AI Article Synopsis

  • Spermatogenesis occurs in the seminiferous epithelium and is regulated by estrogen receptors alpha (ERα) and beta (ERβ), which bind to DNA and influence gene transcription.
  • A study used chromatin immunoprecipitation (ChIP) sequencing to identify over 27,000 binding regions for ERα and over 20,000 for ERβ, mainly found in intronic regions near transcription start sites.
  • The analysis revealed several biological pathways linked to spermatogenesis, including prolactin, GnRH, and oxytocin signaling, with further validation confirming that estrogen regulates these genes through its receptors in both cultured seminiferous tubules and in vivo rat models.

Article Abstract

Spermatogenesis occurs in the seminiferous epithelium that shows the presence of estrogen receptors alpha (ERα) and beta (ERβ), both of which regulate gene transcription by binding to the DNA. Estrogen responsive phases of spermatogenesis are well documented; however, the genes regulated remain inexplicit. To study the regulation of genes by estrogen in male germ cells, we performed chromatin immunoprecipitation (ChIP) sequencing for ERα and ERβ under normal physiological conditions. A total of 27 221 DNA binding regions were enriched with ERα and 20 926 binding sites with ERβ. Majority of the peaks were present in the intronic regions and located 20 kb upstream or downstream from the transcription start site (TSS). Pathway analysis of the genes enriched by ChIP-Seq showed involvement in several biological pathways. Genes involved in pathways whose role in spermatogenesis is unexplored were validated; these included prolactin, GnRH, and oxytocin signaling. All the selected genes showed the presence of estrogen response elements (EREs) in their binding region and were also found to be significantly enriched by ChIP-qPCR. Functional validation using seminiferous tubule culture after treatment with estrogen receptor subtype-specific agonist and antagonist confirmed the regulation of these genes by estrogen through its receptors. The genes involved in these pathways were also found to be regulated by the respective receptor subtypes at the testicular level in our in vivo estrogen receptor agonist rat models. Our study provides a genome-wide map of ERα and ERβ binding sites and identifies the genes regulated by them in the male germ cells under normal physiological conditions.

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Source
http://dx.doi.org/10.1042/BCJ20190946DOI Listing

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