E2F1 regulates testicular descent and controls spermatogenesis by influencing WNT4 signaling

Carolina J. Jorgez; Abhishek Seth; Nathan Wilken; Juan C. Bournat; Ching H. Chen; Dolores J. Lamb

doi:10.1242/dev.191189

E2F1 regulates testicular descent and controls spermatogenesis by influencing WNT4 signaling

Carolina J. Jorgez, Abhishek Seth, Nathan Wilken, Juan C. Bournat, Ching H. Chen, Dolores J. Lamb

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Cryptorchidism is the most common urologic birth defect in men and is a predisposing factor of male infertility and testicular cancer, yet the etiology remains largely unknown. E2F1 microdeletions and microduplications contribute to cryptorchidism, infertility and testicular tumors. Although E2f1 deletion or overexpression in mice causes spermatogenic failure, the mechanism by which E2f1 influences testicular function is unknown. This investigation revealed that E2f1-null mice develop cryptorchidism with severe gubernacular defects and progressive loss of germ cells resulting in infertility and, in rare cases, testicular tumors. It was hypothesized that germ cell depletion resulted from an increase in WNT4 levels. To test this hypothesis, the phenotype of a double-null mouse model lacking both Wnt4 and E2f1 in germ cells was analyzed. Double-null mice are fertile. This finding indicates that germ cell maintenance is dependent on E2f1 repression of Wnt4, supporting a role for Wnt4 in germ cell survival. In the future, modulation of WNT4 expression in men with cryptorchidism and spermatogenic failure due to E2F1 copy number variations may provide a novel approach to improve their spermatogenesis and perhaps their fertility potential after orchidopexy.

Original language	English (US)
Article number	dev191189
Journal	Development (Cambridge)
Volume	148
Issue number	1
DOIs	https://doi.org/10.1242/dev.191189
State	Published - Jan 2021

Keywords

Copy number variations
Cryptorchidism
E2f1
Infertility
Testicular cancer
Wnt4

ASJC Scopus subject areas

Molecular Biology
Developmental Biology

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10.1242/dev.191189

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@article{3d4657d0e4e044dabedf68348934e3ab,

title = "E2F1 regulates testicular descent and controls spermatogenesis by influencing WNT4 signaling",

abstract = "Cryptorchidism is the most common urologic birth defect in men and is a predisposing factor of male infertility and testicular cancer, yet the etiology remains largely unknown. E2F1 microdeletions and microduplications contribute to cryptorchidism, infertility and testicular tumors. Although E2f1 deletion or overexpression in mice causes spermatogenic failure, the mechanism by which E2f1 influences testicular function is unknown. This investigation revealed that E2f1-null mice develop cryptorchidism with severe gubernacular defects and progressive loss of germ cells resulting in infertility and, in rare cases, testicular tumors. It was hypothesized that germ cell depletion resulted from an increase in WNT4 levels. To test this hypothesis, the phenotype of a double-null mouse model lacking both Wnt4 and E2f1 in germ cells was analyzed. Double-null mice are fertile. This finding indicates that germ cell maintenance is dependent on E2f1 repression of Wnt4, supporting a role for Wnt4 in germ cell survival. In the future, modulation of WNT4 expression in men with cryptorchidism and spermatogenic failure due to E2F1 copy number variations may provide a novel approach to improve their spermatogenesis and perhaps their fertility potential after orchidopexy.",

keywords = "Copy number variations, Cryptorchidism, E2f1, Infertility, Testicular cancer, Wnt4",

author = "Jorgez, {Carolina J.} and Abhishek Seth and Nathan Wilken and Bournat, {Juan C.} and Chen, {Ching H.} and Lamb, {Dolores J.}",

note = "Funding Information: This study was supported in part by National Institutes of Health (NIH) grants K12DK0083014 and the Multidisciplinary K12 Urologic Research (KURe) Career Development Program award (C.J.J. and A.S. were KURe K12 Scholars), and grant 1R01DK078121 from the National Institute of Diabetes and Digestive and Kidney Diseases (both awarded to D.J.L.), and the Junior Faculty Seed Award from the Caroline Wiess Law Fund for Research in Molecular Medicine to C.J.J. D.J.L. is also supported in part by grants 1U54HD100549-01 (T. Levin), 1R01HD095341 (T. Garcia) and 5P01HD087157 (M. M. Matzuk) from the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) of the NIH. D.J.L. is also supported in part by the Frederick J. and Theresa Dow Wallace Fund of the New York Community Trust. C.J.J. and A.S. are supported in part by NIH grant 1R01HD100985 from the NICHD. Deposited in PMC for release after 12 months. Publisher Copyright: {\textcopyright} 2021. Published by The Company of Biologists Ltd",

year = "2021",

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doi = "10.1242/dev.191189",

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AU - Jorgez, Carolina J.

