SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis

SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis

Male factor infertility accounts for approximately 50 percent of infertile couples. The male factor-related causes of intracytoplasmic sperm injection failure include the absence of sperm, immotile sperm, immature sperm, abnormally structured sperm, and sperm with nuclear damage. Our knockout and kn...

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Main Authors: Tsung-Hsuan Lai, Ying-Yu Wu, Ya-Yun Wang, Mei-Feng Chen, Pei Wang, Tsung-Ming Chen, Yi-No Wu, Han-Sun Chiang, Pao-Lin Kuo, Ying-Hung Lin
Format: Article
Language:English
Published: MDPI AG 2016-11-01
Series:International Journal of Molecular Sciences
Subjects:
male infertility
SEPT12
NDC1
Online Access:http://www.mdpi.com/1422-0067/17/11/1911
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spelling doaj-6913c955e902462e94363f681c6065102020-11-25T02:30:51ZengMDPI AGInternational Journal of Molecular Sciences1422-00672016-11-011711191110.3390/ijms17111911ijms17111911SEPT12–NDC1 Complexes Are Required for Mammalian SpermiogenesisTsung-Hsuan Lai0Ying-Yu Wu1Ya-Yun Wang2Mei-Feng Chen3Pei Wang4Tsung-Ming Chen5Yi-No Wu6Han-Sun Chiang7Pao-Lin Kuo8Ying-Hung Lin9Department of Obstetrics and Gynecology, Cathay General Hospital, Taipei 106, TaiwanGraduate Institute of Biomedical and Pharmaceutical Science, Fu Jen Catholic University, New Taipei City 242, TaiwanDepartment of Chemistry, Fu Jen Catholic University, New Taipei City 242, TaiwanBone and Joint Research Center, Chang Gung Memorial Hospital, Taoyuan 333, TaiwanSchool of Medicine, Fu Jen Catholic University, New Taipei City 242, TaiwanDepartment and Graduate Institute of Aquaculture, National Kaohsiung Marine University, Kaohsiung 811, TaiwanGraduate Institute of Biomedical and Pharmaceutical Science, Fu Jen Catholic University, New Taipei City 242, TaiwanGraduate Institute of Biomedical and Pharmaceutical Science, Fu Jen Catholic University, New Taipei City 242, TaiwanDepartment of Obstetrics & Gynecology, College of Medicine, National Cheng Kung University, Tainan 701, TaiwanGraduate Institute of Biomedical and Pharmaceutical Science, Fu Jen Catholic University, New Taipei City 242, TaiwanMale factor infertility accounts for approximately 50 percent of infertile couples. The male factor-related causes of intracytoplasmic sperm injection failure include the absence of sperm, immotile sperm, immature sperm, abnormally structured sperm, and sperm with nuclear damage. Our knockout and knock-in mice models demonstrated that SEPTIN12 (SEPT12) is vital for the formation of sperm morphological characteristics during spermiogenesis. In the clinical aspect, mutated SEPT12 in men results in oligozoospermia or teratozoospermia or both. Sperm with mutated SEPT12 revealed abnormal head and tail structures, decreased chromosomal condensation, and nuclear damage. Furthermore, several nuclear or nuclear membrane-related proteins have been identified as SEPT12 interactors through the yeast 2-hybrid system, including NDC1 transmembrane nucleoporin (NDC1). NDC1 is a major nuclear pore protein, and is critical for nuclear pore complex assembly and nuclear morphology maintenance in mammalian cells. Mutated NDC1 cause gametogenesis defects and skeletal malformations in mice, which were detected spontaneously in the A/J strain. In this study, we characterized the functional effects of SEPT12–NDC1 complexes during mammalian spermiogenesis. In mature human spermatozoa, SEPT12 and NDC1 are majorly colocalized in the centrosome regions; however, NDC1 is only slightly co-expressed with SEPT12 at the annulus of the sperm tail. In addition, SEPT12 interacts with NDC1 in the male germ cell line through coimmunoprecipitation. During murine spermiogenesis, we observed that NDC1 was located at the nuclear membrane of spermatids and at the necks of mature spermatozoa. In male germ cell lines, NDC1 overexpression restricted the localization of SEPT12 to the nucleus and repressed the filament formation of SEPT12. In mice sperm with mutated SEPT12, NDC1 dispersed around the manchette region of the sperm head and annulus, compared with concentrating at the sperm neck of wild-type sperm. These results indicate that SEPT12–NDC1 complexes are involved in mammalian spermiogenesis.http://www.mdpi.com/1422-0067/17/11/1911male infertilitySEPT12NDC1
