Your search keyword '"Yuan-Jing Zou"' showing total 7 results

1. Age‐related SUMOylation of PLK1 is essential to meiosis progression in mouse oocytes

Author

Xiao‐Long Mo, Feng Liu, Chun‐Hua Xing, Meng‐Meng Shan, Bo Yao, Qi‐Qi Sun, Yuan‐Jing Zou, Kun‐Huan Zhang, Jun Tan, Shao‐Chen Sun, and Yan‐Ping Ren

Subjects

Physiology, Clinical Biochemistry, Cell Biology

Abstract

Polo like kinase 1 (PLK1) is a protein kinase involved in regulating the spindle assembly and cell cycle control in mammalian oocytes. SUMOylation, one way of post-translational modification, regulates oocyte meiosis by controlling several substrates. However, the relation between PLK1 and SUMOylation in oocytes is still unknown. In this study, we investigated that whether PLK1 was modified by SUMOylation in oocytes and its potential relationship with age-related meiotic abnormalities. We showed that PLK1 had colocalization and protein interaction with Small Ubiquitin-Like Modifier (SUMO)-1 and SUMO-2/3 in mouse oocytes, indicating that PLK1 could be modified by SUMO-1 and SUMO-2/3. Overexpression of PLK1 SUMOylation site mutants PLK1

Published

2022

2. Kinesin KIF15 regulates tubulin acetylation and spindle assembly checkpoint in mouse oocyte meiosis

Author

Yuan-Jing Zou, Meng-Meng Shan, Xiang Wan, Jing-Cai Liu, Kun-Huan Zhang, Jia-Qian Ju, Chun-Hua Xing, and Shao-Chen Sun

Subjects

Pharmacology, Kinesins, Acetylation, Cell Biology, Spindle Apparatus, Microtubules, Cellular and Molecular Neuroscience, Meiosis, Mice, Tubulin, Oocytes, Molecular Medicine, Animals, M Phase Cell Cycle Checkpoints, Molecular Biology

Abstract

Microtubule dynamics ensure multiple cellular events during oocyte meiosis, which is critical for the fertilization and early embryo development. KIF15 (also termed Hklp2) is a member of kinesin-12 family motor proteins, which participates in Eg5-related bipolar spindle formation in mitosis. In present study, we explored the roles of KIF15 in mouse oocyte meiosis. KIF15 expressed during oocyte maturation and localized with microtubules. Depletion or inhibition of KIF15 disturbed meiotic cell cycle progression, and the oocytes which extruded the first polar body showed a high aneuploidy rate. Further analysis showed that disruption of KIF15 did not affect spindle morphology but resulted in chromosome misalignment. This might be due to the reduced stability of the K-fibers, which further induced the loss of kinetochore-microtubule attachment and activated spindle assembly checkpoint, showing with the failed release of Bub3 and BubR1. Based on mass spectroscopy analysis and coimmunoprecipitation data we showed that KIF15 was responsible for recruiting HDAC6, NAT10 and SIRT2 to maintain the acetylated tubulin level, which further affected tubulin acetylation for microtubule stability. Taken together, these results suggested that KIF15 was essential for the microtubule acetylation and cell cycle control during mouse oocyte meiosis.

Published

2022

3. Kinesin motor KIFC1 is required for tubulin acetylation and actin-dependent spindle migration in mouse oocyte meiosis

Author

Meng-Meng Shan, Yuan-Jing Zou, Zhen-Nan Pan, Hao-Lin Zhang, Yi Xu, Jia-Qian Ju, and Shao-Chen Sun

Subjects

Mammals, Kinesins, Acetylation, Spindle Apparatus, macromolecular substances, beta Karyopherins, Actins, Meiosis, Mice, Tubulin, Oocytes, Animals, Molecular Biology, Developmental Biology

