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张晓涵
发布时间: 2022-04-27  浏览次数: 844

张晓涵简介

 



 

 

张晓涵,女,19926月,贵州大学副教授,韩国全南国立大学博士学位,硕士研究生导师,主要从事G蛋白偶联受体信号通路与重大疾病(神经退行性疾病、肿瘤、代谢性疾病等)相关性及机制研究。 

邮箱:xhzhang0606@126.com



20089-20126月,沈阳药科大学,生命科学与生物制ob体育平台,学士;

20128-20148月,韩国全南国立大学,ob体育平台,硕士;

20149-20188月,韩国全南国立大学,ob体育平台,博士;

20193-202111月,贵州大学,ob体育平台,校聘副教授,讲师;

202112月至今,贵州大学,ob体育平台,副教授;

  

【主持项目】

1.   国家自然科学基金,Mdm2核定位介导b-arrestin2去泛素化和诱捕GbgD3R脱敏负反馈调控机制的研究,820602632021-012024-12,在研,主持

2.   贵州省科技计划项目, 多巴胺D2受体通过调控PDK1活性介导胰岛素抵抗作用的分子机制研究,黔科合基础[2020]1Y0842020-032023-02,在研,主持

3.   贵州省普通高等学校青年科技人才成长项目,去泛素化的b-Arr2调控多巴胺D3 受体脱敏作用的分子机制研究,黔教合KY[2021]0852021-012023-12,在研,主持

4.   贵州大学引进人才科研项目,b-Arr2调节自身泛素化水平介导多巴胺D3受体脱敏作用的分子机制研究,贵大人基合字[2020] 07号,2021-012023-12,在研,主持

5.   贵州大学培育项目,Mdm2核定位介导β-arrestin2去泛素化和诱捕GbgD3R脱敏负反馈调控机制研究,贵大培育[2019]66号,2020-102023-10,在研,主持

6.   贵州省科技计划项目, 新型SHP2变构抑制剂的设计、合成及活性研究,黔科合基础[2020]1Y3932020-032023-03,在研,参与

【近期发表论文】

1.  Zhang, X., Min, X., Wang, S., Sun, N., & Kim, K. M. (2020). Mdm2-mediated ubiquitination of β-arrestin2 in the nucleus occurs in a Gβγ-and clathrin-dependent manner. Biochemical Pharmacology, 178, 114049.

2. Zhang, X., Zheng, M., & Kim, K. M. (2020). GRK2-mediated receptor phosphorylation and Mdm2-mediated β-arrestin2 ubiquitination drive clathrin-mediated endocytosis of G protein-coupled receptors. Biochemical and Biophysical Research Communications, 533(3), 383-390.

3.  Zhang, X., Min, X., Zhu, A., & Kim, K. M. (2020). A novel molecular mechanism involved in the crosstalks between homologous and PKC-mediated heterologous regulatory pathway of dopamine D2 receptor. Biochemical Pharmacology, 174, 113791.

4.  Min, X., Zhang, X.(co-first author), Sun, N., Acharya, S., & Kim, K. M. (2019). Mdm2-mediated ubiquitination of PKCβII in the nucleus mediates clathrin-mediated endocytic activity. Biochemical Pharmacology, 170, 113675.

5.  Zhang, X., Zheng, M., Sun, N., & Kim, K. M. (2018). β-Arrestin2 directly or through GRK2 inhibits PKCβII activation in a ubiquitination-dependent manner. Biochimica et Biophysica Acta (BBA)-Molecular Cell Research, 1865(1), 142-157.

6.  Zhang, X., & Kim, K. M. (2017). Multifactorial regulation of G protein-coupled receptor endocytosis. Biomolecules & therapeutics, 25(1), 26.7:

7.  Zheng, M., Zhang, X. (co-first author), Guo, S., Zhang, X., Min, C., Cheon, S. H., ... & Kim, K. M. (2016). Agonist-induced changes in RalA activities allows the prediction of the endocytosis of G protein-coupled receptors. Biochimica et Biophysica Acta (BBA)-Molecular Cell Research, 1863(1), 77-90.

8.  Zheng, M., Zhang, X. (co-first author), Sun, N., Min, C., Zhang, X., & Kim, K. M. (2016). RalA employs GRK2 and β-arrestins for the filamin A-mediated regulation of trafficking and signaling of dopamine D2 and D3 receptor. Biochimica et Biophysica Acta (BBA)-Molecular Cell Research, 1863(8), 2072-2083.

9.  Zhang, X., Sun, N., Zheng, M., & Kim, K. M. (2016). Clathrin-mediated endocytosis is responsible for the lysosomal degradation of dopamine D3 receptor. Biochemical and biophysical research communications, 476(4), 245-251.

10. Zhang, X., Choi, B. G., & Kim, K. M. (2016). Roles of dopamine D2 receptor subregions in interactions with β-Arrestin2. Biomolecules & Therapeutics, 24(5), 517.

11. Zheng, M., Zhang, X. (co-first author), Min, C., Choi, B. G., Oh, I. J., & Kim, K. M. (2016). Functional regulation of dopamine D3 receptor through interaction with PICK1. Biomolecules & Therapeutics, 24(5), 475.

12. Guo, S., Zhang, X. (co-first author), Zheng, M., Zhang, X., Min, C., Wang, Z., ... & Kim, K. M. (2015). Selectivity of commonly used inhibitors of clathrin-mediated and caveolae-dependent endocytosis of G protein–coupled receptors. Biochimica et Biophysica Acta (BBA)-Biomembranes, 1848(10), 2101-2110.

 


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