-amyloid precursor protein 770 messenger RNA. Our results show differences both inter- and intraspecies of the relative abundance and distribution of four beta-amyloid precursor protein messenger RNAs in rat, mouse and human brain.
The β-amyloid precursor protein is the precursor of the main component of senile plaques (the β-amyloid peptide or β/A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of β-amyloid precursor protein messenger RNAs have been described in humans and rodents: β-amyloid precursor protein 695, β-amyloid precursor protein 714, β-amyloid precursor protein 751 and β-amyloid precursor protein 770 messenger RNAs (numbers corresponding to the number of encoded amino acids). The two latter forms are characterized by containing in their sequence a region with high homology to the Kunitz family of serine protease inhibitors. We have used oligonucleotide probes to study the distribution of the different messenger RNAs encoding each of the four β-amyloid precursor proteins by in situ hybridization histochemistry in human, rat and mouse brain. We found that β-amyloid precursor protein 695, β-amyloid precursor protein 714 and β-amyloid precursor protein 751 messenger RNAs were widely distributed in the human, rat and mouse brain and that their distribution was roughly similar in most brain areas in these three species. The distribution of β-amyloid precursor protein 770 messenger RNA was not so wide and differed among the three species studied, β-amyloid precursor protein 751 and 770 messenger RNAs were the only forms present at significant levels in rodent choroid plexus and meninges, while β-amyloid precursor protein messenger RNA isoforms containing and lacking the Kunitz domain were detected in the human choroid plexus. We also observed that the relative levels of β-amyloid precursor protein 751 and 770 messenger RNAs in the rat cerebral white matter as well as in the mouse and human striatum were higher than those of the β-amyloid precursor protein messenger RNAs lacking the Kunitz domain. While the most abundant β-amyloid precursor protein messenger RNAs in the brain of all three species under study were, in descending order, β-amyloid precursor protein 695 and β-amyloid precursor protein 751 messenger RNAs, the least abundant form was not the same for all species: in human it was β-amyloid precursor protein 714 messenger RNA and in rat and mouse brain it was β-amyloid precursor protein 770 messenger RNA. Our results show differences both inter- and intraspecies of the relative abundance and distribution of four β-amyloid precursor protein messenger RNAs in rat, mouse and human brain. The non-coincidence of the distribution of β-amyloid precursor protein messenger RNA isoforms suggests different physiological functions for the β-amyloid precursor proteins. Interspecies differences should be considered when comparing results from animal and human studies.
The beta-amyloid precursor protein is the precursor of the main component of senile plaques (the beta-amyloid peptide or beta/A4) found in the brain of aged humans and, in higher amounts, in the brain of Alzheimer's disease and Down's syndrome subjects. Four different forms of beta-amyloid precursor protein messenger RNAs have been described in humans and rodents: beta-amyloid precursor protein 695, beta-amyloid precursor protein 714, beta-amyloid precursor protein 751 and beta-amyloid precursor protein 770 messenger RNAs (numbers corresponding to the number of encoded amino acids). The two latter forms are characterized by containing in their sequence a region with high homology to the Kunitz family of serine protease inhibitors. We have used oligonucleotide probes to study the distribution of the different messenger RNAs encoding each of the four beta-amyloid precursor proteins by in situ hybridization histochemistry in human, rat and mouse brain. We found that beta-amyloid precursor protein 695, beta-amyloid precursor protein 714 and beta-amyloid precursor protein 751 messenger RNAs were widely distributed in the human, rat and mouse brain and that their distribution was roughly similar in most brain areas in these three species. The distribution of beta-amyloid precursor protein 770 messenger RNA was not so wide and differed among the three species studied. beta-amyloid precursor protein 751 and 770 messenger RNAs were the only forms present at significant levels in rodent choroid plexus and meninges, while beta-amyloid precursor protein messenger RNA isoforms containing and lacking the Kunitz domain were detected in the human choroid plexus. We also observed that the relative levels of beta-amyloid precursor protein 751 and 770 messenger RNAs in the rat cerebral white matter as well as in the mouse and human striatum were higher than those of the beta-amyloid precursor protein messenger RNAs lacking the Kunitz domain. While the most abundant beta-amyloid precursor protein messenger RNAs in the brain of all three species under study were, in descending order, beta-amyloid precursor protein 695 and beta-amyloid precursor protein 751 messenger RNAs, the least abundant form was not the same for all species: in human it was beta-amyloid precursor protein 714 messenger RNA and in rat and mouse brain it was beta-amyloid precursor protein 770 messenger RNA. Our results show differences both inter- and intraspecies of the relative abundance and distribution of four beta-amyloid precursor protein messenger RNAs in rat, mouse and human brain.
Author Sola`, C.
Mengod, G.
Probst, A.
Palacios, J.M.
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  fullname: Palacios, J.M.
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Issue 1
Keywords βAPP
PBS
SSC
SDS
KPI
Human
Nervous system diseases
Kunitz inhibitor
Rat
Enzyme
Alzheimer disease
Proteinase
Rodentia
Central nervous system
Amyloid precursor protein
Autoradiography
Vertebrata
Mammalia
Mouse
Animal
Distribution
Degenerative disease
Aminoacid sequence
Brain (vertebrata)
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Snippet The β-amyloid precursor protein is the precursor of the main component of senile plaques (the β-amyloid peptide or β/A4) found in the brain of aged humans and,...
The beta-amyloid precursor protein is the precursor of the main component of senile plaques (the beta-amyloid peptide or beta/A4) found in the brain of aged...
The beta -amyloid precursor protein is the precursor of the main component of senile plaques (the beta -amyloid peptide or beta /A4) found in the brain of aged...
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pubmed
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crossref
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SourceType Aggregation Database
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StartPage 267
SubjectTerms Adult
Aged
Aged, 80 and over
Amyloid beta-Protein Precursor - biosynthesis
Animals
Base Sequence
Biological and medical sciences
Blotting, Northern
Brain - anatomy & histology
Brain - metabolism
Degenerative and inherited degenerative diseases of the nervous system. Leukodystrophies. Prion diseases
Humans
In Situ Hybridization
Male
Medical sciences
Mice
Middle Aged
Molecular Sequence Data
Neurology
Oligonucleotides
Peptide Mapping
Rats
Rats, Wistar
RNA Probes
RNA, Messenger - metabolism
Rodentia
Serine Proteinase Inhibitors - metabolism
Title Differential regional and cellular distribution of β-amyloid precursor protein messenger RNAs containing and lacking the kunitz protease inhibitor domain in the brain of human, rat and mouse
URI https://dx.doi.org/10.1016/0306-4522(93)90304-X
https://www.ncbi.nlm.nih.gov/pubmed/8469310
https://www.proquest.com/docview/16872220
https://www.proquest.com/docview/75676378
Volume 53
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