Yi-Xin Ye scite author profile

Yi-Xin Ye

4Publications

12Citation Statements Received

100Citation Statements Given

How they've been cited

How they cite others

136

Affiliations

Guangxi University of Chinese Medicine, Shantou University Medical College, Michigan State University

Publications

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The Role of Syncytin in Placental Angiogenesis and Fetal Growth

Wang

Zhou

et al. 2022

Front. Cell Dev. Biol.

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Background: Syncytin, a retroviral envelope protein, is specifically expressed on trophoblast cells and mediates formation of the syncytiotrophoblast through fusogenic activity. Decreased expression of Syncytin was found in fetal growth restriction placentas.Results: By generating an inducible knockout of the syncytin-a gene in mice, we show a specific disruption of placental angiogenesis with abnormal formation of two syncytiotrophoblast layers. Consistent with the defects observed in vivo, conditioned medium collected from trophoblast cells, following Syncytin-1 knockdown, contains lower expression of vascular endothelial growth factor and placental growth factor, and higher levels of soluble fms-like protein kinase-1 in BeWo and HTR-8/SVneo cells which related with suppressed PI3K/Akt/mTOR pathway, and is reduced in ability to induce tube formation by HUVECs.Conclusion: Syncytin participates in angiogenesis during placental development was first identified both in vivo and in vitro. Here, we give a new sight on understanding syncytin and pathophysiology of placenta related disease such as fetal growth restriction.

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The modulation of gap junctional communication by gossypol in various mammalian cell lines in vitro*1

Ye¹,

Bombick²,

Hirst³

et al. 1990

Fundamental and Applied Toxicology

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2.5D induced polarization forward modeling using the adaptive finite-element method

Deng³

et al. 2014

Appl. Geophys.

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DNAJC12 as a Mediator Between ESR1 and ERBB4 in Breast Carcinoma Cells

Lin

Wang

et al. 2021

Front. Oncol.

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Mutation of the DNAJC12 gene is typically associated with non-progressive Parkinsonism, but is also detectable in breast carcinoma where its contribution and mechanisms are unexplored. In breast carcinoma, ESR1 was positively correlated with DNAJC12 and ERBB4, and DNAJC12 was positively correlated with ERBB4. We used the GEO2R tool to compare differential gene expression of MCF-7 cells, following ESR1 knockdown (GEO database, E-GEOD-27473 array), and found decreased expression of DNAJC12 and ERBB4 in ESR1-silenced MCF-7 cells. The number of identical genes having correlativity with ESR1, DNAJC12, or ERBB4 was 12,165 (66.41%). These results suggest that ESR1 can promote the expression of DNAJC12 and ERBB4, and DNAJC12 can enhance the expression of ERBB4 in MCF-7 cells, implying that there may be a regulatory network among these three genes.

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Yi-Xin Ye

The Role of Syncytin in Placental Angiogenesis and Fetal Growth

The modulation of gap junctional communication by gossypol in various mammalian cell lines in vitro*1

2.5D induced polarization forward modeling using the adaptive finite-element method

DNAJC12 as a Mediator Between ESR1 and ERBB4 in Breast Carcinoma Cells

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