Your search keyword '"Yiqiang Cui"' showing total 48 results

1. STYXL1 regulates CCT complex assembly and flagellar tubulin folding in sperm formation

Author

Yu Chen, Mengjiao Luo, Haixia Tu, Yaling Qi, Yueshuai Guo, Xiangzheng Zhang, Yiqiang Cui, Mengmeng Gao, Xin Zhou, Tianyu Zhu, Hui Zhu, Chenghao Situ, Yan Li, and Xuejiang Guo

Subjects

Science

Abstract

Abstract Tubulin-based microtubule is a core component of flagella axoneme and essential for sperm motility and male fertility. Structural components of the axoneme have been well explored. However, how tubulin folding is regulated in sperm flagella formation is still largely unknown. Here, we report a germ cell-specific co-factor of CCT complex, STYXL1. Deletion of Styxl1 results in male infertility and microtubule defects of sperm flagella. Proteomic analysis of Styxl1 -/- sperm reveals abnormal downregulation of flagella-related proteins including tubulins. The N-terminal rhodanese-like domain of STYXL1 is important for its interactions with CCT complex subunits, CCT1, CCT6 and CCT7. Styxl1 deletion leads to defects in CCT complex assembly and tubulin polymerization. Collectively, our findings reveal the vital roles of germ cell-specific STYXL1 in CCT-facilitated tubulin folding and sperm flagella development.

Published

2024

2. Single-cell RNA-seq uncovers dynamic processes orchestrated by RNA-binding protein DDX43 in chromatin remodeling during spermiogenesis

Author

Huanhuan Tan, Weixu Wang, Congjin Zhou, Yanfeng Wang, Shu Zhang, Pinglan Yang, Rui Guo, Wei Chen, Jinwen Zhang, Lan Ye, Yiqiang Cui, Ting Ni, and Ke Zheng

Subjects

Science

Abstract

Abstract Mammalian spermatogenesis shows prominent chromatin and transcriptomic switches in germ cells, but it is unclear how such dynamics are controlled. Here we identify RNA helicase DDX43 as an essential regulator of the chromatin remodeling process during spermiogenesis. Testis-specific Ddx43 knockout mice show male infertility with defective histone-to-protamine replacement and post-meiotic chromatin condensation defects. The loss of its ATP hydrolysis activity by a missense mutation replicates the infertility phenotype in global Ddx43 knockout mice. Single-cell RNA sequencing analyses of germ cells depleted of Ddx43 or expressing the Ddx43 ATPase-dead mutant reveals that DDX43 regulates dynamic RNA regulatory processes that underlie spermatid chromatin remodeling and differentiation. Transcriptomic profiling focusing on early-stage spermatids combined with enhanced crosslinking immunoprecipitation and sequencing further identifies Elfn2 as DDX43-targeted hub gene. These findings illustrate an essential role for DDX43 in spermiogenesis and highlight the single-cell-based strategy to dissect cell-state-specific regulation of male germline development.

Published

2023

3. A novel protein encoded by circRsrc1 regulates mitochondrial ribosome assembly and translation during spermatogenesis

Author

Shu Zhang, Chang Wang, Yue Wang, Hao Zhang, Chen Xu, Yiwei Cheng, Yan Yuan, Jiahao Sha, Xuejiang Guo, and Yiqiang Cui

Subjects

circRsrc1, Translation, Mitochondrial ribosome, C1qbp, Spermatogenesis, Biology (General), QH301-705.5

Abstract

Abstract Background Circular RNAs (circRNAs) are a large class of mammalian RNAs. Several protein products translated by circRNAs have been reported to be involved in the development of various tissues and systems; however, their physiological functions in male reproduction have yet not been explored. Results Here, we report an endogenous circRNA (circRsrc1) that encodes a novel 161-amino-acid protein which we named Rsrc1-161aa through circRNA sequencing coupled with mass spectrometry analysis on mouse testicular tissues. Deletion of Rsrc1-161aa in mice impaired male fertility with a significant decrease in sperm count and motility due to dysfunctions of mitochondrial energy metabolism. A series of in vitro rescue experiments revealed that circRsrc1 regulates mitochondrial functions via its encoded protein Rsrc1-161aa. Mechanistically, Rsrc1-161aa directly interacts with mitochondrial protein C1qbp and enhances its binding activity to mitochondrial mRNAs, thereby regulating the assembly of mitochondrial ribosomes and affecting the translation of oxidative phosphorylation (OXPHOS) proteins and mitochondrial energy metabolism. Conclusions Our studies reveal that Rsrc1-161aa protein encoded by circRsrc1 regulates mitochondrial ribosome assembly and translation during spermatogenesis, thereby affecting male fertility.

Published

2023

4. Regulation of Miwi-mediated mRNA stabilization by Ck137956/Tssa is essential for male fertility

Author

Yu Chen, Xiangzheng Zhang, Jiayin Jiang, Mengjiao Luo, Haixia Tu, Chen Xu, Huanhuan Tan, Xin Zhou, Hong Chen, Xudong Han, Qiuling Yue, Yueshuai Guo, Ke Zheng, Yaling Qi, Chenghao Situ, Yiqiang Cui, and Xuejiang Guo

Subjects

Ck137956/Tssa, Miwi, mRNA stability, Spermiogenesis, Male infertility, Biology (General), QH301-705.5

Abstract

Abstract Background Sperm is formed through spermiogenesis, a highly complex process involving chromatin condensation that results in cessation of transcription. mRNAs required for spermiogenesis are transcribed at earlier stages and translated in a delayed fashion during spermatid formation. However, it remains unknown that how these repressed mRNAs are stabilized. Results Here we report a Miwi-interacting testis-specific and spermiogenic arrest protein, Ck137956, which we rename Tssa. Deletion of Tssa led to male sterility and absence of sperm formation. The spermiogenesis arrested at the round spermatid stage and numerous spermiogenic mRNAs were down-regulated in Tssa −/− mice. Deletion of Tssa disrupted the localization of Miwi to chromatoid body, a specialized assembly of cytoplasmic messenger ribonucleoproteins (mRNPs) foci present in germ cells. We found that Tssa interacted with Miwi in repressed mRNPs and stabilized Miwi-interacting spermiogenesis-essential mRNAs. Conclusions Our findings indicate that Tssa is indispensable in male fertility and has critical roles in post-transcriptional regulations by interacting with Miwi during spermiogenesis.

Published

2023

5. A prime editor efficiently repaired human induced pluripotent stem cells with AR gene mutation (c.2710G > A; p. V904M)

Author

Ruiqi Sun, Yiqiang Cui, Zhaode Liu, Jiayin Guo, Xin Zhang, Pinmou Zhu, Jiahao Sha, Xiaoyu Yang, and Yan Yuan

Subjects

Induced pluripotent stem cell, Gene editing, Androgen insensitivity syndrome, Prime editors, CRISPR-Cas9, Biology (General), QH301-705.5

Abstract

Prime Editor (PE) is a precise genome manipulation technology based on the CRISPR-Cas9 system, while its application in human induced pluripotent stem cells (iPSCs) remains limited. Here, we established a repaired hiPS cell line (SKLRMi001-A-1) from hiPSCs with androgen receptor (AR) mutation (c.2710G > A; p.V904M). The repaired iPSC line expressed pluripotency markers, retained normal karyotype, showed the capability of differentiating into three germ layers and was absence of mycoplasma infection. The repaired iPSC line will help to elucidate the mechanism of androgen insensitivity syndrome (AIS) and benefit treatment for AIS in the future.

Published

2023

6. SOX-5 activates a novel RORγt enhancer to facilitate experimental autoimmune encephalomyelitis by promoting Th17 cell differentiation

Author

Yi Tian, Chao Han, Zhiyuan Wei, Hui Dong, Xiaohe Shen, Yiqiang Cui, Xiaolan Fu, Zhiqiang Tian, Shufeng Wang, Jian Zhou, Di Yang, Yi Sun, Jizhao Yuan, Bing Ni, and Yuzhang Wu

Subjects

Science

Abstract

T helper 17 (Th17) cells are important mediators of inflammatory diseases and fungal infection protection, and are critically regulated by the transcription factor (TF), RORγt. Here the authors identify a new enhancer for RORγt, RORCE2, which synergizes with another TF, Sox5, for binding with RORγt promoter and thereby modulation of RORγt expression.

Published

2021

7. T-complex protein 1 subunit zeta-2 (CCT6B) deficiency induces murine teratospermia

Author

Peiyin Yang, Wenjing Tang, Huiling Li, Rong Hua, Yan Yuan, Yue Zhang, Yunfei Zhu, Yiqiang Cui, and Jiahao Sha

Subjects

CCT6B, Spermatogenesis, Gene knockout, Protein folding, Medicine, Biology (General), QH301-705.5

Abstract

Background The CCT complex is an important mediator of microtubule assembly and intracellular protein folding. Owing to its high expression in spermatids, CCT knockdown can disrupt spermatogenesis. In the present report, we therefore evaluated the in vivo functionality of the testis-specific CCT complex component CCT6B using a murine knockout model system. Methods A CRISPR/Cas9 approach was used to generate Cct6b−/− mice, after which candidate gene expression in these animals was evaluated via qPCR and Western blotting. Testicular and epididymal phenotypes were assessed through histological and immunofluorescent staining assays, while a computer-assisted sperm analyzer was employed to assess semen quality. Results Cct6b−/− mice were successfully generated, and exhibited no differences in development, fertility, appearance, testis weight, or sperm counts relative to control littermates. In addition, no differences in spermatogenesis were detected when comparingCct6b+/+ and Cct6b−/− testes. However, when progressive motility was analyzed, the ratio of normal sperm was significantly decreased in Cct6b−/− male mice, with nuclear base bending being the primary detected abnormality. In addition, slight decreases in Cct4 and Cct7 expression were detected. Conclusion These data indicated that CCT6B is an important regulator of murine spermatogenesis, with the loss of this protein resulting in CCT complex dysfunction, providing a foundation for further studies.

