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Once and only once: mechanisms of centriole duplication and their deregulation in disease
by
Nigg, Erich A
, Holland, Andrew J
in
Biosynthesis
/ Cancer
/ Cell cycle
/ Cell division
/ Cell proliferation
/ Centrioles
/ Cilia
/ Deregulation
/ Flagella
/ Genome editing
/ Genomes
/ Molecular chains
/ Molecular modelling
/ Neurodevelopmental disorders
/ Organelles
/ Proteomics
/ Signal transduction
2018
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Once and only once: mechanisms of centriole duplication and their deregulation in disease
by
Nigg, Erich A
, Holland, Andrew J
in
Biosynthesis
/ Cancer
/ Cell cycle
/ Cell division
/ Cell proliferation
/ Centrioles
/ Cilia
/ Deregulation
/ Flagella
/ Genome editing
/ Genomes
/ Molecular chains
/ Molecular modelling
/ Neurodevelopmental disorders
/ Organelles
/ Proteomics
/ Signal transduction
2018
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Once and only once: mechanisms of centriole duplication and their deregulation in disease
by
Nigg, Erich A
, Holland, Andrew J
in
Biosynthesis
/ Cancer
/ Cell cycle
/ Cell division
/ Cell proliferation
/ Centrioles
/ Cilia
/ Deregulation
/ Flagella
/ Genome editing
/ Genomes
/ Molecular chains
/ Molecular modelling
/ Neurodevelopmental disorders
/ Organelles
/ Proteomics
/ Signal transduction
2018
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Once and only once: mechanisms of centriole duplication and their deregulation in disease
Journal Article
Once and only once: mechanisms of centriole duplication and their deregulation in disease
2018
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Overview
Centrioles are conserved microtubule-based organelles that form the core of the centrosome and act as templates for the formation of cilia and flagella. Centrioles have important roles in most microtubule-related processes, including motility, cell division and cell signalling. To coordinate these diverse cellular processes, centriole number must be tightly controlled. In cycling cells, one new centriole is formed next to each pre-existing centriole in every cell cycle. Advances in imaging, proteomics, structural biology and genome editing have revealed new insights into centriole biogenesis, how centriole numbers are controlled and how alterations in these processes contribute to diseases such as cancer and neurodevelopmental disorders. Moreover, recent work has uncovered the existence of surveillance pathways that limit the proliferation of cells with numerical centriole aberrations. Owing to this progress, we now have a better understanding of the molecular mechanisms governing centriole biogenesis, opening up new possibilities for targeting these pathways in the context of human disease.
Publisher
Nature Publishing Group
Subject
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