Bardet–Biedl syndrome type 4 (BBS4)-null mice implicate Bbs4 in flagella formation but not global cilia assembly

Mykytyn, Kirk; Mullins, Robert F.; Andrews, Michael; Chiang, An‐Jen; Swiderski, Ruth E.; Yang, Baoli; Braun, Terry A.; Casavant, Thomas L.; Stone, Edwin M.; Sheffield, Val C.

doi:10.1073/pnas.0402354101

Cited by 308 publications

(333 citation statements)

References 17 publications

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“…Second, there are three relevant knockout mouse models for genes within the linked interval: Pappa (31), Astn1 (paralogue of Astn2) (32), and Tlr4 (33). These models do not have phenotypes that resemble BBS mouse models (34)(35)(36). Finally, functional characterization of other TRIM proteins indicates involvement with components of the cytoskeleton, a finding consistent with the function of other BBS proteins (37)(38)(39).…”

Section: Discussionsupporting

confidence: 56%

Homozygosity mapping with SNP arrays identifiesTRIM32, an E3 ubiquitin ligase, as a Bardet–Biedl syndrome gene (BBS11)

Chiang

Beck

Yen

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

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387

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The identification of mutations in genes that cause human diseases has largely been accomplished through the use of positional cloning, which relies on linkage mapping. In studies of rare diseases, the resolution of linkage mapping is limited by the number of available meioses and informative marker density. One recent advance is the development of high-density SNP microarrays for genotyping. The SNP arrays overcome low marker informativity by using a large number of markers to achieve greater coverage at finer resolution. We used SNP microarray genotyping for homozygosity mapping in a small consanguineous Israeli Bedouin family with autosomal recessive Bardet-Biedl syndrome (BBS; obesity, pigmentary retinopathy, polydactyly, hypogonadism, renal and cardiac abnormalities, and cognitive impairment) in which previous linkage studies using short tandem repeat polymorphisms failed to identify a disease locus. SNP genotyping revealed a homozygous candidate region. Mutation analysis in the region of homozygosity identified a conserved homozygous missense mutation in the TRIM32 gene, a gene coding for an E3 ubiquitin ligase. Functional analysis of this gene in zebrafish and expression correlation analyses among other BBS genes in an expression quantitative trait loci data set demonstrate that TRIM32 is a BBS gene. This study shows the value of high-density SNP genotyping for homozygosity mapping and the use of expression correlation data for evaluation of candidate genes and identifies the proteasome degradation pathway as a pathway involved in BBS.genetic mapping ͉ obesity ͉ SNP genotyping ͉ zebrafish model

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Section: Discussionsupporting

confidence: 56%

Homozygosity mapping with SNP arrays identifiesTRIM32, an E3 ubiquitin ligase, as a Bardet–Biedl syndrome gene (BBS11)

Chiang

Beck

Yen

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

387

295

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“…Since obesity and several of the other phenotypes that accompany BBS are common, studying this disorder potentially will yield new insights into the cellular and molecular mechanisms that underlie these important phenotypes. That several of the disease phenotypes (retinal dystrophy, situs inversus, and anosmia) already were linked to cilia suggested a connection between BBS and cilia, and several recent studies have confirmed this idea [94][95][96][97] (reviewed in Mykytyn and Sheffield 98 ). The BBS1 and BBS4 gene products are essential for formation of normal cilia in mouse olfactory epithelium.…”

Section: Cilia and The Obesity Disorder Bardet-biedl Syndromementioning

confidence: 65%

“…97 Interestingly, BBS4 knockout mice also undergo apoptotic retinal degeneration and males are sterile because their sperm fail to form a flagellum. 95,96 On the other hand, the BBS4 mice (which exhibit anosmia) show normal motile cilia in the airway and respiratory epithelial, as well as cilia of normal appearance in the renal epithelium. Thus, BBS4 protein is not globally required for cilia formation.…”