Published

2021

8. CircAST: Full-length Assembly and Quantification of Alternatively Spliced Isoforms in Circular RNAs

Author

Jing Wu, Yan Li, Cheng Wang, Yiqiang Cui, Tianyi Xu, Chang Wang, Xiao Wang, Jiahao Sha, Bin Jiang, Kai Wang, Zhibin Hu, Xuejiang Guo, and Xiaofeng Song

Subjects

Biology (General), QH301-705.5, Computer applications to medicine. Medical informatics, R858-859.7

Abstract

Circular RNAs (circRNAs), covalently closed continuous RNA loops, are generated from cognate linear RNAs through back splicing events, and alternative splicing events may generate different circRNA isoforms at the same locus. However, the challenges of reconstruction and quantification of alternatively spliced full-length circRNAs remain unresolved. On the basis of the internal structural characteristics of circRNAs, we developed CircAST, a tool to assemble alternatively spliced circRNA transcripts and estimate their expression by using multiple splice graphs. Simulation studies showed that CircAST correctly assembled the full sequences of circRNAs with a sensitivity of 85.63%–94.32% and a precision of 81.96%–87.55%. By assigning reads to specific isoforms, CircAST quantified the expression of circRNA isoforms with correlation coefficients of 0.85–0.99 between theoretical and estimated values. We evaluated CircAST on an in-house mouse testis RNA-seq dataset with RNase R treatment for enriching circRNAs and identified 380 circRNAs with full-length sequences different from those of their corresponding cognate linear RNAs. RT-PCR and Sanger sequencing analyses validated 32 out of 37 randomly selected isoforms, thus further indicating the good performance of CircAST, especially for isoforms with low abundance. We also applied CircAST to published experimental data and observed substantial diversity in circular transcripts across samples, thus suggesting that circRNA expression is highly regulated. CircAST can be accessed freely at https://github.com/xiaofengsong/CircAST. Keywords: Circular RNA, Full-length reconstruction, Isoform quantification, Multiple splice graph model, Transcriptome

Published

2019

9. TULP2, a New RNA-Binding Protein, Is Required for Mouse Spermatid Differentiation and Male Fertility

Author

Meimei Zheng, Xu Chen, Yiqiang Cui, Wen Li, Haiqian Dai, Qiuling Yue, Hao Zhang, Ying Zheng, Xuejiang Guo, and Hui Zhu

Subjects

spermatid differentiation, RNA binding protein, male infertility, oligo-astheno-teratozoospermia, TULP2, Biology (General), QH301-705.5

Abstract

Spermatogenesis requires a large number of proteins to be properly expressed at certain stages, during which post-transcriptional regulation plays an important role. RNA-binding proteins (RBPs) are key players in post-transcriptional regulation, but only a few RBPs have been recognized and preliminary explored their function in spermatogenesis at present. Here we identified a new RBP tubby-like protein 2 (TULP2) and found three potential deleterious missense mutations of Tulp2 gene in dyszoospermia patients. Therefore, we explored the function and mechanism of TULP2 in male reproduction. TULP2 was specifically expressed in the testis and localized to spermatids. Studies on Tulp2 knockout mice demonstrated that the loss of TULP2 led to male sterility; on the one hand, increases in elongated spermatid apoptosis and restricted spermatid release resulted in a decreased sperm count; on the other hand, the abnormal differentiation of spermatids induced defective sperm tail structures and reduced ATP contents, influencing sperm motility. Transcriptome sequencing of mouse testis revealed the potential target molecular network of TULP2, which played its role in spermatogenesis by regulating specific transcripts related to the cytoskeleton, apoptosis, RNA metabolism and biosynthesis, and energy metabolism. We also explored the potential regulator of TULP2 protein function by using immunoprecipitation and mass spectrometry analysis, indicating that TUPL2 might be recognized by CCT8 and correctly folded by the CCT complex to play a role in spermiogenesis. Our results demonstrated the important role of TULP2 in spermatid differentiation and male fertility, which could provide an effective target for the clinical diagnosis and treatment of patients with oligo-astheno-teratozoospermia, and enrich the biological theory of the role of RBPs in male reproduction.

Published

2021

10. The heat shock protein family gene Hspa1l in male mice is dispensable for fertility

Author

Xin Wang, Wenxiu Xie, Yejin Yao, Yunfei Zhu, Jianli Zhou, Yiqiang Cui, Xuejiang Guo, Yan Yuan, Zuomin Zhou, and Mingxi Liu

Subjects

HSPA1L, Spermatogenesis, Male infertility, Gene knockout, Medicine, Biology (General), QH301-705.5

Abstract

Background Heat shock protein family A member 1 like (Hspa1l) is a member of the 70kD heat shock protein (Hsp70) family. HSPA1L is an ancient, evolutionarily conserved gene with a highly conserved domain structure. The gene is highly abundant and constitutively expressed in the mice testes. However, the role of Hspa1l in the testes has still not been elucidated. Methods Hspa1l-mutant mice were generated using the CRISPR/Cas9 system. Histological and immunofluorescence staining were used to analyze the phenotypes of testis and epididymis. Apoptotic cells were detected through TUNEL assays. Fertility and sperm motilities were also tested. Quantitative RT-PCR was used for analyzing of candidate genes expression. Heat treatment was used to induce heat stress of the testis. Results We successfully generated Hspa1l knockout mice. Hspa1l-/- mice exhibited normal development and fertility. Further, Hspa1l-/- mice shown no significant difference in spermatogenesis, the number of apoptotic cells in testes epididymal histology, sperm count and sperm motility from Hspa1l+/+ mice. Moreover, heat stress does not exacerbate the cell apoptosis in Hspa1l-/- testes. These results revealed that HSPA1L is not essential for physiological spermatogenesis, nor is it involved in heat-induced stress responses, which provides a basis for further studies.

Published

2020

11. Derivation of new pluripotent stem cells from human extended pluripotent stem cells with formative features and trophectoderm potential

Author

Pinmou Zhu, Bohang Zhang, Ruiqi Sun, Jiachen Wang, Zhaode Liu, Xiaorui Liu, Min Yan, Yiqiang Cui, Jiahao Sha, and Yan Yuan

Subjects

Cell Biology, General Medicine

Published

2023

12. ZDHHC19 localizes to the cell membrane of spermatids and is involved in spermatogenesis

Author

Yangyang, Wu, Xin, Zhang, Xi, Zhang, Siyu, Liu, Jintao, Zhang, Shuya, Sun, Shuqin, Zhao, Zerui, Wang, Yiqiang, Cui, Xiaoyan, Huang, and Mingxi, Liu

Subjects

Male, Mice, Knockout, endocrine system, urogenital system, Cell Membrane, Cell Biology, General Medicine, Spermatids, Spermatozoa, Mice, Reproductive Medicine, Testis, Sperm Motility, Animals, Spermatogenesis, Acyltransferases, Infertility, Male

Abstract

Sperm is the ultimate executor of male reproductive function. Normal morphology, quantity, and motility of sperm ensure the normal reproductive process. Palmitoylation is a posttranslational modification mediated by palmitoyltransferases whereby palmitoyl is added to proteins. Seven palmitoyltransferases have been identified in Saccharomyces cerevisiae and 23 in humans (including ZDHHC1–9 and ZDHHC11–24), with corresponding homologs in mice. We identified two testis-specific palmitoyltransferases ZDHHC11 and ZDHHC19 in mice. The Zdhhc11 and Zdhhc19-knockout mouse models were constructed, and it was found that the Zdhhc11 knockout males were fertile, while Zdhhc19 knockout males were sterile. ZDHHC19 is located in the cell membrane of step 4–9 spermatids in the mouse testis, and phenotypic analysis showed that the testicular weight ratio in the Zdhhc19−/− mice decreased along with the number and motility of the sperm decreased, while sperm abnormalities increased, mainly due to the “folded” abnormal sperm caused by sperm membrane fusion, suggesting the involvement of ZDHHC19 in maintaining membrane stability in the male reproductive system. In addition, Zdhhc19−/− mice showed abnormal sperm morphologies and apoptosis during spermatogenesis, suggesting that spermatogenesis in the Zdhhc19−/− mice was abnormal. These results indicate that ZDHHC19 promotes membrane stability in male germ cells.

Published

2021

13. STK33 Phosphorylates Fibrous Sheath Protein AKAP3/4 to Regulate Sperm Flagella Assembly in Spermiogenesis

Author

Weiling Yu, Yang Li, Hong Chen, Yiqiang Cui, Chenghao Situ, Liping Yao, Xiangzheng Zhang, Shuai Lu, Li Liu, Laihua Li, Jie Ren, Yueshuai Guo, Zian Huo, Yu Chen, Haojie Li, Tao Jiang, Yayun Gu, Cheng Wang, Tianyu Zhu, Yan Li, Zhibin Hu, and Xuejiang Guo

Subjects

Molecular Biology, Biochemistry, Analytical Chemistry

Published

2023

14. Global phosphoproteomic analysis identified key kinases regulating male meiosis in mouse

Author

Haojie Li, Hong Chen, Xiangzheng Zhang, Yaling Qi, Bing Wang, Yiqiang Cui, Jie Ren, Yichen Zhao, Yu Chen, Tianyu Zhu, Yue Wang, Liping Yao, Yueshuai Guo, Hui Zhu, Yan Li, Chenghao Situ, and Xuejiang Guo

Subjects

Male, Mammals, Pharmacology, Cell Biology, Histones, Meiosis, Mice, Cellular and Molecular Neuroscience, Semen, Spermatocytes, Animals, Molecular Medicine, Phosphorylation, Molecular Biology, Metaphase

Abstract

Meiosis, a highly conserved process in organisms from fungi to mammals, is subjected to protein phosphorylation regulation. Due to the low abundance of phosphorylation, there is a lack of systemic characterization of phosphorylation regulation of meiosis in mammals. Using the phosphoproteomic approach, we profiled large-scale phosphoproteome of purified primary spermatocytes undergoing meiosis I, and identified 14,660 phosphorylation sites in 4419 phosphoproteins. Kinase-substrate phosphorylation network analysis followed by in vitro meiosis study showed that CDK9 was essential for meiosis progression to metaphase I and had enriched substrate phosphorylation sites in proteins involved in meiotic cell cycle. In addition, histones and epigenetic factors were found to be widely phosphorylated. Among those, HASPIN was found to be essential for male fertility. Haspin knockout led to misalignment of chromosomes, apoptosis of metaphase spermatocytes and a decreased number of sperm by deregulation of H3T3ph, chromosomal passenger complex (CPC) and spindle assembly checkpoint (SAC). The complicated protein phosphorylation and its important regulatory functions in meiosis indicated that in-depth studies of phosphorylation-mediated signaling could help us elucidate the mechanisms of meiosis.

Published

2022

15. Single-Cell RNA-seq Uncovers Dynamic Processes Orchestrated by RNA-Binding Protein DDX43 in Chromatin Remodeling during Spermiogenesis

Author

Ke Zheng, Huanhuan Tan, Weixu Wang, Chongjin Zhou, Yanfeng Wang, Shu Zhang, Pinglan Yang, Rui Guo, Wei Chen, Lan Ye, Yiqiang Cui, and Ting Ni

Abstract

Advances in single-cell RNA sequencing (scRNA-seq) have allowed for elucidating biological mechanisms at cell state level. Mammalian spermatogenic process showcases dynamic switches of gene expression pattern with delicate morphological and functional alterations of germ cells, but it is unclear how such dynamics is genetically controlled. Here we demonstrate that mouse testis-enriched RNA helicase DDX43, as well as its ATP hydrolysis site, is required for spermiogenesis. Genetic mutation of Ddx43 renders spermatids heterogeneously defective in multiple steps of chromatin remodeling, resulting in incomplete substitution of transition protein by protamine and less condensed sperm nucleus. Through scRNA-seq analyses of testicular cells derived from adult wild-type and Ddx43 mutant testes in mice, we reveal that the DDX43 deficiency-elicited perturbation in the dynamic RNA regulatory processes underlies the differentiation deficiency of spermatids. Further, focused analyses on early-stage spermatids combined with enhanced CLIP sequencing (eCLIP-seq) identify Elfn2 as DDX43-targeted hub gene, whose in vivo knockdown shows similar phenotypic defects as Ddx43 mutant. Our study illustrates an essential role for DDX43 in post-meiotic chromatin remodeling and highlights the single cell-based strategy for a refined dissection of stage-specific regulation of germline differentiation.

