Transcriptional regulation of BRCA1 expression by a metabolic switch
Alterations in BRCA1 transcription can contribute to sporadic forms of breast cancer. Now the dynamics between transcriptional coactivators and co-repressors at the BRCA1 promoter reveal a central role for the metabolic sensor CtBP in the response to estrogen or cellular metabolic status Though the...
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Veröffentlicht in: | Nature structural & molecular biology 2010-12, Vol.17 (12), p.1406-1413 |
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Sprache: | eng |
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Zusammenfassung: | Alterations in
BRCA1
transcription can contribute to sporadic forms of breast cancer. Now the dynamics between transcriptional coactivators and co-repressors at the
BRCA1
promoter reveal a central role for the metabolic sensor CtBP in the response to estrogen or cellular metabolic status
Though the linkages between germline mutations of
BRCA1
and hereditary breast cancer are well known, recent evidence suggests that altered
BRCA1
transcription may also contribute to sporadic forms of breast cancer. Here we show that
BRCA1
expression is controlled by a dynamic equilibrium between transcriptional coactivators and co-repressors that govern histone acetylation and DNA accessibility at the
BRCA1
promoter. Eviction of the transcriptional co-repressor and metabolic sensor, C terminal–binding protein (CtBP), has a central role in this regulation. Loss of CtBP from the
BRCA1
promoter through estrogen induction, depletion by RNA interference or increased NAD
+
/NADH ratio leads to HDAC1 dismissal, elevated histone acetylation and increased
BRCA1
transcription. The active control of chromatin marks, DNA accessibility and gene expression at the
BRCA1
promoter by this 'metabolic switch' provides an important molecular link between caloric intake and tumor suppressor expression in mammary cells. |
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ISSN: | 1545-9993 1545-9985 |
DOI: | 10.1038/nsmb.1941 |