Liu Bigang相关文献与解析，生知库 | 链接生命科学的每一步

Zhou Jujun, Chen Qin, Ren Ren, Yang Jie, Liu Bigang, Horton John R, Chang Caleb, Li Chuxuan, Maksoud Leora, Yang Yifei, Rotili Dante, Jain Abhinav K, Zhang Xing, Blumenthal Robert M, Chen Taiping, Gao Yang, Valente Sergio, Mai Antonello, Cheng Xiaodong

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发表日期：2024

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The ZBTB24-CDCA7 axis regulates HELLS enrichment at centromeric satellite repeats to facilitate DNA methylation

ZBTB24-CDCA7轴调控着丝粒卫星重复序列处的HELLS富集，从而促进DNA甲基化。

期刊:Protein & Cell

影响因子:12.8

doi:10.1007/s13238-019-00682-w

Hardikar, Swanand; Ying, Zhengzhou; Zeng, Yang; Zhao, Hongbo; Liu, Bigang; Veland, Nicolas; McBride, Kevin; Cheng, Xiaodong; Chen, Taiping

Overactivation of the NF-κB pathway impairs molar enamel formation

NF-κB通路过度激活会损害磨牙釉质的形成。

期刊:Oral Diseases

影响因子:2.9

doi:10.1111/odi.13384

Yamada, Akane; Kawasaki, Maiko; Miake, Yasuo; Yamada, Yurie; Blackburn, James; Kawasaki, Katsushige; Trakanant, Supaluk; Nagai, Takahiro; Nihara, Jun; Kudo, Takehisa; Meguro, Fumiya; Schmidt-Ullrich, Ruth; Liu, Bigang; Hu, Yinling; Page, Angustias; Ramírez, Ángel; Sharpe, Paul T; Maeda, Takeyasu; Takagi, Ritsuo; Ohazama, Atsushi

DNMT3L facilitates DNA methylation partly by maintaining DNMT3A stability in mouse embryonic stem cells.

DNMT3L 通过维持小鼠胚胎干细胞中 DNMT3A 的稳定性来促进 DNA 甲基化

期刊:Nucleic Acids Research

影响因子:13.1

doi:10.1093/nar/gky947

Veland Nicolas, Lu Yue, Hardikar Swanand, Gaddis Sally, Zeng Yang, Liu Bigang, Estecio Marcos R, Takata Yoko, Lin Kevin, Tomida Mary W, Shen Jianjun, Saha Debapriya, Gowher Humaira, Zhao Hongbo, Chen Taiping

Transgenic overexpression of NanogP8 in the mouse prostate is insufficient to initiate tumorigenesis but weakly promotes tumor development in the Hi-Myc mouse model

在小鼠前列腺中转基因过表达NanogP8不足以启动肿瘤发生，但能微弱地促进Hi-Myc小鼠模型中的肿瘤发展。

期刊:Oncotarget

影响因子:

doi:10.18632/oncotarget.17186

Liu, Bigang; Gong, Shuai; Li, Qiuhui; Chen, Xin; Moore, John; Suraneni, Mahipal V; Badeaux, Mark D; Jeter, Collene R; Shen, Jianjun; Mehmood, Rashid; Fan, Qingxia; Tang, Dean G

NANOG reprograms prostate cancer cells to castration resistance via dynamically repressing and engaging the AR/FOXA1 signaling axis

NANOG通过动态抑制和激活AR/FOXA1信号通路，将前列腺癌细胞重编程为去势抵抗细胞。

期刊:Cell Discovery

影响因子:12.5

doi:10.1038/celldisc.2016.41

Jeter, Collene R; Liu, Bigang; Lu, Yue; Chao, Hsueh-Ping; Zhang, Dingxiao; Liu, Xin; Chen, Xin; Li, Qiuhui; Rycaj, Kiera; Calhoun-Davis, Tammy; Yan, Li; Hu, Qiang; Wang, Jianmin; Shen, Jianjun; Liu, Song; Tang, Dean G

miR-199a-3p targets stemness-related and mitogenic signaling pathways to suppress the expansion and tumorigenic capabilities of prostate cancer stem cells.

