Single-cell transcriptome analysis of Bisphenol A exposure reveals the key roles of the testicular microenvironment in male reproduction - 12/12/21
, Mingzhi Liao a, ⁎ Benvenuto su EM|consulte, il riferimento dei professionisti della salute.
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Abstract |
Testicular development during juvenile is crucial for subsequent male reproductive function. However, it remains poorly understood about the contribution of the testis microenvironment to human germ cell maturation. Therefore, we systematically analyzed scRNA-seq transcriptome and found the dramatic changes in cell-type composition in human testis during puberty. Then we constructed cell-cell communication networks between germ cells and somatic cells in the juvenile testis, which may be achieved via immune-related pathways. Our results showed that maturation-promoting factors are the switches of the Sertoli cells that drive sperm maturation. Furthermore, we found that Bisphenol A(BPA) enhanced the maturation and growth of germ cells through the Sertoli cell's secretory protein. Finally, our results indicate Bisphenol A would lead to the dysregulation of secreted protein expression in Sertoli cells during spermatogenesis, which in turn has direct cytotoxicity to Sertoli cells. Bisphenol A is one of the underlying causes of non-obstructive azoospermia (NOA). In summary, our results reveal the reproductive toxicity and molecular mechanism of Bisphenol A in Sertoli cells and male reproduction. Provide a reference for the toxicity of Bisphenol A to human reproduction.
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Highlights |
• | Single cell transcriptome reveals the microenvironment changes of human testis. |
• | Cell communication network was constructed between germ cells and somatic cells. |
• | The BPA promotes the sperm maturation through maturation promoting factor. |
• | BPA may lead to the dysregulation of secretory protein expression by Sertoli cells. |
• | BPA triggers non-obstructive azoospermia (NOA) via their shared molecular signals. |
Keywords : Bisphenol A(BPA), Microenvironment, Secretory proteins, Single-cell transcriptome, Cell-cell communication network, Reproductive toxicology
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Vol 145
Articolo 112449- gennaio 2022 Ritorno al numero
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