2017
DOI: 10.1002/mgg3.296
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Refining genotype–phenotype correlation in Alström syndrome through study of primary human fibroblasts

Abstract: BackgroundAlström syndrome (AS), featuring retinal dystrophy, neuronal deafness, cardiomyopathy, metabolic syndrome, and diffuse fibrosis, is caused by biallelic mutations in the centrosomal protein ALMS1. Genotype–phenotype correlation has been suggested without assessment of ALMS1 expression.Methods ALMS1 expression (real‐time PCR and immunocytochemistry) and cilia formation (immunocytochemistry) were assessed in fibroblasts from deeply phenotyped volunteers diagnosed with AS recruited from a dedicated AS Se… Show more

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Cited by 24 publications
(34 citation statements)
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“…The formation of primary cilia seems to be unaffected in AS patient fibroblasts in vitro [19, 76, 142]. Hh and PDGFA signalling, both of which act through the cilium, also appear to be normal [142].…”
Section: Alms1 Functionmentioning
confidence: 99%
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“…The formation of primary cilia seems to be unaffected in AS patient fibroblasts in vitro [19, 76, 142]. Hh and PDGFA signalling, both of which act through the cilium, also appear to be normal [142].…”
Section: Alms1 Functionmentioning
confidence: 99%
“…Hh and PDGFA signalling, both of which act through the cilium, also appear to be normal [142]. In stark contrast, transient RNAi-mediated depletion of ALMS1 has been reported to cause severe defects in ciliary structure.…”
Section: Alms1 Functionmentioning
confidence: 99%
See 2 more Smart Citations
“…As expected, Kif3a KD resulted in loss of primary cilia, a reduction in axoneme length, and suppressed HH signaling compared to a scramble shRNA control ( Figures 1C-F, Supplementary Figure 1A). Alms1 KD phenocopied Kif3a KD, despite normal primary ciliogenesis in Alms1 -/mice that present similar features as patients with Alström syndrome (Collin et al 2005) and in primary human fibroblasts cultured from Alström syndrome patients (Chen et al 2017). Despite not previously linked to primary cilia or HH signaling, KD of Usher Type 1 genes Cdh23 and Pcdh15 or Usher Type 2 genes Gpr98 and Ush2a also resulted in ciliary loss, reduced axoneme length, and diminished HH signaling compared to scrambled shRNA control ( Figures 1C-F, Supplementary Figure 1A).…”
Section: Disruption Of Alström and Usher Syndrome Genes Suppress Primmentioning
confidence: 84%