2017
DOI: 10.1101/gr.226621.117
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ABCA4 midigenes reveal the full splice spectrum of all reported noncanonical splice site variants in Stargardt disease

Abstract: Stargardt disease is caused by variants in the gene, a significant part of which are noncanonical splice site (NCSS) variants. In case a gene of interest is not expressed in available somatic cells, small genomic fragments carrying potential disease-associated variants are tested for splice abnormalities using in vitro splice assays. We recently discovered that when using small minigenes lacking the proper genomic context, in vitro results do not correlate with splice defects observed in patient cells. We ther… Show more

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Cited by 142 publications
(208 citation statements)
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References 47 publications
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“…Other variants included a stop-gain, c.6088C>T (p.Arg2030*) variant in Patient 3 and 8 noncoding variants: 5 variants in canonical splice site sequences (c.4773+3A>G, c.2160+1G>C, c.768G>T, c.3050+5G>A, and c.5714+5A>G) and 3 deepintronicvariants(c.302+68C>T, c.4539+2028C>T and c.4539+2001G>A) that likely have a negative effect on exon splicing. 36 The sibling pair Patient 11 and Patient 12 harbored a deep intronic variant, c.4539+2028C>T, and a deletion/insertion, c.6148–698_c.6670del/insTGTGCACCTCCCTAG, described in a previous report. 37 Patient 5 harbors another deep intronic variant, c.4539+2001G>A.…”
Section: Resultsmentioning
confidence: 79%
“…Other variants included a stop-gain, c.6088C>T (p.Arg2030*) variant in Patient 3 and 8 noncoding variants: 5 variants in canonical splice site sequences (c.4773+3A>G, c.2160+1G>C, c.768G>T, c.3050+5G>A, and c.5714+5A>G) and 3 deepintronicvariants(c.302+68C>T, c.4539+2028C>T and c.4539+2001G>A) that likely have a negative effect on exon splicing. 36 The sibling pair Patient 11 and Patient 12 harbored a deep intronic variant, c.4539+2028C>T, and a deletion/insertion, c.6148–698_c.6670del/insTGTGCACCTCCCTAG, described in a previous report. 37 Patient 5 harbors another deep intronic variant, c.4539+2001G>A.…”
Section: Resultsmentioning
confidence: 79%
“…Indeed, we cannot exclude the possibility that this variant may affect splicing in vivo since it has already been proven that ABCA4 can have non-canonical splice sites variant with important effects on protein [19,20,21,22,23,59]. …”
Section: Discussionmentioning
confidence: 99%
“…The effect of seven NCSS and three deep‐intronic variants was assessed by midigene‐based splicing assays employing wild‐type (WT) BA constructs described elsewhere (Sangermano et al, ) and a newly designed BA31 construct (Table S3). Details of mutagenesis primers and sequencing primers are given in Table S4.…”
Section: Methodsmentioning
confidence: 99%