Transcriptional repressor REST drives lineage stage–specific chromatin compaction at
            <i>Ptch1</i>
            and increases AKT activation in a mouse model of medulloblastoma

Dobson, Tara; Tao, Rong; Swaminathan, Jyothishmathi; Maegawa, Satoru; Shaik, Shavali; Bravo-Alegría, Javiera; Sharma, Ajay; Kennis, Bridget; Yang, Yanwen; Callegari, Keri; Haltom, Amanda R.; Taylor, Pete; Kogiso, Mari; Qi, Lin; Khatua, Soumen; Goldman, Stewart; Lulla, Rishi; Fangusaro, Jason; MacDonald, Tobey J.; Li, Xiao Nan; Hawkins, Cynthia; Rajaram, Veena; Gopalakrishnan, Vidya

doi:10.1126/scisignal.aan8680

Cited by 19 publications

(44 citation statements)

References 81 publications

(140 reference statements)

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“…In addition to NB, high expression levels of REST have been detected in other cancers including glioma and medulloblastoma (Dobson et al, 2019;Taylor et al, 2012;Zhang et al, 2016). This implicates REST as a key transcription factor important in normal neurogenesis that is hijacked by cancer cells to promote proliferation/survival.…”

Section: Mementioning

confidence: 99%

“…Genome mapping of REST suggests that its intricate function in regulating gene expression depends on co-factors including SIN3A, the CoREST complex, Polycomb Repressive Complex 1 (PRC1), and PRC2 (Dietrich et al, 2012;McGann et al, 2014;Rockowitz et al, 2014). REST is overexpressed in several aggressive tumors of the nervous system, including neuroblastoma (stage 4 MYCN non-amplified) (Liang et al, 2014), medulloblastoma, and glioblastoma (Dobson et al, 2019;Taylor et al, 2012;Zhang et al, 2016).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

ATRX In-Frame Fusion Neuroblastoma Is Sensitive to EZH2 Inhibition via Modulation of Neuronal Gene Signatures

et al. 2019

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Section: Mementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

ATRX In-Frame Fusion Neuroblastoma Is Sensitive to EZH2 Inhibition via Modulation of Neuronal Gene Signatures

et al. 2019

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“…Inhibition of either REST or the enzyme decreased cancer aggressiveness [48]. An additional study of medulloblastoma revealing the chromatin compaction induced by REST via Akt activation identified a new potential subgroup of specific therapeutic targets [49].…”

Section: Cancersmentioning

confidence: 99%

News about the Role of the Transcription Factor REST in Neurons: From Physiology to Pathology

García-Manteiga

D’Alessandro

Meldolesi

2019

IJMS

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RE-1 silencing transcription factor (REST) (known also as NRSF) is a well-known transcription repressor whose strong decrease induces the distinction of neurons with respect to the other cells. Such distinction depends on the marked increased/decreased expression of specific genes, accompanied by parallel changes of the corresponding proteins. Many properties of REST had been identified in the past. Here we report those identified during the last 5 years. Among physiological discoveries are hundreds of genes governed directly/indirectly by REST, the mechanisms of its neuron/fibroblast conversions, and the cooperations with numerous distinct factors induced at the epigenetic level and essential for REST specific functions. New effects induced in neurons during brain diseases depend on the localization of REST, in the nucleus, where functions and toxicity occur, and in the cytoplasm. The effects of REST, including cell aggression or protection, are variable in neurodegenerative diseases in view of the distinct mechanisms of their pathology. Moreover, cooperations are among the mechanisms that govern the severity of brain cancers, glioblastomas, and medulloblastomas. Interestingly, the role in cancers is relevant also for therapeutic perspectives affecting the REST cooperations. In conclusion, part of the new REST knowledge in physiology and pathology appears promising for future developments in research and brain diseases.

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“…Moreover, ARRB1 expression inversely correlates with proliferation of GCPs derived from a transgenic mouse model involving RE1-silencing transcription factor (REST), a transcriptional repressor of neuronal differentiation [32]. For this reason, the fact that miR-326 and ARRB1 appear to exert convergent tumor-suppressive effects in human MBs is by no means incompatible with its demonstrated oncogenic effects in other cancer cells [73][74][75][76]71].…”

Section: Discussionmentioning

confidence: 99%

“…ARRB1, as miR-326, is involved in neuronal differentiation, where its up-regulated expression in cerebellar GCPs and in neural stem cells halts proliferation and induces growth arrest [25,26]. Notably, under-expression of ARRB1 has been documented in brain tumors [23,[27][28][29][30][31][32].…”

Section: Introductionmentioning

confidence: 99%

Downregulation of miR‐326 and its host gene β‐arrestin1 induces pro‐survival activity of E2F1 and promotes medulloblastoma growth

et al. 2020

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Transcriptional repressor REST drives lineage stage–specific chromatin compaction at Ptch1 and increases AKT activation in a mouse model of medulloblastoma

Cited by 19 publications

References 81 publications

ATRX In-Frame Fusion Neuroblastoma Is Sensitive to EZH2 Inhibition via Modulation of Neuronal Gene Signatures

ATRX In-Frame Fusion Neuroblastoma Is Sensitive to EZH2 Inhibition via Modulation of Neuronal Gene Signatures

News about the Role of the Transcription Factor REST in Neurons: From Physiology to Pathology

Downregulation of miR‐326 and its host gene β‐arrestin1 induces pro‐survival activity of E2F1 and promotes medulloblastoma growth

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