A nonsense mutation in <i><scp>CEP55</scp></i> defines a new locus for a Meckel‐like syndrome, an autosomal recessive lethal fetal ciliopathy

Bondeson, Marie-Louise; Ericson, Katharina; Gudmundsson, Sanna; Ameur, Adam; Pontén, Fredrik; Wesström, Jan; Frykholm, Carina; Wilbe, Maria

doi:10.1111/cge.13012

Cited by 36 publications

(58 citation statements)

References 51 publications

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“…The polarized form of cytokinesis in embryonic cortical NSCs is poorly understood, but may influence the segregation of organelles and apical fate determinants to daughter cells as they make fate choices. Recent findings that mutations in Kif20b and other midbody genes cause microcephaly in humans and mice suggest that brain development is especially sensitive to defects in cytokinesis (26,(35)(36)(37)(38)(39). To elucidate these issues, we developed methods to quantitatively analyze furrowing and abscission in NSCs of the developing cerebral cortex.…”

Section: Discussionmentioning

confidence: 99%

Cytokinetic furrowing and abscission dynamics during brain development revealed by live imaging

McNeely

Little²,

Dwyer

2019

Preprint

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Building a brain of the proper size and structure requires neural stem cells (NSCs) to divide with tight temporal and spatial control to produce different daughter cell types in proper numbers and sequence. Mammalian NSCs in the embryonic cortex must maintain their polarized epithelial structure as they undergo both early proliferative divisions and later neurogenic divisions. To do this they undergo a polarized form of cytokinesis at the apical membrane that is not well understood. Here we investigate whether polarized furrowing and abscission in mouse NSCs are regulated differently at earlier and later stages, and in a cytokinesis mutant, Kif20b. We developed methods to live image furrow ingression and midbody microtubule abscission in NSCs within cortical explants. We find that polarized furrow ingression occurs at a steady rate and completes in 15 minutes, regardless of developmental age. However, ingression is slowed in a subset of Kif20b mutant NSCs. Abscission is usually observed on both midbody flanks, and takes 65-75 minutes to complete. Surprisingly, the process is accelerated in the microcephalic Kif20b mutant NSCs. Midbody remnants litter the apical membrane surface, and are more prevalent with early proliferative divisions. These results suggest that abscission is developmentally regulated in NSCs and may influence proper brain growth and structure.

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Section: Discussionmentioning

confidence: 99%

Cytokinetic furrowing and abscission dynamics during brain development revealed by live imaging

McNeely

Little²,

Dwyer

2019

Preprint

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“…Using a zebra fish model, they demonstrated that loss of function of cep55 mimicked the features of MARCH observed in human patients, therefore establishing a strong connection of the protein with a novel multiple congenital anomaly syndrome. Bondeson et al (46) showed that loss of Cep55 is associated with a ciliopathic lethal autosomal recessive syndrome called MKS, characteristics of which involve renal cystic dysplasia, occipital encephalocele, and polydactyly.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, we showed that Akt was destabilized in the homozygous mutants, which was partially rescued by providing either constitutively activated PI3K-CA or AKT1 expression. In addition, 2 recent studies have emphasized the connection between CEP55 loss and genetic diseases like multinucleated neurons, anhydramnios, renal dysplasia, cerebellar hypoplasia, and hydranencephaly (MARCH) (45) and Meckel-Gruber syndrome (MKS) (46), characterized by the presence of multiple congenital anomalies.…”

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confidence: 99%

Cep55 overexpression causes male‐specific sterility in mice by suppressing Foxo1 nuclear retention through sustained activation of PI3K/Akt signaling

Sinha

Kalimutho

Bowles³

et al. 2018

FASEB j.