Published

2022

16. Human X chromosome exome sequencing identifies BCORL1 as contributor to spermatogenesis

Author

Zhibin Hu, Xuejiang Guo, Yunfei Zhu, Hongbing Shen, Zuomin Zhou, Yankai Xia, Mingxi Liu, Antoine M. Snijders, Xin Wu, Jian-Hua Mao, Chuncheng Lu, Xiang Wei, Yufeng Qin, Xinru Wang, Jintao Zhang, Bo Hang, Min Wang, Qiaoqiao Xu, Ran Zhou, Yiqiang Cui, Yan Zhang, and Xin Zhang

Subjects

0301 basic medicine, Genetics, Infertility, Azoospermia, education.field_of_study, Candidate gene, 030219 obstetrics & reproductive medicine, Population, Biology, medicine.disease, Male infertility, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Knockout mouse, medicine, education, Genetics (clinical), Exome sequencing, X chromosome

Abstract

BackgroundInfertility affects approximately 15% of couples worldwide with male infertility being responsible for approximately 50% of cases. Although accumulating evidence demonstrates the critical role of the X chromosome in spermatogenesis during the last few decades, the expression patterns and potential impact of the X chromosome, together with X linked genes, on male infertility are less well understood.MethodsWe performed X chromosome exome sequencing followed by a two-stage independent population validation in 1333 non-obstructive azoospermia cases and 1141 healthy controls to identify variant classes with high likelihood of pathogenicity. To explore the functions of these candidate genes in spermatogenesis, we first knocked down these candidate genes individually in mouse spermatogonial stem cells (SSCs) using short interfering RNA oligonucleotides and then generated candidate genes knockout mice by CRISPR-Cas9 system.ResultsFour low-frequency variants were identified in four genes (BCORL1, MAP7D3, ARMCX4 and H2BFWT) associated with male infertility. Functional studies of the mouse SSCs revealed that knocking down Bcorl1 or Mtap7d3 could inhibit SSCs self-renewal and knocking down Armcx4 could repress SSCs differentiation in vitro. Using CRISPR-Cas9 system, Bcorl1 and Mtap7d3 knockout mice were generated. Excitingly, Bcorl1 knockout mice were infertile with impaired spermatogenesis. Moreover, Bcorl1 knockout mice exhibited impaired sperm motility and sperm cells displayed abnormal mitochondrial structure.ConclusionOur data indicate that the X-linked genes are associated with male infertility and involved in regulating SSCs, which provides a new insight into the role of X-linked genes in spermatogenesis.

Published

2020

17. Affordance Characteristics Identification Method on Maintenance Requirements Satisfactory Prediction

Author

null Sarina, Yi Wu, Jing Zhang, Yiqiang Cui, and Congxuan Wang

Published

2022

18. A male germ-cell-specific ribosome controls male fertility

Author

Huiling Li, Yangao Huo, Xi He, Liping Yao, Hao Zhang, Yiqiang Cui, Huijuan Xiao, Wenxiu Xie, Dejiu Zhang, Yue Wang, Shu Zhang, Haixia Tu, Yiwei Cheng, Yueshuai Guo, Xintao Cao, Yunfei Zhu, Tao Jiang, Xuejiang Guo, Yan Qin, and Jiahao Sha

Subjects

Male, Mammals, Mice, Protein Folding, Multidisciplinary, Germ Cells, Semen, Protein Biosynthesis, Cryoelectron Microscopy, Animals, Peptides, Ribosomes

Abstract

Ribosomes are highly sophisticated translation machines that have been demonstrated to be heterogeneous in the regulation of protein synthesis

Published

2021

19. Single-cell RNA-Seq reveals a highly coordinated transcriptional program in mouse germ cells during primordial follicle formation

Author

Qiuzhen Chen, Chi Zhang, Zhibin Hu, Yuanlin He, Juncheng Dai, Xiaoxu Peng, Jiahao Sha, Jiazhao Li, Wenjie Shu, Jing Li, Bin Shen, Mingxi Liu, Yue Xiao, Xidong Wen, and Yiqiang Cui

Subjects

0301 basic medicine, Aging, Ovary, Biology, 03 medical and health sciences, Follicle, Mice, 0302 clinical medicine, Transcription (biology), medicine, Animals, RNA-Seq, single‐cell RNA‐seq, oocyte, Gene, Transcription factor, Original Paper, cyst breakdown, Cell Biology, Original Articles, Oocyte, Germ Cell Ribonucleoprotein Granules, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Germ Cells, Oocytes, ovary, Folliculogenesis, Single-Cell Analysis, primordial follicle, 030217 neurology & neurosurgery, Germ cell

Abstract

The assembly of primordial follicles in mammals represents one of the most critical processes in ovarian biology. It directly affects the number of oocytes available to a female throughout her reproductive life. Premature depletion of primordial follicles contributes to the ovarian pathology primary ovarian insufficiency (POI). To delineate the developmental trajectory and regulatory mechanisms of oocytes during the process, we performed RNA‐seq on single germ cells from newborn (P0.5) ovaries. Three cell clusters were classified which corresponded to three cell states (germ cell cyst, cyst breakdown, and follicle) in the newborn ovary. By Monocle analysis, a uniform trajectory of oocyte development was built with a series of genes showed dynamic changes along the pseudo‐timeline. Gene Ontology term enrichment revealed a significant decrease in meiosis‐related genes and a dramatic increase in oocyte‐specific genes which marked the transition from a germ cell to a functional oocyte. We then established a network of regulons by using single‐cell regulatory network inference and clustering (SCENIC) algorithm and identified possible candidate transcription factors that may maintain transcription programs during follicle formation. Following functional studies further revealed the differential regulation of the identified regulon Id2 and its family member Id1, on the establishment of primordial follicle pool by using siRNA knockdown and genetic modified mouse models. In summary, our study systematically reconstructed molecular cascades in oocytes and identified a series of genes and molecular pathways in follicle formation and development., The assembly of primordial follicle determines the number of oocytes available to a female throughout her reproductive life. Premature depletion of primordial follicles contributes to the ovarian pathology primary ovarian insufficiency. We performed RNA‐seq on single germ cells from newborn mouse ovary and the data revealed dynamic gene expressions along with the transition of germ cells to a functional oocyte. Our study highlights the importance of transcriptional regulations on the process.

Published

2021

20. T-complex protein 1 subunit zeta-2 (CCT6B) deficiency induces murine teratospermia

Author

Wenjing Tang, Rong Hua, Peiyin Yang, Huiling Li, Yue Zhang, Yunfei Zhu, Yiqiang Cui, Jiahao Sha, and Yan Yuan

Subjects

Teratospermia, Histology, Protein subunit, Motility, Biochemistry, General Biochemistry, Genetics and Molecular Biology, Gene knockout, 03 medical and health sciences, In vivo, medicine, Protein folding, Spermatogenesis, Molecular Biology, 030304 developmental biology, 0303 health sciences, Gene knockdown, Chemistry, General Neuroscience, 030302 biochemistry & molecular biology, CCT6B, General Medicine, Molecular biology, Sperm, Medicine, medicine.symptom, General Agricultural and Biological Sciences, Developmental Biology

Abstract

Background The CCT complex is an important mediator of microtubule assembly and intracellular protein folding. Owing to its high expression in spermatids, CCT knockdown can disrupt spermatogenesis. In the present report, we therefore evaluated the in vivo functionality of the testis-specific CCT complex component CCT6B using a murine knockout model system. Methods A CRISPR/Cas9 approach was used to generate Cct6b−/− mice, after which candidate gene expression in these animals was evaluated via qPCR and Western blotting. Testicular and epididymal phenotypes were assessed through histological and immunofluorescent staining assays, while a computer-assisted sperm analyzer was employed to assess semen quality. Results Cct6b−/− mice were successfully generated, and exhibited no differences in development, fertility, appearance, testis weight, or sperm counts relative to control littermates. In addition, no differences in spermatogenesis were detected when comparingCct6b+/+ and Cct6b−/− testes. However, when progressive motility was analyzed, the ratio of normal sperm was significantly decreased in Cct6b−/− male mice, with nuclear base bending being the primary detected abnormality. In addition, slight decreases in Cct4 and Cct7 expression were detected. Conclusion These data indicated that CCT6B is an important regulator of murine spermatogenesis, with the loss of this protein resulting in CCT complex dysfunction, providing a foundation for further studies.

Published

2021

21. Deficiency of TPPP2, a factor linked to oligoasthenozoospermia, causes subfertility in male mice

Author

Meimei Zheng, Yueshuai Guo, Xiaoyu Yang, Feng Zhu, Hui Zhu, Xuejiang Guo, Jingjing Zhang, Yiqiang Cui, Peipei Yan, and Yiwei Cheng

Subjects

Male, 0301 basic medicine, Litter Size, Gene Expression, Motility, Nerve Tissue Proteins, Biology, Mitochondrion, Male infertility, Andrology, Mice, 03 medical and health sciences, Adenosine Triphosphate, 0302 clinical medicine, Eukaryotic translation, Testis, energy metabolism, oligoasthenozoospermia, medicine, Animals, Humans, Protein Isoforms, Epididymis, Mice, Knockout, Sperm Count, Acrosome Reaction, Elongation Factor 1-Beta, sperm function, Oligospermia, Original Articles, Cell Biology, Peptide Elongation Factors, male subfertility, medicine.disease, Spermatozoa, Sperm, Mitochondria, 030104 developmental biology, medicine.anatomical_structure, Apoptosis, 030220 oncology & carcinogenesis, Sperm Motility, Molecular Medicine, Female, Original Article, Sperm Capacitation, TPPP2

Abstract

Oligoasthenozoospermia is a major cause of male infertility; however, its etiology and pathogenesis are unclear and may be associated with specific gene abnormalities. This study focused on Tppp2 (tubulin polymerization promoting protein family member 2), whose encoded protein localizes in elongating spermatids at stages IV‐VIII of the seminiferous epithelial cycle in testis and in mature sperm in the epididymis. In human and mouse sperm, in vitro inhibition of TPPP2 caused significantly decreased motility and ATP content. Studies on Tppp2 knockout (KO) mice demonstrated that deletion of TPPP2 resulted in male subfertility with a significantly decreased sperm count and motility. In Tppp2 −/− mice, increased irregular mitochondria lacking lamellar cristae, abnormal expression of electron transfer chain molecules, lower ATP levels, decreased mitochondrial membrane potential and increased apoptotic index were observed in sperm, which could be the potential causes for its oligoasthenozoospermia phenotype. Moreover, we identified a potential TPPP2‐interactive protein, eEf1b (eukaryotic translation elongation factor 1 beta), which plays an important role in protein translation extension. Thus, TPPP2 is probably a potential pathogenic factor in oligoasthenozoospermia. Deficiency of TPPP2 might affect the translation of specific proteins, altering the structure and function of sperm mitochondria, and resulting in decreased sperm count, motility and fertility.

