2021
DOI: 10.1016/j.trecan.2020.08.007
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Mice Are Not Humans: The Case of p53

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Cited by 30 publications
(23 citation statements)
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“…An increasing number of available high-throughput datasets enabled us to generate ranked lists of p63-regulated genes and p63-bound DNA sites that together reveal high-probability direct p63 target genes regulated by p63 across cells of multiple origins. Because p63 target genes, very much like p53 target genes ( Fischer, 2020 ; Fischer, 2019 ), differ substantially between mouse and human ( Sethi et al, 2017 ), many p63 target genes initially described in mouse could not be confirmed to be p63-regulated in this study using human data. Given that p63-binding sites are frequently associated with enhancer regions and enhancer identity, we have integrated enhancer:gene associations to identify target genes that are regulated by p63 through direct binding to associated enhancers.…”
Section: Discussionmentioning
confidence: 72%
See 1 more Smart Citation
“…An increasing number of available high-throughput datasets enabled us to generate ranked lists of p63-regulated genes and p63-bound DNA sites that together reveal high-probability direct p63 target genes regulated by p63 across cells of multiple origins. Because p63 target genes, very much like p53 target genes ( Fischer, 2020 ; Fischer, 2019 ), differ substantially between mouse and human ( Sethi et al, 2017 ), many p63 target genes initially described in mouse could not be confirmed to be p63-regulated in this study using human data. Given that p63-binding sites are frequently associated with enhancer regions and enhancer identity, we have integrated enhancer:gene associations to identify target genes that are regulated by p63 through direct binding to associated enhancers.…”
Section: Discussionmentioning
confidence: 72%
“…Also, the frequent binding of p63 to enhancers ( Kouwenhoven et al, 2015a ; Lin-Shiao et al, 2019 ; Lin-Shiao et al, 2018 ; Qu et al, 2018 ; Somerville et al, 2018 ) and the difficulty to associate such enhancers with target gene regulation adds another level of complexity to the quest of describing the GRN. To overcome these limitations, we utilize a recently developed meta-analysis approach ( Fischer et al, 2016a ), which helped us to dissect the GRNs of the mouse and human orthologue of p53 ( Fischer, 2020 ; Fischer, 2019 ). The analysis rests upon a ranking of potential p63 target genes based on the number of datasets supporting a p63-dependent regulation.…”
Section: Introductionmentioning
confidence: 99%
“…For example, p53 regulates the largest subset of genes indirectly through its direct target gene CDKN1A , encoding cyclin-dependent kinase inhibitor p21 and reactivating DREAM and RB:E2F trans -repressor complexes to down-regulate cell cycle genes ( 23–27 ). Intriguingly, indirect down-regulation of cell cycle genes by p53 is well conserved, while direct p53 targets diverged substantially during evolution ( 28 , 29 ). Yet, complex cross-talks between signaling pathways impede the identification of indirect regulations.…”
Section: Introductionmentioning
confidence: 99%
“…Nonetheless, the canonical tumour suppressive functions of p53 are still heavily intertwined with its long-established role in activating apoptotic cell death. Whilst this involves transcriptional upregulation of direct activators of apoptosis-such as PUMA, An emerging concept is that high affinity p53REs are well conserved across species and are present at cell cycle arrest genes (e.g., CDKN1A/p21) whilst lower affinity, evolutionary divergent p53REs are found at pro-apoptotic genes (e.g., BAX/BAX) [30,31]. However, the underlying molecular mechanisms which dictate p53 binding at distinct p53REs remain poorly defined.…”
Section: P53-a Tumour Suppressive Transcription Factormentioning
confidence: 99%