Your search keyword '"Sun, Yingpu"' showing total 10 results

1. Human trophoblast invasion and migration are mediated by the YAP1-CCN1 pathway: defective signaling in trophoblasts during early-onset severe preeclampsia†

Author

Wu, Liang, Wang, Shengfu, Li, Hongyue, Lu, Haotian, Zheng, Yuanke, Feng, Tianfei, and Sun, Yingpu

Abstract

The transcription coactivator YAP1 mediates the major effects of the Hippo signaling pathway. The CCN family is a small group of glycoproteins known to be downstream effectors of YAP1 in diverse tissues. However, whether CCN family members mediate the effects of YAP1 in human trophoblasts is unknown. In this study, placental expression of both YAP1and CCN1was found to be impaired in pregnancies complicated by early-onset severe preeclampsia. CCN1 was expressed not only in cytotrophoblasts, trophoblast columns, and mesenchymal cells, similar to active YAP1, but also in syncytiotrophoblasts of normal first-trimester placental villi; moreover, decidual staining of active YAP1 and CCN1 was found in both interstitial and endovascular extravillous trophoblasts. In cultured immortalized human trophoblastic HTR-8/SVneo cells, knockdown of YAP1decreased CCN1mRNA and protein expression and led to impaired cell invasion and migration. Also, CCN1knockdown negatively affected HTR-8/SVneo cell invasion and migration but not viability. YAP1knockdown was further found to impair HTR-8/SVneo cell viability via G0/G1 cell cycle arrest and apoptosis, while CCN1knockdown had minimal effect on cell cycle arrest and no effect on apoptosis. Accordingly, treatment with recombinant CCN1 partially reversed the YAP1knockdown-induced impairment in trophoblast invasion and migration but not in viability. Thus, CCN1 mediates the effects of YAP1 on human trophoblast invasion and migration but not apoptosis, and decreased placental expression of YAP1and CCN1in pregnancies complicated by early-onset severe preeclampsia might contribute to the pathogenesis of this disease.CCN1 mediates the effects of YAP1 on human trophoblast invasion and migration but not on apoptosis. Decreased placental YAP1and CCN1expression in early-onset severe preeclampsia might contribute to the pathogenesis of this disease.Graphical AbstractDecreased placental YAP1 and CCN1 expression might contribute to the pathogenesis of early-onset sPE. Abnormally reduced expression of YAP1 in first-trimester placentas results in correspondingly decreased expression of CCN1 via transcriptional regulation by TEAD transcription factors; attenuated autocrine/paracrine effects of CCN1 on EVT invasion and migration might contribute to incomplete remodelling of uterine spiral arteries, which ultimately leads to early-onset sPE. CT, cytotrophoblast; ST, syncytiotrophoblast; TC, trophoblast column; EVT, extravillous trophoblast; iEVT, interstitial EVT; eEVT, endovascular EVT. This graphical abstract was generated using Illustrator CS6 (Adobe Systems) with some graphics from ScienceSlides 2016 (VisiScience, Chapel Hill, NC, USA).

Published

2024

2. Sestrin2 and Sestrin3 protect spermatogenesis against heat-induced meiotic defects†

Author

Chen, Wenhui, Wang, Mengchen, Wang, Huan, Jiang, Yuqing, Zhu, Jing, Zeng, Xinxin, Xie, Huihui, Yang, Qingling, and Sun, Yingpu

Abstract

Heat stress induces testicular oxidative stress, impairs spermatogenesis, and increases the risk of male infertility. Recent studies have highlighted the antioxidative properties of the Sestrins family in reducing cellular oxidative damage. However, the role of Sestrins (Sestrin1, 2, and 3) in the testicular response to heat stress remains unclear. Here, we found that Sestrin2 and 3 were highly expressed in the testis relative to Sestrin1. Then, the Sestrin2−/−and Sestrin3−/−mice were generated by CRISPR/Cas9 to investigate the role of them on spermatogenesis after heat stress. Our data showed that Sestrin2−/−and Sestrin3−/−mice testes exhibited more severe damage manifested by exacerbated loss of germ cells and higher levels of oxidative stress as compared to wild-type counterparts after heat stress. Notably, Sestrin2−/−and Sestrin3−/−mice underwent a remarkable increase in heat-induced spermatocyte apoptosis than that of controls. Furthermore, the transcriptome landscape of spermatocytes and chromosome spreading showed that loss of Sestrin2and Sestrin3exacerbated meiotic failure by compromising DNA double-strand breaks repair after heat stress. Taken together, our work demonstrated a critical protective function of Sestrin2 and Sestrin3 in mitigating the impairments of spermatogenesis against heat stress.Summary SentenceSestrin2 and Sestrin3 play an important role in safeguarding spermatogenesis against heat-induced meiotic defects, highlighting their importance in preserving male fertility after heat stress.Graphical Abstract