miR-199a-3p 靶向干细胞相关和促有丝分裂信号通路，以抑制前列腺癌干细胞的扩增和致瘤能力

期刊:Oncotarget

影响因子:

doi:10.18632/oncotarget.10652

Liu Ruifang, Liu Can, Zhang Dingxiao, Liu Bigang, Chen Xin, Rycaj Kiera, Jeter Collene, Calhoun-Davis Tammy, Li Yandong, Yang Tao, Wang Junchen, Tang Dean G

Regulation of NANOG in cancer cells

癌细胞中NANOG的调控

期刊:Molecular Carcinogenesis

影响因子:3.2

doi:10.1002/mc.22340

Gong, Shuai; Li, Qiuhui; Jeter, Collene R; Fan, Qingxia; Tang, Dean G; Liu, Bigang

miRNA-128 suppresses prostate cancer by inhibiting BMI-1 to inhibit tumor-initiating cells

miRNA-128通过抑制BMI-1来抑制肿瘤起始细胞，从而抑制前列腺癌。

期刊:Cancer Research

影响因子:16.6

doi:10.1158/0008-5472.CAN-14-0404

Jin, Min; Zhang, Tao; Liu, Can; Badeaux, Mark A; Liu, Bigang; Liu, Ruifang; Jeter, Collene; Chen, Xin; Vlassov, Alexander V; Tang, Dean G

Dissociated primary human prostate cancer cells coinjected with the immortalized Hs5 bone marrow stromal cells generate undifferentiated tumors in NOD/SCID-γ mice

将分离的原代人前列腺癌细胞与永生化的Hs5骨髓基质细胞共同注射到NOD/SCID-γ小鼠体内，可形成未分化肿瘤。

期刊:PLoS One

影响因子:2.6

doi:10.1371/journal.pone.0056903

Chen, Xin; Liu, Bigang; Li, Qiuhui; Honorio, Sofia; Liu, Xin; Liu, Can; Multani, Asha S; Calhoun-Davis, Tammy; Tang, Dean G

Quinoline-based compounds can inhibit diverse enzymes that act on DNA.

喹啉类化合物可以抑制多种作用于 DNA 的酶

The ZBTB24-CDCA7 axis regulates HELLS enrichment at centromeric satellite repeats to facilitate DNA methylation

ZBTB24-CDCA7轴调控着丝粒卫星重复序列处的HELLS富集，从而促进DNA甲基化。

Overactivation of the NF-κB pathway impairs molar enamel formation

NF-κB通路过度激活会损害磨牙釉质的形成。

DNMT3L facilitates DNA methylation partly by maintaining DNMT3A stability in mouse embryonic stem cells.

DNMT3L 通过维持小鼠胚胎干细胞中 DNMT3A 的稳定性来促进 DNA 甲基化

Transgenic overexpression of NanogP8 in the mouse prostate is insufficient to initiate tumorigenesis but weakly promotes tumor development in the Hi-Myc mouse model

在小鼠前列腺中转基因过表达NanogP8不足以启动肿瘤发生，但能微弱地促进Hi-Myc小鼠模型中的肿瘤发展。

NANOG reprograms prostate cancer cells to castration resistance via dynamically repressing and engaging the AR/FOXA1 signaling axis

NANOG通过动态抑制和激活AR/FOXA1信号通路，将前列腺癌细胞重编程为去势抵抗细胞。

miR-199a-3p targets stemness-related and mitogenic signaling pathways to suppress the expansion and tumorigenic capabilities of prostate cancer stem cells.

miR-199a-3p 靶向干细胞相关和促有丝分裂信号通路，以抑制前列腺癌干细胞的扩增和致瘤能力

Regulation of NANOG in cancer cells

癌细胞中NANOG的调控

miRNA-128 suppresses prostate cancer by inhibiting BMI-1 to inhibit tumor-initiating cells

miRNA-128通过抑制BMI-1来抑制肿瘤起始细胞，从而抑制前列腺癌。

Dissociated primary human prostate cancer cells coinjected with the immortalized Hs5 bone marrow stromal cells generate undifferentiated tumors in NOD/SCID-γ mice

将分离的原代人前列腺癌细胞与永生化的Hs5骨髓基质细胞共同注射到NOD/SCID-γ小鼠体内，可形成未分化肿瘤。