TY - JOUR
T1 - PAX7 expression defines germline stem cells in the adult testis
AU - Aloisio, Gina M.
AU - Nakada, Yuji
AU - Saatcioglu, Hatice D.
AU - Peña, Christopher G.
AU - Baker, Michael D.
AU - Tarnawa, Edward D.
AU - Mukherjee, Jishnu
AU - Manjunath, Hema
AU - Bugde, Abhijit
AU - Sengupta, Anita L.
AU - Amatruda, James F.
AU - Cuevas, Ileana
AU - Hamra, F. Kent
AU - Castrillon, Diego H.
PY - 2014/9/2
Y1 - 2014/9/2
N2 - Spermatogenesis is a complex, multistep process that maintains male fertility and is sustained by rare germline stem cells. Spermatogenic progression begins with spermatogonia, populations of which express distinct markers. The identity of the spermatogonial stem cell population in the undisturbed testis is controversial due to a lack of reliable and specific markers. Here we identified the transcription factor PAX7 as a specific marker of a rare subpopulation of Asinglespermatogonia in mice. PAX7+cells were present in the testis at birth. Compared with the adult testis, PAX7+cells constituted a much higher percentage of neonatal germ cells. Lineage tracing in healthy adult mice revealed that PAX7+spermatogonia self-maintained and produced expanding clones that gave rise to mature spermatozoa. Interestingly, in mice subjected to chemotherapy and radiotherapy, both of which damage the vast majority of germ cells and can result in sterility, PAX7+spermatogonia selectively survived, and their subsequent expansion contributed to the recovery of spermatogenesis. Finally, PAX7+spermatogonia were present in the testes of a diverse set of mammals. Our data indicate that the PAX7+subset of Asinglespermatogonia functions as robust testis stem cells that maintain fertility in normal spermatogenesis in healthy mice and mediate recovery after severe germline injury, such as occurs after cancer therapy.
AB - Spermatogenesis is a complex, multistep process that maintains male fertility and is sustained by rare germline stem cells. Spermatogenic progression begins with spermatogonia, populations of which express distinct markers. The identity of the spermatogonial stem cell population in the undisturbed testis is controversial due to a lack of reliable and specific markers. Here we identified the transcription factor PAX7 as a specific marker of a rare subpopulation of Asinglespermatogonia in mice. PAX7+cells were present in the testis at birth. Compared with the adult testis, PAX7+cells constituted a much higher percentage of neonatal germ cells. Lineage tracing in healthy adult mice revealed that PAX7+spermatogonia self-maintained and produced expanding clones that gave rise to mature spermatozoa. Interestingly, in mice subjected to chemotherapy and radiotherapy, both of which damage the vast majority of germ cells and can result in sterility, PAX7+spermatogonia selectively survived, and their subsequent expansion contributed to the recovery of spermatogenesis. Finally, PAX7+spermatogonia were present in the testes of a diverse set of mammals. Our data indicate that the PAX7+subset of Asinglespermatogonia functions as robust testis stem cells that maintain fertility in normal spermatogenesis in healthy mice and mediate recovery after severe germline injury, such as occurs after cancer therapy.
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U2 - 10.1172/JCI75943
DO - 10.1172/JCI75943
M3 - Article
C2 - 25133429
AN - SCOPUS:84907009214
SN - 0021-9738
VL - 124
SP - 3929
EP - 3944
JO - Journal of Clinical Investigation
JF - Journal of Clinical Investigation
IS - 9
ER -