Published

2024

3. Dynamic DNA 5-Hydroxylmethylcytosine and RNA 5-Methycytosine Reprogramming During Early Human Development

Author

Han, Xiao, Guo, Jia, Wang, Mengke, Zhang, Nan, Ren, Jie, Yang, Ying, Chi, Xu, Chen, Yusheng, Yao, Huan, Zhao, Yong-Liang, Yang, Yun-Gui, Sun, Yingpu, and Xu, Jiawei

Abstract

After implantation, complex and highly specialized molecular events render functionally distinct organ formation, whereas how the epigenome shapes organ-specific development remains to be fully elucidated. Here, nano-hmC-Seal, RNA bisulfite sequencing (RNA-BisSeq), and RNA sequencing (RNA-Seq) were performed, and the first multilayer landscapes of DNA 5-hydroxymethylcytosine (5hmC) and RNA 5-methylcytosine (m5C) epigenomes were obtained in the heart, kidney, liver, and lung of the human foetuses at 13–28 weeks with 123 samples in total. We identified 70,091 and 503 organ- and stage-specific differentially hydroxymethylated regions (DhMRs) and m5C-modified mRNAs, respectively. The key transcription factors (TFs), T-box transcription factor 20 (TBX20), paired box 8 (PAX8), krueppel-like factor 1 (KLF1), transcription factor 21 (TCF21), and CCAAT enhancer binding protein beta (CEBPB), specifically contribute to the formation of distinct organs at different stages. Additionally, 5hmC-enriched Alu elements may participate in the regulation of expression of TF-targeted genes. Our integrated studies reveal a putative essential link between DNA modification and RNA methylation, and illustrate the epigenetic maps during human foetal organogenesis, which provide a foundation for for an in-depth understanding of the epigenetic mechanisms underlying early development and birth defects.

Published

2023

4. NAD+ deficiency and mitochondrial dysfunction in granulosa cells of women with polycystic ovary syndrome‡.

Author

Wang, Yujiao, Yang, Qingling, Wang, Huan, Zhu, Jing, Cong, Luping, Li, Hui, and Sun, Yingpu

Abstract

Polycystic ovary syndrome (PCOS) is a prevalent heterogeneous endocrine disorder characterized by ovulation dysfunction, androgen excess, ovarian polycystic changes, insulin resistance, and infertility. Although underlying mechanisms for PCOS are still unknown, inflammation and mitochondrial dysfunction in granulosa cells (GCs) of PCOS patients have been reported. Here, we found that Nicotinamide Adenine Dinucleotide (NAD+) levels in GCs of PCOS patients was significantly decreased when compared with controls. Also, we found that higher expression of inflammation factors, increased reactive oxygen species (ROS) accumulation, lower adenosine triphosphate (ATP) generation, and decreased mitochondrial membrane potential, as well as abnormal mitochondrial dynamics in GCs of PCOS patients. In addition, the NAD+ levels were decreased after activation of inflammation in human granulosa-like tumor cell line (KGN) treated by Lipopolysaccharide (LPS). However, supplementation of nicotinamide riboside (NR), a NAD+ precursor, could largely restore the NAD+ content, reduce ROS levels and improve mitochondrial function demonstrated by increased mitochondrial membrane potential and ATP generation in LPS-treated KGN cells. Our data suggested that inflammation decreased NAD+ levels in GCs of PCOS patients, while supplementation of NR could restore NAD+ levels and alleviated mitochondrial dysfunction in GCs of PCOS patients.

Published

2021

5. Parental methylome reprogramming in human uniparental blastocysts reveals germline memory transition

Author

Xu, Jiawei, Shu, Yimin, Yao, Guidong, Zhang, Yu, Niu, Wenbin, Zhang, Yile, Ma, Xueshan, Jin, Haixia, Zhang, Fuli, Shi, Senlin, Wang, Yang, Song, Wenyan, Dai, Shanjun, Cheng, Luyao, Zhang, Xiangyang, Xie, Wei, Hsueh, Aaron J., and Sun, Yingpu

