Epididymal mRNA expression profiles for the protein disulfide isomerase gene family: Modulation by development and androgens.

Andrology

Laboratory of Molecular, Endocrine and Reproductive Pharmacology, Department of Pharmacology, Universidade Federal de São Paulo - Escola Paulista de Medicina, São Paulo, Brazil.

Published: August 2024

AI Article Synopsis

  • The endoplasmic reticulum (ER) is crucial for protein quality control and involves protein disulfide isomerases (PDIs), which assist in protein folding and modifications and may play roles in hormone function, particularly in sperm maturation within the epididymis.
  • This study focuses on the transcriptional activity of Pdi genes in the epididymis, using adult Wistar rats to assess how these genes respond to various conditions, including developmental changes and surgical interventions.
  • Results showed certain PDI transcripts were present in both reproductive and non-reproductive tissues, with specific patterns of expression related to developmental stages and hormonal influences, suggesting their significance in epididymal function and sperm maturation.

Article Abstract

Background: The endoplasmic reticulum (ER) is the central hub for protein quality control, where the protein disulfide isomerases (PDIs), encoded by at least 21 genes, play a pivotal role. These multifunctional proteins contribute to disulfide bond formation, proper folding, and protein modifications, and may act as hormone-binding proteins (e.g., steroids), influencing hormone biology. The interplay between ER proteostasis, PDIs, and epididymis-a crucial site for sperm maturation-remains largely understudied.

Objectives: This study characterizes transcriptional signatures of Pdi genes in the epididymis.

Material And Methods: Transcriptional profiles of selected Pdi genes were assessed in adult Wistar rat tissues, and epididymis under different experimental conditions (developmental stages, surgical castration, and efferent ductules ligation [EDL]). In silico bioinformatic analyses identified expression trends of this gene family in human epididymal segments.

Results: P4hb, Pdia3, Pdia5, Pdia6, Erp44, Erp29, and Casq1 transcripts were detected in both reproductive and non-reproductive tissues, while Casq2 exhibited higher abundance in vas deferens, prostate, and heart. Pdilt, highly expressed in testis, and Pdia2, highly expressed in heart, showed minimal mRNA levels in the epididymis. In the mesonephric duct, epididymal embryonic precursor, P4hb, Pdia3, Pdia5, Pdia6, and Erp29 mRNAs were found at gestational day (GD) 17.5. Except for Erp29, which remained stable, these Pdi transcript levels increased from GD17.5 to GD20.5, when epididymal morphogenesis occurs, and were maintained to varying degrees in the epididymis during postnatal development. Surgical castration downregulated P4hb, Pdia3, Pdia5, Pdia6, Pdilt and Erp29 transcripts, an effect reversed by testosterone replacement. Conversely, transcript levels remained unaffected by EDL, except P4hb, which was reduced in caput epididymis. All 21 PDI genes exhibited diverse transcriptional profiles across the human epididymis.

Discussion And Conclusion: The findings lay the foundations to explore Pdi genes in epididymal biology. As a considerable proportion of male infertility cases are idiopathic, targeting hormonal regulation of protein quality control in epididymis represents a route to address male infertility and advance therapeutic interventions in this domain.

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Source
http://dx.doi.org/10.1111/andr.13700DOI Listing

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