PUBLICATION

Copy-Number Variation Contributes to the Mutational Load of Bardet-Biedl Syndrome

Authors
Lindstrand, A., Frangakis, S., Carvalho, C.M., Richardson, E.B., McFadden, K.A., Willer, J.R., Pehlivan, D., Liu, P., Pediaditakis, I.L., Sabo, A., Lewis, R.A., Banin, E., Lupski, J.R., Davis, E.E., Katsanis, N.
ID
ZDB-PUB-160804-5
Date
2016
Source
American journal of human genetics   99: 318-336 (Journal)
Registered Authors
Davis, Erica, Katsanis, Nicholas, Willer, Jason
Keywords
ciliopathy, mechanism of rearrangements, oligogenic disease, zebrafish model
MeSH Terms
  • Adolescent
  • Adult
  • Alleles
  • Animals
  • Bardet-Biedl Syndrome/genetics*
  • Child
  • Child, Preschool
  • Chromosome Breakpoints
  • Cytoskeletal Proteins/genetics
  • Cytoskeletal Proteins/metabolism
  • DNA Copy Number Variations/genetics*
  • Exons/genetics
  • Female
  • Gastrulation/genetics
  • Genes, Recessive
  • Humans
  • Infant
  • Male
  • Mutation*
  • Pedigree
  • Young Adult
  • Zebrafish/embryology
  • Zebrafish/genetics
  • Zebrafish Proteins/genetics
  • Zebrafish Proteins/metabolism
(all 25)
PubMed
27486776 Full text @ Am. J. Hum. Genet.
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 burden. We identified 17 individuals with exon-disruptive CNVs (18.5%), including 13 different deletions in eight BBS genes (BBS1, BBS2, ARL6/BBS3, BBS4, BBS5, BBS7, BBS9, and NPHP1) and a deletion and a duplication in other ciliopathy-associated genes (ALMS1 and NPHP4, respectively). By contrast, we found a single heterozygous exon-disruptive event in a BBS-associated gene (BBS9) in 229 control subjects. Superimposing these data with resequencing revealed CNVs to (1) be sufficient to cause disease, (2) Mendelize heterozygous deleterious alleles, and (3) contribute oligogenic alleles by combining point mutations and exonic CNVs in multiple genes. Finally, we report a deletion and a splice site mutation in IFT74, inherited under a recessive paradigm, defining a candidate BBS locus. Our data suggest that CNVs contribute pathogenic alleles to a substantial fraction of BBS-affected individuals and highlight how either deletions or point mutations in discrete splice isoforms can induce hypomorphic mutations in genes otherwise intolerant to deleterious variation. Our data also suggest that CNV analyses and resequencing studies unbiased for previous mutational burden is necessary to delineate the complexity of disease architecture.
Genes / Markers
Marker Marker Type Name
alms1GENEALMS1 centrosome and basal body associated protein
arl6GENEARF like GTPase 6
bbs1GENEBardet-Biedl syndrome 1
bbs10GENEBardet-Biedl syndrome 10
bbs2GENEBardet-Biedl syndrome 2
bbs4GENEBardet-Biedl syndrome 4
bbs5GENEBardet-Biedl syndrome 5
bbs7GENEBardet-Biedl syndrome 7
bbs9GENEBardet-Biedl syndrome 9
cep290GENEcentrosomal protein 290
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Figures
No images available
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Expression
Phenotype
Fish Conditions Stage Phenotype Figure
WT + CRISPR1-ift74standard conditions10-13 somites
WT + CRISPR1-ift74standard conditions10-13 somites
WT + CRISPR1-ift74standard conditions10-13 somites
WT + CRISPR1-ift74standard conditions10-13 somites
WT + CRISPR1-ift74standard conditions10-13 somites
WT + CRISPR1-ift74standard conditions10-13 somites
WT + CRISPR1-ift74standard conditionsDay 4
WT + CRISPR1-ift74standard conditionsDay 4
WT + MO1-bbs10standard conditions10-13 somites
WT + MO1-bbs10standard conditionsDay 4
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Mutations / Transgenics
No data available
Human Disease / Model
Human Disease Fish Conditions Evidence
Bardet-Biedl syndromeTAS
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Sequence Targeting Reagents
Target Reagent Reagent Type
alms1MO2-alms1MRPHLNO
arl6MO4-arl6MRPHLNO
bbs1MO4-bbs1MRPHLNO
bbs2MO4-bbs2MRPHLNO
bbs4MO6-bbs4MRPHLNO
bbs5MO3-bbs5MRPHLNO
bbs7MO4-bbs7MRPHLNO
bbs9MO5-bbs9MRPHLNO
bbs10MO1-bbs10MRPHLNO
cep290MO8-cep290MRPHLNO
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Fish
Fish
WT + CRISPR1-ift74
WT + MO1-bbs10
WT + MO1-bbs10 + MO3-bbs5
WT + MO1-ift74
WT + MO2-alms1 + MO5-bbs9
WT + MO2-alms1 + MO5-bbs9 + MO6-bbs4
WT + MO2-alms1 + MO6-bbs4
WT + MO2-ift74
WT + MO2-ttc8
WT + MO3-bbs5
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Antibodies
Orthology
Engineered Foreign Genes
No data available
Mapping
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Citation
Lindstrand, A., Frangakis, S., Carvalho, C.M., Richardson, E.B., McFadden, K.A., Willer, J.R., Pehlivan, D., Liu, P., Pediaditakis, I.L., Sabo, A., Lewis, R.A., Banin, E., Lupski, J.R., Davis, E.E., Katsanis, N. (2016) Copy-Number Variation Contributes to the Mutational Load of Bardet-Biedl Syndrome. American journal of human genetics. 99:318-336.