Abstract

Uniparental embryos derived from only the mother (gynogenetic [GG]) or the father (androgenetic [AG]) are unique models for studying genomic imprinting and parental contributions to embryonic development. Human parthenogenetic embryos can be obtained following artificial activation of unfertilized oocytes, but the production of AG embryos by injection of two sperm into one denucleated oocyte leads to an extra centriole, resulting in multipolar spindles, abnormal cell division, and developmental defects. Here, we improved androgenote production by transferring the male pronucleus from one zygote into another haploid androgenote to prevent extra centrioles and successfully generated human diploid AG embryos capable of developing into blastocysts with an identifiable inner cell mass (ICM) and trophectoderm (TE). The GG embryos were also generated. The zygotic genome was successfully activated in both the AG and GG embryos. DNA methylome analysis showed that the GG blastocysts partially retain the oocyte transcription-dependent methylation pattern, whereas the AG blastocyst methylome showed more extensive demethylation. The methylation states of most known imprinted differentially methylated regions (DMRs) were recapitulated in the AG and GG blastocysts. Novel candidate imprinted DMRs were also identified. The production of uniparental human embryos followed by transcriptome and methylome analysis is valuable for identifying parental contributions and epigenome memory transitions during early human development.

Published

2021

6. Chromatin analysis in human early development reveals epigenetic transition during ZGA

Author

Wu, Jingyi, Xu, Jiawei, Liu, Bofeng, Yao, Guidong, Wang, Peizhe, Lin, Zili, Huang, Bo, Wang, Xuepeng, Li, Tong, Shi, Senlin, Zhang, Nan, Duan, Fuyu, Ming, Jia, Zhang, Xiangyang, Niu, Wenbin, Song, Wenyan, Jin, Haixia, Guo, Yihong, Dai, Shanjun, Hu, Linli, Fang, Lanlan, Wang, Qiujun, Li, Yuanyuan, Li, Wei, Na, Jie, Xie, Wei, and Sun, Yingpu

Abstract

Upon fertilization, drastic chromatin reorganization occurs during preimplantation development1 . However, the global chromatin landscape and its molecular dynamics in this period remain largely unexplored in humans. Here we investigate chromatin states in human preimplantation development using an improved assay for transposase-accessible chromatin with high-throughput sequencing (ATAC-seq)2 . We find widespread accessible chromatin regions in early human embryos that overlap extensively with putative cis-regulatory sequences and transposable elements. Integrative analyses show both conservation and divergence in regulatory circuitry between human and mouse early development, and between human pluripotency in vivo and human embryonic stem cells. In addition, we find widespread open chromatin regions before zygotic genome activation (ZGA). The accessible chromatin loci are readily found at CpG-rich promoters. Unexpectedly, many others reside in distal regions that overlap with DNA hypomethylated domains in human oocytes and are enriched for transcription factor-binding sites. A large portion of these regions then become inaccessible after ZGA in a transcription-dependent manner. Notably, such extensive chromatin reorganization during ZGA is conserved in mice and correlates with the reprogramming of the non-canonical histone mark H3K4me3, which is uniquely linked to genome silencing3–5. Taken together, these data not only reveal a conserved principle that underlies the chromatin transition during mammalian ZGA, but also help to advance our understanding of epigenetic reprogramming during human early development and in vitro fertilization. By applying an optimized ATAC-seq protocol to human early embryos, distinct accessible chromatin landscapes are found before and after zygotic genome activation, revealing a marked epigenetic transition during zygotic genome activation and putative regulatory elements wiring human early development.

Published

2018

7. In Vitro Activation of Follicles and Fresh Tissue Auto-transplantation in Primary Ovarian Insufficiency Patients

Author

Zhai, Jun, Yao, Guidong, Dong, Fangli, Bu, Zhiqin, Cheng, Yuan, Sato, Yorino, Hu, Linli, Zhang, Yingying, Wang, Jingyuan, Dai, Shanjun, Li, Jing, Sun, Jing, Hsueh, Aaron J., Kawamura, Kazuhiro, and Sun, Yingpu

Abstract

Context:Recently, two patients with primary ovarian insufficiency (POI) delivered healthy babies after in vitro activation (IVA) treatment followed by auto-transplantation of frozen-thawed ovarian tissues.Objective:This study sought to report the first case of live birth after IVA treatment following fresh ovarian tissue grafting in patients with POI, together with monitoring of follicle development and serum hormonal changes.Design:This was a prospective observational cohort study.Setting:We performed IVA treatment in 14 patients with POI with mean age of 29 years, mean duration since last menses of 3.8 years, and average basal FSH level of 94.5 mIU/mL.Interventions:Prior to IVA treatment, all patients received routine hormonal treatments with no follicle development. We removed one ovary from patients with POI and treated them with Akt stimulators. We improved upon early procedures by grafting back fresh tissues using a simplified protocol.Main Outcome Measures:In six of the 14 patients (43%), a total of 15 follicle development waves were detected, and four patients had successful oocyte retrieval to yield six oocytes. For two patients showing no spontaneous follicle growth, human menopausal gonadotropin treatment induced follicle growth at 6–8 months after grafting. After vitro fertilization of oocyte retrieved, four early embryos were derived. Following embryo transfer, one patient became pregnant and delivered a healthy baby boy, with three other embryos under cryopreservation.Conclusion:IVA technology can effectively activate residual follicles in some patients with POI and allow them to conceive their own genetic offspring. IVA may also be useful for treating patients with ovarian dysfunction including aging women and cancer survivors.

