2016
DOI: 10.1016/j.ajhg.2015.04.023
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Copy-Number Variation Contributes to the Mutational Load of Bardet-Biedl Syndrome

Abstract: Bardet-Biedl syndrome (BBS) is a defining ciliopathy, notable for extensive allelic and genetic heterogeneity, almost all of which has been identified through sequencing. Recent data have suggested that copy-number variants (CNVs) also contribute to BBS. We used a custom oligonucleotide array comparative genomic hybridization (aCGH) covering 20 genes that encode intraflagellar transport (IFT) components and 74 ciliopathy loci to screen 92 unrelated individuals with BBS, irrespective of their known mutational b… Show more

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Cited by 114 publications
(115 citation statements)
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“…Recently, two cases affected with nonBBS ciliopathy phenotypes were associated with retrotransposon insertions; a L1 in exon 7 of CC2D2A and an Alu in exon 16 of ALMS1 (Takenouchi et al, ; Taschner et al, ). A recent study of BBS cases also found that 40% (6 out of 15) of the CNV deletions detected in their cohort (in BBS1 , BBS4 , BBS5 , and IFT74 ) were mediated by Alu – Alu recombination (Lindstrand et al, ).…”
Section: Discussionmentioning
confidence: 91%
“…Recently, two cases affected with nonBBS ciliopathy phenotypes were associated with retrotransposon insertions; a L1 in exon 7 of CC2D2A and an Alu in exon 16 of ALMS1 (Takenouchi et al, ; Taschner et al, ). A recent study of BBS cases also found that 40% (6 out of 15) of the CNV deletions detected in their cohort (in BBS1 , BBS4 , BBS5 , and IFT74 ) were mediated by Alu – Alu recombination (Lindstrand et al, ).…”
Section: Discussionmentioning
confidence: 91%
“…The literature search was performed according to the protocol preregistered in Prospero (CRD42018096099) and it followed the PRISMA guidelines whenever applicable (Table S1 and Figure S1). In total, we identified 85 relevant studies (Abu Safieh et al, ; Agha et al, ; Ajmal et al, ; Al‐Hamed et al, ; Alazami et al, ; Aldahmesh et al, ; Azari et al, ; Badano, ; Baker et al, ; Bee, Chawla, & Zhao, ; Bennouna‐Greene et al, ; Billingsley et al, ; Billingsley, Vincent, Deveault, & Heon, ; Branfield Day et al, ; Braun et al, ; Bujakowska et al, ; Castro‐Sanchez et al, ; Chaki et al, ; Chul Yoon et al, ; Cox et al, ; Davies, ; Deveault et al, ; Ece Solmaz et al, ; Esposito et al, ; Estrada‐Cuzcano, Koenekoop, et al, ; Estrada‐Cuzcano, Neveling, et al, ; Fan et al, ; Fattahi et al, ; Fedick et al, ; Frank et al, ; Gerth, Zawadzki, Werner, & Heon, ; Ghadami et al, ; González‐del Pozo et al, ; Harville et al, ; Heon et al, ; Hjortshoj, Gronskov, Brondum‐Nielsen, & Rosenberg, ; Hjortshoj et al, ; Hulleman et al, ; Iannaccone et al, ; Innes et al, ; Iurian, Arts, Brunner, & Fintina, ; Janssen et al, ; Kamme, Mayer, Strom, Andréasson, & Weisschuh, ; Katsanis et al, ; Katsanis et al, ; Kerr, Bhan, & Héon, ; A. O. Khan, Decker, Bachmann, Bolz, & Bergmann, ; S. Khan et al, , S. A. Khan et al, ; Laurier et al, ; Leitch et al, ; Lim et al, ; Lindstrand et al, ; Lindstrand et al, ; M'Hamdi et al, ; Maria et al,…”
Section: Resultsmentioning
confidence: 99%
“…Structural variants also represent an underestimated mutational burden that contributes to missing heritability and oligogenic mechanisms, not only in non-syndromic RD, but also in BBS and Joubert syndrome 20,2426,51,52 . Here, we report novel heterozygous multi-exon structural variants for BBS1 and RPGRIP1 that were identified by targeted comparative read-depth analysis.…”
Section: Discussionmentioning
confidence: 99%