Published

2019

22. The testis-specifically expressed gene

Author

Xi, He, Wenxiu, Xie, Huiling, Li, Yiqiang, Cui, Ya, Wang, Xuejiang, Guo, and Jiahao, Sha

Subjects

E3 ubiquitin ligase, Trim69, Original Article, spermatogenesis, male fertility, gene knockout

Abstract

Protein ubiquitination is essential for diverse cellular functions including spermatogenesis. The tripartite motif (TRIM) family proteins, most of which have E3 ubiquitin ligase activity, are highly conserved in mammals. They are involved in important cellular processes such as embryonic development, immunity, and fertility. Our previous studies indicated that Trim69, a testis-specific expressed TRIM family gene, potentially participates in the spermatogenesis by mediating testicular cells apoptosis. In this study, we investigated the biological functions of Trim69 in male mice by established Trim69 knockout mice with CRISPR/Cas9 genomic editing technology. Here, we reported that the male Trim69 knockout mice had normal fertility. The adult knockout mice have shown that the appearance of testes, testis/body weight ratios, testicular histomorphology, and the number and quality of sperm were consistent with wild-type mice. These results indicated that the E3 ubiquitin ligase protein Trim69 was not essential for male mouse fertility, and it might be compensated by other TRIM family members such as Trim58 in Trim69-deficiency testis. This study would help to elucidate the functions of tripartite motif protein family and the regulation of spermatogenesis.

Published

2020

23. TULP2, a New RNA-Binding Protein, Is Required for Mouse Spermatid Differentiation and Male Fertility

Author

Meimei Zheng, Xu Chen, Yiqiang Cui, Wen Li, Haiqian Dai, Qiuling Yue, Hao Zhang, Ying Zheng, Xuejiang Guo, and Hui Zhu

Subjects

oligo-astheno-teratozoospermia, Spermatid, Spermiogenesis, Spermatid differentiation, RNA-binding protein, Cell Biology, Biology, Sperm, RNA binding protein, male infertility, Cell biology, Cell and Developmental Biology, TULP2, medicine.anatomical_structure, lcsh:Biology (General), Knockout mouse, spermatid differentiation, medicine, Spermatogenesis, lcsh:QH301-705.5, Sperm motility, Developmental Biology, Original Research

Abstract

Spermatogenesis requires a large number of proteins to be properly expressed at certain stages, during which post-transcriptional regulation plays an important role. RNA-binding proteins (RBPs) are key players in post-transcriptional regulation, but only a few RBPs have been recognized and preliminary explored their function in spermatogenesis at present. Here we identified a new RBP tubby-like protein 2 (TULP2) and found three potential deleterious missense mutations of Tulp2 gene in dyszoospermia patients. Therefore, we explored the function and mechanism of TULP2 in male reproduction. TULP2 was specifically expressed in the testis and localized to spermatids. Studies on Tulp2 knockout mice demonstrated that the loss of TULP2 led to male sterility; on the one hand, increases in elongated spermatid apoptosis and restricted spermatid release resulted in a decreased sperm count; on the other hand, the abnormal differentiation of spermatids induced defective sperm tail structures and reduced ATP contents, influencing sperm motility. Transcriptome sequencing of mouse testis revealed the potential target molecular network of TULP2, which played its role in spermatogenesis by regulating specific transcripts related to the cytoskeleton, apoptosis, RNA metabolism and biosynthesis, and energy metabolism. We also explored the potential regulator of TULP2 protein function by using immunoprecipitation and mass spectrometry analysis, indicating that TUPL2 might be recognized by CCT8 and correctly folded by the CCT complex to play a role in spermiogenesis. Our results demonstrated the important role of TULP2 in spermatid differentiation and male fertility, which could provide an effective target for the clinical diagnosis and treatment of patients with oligo-astheno-teratozoospermia, and enrich the biological theory of the role of RBPs in male reproduction.

Published

2020

24. PRSS55 plays an important role in the structural differentiation and energy metabolism of sperm and is required for male fertility in mice

Author

Xiaofei Liu, Feng Zhu, Yiqiang Cui, Meimei Zheng, Wen Li, Hui Zhu, Xinli Zhou, Xuejiang Guo, and Xu Chen

Subjects

0301 basic medicine, Male, Proteases, endocrine system, Genotype, Spermiogenesis, Fluorescent Antibody Technique, Gene Expression, Apoptosis, Teratozoospermia, Biology, male infertility, PRSS55, Male infertility, 03 medical and health sciences, Mice, 0302 clinical medicine, Adenosine Triphosphate, Myosin, Testis, energy metabolism, medicine, Animals, Humans, sperm motility, Spermatogenesis, Sperm motility, reproductive and urinary physiology, Mice, Knockout, urogenital system, Cell Biology, Original Articles, medicine.disease, Sperm, Immunohistochemistry, Spermatozoa, spermiogenesis, Cell biology, 030104 developmental biology, Fertility, Phenotype, 030220 oncology & carcinogenesis, Molecular Medicine, Original Article, Serine Proteases, Biomarkers

Abstract

Orderly and stage‐specifically expressed proteins are essential for spermatogenesis, and proteases play a key role in protein activation and function. The present study aimed to investigate serine protease 55 (PRSS55), which was reported to play a role in sperm‐uterotubal junction (UTJ) migration and sperm‐zona pellucida (ZP) binding. We found that PRSS55 was specifically expressed in testicular spermatids and epididymal spermatozoa. By constructing knockout mice targeting all transcripts of Prss55, we demonstrated that deletion of Prss55 resulted in a serious decline of male fertility, with significantly increased sperm malformation and decreased sperm motility. In Prss55 −/− mice, increased structural abnormality, including deficient “9 + 2” microtubules, damaged peripheral dense fibre, and defective mitochondrial cristae, were found in sperm. In addition, sperm showed decreased expression of electron transfer chain molecules and lower ATP contents. These could be the potential causes of the astheno/teratozoospermia phenotype of the Prss55 −/− mice, and provided new evidence for the previously reported impaired sperm‐UTJ migration. Moreover, preliminary studies allowed us to speculate that PRSS55 might function by activating type II muscle myosin in the testis, which is involved in many processes requiring motivation and cytoskeleton translocation. Thus, PRSS55 is essential for the structural differentiation and energy metabolism of sperm, and might be a potential pathogenic factor in astheno/teratozoospermia. Our results provide an additional explanation for the male sterility of Prss55 −/− mice, and further reveal the role of PRSS55.

Published

2020

25. The heat shock protein family gene Hspa1l in male mice is dispensable for fertility

Author

Yan Yuan, Mingxi Liu, Wenxiu Xie, Jianli Zhou, Yejin Yao, Zuomin Zhou, Yunfei Zhu, Xuejiang Guo, Xin Wang, and Yiqiang Cui

Subjects

lcsh:Medicine, Biology, General Biochemistry, Genetics and Molecular Biology, Gene knockout, 03 medical and health sciences, 0302 clinical medicine, Heat shock protein, medicine, HSPA1L, Spermatogenesis, Sperm motility, 030304 developmental biology, 0303 health sciences, Male infertility, 030219 obstetrics & reproductive medicine, General Neuroscience, lcsh:R, General Medicine, Epididymis, Sperm, Cell biology, Hsp70, medicine.anatomical_structure, General Agricultural and Biological Sciences

Abstract

BackgroundHeat shock protein family A member 1 like (Hspa1l) is a member of the 70kD heat shock protein (Hsp70) family. HSPA1L is an ancient, evolutionarily conserved gene with a highly conserved domain structure. The gene is highly abundant and constitutively expressed in the mice testes. However, the role ofHspa1lin the testes has still not been elucidated.MethodsHspa1l-mutant mice were generated using the CRISPR/Cas9 system. Histological and immunofluorescence staining were used to analyze the phenotypes of testis and epididymis. Apoptotic cells were detected through TUNEL assays. Fertility and sperm motilities were also tested. Quantitative RT-PCR was used for analyzing of candidate genes expression. Heat treatment was used to induce heat stress of the testis.ResultsWe successfully generatedHspa1lknockout mice.Hspa1l-/-mice exhibited normal development and fertility. Further,Hspa1l-/-mice shown no significant difference in spermatogenesis, the number of apoptotic cells in testes epididymal histology, sperm count and sperm motility fromHspa1l+/+mice. Moreover, heat stress does not exacerbate the cell apoptosis inHspa1l-/-testes. These results revealed that HSPA1L is not essential for physiological spermatogenesis, nor is it involved in heat-induced stress responses, which provides a basis for further studies.

Published

2020

26. SOX-5 activates a novel RORγt enhancer to facilitate experimental autoimmune encephalomyelitis by promoting Th17 cell differentiation

Author

Yi Tian, Shen Xiaohe, Hui Dong, Bing Ni, Chao Han, Shufeng Wang, Zhiqiang Tian, Sun Yi, Zhiyuan Wei, Yuzhang Wu, Di Yang, Xiaolan Fu, Jizhao Yuan, Jian Zhou, and Yiqiang Cui

Subjects

0301 basic medicine, Epigenomics, STAT3 Transcription Factor, Encephalomyelitis, Autoimmune, Experimental, Cellular differentiation, Science, General Physics and Astronomy, Autoimmunity, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Transcriptional regulation, Animals, T-helper 17 cells, Enhancer, STAT3, Transcription factor, Regulation of gene expression, Mice, Knockout, Multidisciplinary, Experimental autoimmune encephalomyelitis, Cell Differentiation, General Chemistry, Nuclear Receptor Subfamily 1, Group F, Member 3, medicine.disease, Cell biology, Mice, Inbred C57BL, Gene regulation in immune cells, 030104 developmental biology, Gene Expression Regulation, 030220 oncology & carcinogenesis, STAT protein, biology.protein, Th17 Cells, Epigenetics, SOXD Transcription Factors, Signal Transduction

Abstract

T helper type 17 (Th17) cells have important functions in the pathogenesis of inflammatory and autoimmune diseases. Retinoid-related orphan receptor-γt (RORγt) is necessary for Th17 cell differentiation and functions. However, the transcriptional regulation of RORγt expression, especially at the enhancer level, is still poorly understood. Here we identify a novel enhancer of RORγt gene in Th17 cells, RORCE2. RORCE2 deficiency suppresses RORγt expression and Th17 differentiation, leading to reduced severity of experimental autoimmune encephalomyelitis. Mechanistically, RORCE2 is looped to RORγt promoter through SRY-box transcription factor 5 (SOX-5) in Th17 cells, and the loss of SOX-5 binding site in RORCE abolishes RORCE2 function and affects the binding of signal transducer and activator of transcription 3 (STAT3) to the RORγt locus. Taken together, our data highlight a molecular mechanism for the regulation of Th17 differentiation and functions, which may represent a new intervening clue for Th17-related diseases., T helper 17 (Th17) cells are important mediators of inflammatory diseases and fungal infection protection, and are critically regulated by the transcription factor (TF), RORγt. Here the authors identify a new enhancer for RORγt, RORCE2, which synergizes with another TF, Sox5, for binding with RORγt promoter and thereby modulation of RORγt expression.

