Hypomorphism in human NSMCE2 linked to primordial dwarfism and insulin resistance

Payne, Felicity; Colnaghi, Rita; Rocha, Nuno; Asha, S; Harris, J. Ieuan; Carpenter, Gillian; Bottomley, William; Wheeler, Eleanor; Wong, Stephen Q.; Saudek, Vladimı́r; Savage, David B.; O’Rahilly, Stephen; Carel, Jean‐Claude; Barroso, Inês; O’Driscoll, Mark; Semple, Robert K.

doi:10.1172/jci73264

Cited by 94 publications

(114 citation statements)

References 43 publications

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“…Misregulation of condensin II has been implicated in the neurodevelopmental disorder autosomal recessive primary microcephaly (MCPH) (Hirano, 2012;Trimborn et al, 2006). Recently, hypomorphic mutations of a Smc5/6 component, NSMCE2, have been reported to cause primordial dwarfism and microcephaly in human (Payne et al, 2014). Furthermore, SMC mutations are associated with cancer (Leiserson et al, 2015;Jacome et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Conditional mutation of Smc5 in mouse embryonic stem cells perturbs condensin localization and mitotic progression

Pryzhkova

Jordan

2016

Journal of Cell Science

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Correct duplication of stem cell genetic material and its appropriate segregation into daughter cells are requisites for tissue, organ and organism homeostasis. Disruption of stem cell genomic integrity can lead to developmental abnormalities and cancer. Roles of the Smc5/6 structural maintenance of chromosomes complex in pluripotent stem cell genome maintenance have not been investigated, despite its important roles in DNA synthesis, DNA repair and chromosome segregation as evaluated in other model systems. Using mouse embryonic stem cells (mESCs) with a conditional knockout allele of Smc5, we showed that Smc5 protein depletion resulted in destabilization of the Smc5/6 complex, accumulation of cells in G2 phase of the cell cycle and apoptosis. Detailed assessment of mitotic mESCs revealed abnormal condensin distribution and perturbed chromosome segregation, accompanied by irregular spindle morphology, lagging chromosomes and DNA bridges. Mutation of Smc5 resulted in retention of Aurora B kinase and enrichment of condensin on chromosome arms. Furthermore, we observed reduced levels of Polo-like kinase 1 at kinetochores during mitosis. Our study reveals crucial requirements of the Smc5/6 complex during cell cycle progression and for stem cell genome maintenance.

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Section: Introductionmentioning

confidence: 99%

Conditional mutation of Smc5 in mouse embryonic stem cells perturbs condensin localization and mitotic progression

Pryzhkova

Jordan

2016

Journal of Cell Science

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“…The truncated mutant protein corresponding to S116Lfs*18 was not readily detectable in the patient's cells whereas the A234Efs*4 mutant protein was less stable and expressed at a lower level in patient derived LCL (Epstein Barr virus immortalized lymphoblastoid cell lines) and dermal fibroblasts. The S116Lfs*18 mutant protein was autosumoylation defective while the auto-sumoylation of the A234Efs*4 mutant protein was not significantly different from the wild-type NSMCE2 protein [24]. However, the patient derived LCLs showed mild reduction of SMC5 and SMC6 proteins in whole cell extracts and chromatin fractions indicating some instability of the Smc5/6 complex in these cells.…”

Section: Introductionmentioning

confidence: 85%

“…The NSMCE2 hypomorphic patients displayed multiple developmental defects most notably primordial dwarfism, facial dysmorphism, primary gonadal failure and insulin resistant diabetes [24]. Numerous cellular defects were also observed in patient dermal fibroblasts and LCLs.…”

Section: Introductionmentioning

confidence: 99%

“…Numerous cellular defects were also observed in patient dermal fibroblasts and LCLs. The frequencies of micronuclei (MN) that may form from acentric broken chromosome fragments, and of nucleoplasmic bridges (NPB) that represent unresolved chromosome strands connecting two nuclei of a binucleate cell prior to cytokinesis, are indicative of chromosome instability, and were enhanced in patient cells especially following treatment with HU that induces replication fork stalling and collapse [24]. In addition, patient derived LCLs treated with low concentrations of HU showed impairment in recovery of replication relative to wild-type.…”

Section: Introductionmentioning

confidence: 99%

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Emerging Roles for Human MMS21, NSMCE2, in Development and Disease

Laloraya¹

2017

Down Syndr Chr Abnorm

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The maintenance of chromosome stability during cell division is crucial for inheritance of complete genetic information by progeny cells. Errors in mechanisms safeguarding genomic stability during cell division can result in chromosome aberrations during gametogenesis and development that may manifest as disease phenotypes. Structural maintenance of chromosomes (SMC) protein complexes play important roles in chromosome organization and function and impact a wide variety of chromosomal transactions. The conserved Smc5/6 complex is essential for viability, repair of DNA double strand breaks and recovery of collapsed replication forks and is crucial for chromosome stability. This mini review is focussed on hMMS21/NSMCE2, the human homolog of MMS21/NSE2 that is a non-smc subunit of the Smc5/6 complex having SUMO E3 ligase activity, and aims to provide insights into the role of hMMS21/NSMCE2 in human development and disease associated with deficiency of NSMCE2.

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“…2 Moreover, NSMCE2 hypomorphism in humans also leads to a genomic instability syndrome that limits lifespan. 7 Hence, understanding the function of the SMC5/6 complex is still an important task, which beyond its academic interest might yield unanticipated insights with potential applications to human health.…”

mentioning

confidence: 99%

The (elusive) role of the SMC5/6 complex

Fernández-Capetillo

2016

Cell Cycle

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Hypomorphism in human NSMCE2 linked to primordial dwarfism and insulin resistance

Cited by 94 publications

References 43 publications

Conditional mutation of Smc5 in mouse embryonic stem cells perturbs condensin localization and mitotic progression

Conditional mutation of Smc5 in mouse embryonic stem cells perturbs condensin localization and mitotic progression

Emerging Roles for Human MMS21, NSMCE2, in Development and Disease

The (elusive) role of the SMC5/6 complex

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