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Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization

Squamous cell carcinoma–related oncogene (SCCRO, also known as DCUN1D1) is a component of the E3 for neddylation. As such, DCUN1D1 regulates the neddylation of cullin family members. Targeted inactivation of DCUN1D1 in mice results in male-specific infertility. Infertility in DCUN1D1(-/-) mice is se...

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Autores principales: Huang, Guochang, Kaufman, Andrew J., Ryan, Russell J. H., Romin, Yevgeniy, Huryn, Laryssa, Bains, Sarina, Manova-Todorova, Katia, Morris, Patricia L., Hunnicutt, Gary R., Adelman, Carrie A., Petrini, John H. J., Ramanathan, Y., Singh, Bhuvanesh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6336273/
https://www.ncbi.nlm.nih.gov/pubmed/30653527
http://dx.doi.org/10.1371/journal.pone.0209995
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author Huang, Guochang
Kaufman, Andrew J.
Ryan, Russell J. H.
Romin, Yevgeniy
Huryn, Laryssa
Bains, Sarina
Manova-Todorova, Katia
Morris, Patricia L.
Hunnicutt, Gary R.
Adelman, Carrie A.
Petrini, John H. J.
Ramanathan, Y.
Singh, Bhuvanesh
author_facet Huang, Guochang
Kaufman, Andrew J.
Ryan, Russell J. H.
Romin, Yevgeniy
Huryn, Laryssa
Bains, Sarina
Manova-Todorova, Katia
Morris, Patricia L.
Hunnicutt, Gary R.
Adelman, Carrie A.
Petrini, John H. J.
Ramanathan, Y.
Singh, Bhuvanesh
author_sort Huang, Guochang
collection PubMed
description Squamous cell carcinoma–related oncogene (SCCRO, also known as DCUN1D1) is a component of the E3 for neddylation. As such, DCUN1D1 regulates the neddylation of cullin family members. Targeted inactivation of DCUN1D1 in mice results in male-specific infertility. Infertility in DCUN1D1(-/-) mice is secondary to primary defects in spermatogenesis. Time-dam experiments mapped the onset of the defect in spermatogenesis to 5.5 to 6 weeks of age, which temporally corresponds to defects in spermiogenesis. Although the first round of spermatogenesis progressed normally, the number of spermatozoa released into the seminiferous lumen and epididymis of DCUN1D1(-/-) mice was significantly reduced. Spermatozoa in DCUN1D1(-/-) mice had multiple abnormalities, including globozoospermia, macrocephaly, and multiple flagella. Many of the malformed spermatozoa in DCUN1D1(-/-) mice were multinucleated, with supernumerary and malpositioned centrioles, suggesting a defect in the resolution of intercellular bridges. The onset of the defect in spermatogenesis in DCUN1D1(-/-) mice corresponds to an increase in DCUN1D1 expression observed during normal spermatogenesis. Moreover, consistent with its known function as a component of the E3 in neddylation, the pattern of DCUN1D1 expression temporally correlates with an increase in the neddylated cullin fraction and stage-specific increases in the total ubiquitinated protein pool in wild-type mice. Levels of neddylated Cul3 were decreased in DCUN1D1(-/-) mice, and ubiquitinated proteins did not accumulate during the stages in which DCUN1D1 expression peaks during spermatogenesis in wild-type mice. Combined, these findings suggest that DCUN1D1(-/-) mice fail to release mature spermatozoa into the seminiferous lumen, possibly due to unresolved intercellular bridges. Furthermore, the effects of DCUN1D1 on spermatogenesis likely involve its regulation of cullin-RING-ligase (CRL)–type ubiquitin E3 activity during spermiogenesis through its role in promoting Cul3 neddylation. The specific CRLs required for spermiogenesis and their protein targets require identification.
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spelling pubmed-63362732019-01-30 Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization Huang, Guochang Kaufman, Andrew J. Ryan, Russell J. H. Romin, Yevgeniy Huryn, Laryssa Bains, Sarina Manova-Todorova, Katia Morris, Patricia L. Hunnicutt, Gary R. Adelman, Carrie A. Petrini, John H. J. Ramanathan, Y. Singh, Bhuvanesh PLoS One Research Article Squamous cell carcinoma–related oncogene (SCCRO, also known as DCUN1D1) is a component of the E3 for neddylation. As such, DCUN1D1 regulates the neddylation of cullin family members. Targeted inactivation of DCUN1D1 in mice results in male-specific infertility. Infertility in DCUN1D1(-/-) mice is secondary to primary defects in spermatogenesis. Time-dam experiments mapped the onset of the defect in spermatogenesis to 5.5 to 6 weeks of age, which temporally corresponds to defects in spermiogenesis. Although the first round of spermatogenesis progressed normally, the number of spermatozoa released into the seminiferous lumen and epididymis of DCUN1D1(-/-) mice was significantly reduced. Spermatozoa in DCUN1D1(-/-) mice had multiple abnormalities, including globozoospermia, macrocephaly, and multiple flagella. Many of the malformed spermatozoa in DCUN1D1(-/-) mice were multinucleated, with supernumerary and malpositioned centrioles, suggesting a defect in the resolution of intercellular bridges. The onset of the defect in spermatogenesis in DCUN1D1(-/-) mice corresponds to an increase in DCUN1D1 expression observed during normal spermatogenesis. Moreover, consistent with its known function as a component of the E3 in neddylation, the pattern of DCUN1D1 expression temporally correlates with an increase in the neddylated cullin fraction and stage-specific increases in the total ubiquitinated protein pool in wild-type mice. Levels of neddylated Cul3 were decreased in DCUN1D1(-/-) mice, and ubiquitinated proteins did not accumulate during the stages in which DCUN1D1 expression peaks during spermatogenesis in wild-type mice. Combined, these findings suggest that DCUN1D1(-/-) mice fail to release mature spermatozoa into the seminiferous lumen, possibly due to unresolved intercellular bridges. Furthermore, the effects of DCUN1D1 on spermatogenesis likely involve its regulation of cullin-RING-ligase (CRL)–type ubiquitin E3 activity during spermiogenesis through its role in promoting Cul3 neddylation. The specific CRLs required for spermiogenesis and their protein targets require identification. Public Library of Science 2019-01-17 /pmc/articles/PMC6336273/ /pubmed/30653527 http://dx.doi.org/10.1371/journal.pone.0209995 Text en © 2019 Huang et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Huang, Guochang
Kaufman, Andrew J.
Ryan, Russell J. H.
Romin, Yevgeniy
Huryn, Laryssa
Bains, Sarina
Manova-Todorova, Katia
Morris, Patricia L.
Hunnicutt, Gary R.
Adelman, Carrie A.
Petrini, John H. J.
Ramanathan, Y.
Singh, Bhuvanesh
Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization
title Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization
title_full Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization
title_fullStr Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization
title_full_unstemmed Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization
title_short Mouse DCUN1D1 (SCCRO) is required for spermatogenetic individualization
title_sort mouse dcun1d1 (sccro) is required for spermatogenetic individualization
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6336273/
https://www.ncbi.nlm.nih.gov/pubmed/30653527
http://dx.doi.org/10.1371/journal.pone.0209995
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