AU - Seth, Abhishek

AU - Wilken, Nathan

AU - Bournat, Juan C.

AU - Chen, Ching H.

AU - Lamb, Dolores J.

N1 - Funding Information: This study was supported in part by National Institutes of Health (NIH) grants K12DK0083014 and the Multidisciplinary K12 Urologic Research (KURe) Career Development Program award (C.J.J. and A.S. were KURe K12 Scholars), and grant 1R01DK078121 from the National Institute of Diabetes and Digestive and Kidney Diseases (both awarded to D.J.L.), and the Junior Faculty Seed Award from the Caroline Wiess Law Fund for Research in Molecular Medicine to C.J.J. D.J.L. is also supported in part by grants 1U54HD100549-01 (T. Levin), 1R01HD095341 (T. Garcia) and 5P01HD087157 (M. M. Matzuk) from the Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) of the NIH. D.J.L. is also supported in part by the Frederick J. and Theresa Dow Wallace Fund of the New York Community Trust. C.J.J. and A.S. are supported in part by NIH grant 1R01HD100985 from the NICHD. Deposited in PMC for release after 12 months. Publisher Copyright: © 2021. Published by The Company of Biologists Ltd

PY - 2021/1

Y1 - 2021/1

N2 - Cryptorchidism is the most common urologic birth defect in men and is a predisposing factor of male infertility and testicular cancer, yet the etiology remains largely unknown. E2F1 microdeletions and microduplications contribute to cryptorchidism, infertility and testicular tumors. Although E2f1 deletion or overexpression in mice causes spermatogenic failure, the mechanism by which E2f1 influences testicular function is unknown. This investigation revealed that E2f1-null mice develop cryptorchidism with severe gubernacular defects and progressive loss of germ cells resulting in infertility and, in rare cases, testicular tumors. It was hypothesized that germ cell depletion resulted from an increase in WNT4 levels. To test this hypothesis, the phenotype of a double-null mouse model lacking both Wnt4 and E2f1 in germ cells was analyzed. Double-null mice are fertile. This finding indicates that germ cell maintenance is dependent on E2f1 repression of Wnt4, supporting a role for Wnt4 in germ cell survival. In the future, modulation of WNT4 expression in men with cryptorchidism and spermatogenic failure due to E2F1 copy number variations may provide a novel approach to improve their spermatogenesis and perhaps their fertility potential after orchidopexy.

AB - Cryptorchidism is the most common urologic birth defect in men and is a predisposing factor of male infertility and testicular cancer, yet the etiology remains largely unknown. E2F1 microdeletions and microduplications contribute to cryptorchidism, infertility and testicular tumors. Although E2f1 deletion or overexpression in mice causes spermatogenic failure, the mechanism by which E2f1 influences testicular function is unknown. This investigation revealed that E2f1-null mice develop cryptorchidism with severe gubernacular defects and progressive loss of germ cells resulting in infertility and, in rare cases, testicular tumors. It was hypothesized that germ cell depletion resulted from an increase in WNT4 levels. To test this hypothesis, the phenotype of a double-null mouse model lacking both Wnt4 and E2f1 in germ cells was analyzed. Double-null mice are fertile. This finding indicates that germ cell maintenance is dependent on E2f1 repression of Wnt4, supporting a role for Wnt4 in germ cell survival. In the future, modulation of WNT4 expression in men with cryptorchidism and spermatogenic failure due to E2F1 copy number variations may provide a novel approach to improve their spermatogenesis and perhaps their fertility potential after orchidopexy.

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E2F1 regulates testicular descent and controls spermatogenesis by influencing WNT4 signaling

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Keywords

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