A large "gene desert" located far upstream from Fshb and Kcna4 contains several gonadotrope-specific accessible chromatin sites that were seen in chromatin conformation capture to make distinct contacts with both genes. Expression of Fshb and Kcna4 was strongly inhibited by JQ-1, which represses super-enhancer activity, and the region displays super-enhancer characteristics. The sites of open chromatin were seen, in chromatin immunoprecipitation, to bind Brd4 and Med1, most notably at a site -67â kb from the Fshb gene, as well as binding Ctcf further upstream (-123â kb), all of which were increased following activin exposure. The locus is transcribed to chromatin-associated long noncoding RNAs whose levels correlate with Fshb and Kcna4 mRNA levels in vivo and in cultured gonadotrope cells, indicating coordinated regulation. CRISPR interference confirmed distinct functions for each element and, together with the chromatin conformation capture data, indicate that the -67â kb locus mediates basal and activin-stimulated Fshb expression, whereas the site at -59â kb contributes to activin-stimulation of both genes. Single-cell multiomics revealed that the -67â kb locus is accessible in pituitary stem cells and throughout gonadotrope differentiation, preceding opening of the Fshb promoter, although it is closed in other differentiated cell types, suggesting a gonadotrope-specific factor that keeps it open at this stage. Foxl2 was found to bind this element, contributes to maintaining its chromatin accessibility, and recruits Supt16h, a component of the Facilitates Active Chromatin Transcription histone chaperone complex. These findings define a distal, Foxl2-bound super-enhancer that regulates Fshb transcription and shapes the gonadotrope regulatory landscape.
Accessibility at a primed distal Fshb-Kcna4 super-enhancer is facilitated by Foxl2 during gonadotrope differentiation.
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作者:Refael Tal, Golan Gil, Darsa Daniella, Pnueli Lilach, Chakravarty Probir, Rizzoti Karine, Melamed Philippa
| 期刊: | Endocrinology | 影响因子: | 3.300 |
| 时间: | 2026 | 起止号: | 2026 Apr 7; 167(5):bqag028 |
| doi: | 10.1210/endocr/bqag028 | ||
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