Literature DB >> 21820037

A new human dyskerin isoform with cytoplasmic localization.

Alberto Angrisani1, Mimmo Turano, Lorella Paparo, Concetta Di Mauro, Maria Furia.   

Abstract

BACKGROUND: The human DKC1 gene is causative of X-linked dyskeratosis congenita (X-DC), a syndrome characterized by mucocutaneous features, bone marrow failure, tumor susceptibility, perturbation of stem cell function, and premature aging. DKC1 is thought to produce a single protein, named dyskerin, which shows strict nucleolar localization and participates in at least two distinct nuclear functional complexes: the H/ACA small nucleolar ribonucleoproteic complex involved in RNA pseudouridylation and the active telomerase complex.
METHODS: By bioinformatics and molecular analyses we identified a DKC1 splice variant able to encode a truncated form of dyskerin, confirmed its active expression in diverse human tissues by RT-PCR, and showed by immunoblotting and immunocytochemistry experiments that it actually encodes a novel protein. Stably transfected clones over-expressing the new isoform were analyzed for growth, morphology and adhesion properties.
RESULTS: Our results show that DKC1 encodes a new alternatively spliced mRNA able to direct the synthesis of a variant dyskerin with unexpected cytoplasmic localization. Intriguingly, when over-expressed in HeLa cells, the new isoform promotes cell to cell and cell to substratum adhesion, increases the cell proliferation rate and leads to cytokeratin hyper-expression. CONCLUSIONS AND GENERAL SIGNIFICANCE: Our results highlight a novel degree of complexity and regulation of the human DKC1 gene and reveal that it can play a further, unpredicted role in cell adhesion. The identification of a dyskerin cytoplasmic variant reinforces the view that other mechanisms, in addition to telomere instability, can significantly contribute to the pathogenesis of the X-DC, and suggests that DKC1 nucleolar and cytoplasmic functions might cumulatively account for the plethora of manifestations displayed by this syndrome. 2011 Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 21820037     DOI: 10.1016/j.bbagen.2011.07.012

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  11 in total

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4.  Dyskerin depletion increases VEGF mRNA internal ribosome entry site-mediated translation.

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Review 7.  Replication Stress at Telomeric and Mitochondrial DNA: Common Origins and Consequences on Ageing.

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9.  A new role for human dyskerin in vesicular trafficking.

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10.  Characterisation of mesenchymal colon tumour-derived cells in tumourspheres as a model for colorectal cancer progression.

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