Abstract

BackgroundThe most common sex chromosomal aneuploidy in males is Klinefelter syndrome, which is characterized by at least one supernumerary X chromosome. While these men have long been considered infertile, focal spermatogenesis can be observed in some patients, and sperm can be surgically retrieved and used for artificial reproductive techniques. Although these gametes can be used for fertility treatments, little is known about the molecular biology of the germline in Klinefelter men. Specifically, it is unclear if germ cells in Klinefelter syndrome correctly establish the androgenetic DNA methylation profile and transcriptome. This is due to the low number of germ cells in the Klinefelter testes available for analysis.ResultsHere, we overcame these difficulties and successfully investigated the epigenetic and transcriptional profiles of germ cells in Klinefelter patients employing deep bisulfite sequencing and single-cell RNA sequencing. On the transcriptional level, the germ cells from Klinefelter men clustered together with the differentiation stages of normal spermatogenesis. Klinefelter germ cells showed a normal DNA methylation profile of selected germ cell-specific markers compared with spermatogonia and sperm from men with normal spermatogenesis. However, germ cells from Klinefelter patients showed variations in the DNA methylation of imprinted regions.ConclusionsThese data indicate that Klinefelter germ cells have a normal transcriptome but might present aberrant imprinting, showing impairment in germ cell development that goes beyond mere germ cell loss.

Highlights

  • The most common sex chromosomal aneuploidy in males is Klinefelter syndrome, which is characterized by at least one supernumerary X chromosome

  • Individual tubules showing focal spermatogenesis could be detected in selected Klinefelter tissues (Fig. 1b, f)

  • Germ cells at different stages of differentiation display normal transcriptome in Klinefelter testis Using testicular tissues with qualitatively normal spermatogenesis, germ cells were enriched from testicular tissues using a differential plating approach

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Summary

Introduction

The most common sex chromosomal aneuploidy in males is Klinefelter syndrome, which is characterized by at least one supernumerary X chromosome While these men have long been considered infertile, focal spermatogenesis can be observed in some patients, and sperm can be surgically retrieved and used for artificial reproductive techniques. These gametes can be used for fertility treatments, little is known about the molecular biology of the germline in Klinefelter men It is unclear if germ cells in Klinefelter syndrome correctly establish the androgenetic DNA methylation profile and transcriptome. Analysis of children born to men with non-mosaic KS after testicular sperm extraction and intracytoplasmic sperm injection revealed normal karyotypes in cohorts of 16 and 17 children, respectively [8, 9] These euploid sperms likely originate from focal populations of euploid spermatogonia amidst XXY Sertoli cells [10]. Available data suggests that the risk of transmission of chromosomal aneuploidy through the germline may be rather low

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