2017
DOI: 10.1016/j.nbd.2017.04.020
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Deletion of exons 9 and 10 of the Presenilin 1 gene in a patient with Early-onset Alzheimer Disease generates longer amyloid seeds

Abstract: Presenilin 1 (PSEN1) mutations are the main cause of autosomal dominant early onset Alzheimer Disease (EOAD). Among them, deletions of exon 9 have been reported to be associated with a phenotype of spastic paraparesis.Using exome data from a large sample of 522 EOAD cases and 584 controls to search for genomic copy-number variations (CNVs), we report here a novel partial, in-frame deletion of PSEN1, removing both exons 9 and 10. The patient presented with memory impairment associated with spastic paraparesis, … Show more

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Cited by 24 publications
(15 citation statements)
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“…PSEN1 Gly183Val revealed in skipping exon 6 or both exon 6-7, resulting in reduced PSEN1 function [31]. PSEN1 Ser290Cys was located at the splice junction of exon 8 and 10, causing deletion of entire exon 9 [32,33]. Additional mutations indicated significant impacts on PSEN1 mRNA splicing, such as Leu113Pro [34], Leu113Gln [35], Glu184Gly [19], Glu184Asp [24], and Arg377Trp [19].…”
Section: Discussionmentioning
confidence: 99%
“…PSEN1 Gly183Val revealed in skipping exon 6 or both exon 6-7, resulting in reduced PSEN1 function [31]. PSEN1 Ser290Cys was located at the splice junction of exon 8 and 10, causing deletion of entire exon 9 [32,33]. Additional mutations indicated significant impacts on PSEN1 mRNA splicing, such as Leu113Pro [34], Leu113Gln [35], Glu184Gly [19], Glu184Asp [24], and Arg377Trp [19].…”
Section: Discussionmentioning
confidence: 99%
“…Aβ length is under the control of the carboxypeptidase activity of the gamma-secretase which cleaves the Aβ peptide from its carboxy-terminal region. Thus, lack of PS1 exon 9 and exon 10 generates longer Aβ peptides (Le Guennec et al, 2017 ). Although speculative, MSX3 could promote the carboxypeptidase activity of the gamma-secretase and thus modify the ratio of Aβ towards the production of shorter species of Aβ peptides.…”
Section: Discussionmentioning
confidence: 99%
“…Mutations/variants in PSEN1, located near the 5 and 3 may eliminate the acceptor or donor splicing site, and result in exon skipping. One of the most known splice site mutations in PSEN1 is the deletion of exon 9 (Ser290Cys) or exon 9 -10 (Ser290Trp), associated with aggressive AD phenotypes [66,67]. Additional exon-skipping mutations were also described, which could result in abnormal splicings, such as Leu113_I114insTyr [68], Leu271Val [69], or Ile416Thr [70].…”
Section: Alternative Splicing Copy Number Variants (Cnvs) In Admentioning
confidence: 99%