2019
DOI: 10.1101/509869
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A pseudo-meiotic centrosomal function of TEX12 in cancer

Abstract: Cell division by meiosis involves an extraordinary chromosome choreography including pairing, synapsis and crossing over between homologous chromosomes. The many meiosis-specific genes involved in these processes also constitute a latent toolbox of chromosome remodelling and recombination factors that may be exploited through aberrant expression in cancer. Here, we report that TEX12, a structural protein involved in meiotic chromosome synapsis, is aberrantly expressed in human cancers, with high TEX12 levels c… Show more

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Cited by 4 publications
(7 citation statements)
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“…It successfully predicted several important aspects of SYCE2-TEX12 structure, such as the parallel arrangement of elongated SYCE2 chains and a dominant interaction between SYCE2 N-termini and TEX12 C-termini within the 4:4 complex (Davies et al, 2012). However, a notable difference is that our previous model was built on the assumption of constituent TEX12 dimers, owing to their behaviour as such in solution, which we now know represents an entirely distinct structural and functional form of TEX12 (Sandhu et al, 2019). This led to the incorrect placement of TEX12 dimers flanking an SYCE2 core rather than intertwined within the hetero-octamer, and the prediction that the over-estimated 40-nm length of a heteroctamer could account for the width of the SYCE2-TEX12 fibres.…”
Section: Discussionmentioning
confidence: 99%
“…It successfully predicted several important aspects of SYCE2-TEX12 structure, such as the parallel arrangement of elongated SYCE2 chains and a dominant interaction between SYCE2 N-termini and TEX12 C-termini within the 4:4 complex (Davies et al, 2012). However, a notable difference is that our previous model was built on the assumption of constituent TEX12 dimers, owing to their behaviour as such in solution, which we now know represents an entirely distinct structural and functional form of TEX12 (Sandhu et al, 2019). This led to the incorrect placement of TEX12 dimers flanking an SYCE2 core rather than intertwined within the hetero-octamer, and the prediction that the over-estimated 40-nm length of a heteroctamer could account for the width of the SYCE2-TEX12 fibres.…”
Section: Discussionmentioning
confidence: 99%
“…To address this issue, the term Germ Cell Cancer Genes (GCCG) has been proposed to describe the variety of meiotic genes re-expressed in cancer cells [121]. Currently over a thousand GCCGs have been reported widely re-expressed across cancer types, highlighting the importance of this process (see below) [105,[121][122][123][124].…”
Section: Emerging Links Between Meiotic Initiation and Oncogenesismentioning
confidence: 99%
“…The presence of meiotic proteins in cells other than germ also brings into to question the validity of the Weismann barrier hypothesis [ 121 , 122 , 125 ], which now needs to be evaluated experimentally through a combination of cell signalling, epigenetic and transcriptional analyses. Indeed, it is now timely to consider whether genes required for meiosis specific processes might also possess non-meiotic functions; such ‘moonlighting’ functions have been characterised for a number of human mitotic proteins including the HSP family members, clathrin and dynein [ 126 ].…”
Section: Emerging Links Between Meiotic Initiation and Oncogenesismentioning
confidence: 99%
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