Mks6 mutations reveal tissue‐ and cell type‐specific roles for the cilia transition zone

Lewis, Wesley R.; Bales, Katie; Revell, Dustin Z.; Croyle, Mandy J.; Engle, Staci E.; Song, Chun-Yan; Malarkey, Erik B.; Uytingco, Cedric; Shan, Dan; Antonellis, Patrick J.; Nagy, Tim R.; Kesterson, Robert A.; Mrug, Michal; Martens, Jeffrey R.; Berbari, Nicolas F.; Gross, Alecia K.; Yoder, Bradley K.

doi:10.1096/fj.201801149r

Cited by 21 publications

(23 citation statements)

References 48 publications

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“…Mice with null mutations in Cc2d2a experience embryonic lethality due to the absence of subdistal appendages and nodal cilia [88]. The retinas of adult mice with tamoxifen-induced deletion of Cc2d2a in PRs have a significantly diminished ONL (2-3 layers) 12 weeks post-injection [92], suggesting that CC2D2A is necessary for ciliary homeostasis.…”

Section: Category 01: Ciliary Function and Traffickingmentioning

confidence: 99%

Mouse Models of Inherited Retinal Degeneration with Photoreceptor Cell Loss

Collin

Gogna

Chang

et al. 2020

Cells

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Inherited retinal degeneration (RD) leads to the impairment or loss of vision in millions of individuals worldwide, most frequently due to the loss of photoreceptor (PR) cells. Animal models, particularly the laboratory mouse, have been used to understand the pathogenic mechanisms that underlie PR cell loss and to explore therapies that may prevent, delay, or reverse RD. Here, we reviewed entries in the Mouse Genome Informatics and PubMed databases to compile a comprehensive list of monogenic mouse models in which PR cell loss is demonstrated. The progression of PR cell loss with postnatal age was documented in mutant alleles of genes grouped by biological function. As anticipated, a wide range in the onset and rate of cell loss was observed among the reported models. The analysis underscored relationships between RD genes and ciliary function, transcription-coupled DNA damage repair, and cellular chloride homeostasis. Comparing the mouse gene list to human RD genes identified in the RetNet database revealed that mouse models are available for 40% of the known human diseases, suggesting opportunities for future research. This work may provide insight into the molecular players and pathways through which PR degenerative disease occurs and may be useful for planning translational studies.

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Section: Category 01: Ciliary Function and Traffickingmentioning

confidence: 99%

Mouse Models of Inherited Retinal Degeneration with Photoreceptor Cell Loss

Collin

Gogna

Chang

et al. 2020

Cells

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“…However, loss of Nphp1, Nphp4 and Invs did not alter the ciliary amount of Arl13b or Sstr3 in MEFs and NIH3T3 cells ( Figure 1B and Figure 2) indicating that they are not involved in gating these proteins in vertebrate primary cilia. Remarkably, several reports point to cell type-specific functions of some TZ proteins [14,16,27,41,42] making a potential regulation of ciliary gating by Nphp1, Nphp4 and Invs in other vertebrate cell types conceivable. Rpgrip1l -/and Cep290 -/mice have a much more severe phenotype than Nphp1 -/-, Nphp4 -/and Invs -/mice [20,25,27,[42][43][44][45][46][47][48][49][50][51][52][53][54][55][56][57][58][59].…”

Section: Discussionmentioning

confidence: 99%

“…For this reason, the assembly and function of the TZ is a hot topic in biomedical research. A lot of proteins participate in TZ assembly and/or function as ciliary gatekeepers at the TZ [12- 14,16,17,19,23,24,27,29,30,33,34,37,41,69,70,[73][74][75][76][77][78][79][80][81][82][83][84][85][86][87][88][89][90]. However, the relationships between these proteins and hence the mechanisms underlying ciliary gating at the TZ remain largely elusive.…”

Section: Interestingly Garcia-gonzalo Et Al Revealed That the Loss mentioning

confidence: 99%

“…Proteins were detected with secondary antibodies conjugated to horseradish peroxidase (RPN4201 and RPN4301) and the ECL detection kit (both GE Healthcare). Visualization of 16 protein bands was realized by LAS-4000 mini (Fujifilm). Band intensities were measured by using ImageJ (National Institutes of Health).…”

Section: Western Blottingmentioning

confidence: 99%

“…In many cases, ciliopathies are caused by mutations in genes encoding TZ proteins [3,4]. As the TZ functions as the ciliary gatekeeper governing ciliary protein import and export [4][5][6][7][8][9][10][11][12], a defective TZ can affect the proper formation of cilia and alter signalling pathways transduction [13][14][15][16][17][18][19][20][21][22][23][24]. Thus, the investigation of the molecular mechanisms underlying TZ function is an important prerequisite for the development of curative ciliopathy therapies.…”

Section: Introductionmentioning

confidence: 99%

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Rpgrip1l controls ciliary gating by ensuring the proper amount of Cep290 at the vertebrate transition zone

Wiegering

Dildrop

Vesque

et al. 2020

Preprint

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A range of severe human diseases called ciliopathies are caused by the dysfunction of primary cilia. Primary cilia are cytoplasmic protrusions consisting of the basal body (BB), the axoneme and the transition zone (TZ). The BB is a modified mother centriole from which the axoneme, the microtubule-based ciliary scaffold, is formed. At the proximal end of the axoneme, the TZ functions as the ciliary gate governing ciliary protein entry and exit. Since ciliopathies often develop due to mutations in genes encoding proteins that localise to the TZ, the understanding of the mechanisms underlying TZ function is of eminent importance. Here, we show that the ciliopathy protein Rpgrip1l governs ciliary gating by ensuring the proper amount of Cep290 at the vertebrate TZ. Further, we identified the flavonoid eupatilin as a potential agent to tackle ciliopathies caused by mutations in RPGRIP1L as it rescues ciliary gating in the absence of Rpgrip1l.

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