Published

2020

27. The heat shock protein family gene

Author

Xin, Wang, Wenxiu, Xie, Yejin, Yao, Yunfei, Zhu, Jianli, Zhou, Yiqiang, Cui, Xuejiang, Guo, Yan, Yuan, Zuomin, Zhou, and Mingxi, Liu

Subjects

Male infertility, Andrology, HSPA1L, Spermatogenesis, Biochemistry, Gene knockout

Abstract

Background Heat shock protein family A member 1 like (Hspa1l) is a member of the 70kD heat shock protein (Hsp70) family. HSPA1L is an ancient, evolutionarily conserved gene with a highly conserved domain structure. The gene is highly abundant and constitutively expressed in the mice testes. However, the role of Hspa1l in the testes has still not been elucidated. Methods Hspa1l-mutant mice were generated using the CRISPR/Cas9 system. Histological and immunofluorescence staining were used to analyze the phenotypes of testis and epididymis. Apoptotic cells were detected through TUNEL assays. Fertility and sperm motilities were also tested. Quantitative RT-PCR was used for analyzing of candidate genes expression. Heat treatment was used to induce heat stress of the testis. Results We successfully generated Hspa1l knockout mice. Hspa1l-/- mice exhibited normal development and fertility. Further, Hspa1l-/- mice shown no significant difference in spermatogenesis, the number of apoptotic cells in testes epididymal histology, sperm count and sperm motility from Hspa1l+/+ mice. Moreover, heat stress does not exacerbate the cell apoptosis in Hspa1l-/- testes. These results revealed that HSPA1L is not essential for physiological spermatogenesis, nor is it involved in heat-induced stress responses, which provides a basis for further studies.

Published

2019

28. APOBEC3 induces mutations during repair of CRISPR–Cas9-generated DNA breaks

Author

Jia Wei, Jianying Wang, Lei Yan, Wei Li, Xingxu Huang, Bian Hu, Min Zhuang, Bei Yang, Liqun Lei, Jimin Gao, Hongquan Chen, Wei Xue, Jia Chen, Yiqiang Cui, Lijie Wang, Bin Shen, Jiahao Sha, Wanjing Shang, and Li Yang

Subjects

0301 basic medicine, DNA Repair, DNA repair, Oligonucleotides, Deamination, DNA, Single-Stranded, Cytidine, medicine.disease_cause, Cytosine Deaminase, 03 medical and health sciences, chemistry.chemical_compound, Cytidine deamination, INDEL Mutation, Structural Biology, Cytidine Deaminase, medicine, Humans, DNA Breaks, Double-Stranded, APOBEC Deaminases, RNA, Small Interfering, Molecular Biology, Mutation, Mutagenesis, Recombinational DNA Repair, food and beverages, Sequence Analysis, DNA, Cytidine deaminase, Cell biology, genomic DNA, HEK293 Cells, 030104 developmental biology, chemistry, CRISPR-Cas Systems, DNA, HeLa Cells

Abstract

The APOBEC-AID family of cytidine deaminase prefers single-stranded nucleic acids for cytidine-to-uridine deamination. Single-stranded nucleic acids are commonly involved in the DNA repair system for breaks generated by CRISPR-Cas9. Here, we show in human cells that APOBEC3 can trigger cytidine deamination of single-stranded oligodeoxynucleotides, which ultimately results in base substitution mutations in genomic DNA through homology-directed repair (HDR) of Cas9-generated double-strand breaks. In addition, the APOBEC3-catalyzed deamination in genomic single-stranded DNA formed during the repair of Cas9 nickase-generated single-strand breaks in human cells can be further processed to yield mutations mainly involving insertions or deletions (indels). Both APOBEC3-mediated deamination and DNA-repair proteins play important roles in the generation of these indels. Therefore, optimizing conditions for the repair of CRISPR-Cas9-generated DNA breaks, such as using double-stranded donors in HDR or temporarily suppressing endogenous APOBEC3s, can repress these unwanted mutations in genomic DNA.

Published

2017

29. FBXO47 regulates telomere-inner nuclear envelope integration by stabilizing TRF2 during meiosis

Author

Yiqiang Cui, Huafang Wei, Siyu Liu, Mingxi Liu, Rong Hua, Wei Li, Chao Liu, Xuejiang Guo, Yueshuai Guo, Yue Zhang, and Xin Zhang

Subjects

Male, Nuclear Envelope, Protein subunit, Regulator, Cell Cycle Proteins, Biology, Prophase, Mice, 03 medical and health sciences, Meiotic Prophase I, 0302 clinical medicine, Meiosis, Spermatocytes, Genetics, Homologous chromosome, Animals, Humans, Telomeric Repeat Binding Protein 2, Molecular Biology, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Protein Stability, F-Box Proteins, Telomere, Shelterin, Cell biology, Synaptonemal complex, HEK293 Cells, 030220 oncology & carcinogenesis, Female, Transcription Factors

Abstract

During meiosis, telomere attachment to the inner nuclear envelope is required for proper pairing of homologous chromosomes and recombination. Here, we identified F-box protein 47 (FBXO47) as a regulator of the telomeric shelterin complex that is specifically expressed during meiotic prophase I. Knockout of Fbxo47 in mice leads to infertility in males. We found that the Fbxo47 deficient spermatocytes are unable to form a complete synaptonemal complex. FBXO47 interacts with TRF1/2, and the disruption of Fbxo47 destabilizes TRF2, leading to unstable telomere attachment and slow traversing through the bouquet stage. Our findings uncover a novel mechanism of FBXO47 in telomeric shelterin subunit stabilization during meiosis.

Published

2019

30. Human X chromosome exome sequencing identifies

Author

Chuncheng, Lu, Yan, Zhang, Yufeng, Qin, Qiaoqiao, Xu, Ran, Zhou, Yiqiang, Cui, Yunfei, Zhu, Xin, Zhang, Jintao, Zhang, Xiang, Wei, Min, Wang, Bo, Hang, Jian-Hua, Mao, Antoine M, Snijders, Mingxi, Liu, Zhibin, Hu, Hongbing, Shen, Zuomin, Zhou, Xuejiang, Guo, Xin, Wu, Xinru, Wang, and Yankai, Xia

Subjects

Male, Mice, Knockout, Chromosomes, Human, X, Spermatogonia, Repressor Proteins, Mice, Testis, Exome Sequencing, Sperm Motility, Animals, Humans, Exome, CRISPR-Cas Systems, Spermatogenesis

Abstract

Infertility affects approximately 15% of couples worldwide with male infertility being responsible for approximately 50% of cases. Although accumulating evidence demonstrates the critical role of the X chromosome in spermatogenesis during the last few decades, the expression patterns and potential impact of the X chromosome, together with X linked genes, on male infertility are less well understood.We performed X chromosome exome sequencing followed by a two-stage independent population validation in 1333 non-obstructive azoospermia cases and 1141 healthy controls to identify variant classes with high likelihood of pathogenicity. To explore the functions of these candidate genes in spermatogenesis, we first knocked down these candidate genes individually in mouse spermatogonial stem cells (SSCs) using short interfering RNA oligonucleotides and then generated candidate genes knockout mice by CRISPR-Cas9 system.Four low-frequency variants were identified in four genes (Our data indicate that the X-linked genes are associated with male infertility and involved in regulating SSCs, which provides a new insight into the role of X-linked genes in spermatogenesis.

Published

2019

31. Correction: Sox30 initiates transcription of haploid genes during late meiosis and spermiogenesis in mouse testes (doi:10.1242/dev.164855)

Author

Mingyan Lin, Huiqi Yin, Lan Ye, Huanhuan Tan, Bin Shen, Yingwen Zhang, Ke Zheng, Wenbo Li, Qiuling Yue, Shun Bai, Changpeng Xin, Yuanyuan Wang, Wenxiu He, Zheng Sun, Kaiqiang Fu, Yiqiang Cui, Xuejiang Guo, Xiaofei Liu, Yueshuai Guo, Jinwen Zhang, Jie Xie, Le Cheng, and Hua Feng

Subjects

Genetics, 0303 health sciences, urogenital system, Spermiogenesis, Biology, 03 medical and health sciences, 0302 clinical medicine, Meiosis, Transcription (biology), Ploidy, Molecular Biology, Gene, 030217 neurology & neurosurgery, Research Article, 030304 developmental biology, Developmental Biology

Abstract

Transcription factors of the Sox protein family contain a DNA-binding HMG box and are key regulators of progenitor cell fate. Here, we report that expression of Sox30 is restricted to meiotic spermatocytes and postmeiotic haploids. Sox30 mutant males are sterile owing to spermiogenic arrest at the early round spermatid stage. Specifically, in the absence of Sox30, proacrosomic vesicles fail to form a single acrosomal organelle, and spermatids arrest at step 2-3. Although most Sox30 mutant spermatocytes progress through meiosis, accumulation of diplotene spermatocytes indicates a delayed or impaired transition from meiotic to postmeiotic stages. Transcriptome analysis of isolated stage-specific spermatogenic cells reveals that Sox30 controls a core postmeiotic gene expression program that initiates as early as the late meiotic cell stage. ChIP-seq analysis shows that Sox30 binds to specific DNA sequences in mouse testes, and its genomic occupancy correlates positively with expression of many postmeiotic genes including Tnp1, Hils1, Ccdc54 and Tsks. These results define Sox30 as a crucial transcription factor that controls the transition from a late meiotic to a postmeiotic gene expression program and subsequent round spermatid development.