Abstract

Mammalian oocyte maturation is a unique asymmetric division, which is mainly because of actin-based spindle migration to the cortex. In the present study, we report that a kinesin motor KIFC1, which is associated with microtubules for the maintenance of spindle poles in mitosis, is also involved in actin dynamics in murine oocyte meiosis, co-localizing with microtubules during mouse oocyte maturation. Depletion of KIFC1 caused the failure of polar body extrusion, and we found that meiotic spindle formation and chromosome alignment were disrupted. This might be because of the effects of KIFC1 on HDAC6 and NAT10-based tubulin acetylation, which further affected microtubule stability. Mass spectroscopy analysis revealed that KIFC1 also associated with several actin nucleation factors and we found that KIFC1 was essential for the distribution of actin filaments, which further affected spindle migration. Depletion of KIFC1 leaded to aberrant expression of formin 2 and the ARP2/3 complex, and endoplasmic reticulum distribution was also disturbed. Exogenous KIFC1 mRNA supplement could rescue these defects. Taken together, as well as its roles in tubulin acetylation, our study reported a previously undescribed role of kinesin KIFC1 on the regulation of actin dynamics for spindle migration in mouse oocytes.

Published

2022

4. Exposure to acrylamide induces zygotic genome activation defects of mouse embryos

Author

Si-Le Wu, Jia-Qian Ju, Yi-Ming Ji, Hao-Lin Zhang, Yuan-Jing Zou, and Shao-Chen Sun

Subjects

General Medicine, Toxicology, Food Science

Published

2023

5. RAB14 GTPase is essential for actin‐based asymmetric division during mouse oocyte maturation

Author

Zhen-Nan Pan, Yuan-Jing Zou, Yi Xu, Jia-Qian Ju, Meng-Hao Pan, Hong-Hui Wang, Meng-Meng Shan, and Shao-Chen Sun

Subjects

Cytoplasm, Endosome, Mice, Polar body, symbols.namesake, Oogenesis, medicine, Animals, Phosphorylation, oocyte, Mice, Inbred ICR, rho-Associated Kinases, Chemistry, Endoplasmic reticulum, Original Articles, spindle, Cell Biology, General Medicine, Golgi apparatus, Oocyte, Actins, Cell biology, Meiosis, medicine.anatomical_structure, rab GTP-Binding Proteins, Oocytes, symbols, Spindle organization, Original Article, Rab, actin, Rab GTPase, Signal Transduction

Abstract

Objectives RAB14 is a member of small GTPase RAB family which localizes at the endoplasmic reticulum (ER), Golgi apparatus and endosomal compartments. RAB14 acts as molecular switches that shift between a GDP‐bound inactive state and a GTP‐bound active state and regulates circulation of vesicles between the Golgi and endosomal compartments. In present study, we investigated the roles of RAB14 during oocyte meiotic maturation. Materials and methods Microinjection with siRNA and exogenous mRNA for knock down and rescue, and immunofluorescence staining, Western blot and real‐time RT‐PCR were utilized for the study. Results Our results showed that RAB14 localized in the cytoplasm and accumulated at the cortex during mouse oocyte maturation, and it was also enriched at the spindle periphery. Depletion of RAB14 did not affect polar body extrusion but caused large polar bodies, indicating the failure of asymmetric division. We found that absence of RAB14 did not affect spindle organization but caused the spindle migration defects, and this might be due to the regulation on cytoplasmic actin assembly via the ROCK‐cofilin signalling pathway. We also found that RAB14 depletion led to aberrant Golgi apparatus distribution. Exogenous Myc‐Rab14 mRNA supplement could significantly rescue these defects caused by Rab14 siRNA injection. Conclusions Taken together, our results suggest that RAB14 affects ROCK‐cofilin pathway for actin‐based spindle migration and Golgi apparatus distribution during mouse oocyte meiotic maturation., RAB14 localized in the cytoplasm and accumulated at the cortex during mouse oocyte maturation, and it was also enriched at the spindle periphery. Depletion of RAB14 caused large polar bodies, indicating the failure of asymmetric division. Absence of RAB14 did not affect spindle organization but caused the spindle migration defects, and this might be due to the regulation on cytoplasmic actin assembly via the ROCK‐cofilin signalling pathway. We also found that RAB14 depletion led to aberrant Golgi apparatus distribution. Exogenous Myc‐Rab14 mRNA supplement could significantly rescue these defects caused by Rab14 siRNA injection. Our results suggest that RAB14 affects ROCK‐cofilin pathway for actin‐based spindle migration and Golgi apparatus distribution during mouse oocyte meiotic maturation.

