AI Article Synopsis
- Infertility impacts 10-15% of men globally, with genetic factors causing issues in about one-third of cases, particularly linked to the protein PICK1 and its deficiency affecting Sertoli cell function.
- The study aims to use multi-omics analysis to explore the effects of PICK1 deficiency on Sertoli cells and find biomarkers that distinguish fertile males from those infertile due to this deficiency.
- Results reveal two mutations in PICK1 associated with infertility, decreased serum inhibin B, and impaired Sertoli cell function, alongside significant metabolic and gene expression changes in a PICK1-deficient mouse model, correlating with reduced testis volume and sperm production.
Article Abstract
Background: Infertility affects approximately 10-15% of reproductive-age men worldwide, and genetic causes play a role in one-third of cases. As a Bin-Amphiphysin-Rvs (BAR) domain protein, protein interacting with C-kinase 1 (PICK1) deficiency could lead to impairment of acrosome maturation. However, its effects on auxiliary germ cells such as Sertoli cells are unknown.
Purpose: The present work was aimed to use multi-omics analysis to research the effects of PICK1 deficiency on Sertoli cells and to identify effective biomarkers to distinguish fertile males from infertile males caused by PICK1 deficiency.
Methods: Whole-exome sequencing (WES) was performed on 20 infertility patients with oligozoospermia to identify pathogenic PICK1 mutations. Multi-omics analysis of a PICK1 knockout (KO) mouse model was utilized to identify pathogenic mechanism. Animal and cell function experiments of Sertoli cell-specific PICK1 KO mouse were performed to verify the functional impairment of Sertoli cells.
Results: Two loss-of-function deletion mutations c.358delA and c.364delA in PICK1 resulting in transcription loss of BAR functional domain were identified in infertility patients with a specific decrease in serum inhibin B, indicating functional impairment of Sertoli cells. Multi-omics analysis of PICK1 KO mouse illustrated that targeted genes of differentially expressed microRNAs and mRNAs are significantly enriched in the negative regulatory role in the vesicle trafficking pathway, while metabolomics analysis showed that the metabolism of amino acids, lipids, cofactors, vitamins, and endocrine factors changed. The phenotype of PICK1 KO mouse showed a reduction in testis volume, a decreased number of mature spermatozoa and impaired secretory function of Sertoli cells. In vitro experiments confirmed that the expression of growth factors secreted by Sertoli cells in PICK1 conditional KO mouse such as Bone morphogenetic protein 4 (BMP4) and Fibroblast growth factor 2 (FGF2) were decreased.
Conclusions: Our study attributed male infertility caused by PICK1 deficiency to impaired vesicle-related secretory function of Sertoli cells and identified a variety of significant candidate biomarkers for male infertility induced by PICK1 deficiency.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10675906 | PMC |
| http://dx.doi.org/10.1186/s12958-023-01163-w | DOI Listing |
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