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. 2017 Oct 1;144(19):3430-3439.
doi: 10.1242/dev.150284. Epub 2017 Aug 21.

Spermatogonial kinetics in humans

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Spermatogonial kinetics in humans

Sara Di Persio et al. Development. .

Abstract

The human spermatogonial compartment is essential for daily production of millions of sperm. Despite this crucial role, the molecular signature, kinetic behavior and regulation of human spermatogonia are poorly understood. Using human testis biopsies with normal spermatogenesis and by studying marker protein expression, we have identified for the first time different subpopulations of spermatogonia. MAGE-A4 marks all spermatogonia, KIT marks all B spermatogonia and UCLH1 all Apale-dark (Ap-d) spermatogonia. We suggest that at the start of the spermatogenic lineage there are Ap-d spermatogonia that are GFRA1High, likely including the spermatogonial stem cells. Next, UTF1 becomes expressed, cells become quiescent and GFRA1 expression decreases. Finally, GFRA1 expression is lost and subsequently cells differentiate into B spermatogonia, losing UTF1 and acquiring KIT expression. Strikingly, most human Ap-d spermatogonia are out of the cell cycle and even differentiating type B spermatogonial proliferation is restricted. A novel scheme for human spermatogonial development is proposed that will facilitate further research in this field, the understanding of cases of infertility and the development of methods to increase sperm output.

Keywords: GFRA1; Human; KIT; Spermatogonia; Spermatogonial differentiation; Stem cell renewal; UCL-H1; UTF1.

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Conflict of interest statement

Competing interestsThe authors declare no competing or financial interests.

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