2018
DOI: 10.1002/mgg3.409
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Interstitial microdeletion of the 1p34.3p34.2 region

Abstract: BackgroundInterstitial microdeletions of chromosome 1p34.3p34.2 are rare, but are continuing to be identified by the use of chromosome microarray. There have been fewer than 10 individuals identified who have deletions of the 1p34.3p34.2 region; all of these previously described individuals have deletions of the AGO1, AGO3, GRIK3, SLC2A1, or RIMS3 genes. Haploinsufficiency of these genes has been associated with neurodevelopmental delays.MethodsChromosome microarray, quantitative PCR, and fluorescence in situ … Show more

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Cited by 8 publications
(8 citation statements)
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“…Large deletions at the 1p34.3 locus including AGO1 together with AGO3 (and sometimes AGO4 ) among other genes were previously reported in five children with psychomotor developmental delay as well as additional non-specific features (feeding difficulty, language impairment, facial dysmorphy) 13 14. In addition, AGO2 was very recently implicated in NDD15: 21 individuals with heterozygous de novo variants in AGO2 were reported, including 11 missense variants, one in-frame deletion and one 235 kb deletion involving the first three exons of AGO2 .…”
Section: Introductionmentioning
confidence: 97%
“…Large deletions at the 1p34.3 locus including AGO1 together with AGO3 (and sometimes AGO4 ) among other genes were previously reported in five children with psychomotor developmental delay as well as additional non-specific features (feeding difficulty, language impairment, facial dysmorphy) 13 14. In addition, AGO2 was very recently implicated in NDD15: 21 individuals with heterozygous de novo variants in AGO2 were reported, including 11 missense variants, one in-frame deletion and one 235 kb deletion involving the first three exons of AGO2 .…”
Section: Introductionmentioning
confidence: 97%
“…Large deletions of 1.1 Mb to 3.1 Mb at the 1p34.3 loci including AGO1 together with AGO3 (and sometimes AGO4 among other genes) were previously reported in children with NDD 13,14 . These five individuals presented with psychomotor developmental delay as well as additional non-specific features (feeding difficulty, language impairment, facial dysmorphy).…”
Section: Introductionmentioning
confidence: 68%
“…together with AGO3 (and sometimes AGO4 among other genes), and a deletion encompassing the AGO2 fist 3 exons challenges this observation [13][14][15] . AGO2 variant functional analysis revealed a complex cellular deregulation: a decrease in mRNA silencing was observed as expected for a LoF mechanism but with a variable impact, depending on the mRNA target and the tested AGO2 variant.…”
Section: Variants Are Predicted To Affect Ago1 Dynamic Conformationalmentioning
confidence: 99%
“…While the pathomolecular outcomes associated with the SNIP1 NM_024700.4:c.1097A>G, p.(Glu366Gly) substitution remain unclear, SNIP1 null mouse models display embryonic lethality indicating that this Amish variant may be unlikely to result in complete loss of function [ 14 ]. While no other biallelic variants in SNIP1 have conclusively been associated with genetic disease to date, Jacher and Innis (2018) reported a 17-year-old female with a de novo 2.3 Mb interstitial deletion at 1q34.3q34.2 that encompassed 43 genes, of which only two ( SNIP1 and RSPO1 ) were potentially linked with genetic disease genes at the time of publication [ 15 ]. This female had global developmental delay, mild intellectual disability, congenital defects, vocal cord paralysis, delayed bone age, and skeletal deformities.…”
Section: Discussionmentioning
confidence: 99%