Published

2021

6. Loss of Arf Guanine Nucleotide Exchange Factor GBF1 Activity Disturbs Organelle Dynamics in Mouse Oocytes

Author

Yuan-Jing Zou, Xiao-Han Li, Shao-Chen Sun, Zhen-Nan Pan, Meng-Meng Shan, and Meng-Hao Pan

Subjects

Golgi Apparatus, Endoplasmic Reticulum, 03 medical and health sciences, chemistry.chemical_compound, symbols.namesake, Mice, Organelle, medicine, Animals, Guanine Nucleotide Exchange Factors, Instrumentation, Endoplasmic Reticulum Chaperone BiP, 030304 developmental biology, 0303 health sciences, ADP-Ribosylation Factors, Endoplasmic reticulum, 030302 biochemistry & molecular biology, COPI, Brefeldin A, Golgi apparatus, Oocyte, Cell biology, medicine.anatomical_structure, chemistry, symbols, Unfolded protein response, Oocytes, Guanine nucleotide exchange factor

Abstract

GBF1 [Golgi brefeldin A (BFA) resistance factor 1] is a member of the guanine nucleotide exchange factors Arf family. GBF1 localizes at the cis-Golgi and endoplasmic reticulum (ER)-Golgi intermediate compartment where it participates in ER-Golgi traffic by assisting in the recruitment of the coat protein COPI. However, the roles of GBF1 in oocyte meiotic maturation are still unknown. In the present study, we investigated the regulatory functions of GBF1 in mouse oocyte organelle dynamics. In our results, GBF1 was stably expressed during oocyte maturation, and GBF1 localized at the spindle periphery during metaphase I. Inhibiting GBF1 activity led to aberrant accumulation of the Golgi apparatus around the spindle. This may be due to the effects of GBF1 on the localization of GM130, as GBF1 co-localized with GM130 and inhibiting GBF1 induced condensation of GM130. Moreover, the loss of GBF1 activity affected the ER distribution and induced ER stress, as shown by increased GRP78 expression. Mitochondrial localization and functions were affected, as the mitochondrial membrane potential was altered. Taken together, these results suggest that GBF1 has wide-ranging effects on the distribution and functions of Golgi apparatus, ER, and mitochondria as well as normal polar body formation in mouse oocytes.

Published

2021

7. Aflatoxin B1 exposure disrupts organelle distribution in mouse oocytes

Author

Yan-Zhe, Zhang, Qian-Han, Zhao, Hong-Wei, Duan, Yuan-Jing, Zou, Shao-Chen, Sun, and Lin-Lin, Hu

Subjects

General Neuroscience, General Medicine, General Agricultural and Biological Sciences, General Biochemistry, Genetics and Molecular Biology

Abstract

Aflatoxin B1 (AFB1) is a secondary metabolite produced by the fungus Aspergillus, which is ubiquitous in moldy grain products. Aflatoxin B1 has been reported to possess hepatotoxicity, renal toxicity, and reproductive toxicity. Previous studies have shown that AFB1 is toxic to mammalian oocytes. However, the potential toxicity of AFB1 on the organelles of mouse oocytes is unknown. In this study, we found that exposure to AFB1 significantly reduced mouse oocyte development capacity. Further analysis showed that the endoplasmic reticulum (ER) failed to accumulate around the spindle, and scattered in the cytoplasm under AFB1 exposure. Similar to the ER, the Golgi apparatus showed a uniform localization pattern following AFB1 treatment. In addition, we found that AFB1 exposure caused the condensation of lysosomes in the cytoplasm, presenting as a clustered or spindle peripheral-localization pattern, which indicated that protein modification, transport, and degradation were affected. Mitochondrial distribution was also altered by AFB1 treatment. In summary, our study showed that AFB1 exposure had toxic effects on the distribution of mouse oocyte organelles, which further led to a decline in oocyte quality.

Published

2022