Published

2019

32. Proteomic Analysis of Dpy19l2-Deficient Human Globozoospermia Reveals Multiple Molecular Defects

Author

Xiaoyu Yang, Zhibin Hu, Yiqiang Cui, Gaigai Wang, Xiaofei Liu, Jiayin Jiang, Hao Zhang, Zuomin Zhou, Yan Li, Yueshuai Guo, Jiahao Sha, Jianyu Tian, Daozhen Chen, Haotian Zhang, Xuejiang Guo, Min Jiang, and Yang Wen

Subjects

0301 basic medicine, Adult, Male, Proteomics, Isoantigens, Bioinformatics analysis, Genotype, Proteome, Clinical Biochemistry, Down-Regulation, Immunoglobulins, Computational biology, Biology, 03 medical and health sciences, Teratozoospermia, Young Adult, Human fertilization, Humans, Acrosome, Globozoospermia, 030102 biochemistry & molecular biology, Seminal Plasma Proteins, Membrane Proteins, Sperm, Spermatozoa, Chromatin, Up-Regulation, Blot, 030104 developmental biology, Case-Control Studies

Abstract

Purpose To investigate the differences in protein expression between Dpy19l2-deficient human globozoospermia and normozoospermia. Experimental design Human sperm samples from three globozoospermic donors with Dpy19l2 deletion and three normal controls are subjected to TMT quantitative technology. SPESP1, HIST1H4A, and LYZL1 are randomly selected for western blotting analysis. GO annotations are performed using the Database for Annotation, Visualization, and Integrated Discovery. Results A total of 2567 proteins are identified, of which 2510 proteins are quantified, and 491 are differentially expressed (fold-change > 2), with 370 upregulated and 121 downregulated in globozoospermic patients. The levels of several important proteins, including SPACA 1, IZUMO1, ZPBP1, and PLCZ1, are decreased in globozoospermic sperm. Bioinformatics analysis indicates the Dpy19l2-deficient sperm presented molecular defects in acrosome, chromatin, sperm-egg interaction, and fertilization. Conclusions and clinical relevance The present study is the first to analyze total globozoospermia with Dpy19l2 deletion using high-throughput proteomics. This study may provide insights into the mechanism of globozoospermia.

Published

2019

33. The testis-specifically expressed gene Trim69 is not essential for fertility in mice

Author

Wenxiu Xie, Xuejiang Guo, Jiahao Sha, Ya Wang, Huiling Li, Yiqiang Cui, and Xi He

Subjects

Protein family, biology, 010401 analytical chemistry, 02 engineering and technology, General Medicine, 021001 nanoscience & nanotechnology, 01 natural sciences, General Biochemistry, Genetics and Molecular Biology, Protein ubiquitination, 0104 chemical sciences, Ubiquitin ligase, Cell biology, Knockout mouse, Gene expression, biology.protein, 0210 nano-technology, Gene, TRIM Family, Gene knockout

Abstract

Protein ubiquitination is essential for diverse cellular functions including spermatogenesis. The tripartite motif (TRIM) family proteins, most of which have E3 ubiquitin ligase activity, are highly conserved in mammals. They are involved in important cellular processes such as embryonic development, immunity, and fertility. Our previous studies indicated that Trim69, a testis-specific expressed TRIM family gene, potentially participates in the spermatogenesis by mediating testicular cells apoptosis. In this study, we investigated the biological functions of Trim69 in male mice by established Trim69 knockout mice with CRISPR/Cas9 genomic editing technology. Here, we reported that the male Trim69 knockout mice had normal fertility. The adult knockout mice have shown that the appearance of testes, testis/body weight ratios, testicular histomorphology, and the number and quality of sperm were consistent with wild-type mice. These results indicated that the E3 ubiquitin ligase protein Trim69 was not essential for male mouse fertility, and it might be compensated by other TRIM family members such as Trim58 in Trim69-deficiency testis. This study would help to elucidate the functions of tripartite motif protein family and the regulation of spermatogenesis.

Published

2021

34. 2,2′,4,4′-Tetrabromodiphenyl ether injures cell viability and mitochondrial function of mouse spermatocytes by decreasing mitochondrial proteins Atp5b and Uqcrc1

Author

Shaoping Huang, Jing Wang, and Yiqiang Cui

Subjects

Male, 0301 basic medicine, endocrine system, Cell cycle checkpoint, Cell Survival, Health, Toxicology and Mutagenesis, ATP5B, Cell Culture Techniques, Apoptosis, 010501 environmental sciences, Mitochondrion, Biology, Toxicology, 01 natural sciences, Cell Line, Electron Transport Complex III, Mice, 03 medical and health sciences, Microscopy, Electron, Transmission, Spermatocytes, Halogenated Diphenyl Ethers, Animals, Viability assay, RNA, Small Interfering, Inner mitochondrial membrane, 0105 earth and related environmental sciences, Membrane Potential, Mitochondrial, Pharmacology, chemistry.chemical_classification, Reactive oxygen species, Dose-Response Relationship, Drug, Cell Cycle, General Medicine, Mitochondrial Proton-Translocating ATPases, Cell cycle, Molecular biology, Cell biology, 030104 developmental biology, chemistry, Gene Knockdown Techniques, Mitochondrial Membranes, Environmental Pollutants

Abstract

Our object was to explore direct effects and mechanism of BDE47 on GC2 (immortalized mouse spermatocyte). GC2 were exposed to DMSO, 0.1, 1, 10, 100μM BDE47 for 48h. Cell viability was detected by trypan-blue exclusion; ultrastructure by electron-microscopy; cell cycle, mitochondrial membrane motential (MMP), reactive oxygen species (ROS) by flow-cytometry; ATP production by luminometer; Atp5b, Uqcrc1, Bcl-2 level by WB. To explore whether the decreased mitochondrial proteins play an important role in apoptosis, MMP and apoptosis were detected after Atp5b or Uqcrc1 knockdown in GC2. Results showed BDE47 reduced cell viability, caused condensation of nuclear and vacuolated mitochondria, decreased MMP and ATP, induced ROS, cell cycle arrest at S and G2/M phase, reduced Atp5b, Uqcrc1, Bcl-2 in GC2. Knockdown of Atp5b or Uqcrc1 decreased MMP, induced apoptosis in GC2. Results suggested that BDE47 reduced cell viability, injured mitochondria in spermatocytes probably by decreasing mitochondrial protein Atp5b and Uqcrc1.

Published

2016

35. Sox30 initiates transcription of haploid genes during late meiosis and spermiogenesis in mouse testes

Author

Zheng Sun, Kaiqiang Fu, Hua Feng, Xuejiang Guo, Mingyan Lin, Bin Shen, Lan Ye, Le Cheng, Huanhuan Tan, Jinwen Zhang, Qiuling Yue, Yingwen Zhang, Xiaofei Liu, Shun Bai, Yueshuai Guo, Jie Xie, Wenbo Li, Huiqi Yin, Changpeng Xin, Ke Zheng, Yuanyuan Wang, Wenxiu He, and Yiqiang Cui

Subjects

0301 basic medicine, Male, Spermiogenesis, Mutant, Biology, Response Elements, 03 medical and health sciences, Mice, Meiosis, Transcription (biology), Gene expression, Testis, medicine, Animals, Spermatogenesis, Molecular Biology, Gene, Transcription factor, SOX Transcription Factors, Transcription Initiation, Genetic, Spermatid, urogenital system, Gene Expression Profiling, Correction, Spermatids, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, Developmental Biology

Abstract

Transcription factors of the Sox protein family contain a DNA-binding HMG box and are key regulators of progenitor cell fate. Here, we report that expression of Sox30 is restricted to meiotic spermatocytes and postmeiotic haploids. Sox30 mutant males are sterile due to spermiogenic arrest at the early round spermatid stage. Specifically, in the absence of Sox30, proacrosomic vesicles fail to form a single acrosomal organelle, and spermatids arrest at step 2-3. Although most Sox30 mutant spermatocytes progress through meiosis, accumulation of diplotene spermatocytes indicates a delayed or impaired transition from meiotic to postmeiotic stages. Transcriptome analysis of isolated stage-specific spermatogenic cells reveals that Sox30 controls a core postmeiotic gene expression program that initiates as early as in late meiotic cells. ChIP-seq analysis shows that Sox30 binds to specific DNA sequences in mouse testes, and its genomic occupancy correlates positively with expression of many postmeiotic genes including Tnp1, Hils1, Ccdc54 and Tsks. These results define Sox30 as a crucial transcription factor that controls the transition from a late meiotic to a postmeiotic gene expression program and subsequent round spermatid development.

Published

2018

36. CRISPR/Cas9-mediatedDax1knockout in the monkey recapitulates human AHC-HH

Author

Bo Zheng, Weizhi Ji, Hong Wang, Jianying Wang, Jiahao Sha, Bin Shen, Yuyu Niu, Lei Wang, Bian Hu, Qi Zhou, Xuejiang Guo, Jiankui Zhou, Yongchang Chen, Xingxu Huang, Yu Kang, and Yiqiang Cui

Subjects

Male, medicine.medical_specialty, CRISPR-Associated Proteins, Biology, Animals, Genetically Modified, Sertoli cell-only syndrome, X-linked adrenal hypoplasia congenita, Internal medicine, Testis, Genetics, medicine, Animals, Humans, CRISPR, Clustered Regularly Interspaced Short Palindromic Repeats, Molecular Biology, Genetics (clinical), Sertoli Cells, DAX-1 Orphan Nuclear Receptor, Hypogonadism, Wnt signaling pathway, Gene targeting, Haplorhini, General Medicine, medicine.disease, Sertoli cell, Cell biology, DNA-Binding Proteins, Endocrinology, medicine.anatomical_structure, Knockout mouse, Female, DAX1, Transcription Factors

Abstract

Mutations in the DAX1 locus cause X-linked adrenal hypoplasia congenita (AHC) and hypogonadotropic hypogonadism (HH), which manifest with primary adrenal insufficiency and incomplete or absent sexual maturation, respectively. The associated defects in spermatogenesis can range from spermatogenic arrest to Sertoli cell only syndrome. Conclusions from Dax1 knockout mouse models provide only limited insight into AHC/HH disease mechanisms, because mouse models exhibit more extensive abnormalities in testicular development, including disorganized and incompletely formed testis cords with decreased number of peritubular myoid cells and male-to-female sex reversal. We previously reported successful clustered regularly interspaced short palindromic repeats (CRISPR)/CRISPR-associated protein 9 (Cas9)-mediated genome targeting in cynomolgus monkeys. Here, we describe a male fetal monkey in which targeted genome editing using CRISPR/Cas9 produced Dax1-null mutations in most somatic tissues and in the gonads. This DAX1-deficient monkey displayed defects in adrenal gland development and abnormal testis architecture with small cords, expanded blood vessels and extensive fibrosis. Sertoli cell formation was not affected. This phenotype strongly resembles findings in human patients with AHC-HH caused by mutations in DAX1. We further detected upregulation of Wnt/β-catenin-VEGF signaling in the fetal Dax1-deficient testis, suggesting abnormal activation of signaling pathways in the absence of DAX1 as one mechanism of AHC-HH. Our study reveals novel insight into the role of DAX1 in HH and provides proof-of-principle for the generation of monkey models of human disease via CRISPR/Cas9-mediated gene targeting.