Published

2016

8. Recombinant luteinizing hormone priming in early follicular phase for women undergoing in vitrofertilization: Systematic review and meta-analysis

Author

Hu, Linli, Bu, Zhiqin, Wang, Keyan, and Sun, Yingpu

Abstract

Objectives To investigate the effect of recombinant human luteinizing hormone supplementation (rLH priming) during the early follicular phase on in vitrofertilization (IVF) and intracytoplasmic sperm injection (ICSI) outcomes.Methods In order to evaluate available evidence regarding the efficacy of rLH priming in IVF/ICSI procedures, a systematic review and meta-analysis was preformed. Searches were conducted on MEDLINE®, EMBASE and the Cochrane Database of Clinical Trials without language limitation, but were restricted to randomized controlled trials (RCTs).Results Three RCTs including 346 patients were included in this meta-analysis, which demonstrated that rLH priming did not increase ongoing pregnancy rate. Although less recombinant follicle-stimulating hormone (rFSH) was required and the oestradiol level was higher on the day of human chorionic gonadotropin administration in the rLH priming group, the numbers of oocytes retrieved and embryos produced were comparable between patients treated with rLH priming and those treated with rFSH alone.Conclusions This systematic review and meta-analysis has demonstrated that at present there is insufficient evidence that patients undergoing IVF/ICSI may benefit from rLH priming during the early follicular phase.

Published

2014

9. Dynamic DNA 5-hydroxylmethylcytosine and RNA 5-methycytosine Reprogramming During Early Human Development

Author

Han, Xiao, Guo, Jia, Wang, Mengke, Zhang, Nan, Ren, Jie, Yang, Ying, Chi, Xu, Chen, Yusheng, Yao, Huan, Zhao, Yong-Liang, Yang, Yun-Gui, Sun, Yingpu, and Xu, Jiawei

Abstract

After implantation, complex and highly specialized molecular events render functionally distinct organ formation, whereas how the epigenome shapes organ-specific development remains to be fully elucidated. Here, nano-hmC-Seal, RNA bisulfite sequencing (RNA-BisSeq), and RNA sequencing (RNA-Seq) were performed, and the first multilayer landscapes of DNA 5-hydroxymethylcytosine (5hmC) and RNA 5-methylcytosine (m5C) epigenome were obtained in the heart, kidney, liver, and lung of the human foetuses at 13–28 weeks with 123 samples in total. We identified 70,091 and 503 organ-stage-specific differentially hydroxymethylated regions (DhMRs) and m5C-modified mRNAs, respectively. The key transcription factors (TFs), T-box transcription factor 20 (TBX20), paired box protein pax-8 (PAX8), krueppel-like factor 1 (KLF1), transcription factor 21 (TCF21), and CCAAT enhancer binding protein beta (CEBPB), specifically contribute to the formation of distinct organs at different stages. Additionally, 5hmC-enriched Alu elements may participate in the regulation of expression of TF-targeted genes. Our integrated studies revealed a putative essential link between DNA modification and RNA methylation, and illustrate the epigenetic maps during human foetal organogenesis, which provide a foundation for understanding the in-depth epigenetic mechanisms for early development and birth defects.

Published

2022

10. Publisher Correction: Chromatin analysis in human early development reveals epigenetic transition during ZGA

Author

Wu, Jingyi, Xu, Jiawei, Liu, Bofeng, Yao, Guidong, Wang, Peizhe, Lin, Zili, Huang, Bo, Wang, Xuepeng, Li, Tong, Shi, Senlin, Zhang, Nan, Duan, Fuyu, Ming, Jia, Zhang, Xiangyang, Niu, Wenbin, Song, Wenyan, Jin, Haixia, Guo, Yihong, Dai, Shanjun, Hu, Linli, Fang, Lanlan, Wang, Qiujun, Li, Yuanyuan, Li, Wei, Na, Jie, Xie, Wei, and Sun, Yingpu

Abstract

In this Letter, the ‘Open chromatin’ label in Fig. 4a should have been centred above the first three columns, and the black horizontal line underneath the label should have been removed. In addition, there should have been a vertical black line between the last two sets of panels for consistency. Minor changes have also been made to Fig. 1 and to the legend of Fig. 3. These errrors have been corrected online, and see Supplementary Information to the accompanying Amendment for the original Fig. 4.

Published

2018