The Molecular Signature of Human Testicular Peritubular Cells Revealed by Single-Cell Analysis

Peritubular cells of the human testis form a small compartment surrounding the seminiferous tubules. They are crucial for sperm transport, and they emerge as contributors to the spermatogonial stem cell niche. They are among the least known cell types of the human body. We employed single-cell RNA sequencing of cultured human testicular peritubular cells (HTPCs), which had been isolated from testicular samples of donors with normal spermatogenesis. The significant overlap between our results and recently published ex vivo data indicates that HTPCs are a highly adequate cellular model to define and study these cells. Thus, based on the expression of several markers, HTPCs can be classified as testicular smooth muscle cells. Small differences between the in vivo/in vitro expressed genes may be due to cellular plasticity. Plasticity was also shown upon addition of FCS to the culture medium. Based on transcriptome similarities, four cellular states were identified. Further analyses confirmed the presence of known stem cell niche-relevant factors (e.g., GDNF) and identified unknown functions, e.g., the ability to produce retinoic acid. Therefore, HTPCs allow us to define the signature(s) and delineate the functions of human testicular peritubular cells. The data may also serve as a resource for future studies to better understand male (in)fertility.

Automated summary

Peritubular cells of the human testis play important roles in sperm transport and spermatogonial stem cell niche. In this study, single-cell RNA sequencing was used to study cultured human testicular peritubular cells (HTPCs) isolated from donors with normal spermatogenesis. The expression profile of HTPCs revealed cell plasticity and identified four cellular states. The findings provide insights into the functions of human testicular peritubular cells and serve as a resource for further understanding male (in)fertility.