collection DOAJ
language English
format Article
sources DOAJ
author Tsung-Hsuan Lai
Ying-Yu Wu
Ya-Yun Wang
Mei-Feng Chen
Pei Wang
Tsung-Ming Chen
Yi-No Wu
Han-Sun Chiang
Pao-Lin Kuo
Ying-Hung Lin
spellingShingle Tsung-Hsuan Lai
Ying-Yu Wu
Ya-Yun Wang
Mei-Feng Chen
Pei Wang
Tsung-Ming Chen
Yi-No Wu
Han-Sun Chiang
Pao-Lin Kuo
Ying-Hung Lin
SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis
International Journal of Molecular Sciences
male infertility
SEPT12
NDC1
author_facet Tsung-Hsuan Lai
Ying-Yu Wu
Ya-Yun Wang
Mei-Feng Chen
Pei Wang
Tsung-Ming Chen
Yi-No Wu
Han-Sun Chiang
Pao-Lin Kuo
Ying-Hung Lin
author_sort Tsung-Hsuan Lai
title SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis
title_short SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis
title_full SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis
title_fullStr SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis
title_full_unstemmed SEPT12–NDC1 Complexes Are Required for Mammalian Spermiogenesis
title_sort sept12–ndc1 complexes are required for mammalian spermiogenesis
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2016-11-01
description Male factor infertility accounts for approximately 50 percent of infertile couples. The male factor-related causes of intracytoplasmic sperm injection failure include the absence of sperm, immotile sperm, immature sperm, abnormally structured sperm, and sperm with nuclear damage. Our knockout and knock-in mice models demonstrated that SEPTIN12 (SEPT12) is vital for the formation of sperm morphological characteristics during spermiogenesis. In the clinical aspect, mutated SEPT12 in men results in oligozoospermia or teratozoospermia or both. Sperm with mutated SEPT12 revealed abnormal head and tail structures, decreased chromosomal condensation, and nuclear damage. Furthermore, several nuclear or nuclear membrane-related proteins have been identified as SEPT12 interactors through the yeast 2-hybrid system, including NDC1 transmembrane nucleoporin (NDC1). NDC1 is a major nuclear pore protein, and is critical for nuclear pore complex assembly and nuclear morphology maintenance in mammalian cells. Mutated NDC1 cause gametogenesis defects and skeletal malformations in mice, which were detected spontaneously in the A/J strain. In this study, we characterized the functional effects of SEPT12–NDC1 complexes during mammalian spermiogenesis. In mature human spermatozoa, SEPT12 and NDC1 are majorly colocalized in the centrosome regions; however, NDC1 is only slightly co-expressed with SEPT12 at the annulus of the sperm tail. In addition, SEPT12 interacts with NDC1 in the male germ cell line through coimmunoprecipitation. During murine spermiogenesis, we observed that NDC1 was located at the nuclear membrane of spermatids and at the necks of mature spermatozoa. In male germ cell lines, NDC1 overexpression restricted the localization of SEPT12 to the nucleus and repressed the filament formation of SEPT12. In mice sperm with mutated SEPT12, NDC1 dispersed around the manchette region of the sperm head and annulus, compared with concentrating at the sperm neck of wild-type sperm. These results indicate that SEPT12–NDC1 complexes are involved in mammalian spermiogenesis.
topic male infertility
SEPT12
NDC1
url http://www.mdpi.com/1422-0067/17/11/1911
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