Published

2015

37. Systematic Analysis of the Phosphoproteome and Kinase-substrate Networks in the Mouse Testis

Author

Zuomin Zhou, Jiahao Sha, Yu Xue, Yueshuai Guo, Zexian Liu, Xuejiang Guo, Yiqiang Cui, Jing Wang, Tao Zhou, and Lin Qi

Subjects

Male, Proteome, Cell Cycle Proteins, Protein Serine-Threonine Kinases, Biochemistry, PLK1, Analytical Chemistry, Mice, Proto-Oncogene Proteins, CDC2 Protein Kinase, Testis, Animals, Gene Regulatory Networks, Phosphorylation, Spermatogenesis, Cell Cycle Protein, Protein Kinase Inhibitors, Molecular Biology, Cyclin-dependent kinase 1, Protein-Serine-Threonine Kinases, biology, Kinase, Research, Gene Expression Profiling, Cyclin-Dependent Kinase 2, Cyclin-dependent kinase 2, Molecular Sequence Annotation, Cell cycle, Phosphoproteins, Cell biology, G2 Phase Cell Cycle Checkpoints, Gene Expression Regulation, biology.protein, Mitogen-Activated Protein Kinases

Abstract

Spermatogenesis is a complex process closely associated with the phosphorylation-orchestrated cell cycle. Elucidating the phosphorylation-based regulations should advance our understanding of the underlying molecular mechanisms. Here we present an integrative study of phosphorylation events in the testis. Large-scale phosphoproteome profiling in the adult mouse testis identified 17,829 phosphorylation sites in 3955 phosphoproteins. Although only approximately half of the phosphorylation sites enriched by IMAC were also captured by TiO2, both the phosphoprotein data sets identified by the two methods significantly enriched the functional annotation of spermatogenesis. Thus, the phosphoproteome profiled in this study is a highly useful snapshot of the phosphorylation events in spermatogenesis. To further understand phosphoregulation in the testis, the site-specific kinase-substrate relations were computationally predicted for reconstructing kinase-substrate phosphorylation networks. A core sub-kinase-substrate phosphorylation networks among the spermatogenesis-related proteins was retrieved and analyzed to explore the phosphoregulation during spermatogenesis. Moreover, network-based analyses demonstrated that a number of protein kinases such as MAPKs, CDK2, and CDC2 with statistically more site-specific kinase-substrate relations might have significantly higher activities and play an essential role in spermatogenesis, and the predictions were consistent with previous studies on the regulatory roles of these kinases. In particular, the analyses proposed that the activities of POLO-like kinases (PLKs) might be dramatically higher, while the prediction was experimentally validated by detecting and comparing the phosphorylation levels of pT210, an indicator of PLK1 activation, in testis and other tissues. Further experiments showed that the inhibition of POLO-like kinases decreases cell proliferation by inducing G2/M cell cycle arrest. Taken together, this systematic study provides a global landscape of phosphoregulation in the testis, and should prove to be of value in future studies of spermatogenesis.

Published

2014

38. The testis-specifically expressed gene Trim69 is not essential for fertility in mice.

Author

Xi He, Wenxiu Xie, Huiling Li, Yiqiang Cui, Ya Wang, Xuejiang Guo, and Jiahao Sha

Subjects

SPERMATOGENESIS, TRIM proteins, UBIQUITIN ligases, FERTILITY, GENES, EMBRYOLOGY

Abstract

Protein ubiquitination is essential for diverse cellular functions including spermatogenesis. The tripartite motif (TRIM) family proteins, most of which have E3 ubiquitin ligase activity, are highly conserved in mammals. They are involved in important cellular processes such as embryonic development, immunity, and fertility. Our previous studies indicated that Trim69, a testis-specific expressed TRIM family gene, potentially participates in the spermatogenesis by mediating testicular cells apoptosis. In this study, we investigated the biological functions of Trim69 in male mice by established Trim69 knockout mice with CRISPR/Cas9 genomic editing technology. Here, we reported that the male Trim69 knockout mice had normal fertility. The adult knockout mice have shown that the appearance of testes, testis/body weight ratios, testicular histomorphology, and the number and quality of sperm were consistent with wild-type mice. These results indicated that the E3 ubiquitin ligase protein Trim69 was not essential for male mouse fertility, and it might be compensated by other TRIM family members such as Trim58 in Trim69-deficiency testis. This study would help to elucidate the functions of tripartite motif protein family and the regulation of spermatogenesis. [ABSTRACT FROM AUTHOR]

Published

2021

39. Human X chromosome exome sequencing identifies BCORL1 as contributor to spermatogenesis.

Author

Chuncheng Lu, Yan Zhang, Yufeng Qin, Qiaoqiao Xu, Ran Zhou, Yiqiang Cui, Yunfei Zhu, Xin Zhang, Jintao Zhang, Xiang Wei, Min Wang, Bo Hang, Jian-Hua Mao, Snijders, Antoine M., Mingxi Liu, Zhibin Hu, Hongbing Shen, Zuomin Zhou, Xuejiang Guo, and Xin Wu

Abstract

Background Infertility affects approximately 15% of couples worldwide with male infertility being responsible for approximately 50% of cases. Although accumulating evidence demonstrates the critical role of the X chromosome in spermatogenesis during the last few decades, the expression patterns and potential impact of the X chromosome, together with X linked genes, on male infertility are less well understood. Methods We performed X chromosome exome sequencing followed by a two-stage independent population validation in 1333 non-obstructive azoospermia cases and 1141 healthy controls to identify variant classes with high likelihood of pathogenicity. To explore the functions of these candidate genes in spermatogenesis, we first knocked down these candidate genes individually in mouse spermatogonial stem cells (SSCs) using short interfering RNA oligonucleotides and then generated candidate genes knockout mice by CRISPR-Cas9 system. Results Four low-frequency variants were identified in four genes (BCORL1, MAP7D3, ARMCX4 and H2BFWT) associated with male infertility. Functional studies of the mouse SSCs revealed that knocking down Bcorl1 or Mtap7d3 could inhibit SSCs self-renewal and knocking down Armcx4 could repress SSCs differentiation in vitro. Using CRISPR-Cas9 system, Bcorl1 and Mtap7d3 knockout mice were generated. Excitingly, Bcorl1 knockout mice were infertile with impaired spermatogenesis. Moreover, Bcorl1 knockout mice exhibited impaired sperm motility and sperm cells displayed abnormal mitochondrial structure. Conclusion Our data indicate that the X-linked genes are associated with male infertility and involved in regulating SSCs, which provides a new insight into the role of X-linked genes in spermatogenesis. [ABSTRACT FROM AUTHOR]

Published

2021

40. An essential role for PNLDC1 in piRNA 3′ end trimming and male fertility in mice

Author

Yue Zhang, Lan Ye, Shun Bai, Hao Wu, Mingxi Liu, Zhiping Zhu, Bin Shen, Yingwen Zhang, Qiuling Yue, Ke Zheng, Bo Zheng, Xuejiang Guo, Rui Guo, Jiahao Sha, Zuomin Zhou, Wentao Zeng, and Yiqiang Cui

Subjects

0301 basic medicine, Genetics, 03 medical and health sciences, 030104 developmental biology, Male fertility, Piwi-interacting RNA, Trimming, Cell Biology, Biology, Bioinformatics, Molecular Biology, Letter to the Editor

Published

2017

41. TCTE1 is a conserved component of the dynein regulatory complex and is required for motility and metabolism in mouse spermatozoa

Author

Ramiro Ramirez-Solis, Haruhiko Miyata, Masahito Ikawa, Renata Prunskaite-Hyyryläinen, Zibin Wang, Mingxi Liu, Yiqiang Cui, Rong Hua, Yueshuai Guo, Jiahao Sha, Julio M Castaneda, Martin M. Matzuk, Tao Zhou, Yiwei Cheng, Zhibin Hu, Zhifeng Yu, Xuejiang Guo, Bin Shen, Asami Oji, and Zuomin Zhou

Subjects

0301 basic medicine, Axoneme, Male, Dynein, Green Fluorescent Proteins, Biology, Flagellum, Ciliopathies, Microtubules, 03 medical and health sciences, Mice, 0302 clinical medicine, Adenosine Triphosphate, Radial spoke, Microtubule, Testis, Animals, Humans, Cilia, Sperm motility, Crosses, Genetic, Cytoskeleton, 030219 obstetrics & reproductive medicine, Multidisciplinary, urogenital system, Cilium, Chlamydomonas, Homozygote, Dyneins, Proteins, Spermatids, Spermatozoa, Cell biology, 030104 developmental biology, HEK293 Cells, PNAS Plus, Flagella, Mutation, Sperm Motility, Female

Abstract

Flagella and cilia are critical cellular organelles that provide a means for cells to sense and progress through their environment. The central component of flagella and cilia is the axoneme, which comprises the “9+2” microtubule arrangement, dynein arms, radial spokes, and the nexin-dynein regulatory complex (N-DRC). Failure to properly assemble components of the axoneme leads to defective flagella and in humans leads to a collection of diseases referred to as ciliopathies. Ciliopathies can manifest as severe syndromic diseases that affect lung and kidney function, central nervous system development, bone formation, visceral organ organization, and reproduction. T-Complex-Associated–Testis-Expressed 1 (TCTE1) is an evolutionarily conserved axonemal protein present from Chlamydomonas (DRC5) to mammals that localizes to the N-DRC. Here, we show that mouse TCTE1 is testis-enriched in its expression, with its mRNA appearing in early round spermatids and protein localized to the flagellum. TCTE1 is 498 aa in length with a leucine rich repeat domain at the C terminus and is present in eukaryotes containing a flagellum. Knockout of Tcte1 results in male sterility because Tcte1-null spermatozoa show aberrant motility. Although the axoneme is structurally normal in Tcte1 mutant spermatozoa, Tcte1-null sperm demonstrate a significant decrease of ATP, which is used by dynein motors to generate the bending force of the flagellum. These data provide a link to defining the molecular intricacies required for axoneme function, sperm motility, and male fertility.

Published

2017

42. Generation of Gene-Modified Cynomolgus Monkey via Cas9/RNA-Mediated Gene Targeting in One-Cell Embryos

Author

Yongchang Chen, Fang Wang, Xingxu Huang, Weizhi Ji, Chenyang Si, Tianqing Li, Zuomin Zhou, Yuyu Niu, Wei Li, Xiuqiong Pu, Bin Shen, Tao Tan, Jiankui Zhou, Xuejiang Guo, Qi Zhou, Shaohui Ji, Wei Si, Andy Peng Xiang, Jiahao Sha, Yiqiang Cui, Jianying Wang, Guoying Dong, Xiaoyang Zhao, Yu Kang, Lei Wang, Ye Bi, Bian Hu, and Hong Wang

Subjects

Genetics, Base Sequence, Mosaicism, Biochemistry, Genetics and Molecular Biology(all), Cas9, Molecular Sequence Data, Gene targeting, RNA, Mutagenesis (molecular biology technique), Biology, Embryo, Mammalian, General Biochemistry, Genetics and Molecular Biology, Recombination-activating gene, Cell Line, Genetically modified organism, Cell biology, Macaca fascicularis, Gene Targeting, Animals, Humans, CRISPR, Female, Sequence Alignment, Gene

Abstract

SummaryMonkeys serve as important model species for studying human diseases and developing therapeutic strategies, yet the application of monkeys in biomedical researches has been significantly hindered by the difficulties in producing animals genetically modified at the desired target sites. Here, we first applied the CRISPR/Cas9 system, a versatile tool for editing the genes of different organisms, to target monkey genomes. By coinjection of Cas9 mRNA and sgRNAs into one-cell-stage embryos, we successfully achieve precise gene targeting in cynomolgus monkeys. We also show that this system enables simultaneous disruption of two target genes (Ppar-γ and Rag1) in one step, and no off-target mutagenesis was detected by comprehensive analysis. Thus, coinjection of one-cell-stage embryos with Cas9 mRNA and sgRNAs is an efficient and reliable approach for gene-modified cynomolgus monkey generation.