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Spermatogenesis is a dynamic process involving self-renewal and differentiation of spermatogonial stem cells, meiosis, and ultimately, the differentiation of haploid spermatids into sperm. Centrosomal protein 55 kDa (CEP55) is necessary for somatic cell abscission during cytokinesis. It facilitates equal segregation of cytoplasmic contents between daughter cells by recruiting endosomal sorting complex required for transport machinery (ESCRT) at the midbody. In germ cells, CEP55, in partnership with testes expressed-14 (TEX14) protein, has also been shown to be an integral component of intercellular bridge before meiosis. Various in vitro studies have demonstrated a role for CEP55 in multiple cancers and other diseases. However, its oncogenic potential in vivo remains elusive. To investigate, we generated ubiquitously overexpressing Cep55 transgenic ( Cep55) mice aiming to characterize its oncogenic role in cancer. Unexpectedly, we found that Cep55 male mice were sterile and had severe and progressive defects in spermatogenesis related to spermatogenic arrest and lack of spermatids in the testes. In this study, we characterized this male-specific phenotype and showed that excessively high levels of Cep55 results in hyperactivation of PI3K/protein kinase B (Akt) signaling in testis. In line with this finding, we observed increased phosphorylation of forkhead box protein O1 (FoxO1), and suppression of its nuclear retention, along with the relative enrichment of promyelocytic leukemia zinc finger (PLZF) -positive cells. Independently, we observed that Cep55 amplification favored upregulation of ret ( Ret) proto-oncogene and glial-derived neurotrophic factor family receptor α-1 ( Gfra1). Consistent with these data, we observed selective down-regulation of genes associated with germ cell differentiation in Cep55-overexpressing testes at postnatal day 10, including early growth response-4 ( Egr4) and spermatogenesis and oogenesis specific basic helix-loop-helix-1 ( Sohlh1). Thus, Cep55 amplification leads to a shift toward the initial maintenance of undifferentiated spermatogonia and ultimately results in progressive germ cell loss. Collectively, our findings demonstrate that Cep55 overexpression causes change in germ cell proportions and manifests as a Sertoli cell only tubule phenotype, similar to that seen in many azoospermic men.-Sinha, D., Kalimutho, M., Bowles, J., Chan, A.-L., Merriner, D. J., Bain, A. L., Simmons, J. L., Freire, R., Lopez, J. A., Hobbs, R. M., O'Bryan, M. K., Khanna, K. K. Cep55 overexpression causes male-specific sterility in mice by suppressing Foxo1 nuclear retention through sustained activation of PI3K/Akt signaling.

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“…Abscission, the process through which the membrane connecting the two newly generated cells is severed resulting in physical separation of the siblings, concludes cytokinesis . Few studies have directly examined cytokinesis in NSCs and RGCs during corticogenesis despite mutations of cytokinesis‐regulating proteins in several neurodevelopmental disorders (e.g., microcephaly) . In polarized tissues such as the telencephalon, the orientation of division may be critical to maintain overall tissue structure and daughter cell identity .…”

Section: Cortical Development Neural Stem Cells and Cytokinesismentioning

confidence: 99%

Regulation of cytokinesis during corticogenesis: focus on the midbody

2017

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Development of the cerebral cortices depends on tight regulation of cell divisions. In this system, stem and progenitor cells undergo symmetric and asymmetric divisions to ultimately produce neurons that establish the layers of the cortex. Cell division culminates with the formation of the midbody, a transient organelle that establishes the site of abscission between nascent daughter cells. During cytokinetic abscission, the final stage of cell division, one daughter cell will inherit the midbody remnant, which can then maintain or expel the remnant, but mechanisms and circumstances influencing this decision are unclear. This review describes the midbody and its constituent proteins, as well as the known consequences of their manipulation during cortical development. The potential functional relevance of midbody mechanisms is discussed.

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A nonsense mutation in CEP55 defines a new locus for a Meckel‐like syndrome, an autosomal recessive lethal fetal ciliopathy

Cited by 36 publications

References 51 publications

Cytokinetic furrowing and abscission dynamics during brain development revealed by live imaging

Cytokinetic furrowing and abscission dynamics during brain development revealed by live imaging

Cep55 overexpression causes male‐specific sterility in mice by suppressing Foxo1 nuclear retention through sustained activation of PI3K/Akt signaling

Regulation of cytokinesis during corticogenesis: focus on the midbody

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