SCAPER localizes to primary cilia and its mutation affects cilia length, causing Bardet-Biedl syndrome

Wormser, Ohad; Gradstein, Libe; Yogev, Yuval; Perez, Yonatan; Kadir, Rotem; Goliand, Inna; Sadka, Yair; Riati, Saad El; Flusser, Hagit; Nachmias, Dikla; Birk, Ruth; Iraqi, Muhamad; Kadar, Einat; Gat, Roni; Drabkin, Max; Halpérin, Daniel; Horev, Amir; Sivan, Sara; Elia, Natalie

doi:10.1038/s41431-019-0347-z

Cited by 38 publications

(45 citation statements)

References 46 publications

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“…BBS is an autosomal recessive disorder caused by loss‐of‐function (LOF) mutations in at least 24 genes ( BBS1‐21 , Forsythe, Kenny, Bacchelli, & Beales, ; NPHP1 , Lindstrand et al, ; IFT74 , Lindstrand et al, ; and SCAPER , Wormser et al, ), whose function is closely related to the primary cilium. Most of the BBS patients have mutations in one of the eight genes encoding for the subunits of the octameric protein complex, BBSome ( BBS1 , 2 , 4 , 5 , 7 , 8 , 9 , 18 ; Nachury et al, ).…”

Section: Introductionmentioning

confidence: 99%

Meta‐analysis of genotype‐phenotype associations in Bardet‐Biedl syndrome uncovers differences among causative genes

et al. 2019

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Bardet‐Biedl syndrome (BBS) is a recessive genetic disease causing multiple organ anomalies. Most patients carry mutations in genes encoding for the subunits of the BBSome, an octameric ciliary transport complex, or accessory proteins involved in the BBSome assembly or function. BBS proteins have been extensively studied using in vitro, cellular, and animal models. However, the molecular functions of particular BBS proteins and the etiology of the BBS symptoms are still largely elusive. In this study, we applied a meta‐analysis approach to study the genotype‐phenotype association in humans using our database of all reported BBS patients. The analysis revealed that the identity of the causative gene and the character of the mutation partially predict the clinical outcome of the disease. Besides their potential use for clinical prognosis, our analysis revealed functional differences of particular BBS genes in humans. Core BBSome subunits BBS2, BBS7, and BBS9 manifest as more critical for the function and development of kidneys than peripheral subunits BBS1, BBS4, and BBS8/TTC8, suggesting that incomplete BBSome retains residual function at least in the kidney.

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Section: Introductionmentioning

confidence: 99%

Meta‐analysis of genotype‐phenotype associations in Bardet‐Biedl syndrome uncovers differences among causative genes

et al. 2019

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“…16 Notably, several other BBS genes were later implicated in other ciliopathies and vice versa; for example, CEP290/NPHP6 mutations are associated with BBS and other ciliopathies, such as Meckel-Gruber, Joubert, Senior-Løcken, nephronophtisis, and Leber congenital amaurosis syndromes. 11 The advent of next-generation sequencing has led to the discovery of an increasing number of pathogenic loci; to date, up to 24 genes have been described 10,[17][18][19] (Supplementary Table S1). BBS1, BBS2, and BBS10 are the most commonly mutated genes and account for almost 50% of diagnoses.…”

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confidence: 99%

Exploring Key Challenges of Understanding the Pathogenesis of Kidney Disease in Bardet–Biedl Syndrome

Marchese

Ruoppolo

Perna

et al. 2020

Kidney International Reports

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Bardet-Biedl syndrome (BBS) is a rare pleiotropic inherited disorder known as a ciliopathy. Kidney disease is a cardinal clinical feature; however, it is one of the less investigated traits. This study is a comprehensive analysis of the literature aiming to collect available information providing mechanistic insights into the pathogenesis of kidney disease by analyzing clinical and basic science studies focused on this issue. The analysis revealed that the syndrome is either clinically and genetically heterogenous, with 24 genes discovered to date, but with 3 genes (BBS1, BBS2, and BBS10) accounting for almost 50% of diagnoses; genotype-phenotype correlation studies showed that patients with BBS1 mutations have a less severe renal phenotype than the other 2 most common loci; in addition, truncating rather than missense mutations are more likely to cause kidney disease. However, significant intrafamilial clinical variability has been described, with no clear explanation to date. In mice kidneys, Bbs genes have relative low expression levels, in contrast with other common affected organs, like the retina; surprisingly, Bbs1 is the only locus with basal overexpression in the kidney. In vitro studies indicate that signalling pathways involved in embryonic kidney development and repair are affected in the context of BBS depletion; in mice, kidney disease does not have a full penetrance; when present, it resembles human phenotype and shows an agedependent progression. Data on the exact contribution of local versus systemic consequences of Bbs dysfunction are scanty and further investigations are required to get firm conclusions.

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“…In the current study, we describe clinical and genetic findings, including seven novel SCAPER variants, in six individuals of Amish, Caucasian, and South Asian descent. Together with our molecular data, our comprehensive phenotypic assessments enable a more detailed clinical comparison to be drawn between the patient cohort described here (including previously published individual G001284; Patient 3 in this study, (Carss et al, ) with the 17 individuals in whom SCAPER variants were recently defined (Hu et al, ; Jauregui et al, ; Najmabadi et al, ; Tatour et al, ; Wormser et al, ), permitting a more precise definition of the clinical phenotype arising from pathogenic SCAPER variation.…”

Section: A Comparison Of Clinical Findings Of All Affected Individualmentioning

confidence: 95%

“…Biallelic LOF variants have since been associated with ID with or without retinitis pigmentosa (RP) in seven individuals from five families from Spain, Israel, and Iran (Hu et al, ; Tatour et al, ); in one individual from a Jordanian Arab family, a homozygous SCAPER gene variant was identified as the cause of nonsyndromic RP (Jauregui et al, ). More recently, Wormser et al () described a SCAPER gene variant associated with a Bardet–Biedl syndrome (BBS)‐like presentation comprising of ID, RP, short stature, obesity, and brachydactyly in eight individuals from two consanguineous Bedouin families belonging to the same tribe in southern Israel, alongside preliminary functional studies suggesting a possible role for SCAPER in ciliary dynamics and disassembly. In the current study, we describe clinical and genetic findings, including seven novel SCAPER variants, in six individuals of Amish, Caucasian, and South Asian descent.…”

Section: A Comparison Of Clinical Findings Of All Affected Individualmentioning

confidence: 99%

Delineating the expanding phenotype associated with SCAPER gene mutation

Fasham

Arno

Lin

et al. 2019

American J of Med Genetics Pt A

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SCAPER localizes to primary cilia and its mutation affects cilia length, causing Bardet-Biedl syndrome

Cited by 38 publications

References 46 publications

Meta‐analysis of genotype‐phenotype associations in Bardet‐Biedl syndrome uncovers differences among causative genes

Meta‐analysis of genotype‐phenotype associations in Bardet‐Biedl syndrome uncovers differences among causative genes

Exploring Key Challenges of Understanding the Pathogenesis of Kidney Disease in Bardet–Biedl Syndrome

Delineating the expanding phenotype associated with SCAPER gene mutation

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