Published

2014

43. Germline acquisition of Cas9/RNA-mediated gene modifications in monkeys

Author

Wei Li, Qi Zhou, Jianying Wang, Xiaoyang Zhao, Xingxu Huang, Lei Wang, Weizhi Ji, Bin Shen, Yongchang Chen, Yuyu Niu, Yiqiang Cui, and Jiahao Sha

Subjects

Peroxisome proliferator-activated receptor, Germline, Animals, Clustered Regularly Interspaced Short Palindromic Repeats, DNA Cleavage, Molecular Biology, Gene, Letter to the Editor, RNA metabolism, Genetics, chemistry.chemical_classification, Homeodomain Proteins, biology, Base Sequence, Cas9, Gene targeting, RNA, Cell Biology, Haplorhini, biology.organism_classification, PPAR gamma, Germ Cells, chemistry, Gene Targeting

Published

2014

44. 2,2',4,4'-Tetrabromodiphenyl ether disrupts spermatogenesis, impairs mitochondrial function and induces apoptosis of early leptotene spermatocytes in rats

Author

Ye Bi, Min Lin, Yankai Xia, Xiaoyan Huang, Ying Lu, Shoulin Wang, Lei Wang, Shaoping Huang, Yiqiang Cui, Suying Li, Jiahao Sha, Zuomin Zhou, Xinru Wang, and Xuejiang Guo

Subjects

Male, Proteomics, TUNEL assay, Apoptosis, Biology, Mitochondrion, Toxicology, Cell biology, Cell Line, Mitochondria, Blot, Rats, Sprague-Dawley, Mice, Meiosis, Microscopy, Electron, Transmission, Spermatocytes, Testis, Halogenated Diphenyl Ethers, Immunohistochemistry, Animals, Spermatogenesis, Corn oil, Flame Retardants

Abstract

Our objective was to explore molecular markers and mechanism of BDE47 on spermatogenesis in mammals. Adult male SD rats were gavaged daily with corn oil containing 0, 0.001, 0.03, 1 or 20mg BDE47/kg bw for eight weeks. Testes morphology was analyzed using electron microscopy, TUNEL, immunohistochemistry and morphometry. Differential proteome profile and western blotting were applied to determine molecular markers and protein expression. GC1-spg cells (mouse spermatogonial cells) were used to verify mechanism of BDE47. Data showed BDE47 reduced tubular epithelial thickness, impaired mitochondrial function and induced apoptosis in early leptotene spermatocytes. Proteomic study identified 70 differential spots corresponding to 64 proteins. 20 proteins related to apoptosis, 15 located in mitochondria. Exposure of GC1-spg cells showed BDE47 induced apoptosis, impaired mitochondria and decreased Bcl-2 in cells. Data indicate that BDE47 disrupts spermatogenesis, impairs mitochondrial function and induces apoptosis of early leptotene spermatocytes in rats probably via mitochondrial pathway.

Published

2014

45. Insights into the lysine acetylproteome of human sperm

Author

Yiqiang Cui, Tao Zhou, Guohai Sun, Yueshuai Guo, Jiahao Sha, Xuejiang Guo, and Min Jiang

Subjects

Adult, Male, Glycosylation, Proteome, Lysine, Acrosome reaction, Biophysics, Hydroxamic Acids, complex mixtures, Biochemistry, Histone Deacetylases, chemistry.chemical_compound, Capacitation, Humans, Sperm motility, biology, urogenital system, Acrosome Reaction, Acetylation, Sperm, Spermatozoa, Histone Deacetylase Inhibitors, Histone, chemistry, biology.protein, Sperm Motility, bacteria

Abstract

Protein lysine acetylation is a dynamic and reversible post-modification that is known to play diverse functions in eukaryotes. Nevertheless, the composition and function of non-histone lysine acetylation in gametes remain unknown. In humans, only capacitated sperm have the capacity to fertilize an egg. In the present study, we found complex composition of lysine acetylated proteins in capacitated human sperm. In vitro fertilization inhibition assay by anti-acetyllysine antibody showed essential roles of lysine acetylation in fertilization. And inhibition of lysine deacetylases, the histone deacetylases, by trichostatin A and nicotinamide, could significantly suppress sperm motility. After immunopurification enrichment of acetylpeptides with anti-acetyllysine antibody and high-throughput liquid chromatography–tandem mass spectrometry identification, we characterized 1206 lysine acetylated sites, corresponding to 576 lysine acetylated proteins in human capacitated sperm. Bioinformatics analysis showed that these proteins are associated with sperm functions, including motility, capacitation, acrosome reaction and sperm–egg interaction. Thus, lysine acetylation is expected to be an important regulatory mechanism for sperm functions. And our characterization of lysine acetylproteome could be a rich resource for the study of male fertility. Biological significance Mature sperm are almost transcriptionally and translationally silent, thus post-translational modifications play important roles in sperm functions. Till now, only two types of PTMs, phosphorylation and glycosylation, are well studied in normal human sperm based on large scale proteomics. In the present study, we established the acetylproteome of capacitated human sperm. Over 1000 lysine acetylated sites were identified. Bioinformatics analysis shows that lysine acetylated proteins participate in many biological events of sperm functions. We further provided functional data that the lysine acetylation is essential for sperm motility and fertilization using histone acetylase inhibitors and anti-acetyllysine antibody. These data can be strong evidences for the important function of lysine acetylation in human sperm.

Published

2014

46. Blastomere biopsy influences epigenetic reprogramming during early embryo development, which impacts neural development and function in resulting mice

Author

Yang Yang, Qi Zhou, Liu Wang, Yang Yu, Man Tong, Jiahao Sha, Guoying Dong, Zuomin Zhou, Yibo Wu, Zhuo Lv, Yiqiang Cui, and Hui Zhu

Subjects

Pathology, medicine.medical_specialty, Aging, Blastomeres, Proteome, Reproductive Techniques, Assisted, Embryonic Development, Neural degeneration, Biology, Epigenesis, Genetic, Cellular and Molecular Neuroscience, Mice, Biopsy, medicine, Animals, Methylated DNA immunoprecipitation, Promoter Regions, Genetic, Molecular Biology, Pharmacology, Neurons, Mice, Inbred ICR, Genome, medicine.diagnostic_test, Behavior, Animal, DNA Helicases, Brain, Embryo, Cell Biology, Methylation, DNA Methylation, Embryo, Mammalian, DNA methylation, Molecular Medicine, Neural development, Reprogramming

Abstract

Blastomere biopsy is used in preimplantation genetic diagnosis; however, the long-term implications on the offspring are poorly characterized. We previously reported a high risk of memory defects in adult biopsied mice. Here, we assessed nervous function of aged biopsied mice and further investigated the mechanism of neural impairment after biopsy. We found that aged biopsied mice had poorer spatial learning ability, increased neuron degeneration, and altered expression of proteins involved in neural degeneration or dysfunction in the brain compared to aged control mice. Furthermore, the MeDIP assay indicated a genome-wide low methylation in the brains of adult biopsied mice when compared to the controls, and most of the genes containing differentially methylated loci in promoter regions were associated with neural disorders. When we further compared the genomic DNA methylation profiles of 7.5-days postconception (dpc) embryos between the biopsy and control group, we found the whole genome low methylation in the biopsied group, suggesting that blastomere biopsy was an obstacle to de novo methylation during early embryo development. Further analysis on mRNA profiles of 4.5-dpc embryos indicated that reduced expression of de novo methylation genes in biopsied embryos may impact de novo methylation. In conclusion, we demonstrate an abnormal neural development and function in mice generated after blastomere biopsy. The impaired epigenetic reprogramming during early embryo development may be the latent mechanism contributing to the impairment of the nervous system in the biopsied mice, which results in a hypomethylation status in their brains.

Published

2013

47. TCTE1 is a conserved component of the dynein regulatory complex and is required for motility and metabolism in mouse spermatozoa.

Author

Castaneda, Julio M., Rong Hua, Haruhiko Miyata, Oji, Asami, Guo, Yueshuai, Yiwei Cheng, Tao Zhou, Xuejiang Guo, Yiqiang Cui, Bin Shen, Zibin Wang, Zhibin Hu, Zuomin Zhou, Sha, Jiahao, Prunskaite-Hyyrylainen, Renata, Zhifeng Yu, Ramirez-Solis, Ramiro, Masahito Ikawa, Matzuk, Martin M., and Mingxi Liu

Subjects

DYNEIN, ADENOSINE triphosphatase, SEMEN, MICROTUBULES, GERM cells, SPERMATOZOA, LABORATORY mice

Abstract

Flagella and cilia are critical cellular organelles that provide a means for cells to sense and progress through their environment. The central component of flagella and cilia is the axoneme, which comprises the "9+2" microtubule arrangement, dynein arms, radial spokes and the nexin-dynein regulatory complex (N-DRC). Failure to properly assemble components of the axoneme leads to defective flagella and in humans leads to a collection of diseases referred to as ciliopathies. Ciliopathies can manifest as severe syndromic diseases that affect lung and kidney function, central nervous system development, bone formation, visceral organ organization and reproduction. T-Complex-Associated-Testis-Expressed 1 (TCTE1) is an evolutionarily conserved axonemal protein present from Chlamydomonas (DRC5) to mammals that localizes to the N-DRC. Here, we show that mouse TCTE1 is testis-enriched in its expression, with its mRNA appearing in early round spermatids and protein localized to the flagellum. TCTE1 is 498 aa in length with a leucine rich repeat domain at the C terminus and is present in eukaryotes containing a flagellum. Knockout of Tcte1 results in male sterility because Tcte1-null spermatozoa show aberrant motility. Although the axoneme is structurally normal in Tcte1 mutant spermatozoa, Tcte1-null sperm demonstrate a significant decrease of ATP, which is used by dynein motors to generate the bending force of the flagellum. These data provide a link to defining the molecular intricacies required for axoneme function, sperm motility and male fertility. [ABSTRACT FROM AUTHOR]

Published

2017

48. CRISPR/Cas9-mediated Dax1 knockout in the monkey recapitulates human AHC-HH.

Author

Yu Kang, Bo Zheng, Bin Shen, Yongchang Chen, Lei Wang, Jianying Wang, Yuyu Niu, Yiqiang Cui, Jiankui Zhou, Hong Wang, Xuejiang Guo, Bian Hu, Qi Zhou, Jiahao Sha, Weizhi Ji, and Xingxu Huang

Published

2015