Section: Cilia and The Obesity Disorder Bardet-biedl Syndromementioning

confidence: 99%

Cilium-generated signaling and cilia-related disorders

Pan

Wang

Snell

2005

Laboratory Investigation

210

183

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Biologists have long known that humans experience their environment through cilia. Light, odorant, and sound perception depend on these microtubule-filled, complex organelles present on cells in primary sensory tissues. Recently, discoveries on the mechanism of assembly of cilia (flagella) in the lowly, biflagellated, eucaryotic green alga Chlamydomonas have triggered a renaissance of interest in the organelles along with a recognition of their key sensory roles in nonsensory tissues. Chlamydomonas researchers uncovered an entirely new set of cellular machinery essential for transporting the protein components of cilia and flagella in all ciliated/ flagellated eukaryotic cells between their site of synthesis in the cell body and their site of assembly at the tip of the flagellum (intraflagellar transport: IFT). Prompted by the surprising observations that disruption of IFT genes in mice led to polycystic kidney disease (PKD) and that PKD proteins are present on the sensory cilia of Caenorhabditis elegans, researchers have made a direct connection between PKD and cilia. At least five (and possibly all) of the seven identified human genes disrupted in PKD and a related disorder nephronophthisis encode proteins expressed in the primary cilia that project into the lumen from the epithelial cells that line renal tubules. Moreover, the renal cilia are flow sensors and at least two of the PKD genes encode ciliary transmembrane proteins essential for mechanosensation. Although their roles have not yet been as clearly identified, cilia also are at the center of a rare human disorder, Bardet-Biedl syndrome (BBS), in which patients exhibit phenotypes of common human diseases, including obesity and increased incidence of hypertension and diabetes. Five of the eight known BBS genes encode basal body or cilia proteins in mice or humans, and homologues of two of the remaining genes are present in basal bodies/cilia of model organisms. Here we briefly describe the biology of cilia and flagella, we outline how studies on model organisms have led to our current understanding of the roles of these organelles and their proteins in health and disease, and we highlight the notion that the primary cilia present on cells throughout the body, even those on brain neurons, may be essential for as yet undiscovered cilium-generated signaling functions.

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“…At birth, Bardet-Biedl-Syndrome 4 (Bbs4) mutant mice are runted compared with their wild-type littermates and manifest obesity later on 15 . Penetrance is dependent on sex and age of the animals both in this and another Bbs4 À / À mutant strain 16 . Generally, female mutants are more severely affected than age-matched male mutants.…”

Section: Resultsmentioning

confidence: 99%

Ciliary dysfunction impairs beta-cell insulin secretion and promotes development of type 2 diabetes in rodents

Christou-Savina²,

et al. 2014

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Type 2 diabetes mellitus is affecting more than 382 million people worldwide. Although much progress has been made, a comprehensive understanding of the underlying disease mechanism is still lacking. Here we report a role for the b-cell primary cilium in type 2 diabetes susceptibility. We find impaired glucose handling in young Bbs4 À / À mice before the onset of obesity. Basal body/ciliary perturbation in murine pancreatic islets leads to impaired first phase insulin release ex and in vivo. Insulin receptor is recruited to the cilium of stimulated b-cells and ciliary/basal body integrity is required for activation of downstream targets of insulin signalling. We also observe a reduction in the number of ciliated b-cells along with misregulated ciliary/basal body gene expression in pancreatic islets in a diabetic rat model. We suggest that ciliary function is implicated in insulin secretion and insulin signalling in the b-cell and that ciliary dysfunction could contribute to type 2 diabetes susceptibility.

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Bardet–Biedl syndrome type 4 (BBS4)-null mice implicate Bbs4 in flagella formation but not global cilia assembly

Cited by 308 publications

References 17 publications

Homozygosity mapping with SNP arrays identifiesTRIM32, an E3 ubiquitin ligase, as a Bardet–Biedl syndrome gene (BBS11)

Homozygosity mapping with SNP arrays identifiesTRIM32, an E3 ubiquitin ligase, as a Bardet–Biedl syndrome gene (BBS11)

Cilium-generated signaling and cilia-related disorders

Ciliary dysfunction impairs beta-cell insulin secretion and promotes development of type 2 diabetes in rodents

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