Your search keyword '"Zhaomin Mao"' showing total 8 results

1. TβRII Regulates the Proliferation of Metanephric Mesenchyme Cells through Six2 In Vitro.

Author

Zhaomin Mao, Zhongshi Lyu, Liyuan Huang, Qin Zhou, and Yaguang Weng

Subjects

*TRANSFORMING growth factors, *MESENCHYME, *POLYMERASE chain reaction, *IMMUNOFLUORESCENCE, *GENE regulatory networks

Abstract

The transforming growth factor-β (TGFβ) family signaling pathways play an important role in regulatory cellular networks and exert specific effects on developmental programs during embryo development. However, the function of TGFβ signaling pathways on the early kidney development remains unclear. In this work, we aim to detect the underlying role of TGFβ type II receptor (TβRII) in vitro, which has a similar expression pattern as the crucial regulator Six2 during early kidney development. Firstly, the 5-ethynyl-2′-deoxyuridine (EdU) assay showed knock down of TβRII significantly decreased the proliferation ratio of metanephric mesenchyme (MM) cells. Additionally, real-time Polymerase Chain Reaction (PCR) and Western blot together with immunofluorescence determined that the mRNA and protein levels of Six2 declined after TβRII knock down. Also, Six2 was observed to be able to partially rescue the proliferation phenotype caused by the depletion of TβRII. Moreover, bioinformatics analysis and luciferase assay indicated Smad3 could transcriptionally target Six2. Further, the EdU assay showed that Smad3 could also rescue the inhibition of proliferation caused by the knock down of TβRII. Taken together, these findings delineate the important function of the TGFβ signaling pathway in the early development of kidney and TβRII was shown to be able to promote the expression of Six2 through Smad3 mediating transcriptional regulation and in turn activate the proliferation of MM cells. [ABSTRACT FROM AUTHOR]

Published

2017

2. Six2 Is a Coordinator of LiCl-Induced Cell Proliferation and Apoptosis.

Author

Jianing Liu, Pan Ju, Yuru Zhou, Ya Zhao, Yajun Xie, Yaoshui Long, Yuping Gu, Dongsheng Ni, Zhongshi Lyv, Zhaomin Mao, Jin Hao, Yiman Li, Qianya Wan, Quist Kanyomse, Yamin Liu, Yue Xiang, Ruoli Wang, Xiangling Chen, Junman Zhang, and Xihan Liu

Subjects

*CELL proliferation, *APOPTOSIS, *PROGENITOR cells, *NEPHRONS, *LUCIFERASES, *REVERSE transcriptase polymerase chain reaction, *FLOW cytometry

Abstract

The metanephric mesenchyme (MM) cells are a subset of kidney progenitor cells and play an essential role in mesenchymal-epithelial transition (MET), the key step of nephron generation. Six2, a biological marker related to Wnt signaling pathway, promotes the proliferation, inhibits the apoptosis and maintains the un-differentiation of MM cells. Besides, LiCl is an activator of Wnt signaling pathway. However, the role of LiCl in cellular regulation of MM cells remains unclear, and the relationship between LiCl and Six2 in this process is also little known. Here, we performed EdU assay and flow cytometry assay to, respectively, detect the proliferation and apoptosis of MM cells treated with LiCl of increasing dosages. In addition, reverse transcription-PCR (RT-PCR) and Western-blot were conducted to measure the expression of Six2 and some maker genes of Wnt and bone-morphogenetic-protein (BMP) signaling pathway. Furthermore, luciferase assay was also carried out to detect the transcriptional regulation of Six2. Then we found LiCl promoted MM cell proliferation at low-concentration (10, 20, 30, and 40 mM). The expression of Six2 was dose-dependently increased in low-concentration (10, 20, 30, and 40 mM) at both mRNA and protein level. In addition, both of cell proliferation and Six2 expression in MM cells declined when dosage reached high-concentration (50 mM). However, Six2 knock-down converted the proliferation reduction at 50 mM. Furthermore, Six2 deficiency increased the apoptosis of MM cells, compared with negative control cells at relative LiCl concentration. However, the abnormal rise of apoptosis at 30 mM of LiCl concentration implies that it might be the reduction of GSK3β that increased cell apoptosis. Together, these demonstrate that LiCl can induce the proliferation and apoptosis of MM cells coordinating with Six2. [ABSTRACT FROM AUTHOR]

Published

2016

3. Zeb1 Is a Potential Regulator of Six2 in the Proliferation, Apoptosis and Migration of Metanephric Mesenchyme Cells.

Author

Yuping Gu, Ya Zhao, Yuru Zhou, Yajun Xie, Pan Ju, Yaoshui Long, Jianing Liu, Dongsheng Ni, Fen Cao, Zhongshi Lyu, Zhaomin Mao, Jin Hao, Yiman Li, Qianya Wan, Kanyomse, Quist, Yamin Liu, Die Ren, Yating Ning, Xiaofeng Li, and Qin Zhou

Subjects

*PROGENITOR cells, *NEPHRONS, *CELL proliferation, *MESENCHYMAL stem cells, *APOPTOSIS, *CELL migration

Abstract

Nephron progenitor cells surround around the ureteric bud tips (UB) and inductively interact with the UB to originate nephrons, the basic units of renal function. This process is determined by the internal balance between self-renewal and consumption of the nephron progenitor cells, which is depending on the complicated regulation networks. It has been reported that Zeb1 regulates the proliferation of mesenchymal cells in mouse embryos. However, the role of Zeb1 in nephrons generation is not clear, especially in metanephric mesenchyme (MM). Here, we detected cell proliferation, apoptosis and migration in MM cells by EdU assay, flow cytometry assay and wound healing assay, respectively. Meanwhile, Western and RT-PCR were used to measure the expression level of Zeb1 and Six2 in MM cells and developing kidney. Besides, the dual-luciferase assay was conducted to study the molecular relationship between Zeb1 and Six2. We found that knock-down of Zeb1 decreased cell proliferation, migration and promoted cell apoptosis in MM cells and Zeb1 overexpression leaded to the opposite data. Western-blot and RT-PCR results showed that knock-down of Zeb1 decreased the expression of Six2 in MM cells and Zeb1 overexpression contributed to the opposite results. Similarly, Zeb1 promoted Six2 promoter reporter activity in luciferase assays. However, double knock-down of Zeb1 and Six2 did not enhance the apoptosis of MM cells compared with control cells. Nevertheless, double silence of Zeb1 and Six2 repressed cell proliferation. In addition, we also found that Zeb1 and Six2 had an identical pattern in distinct developing phases of embryonic kidney. These results indicated that there may exist a complicated regulation network between Six2 and Zeb1. Together, we demonstrate Zeb1 promotes proliferation and apoptosis and inhibits the migration of MM cells, in association with Six2. [ABSTRACT FROM AUTHOR]

Published

2016

4. EIYMNVPV Motif is Essential for A1CF Nucleus Localization and A1CF (-8aa) Promotes Proliferation of MDA-MB-231 Cells via Up-Regulation of IL-6.

Author

Li Zhou, Jin Hao, Yue Yuan, Rui Peng, Honglian Wang, Dongsheng Ni, Yuping Gu, Liyuan Huang, Zhaomin Mao, Zhongshi Lyu, Yao Du, Zhicheng Liu, Yiman Li, Pan Ju, Yaoshui Long, Jianing Liu, and Qin Zhou

Subjects

*CELL proliferation, *CELLULAR control mechanisms, *RNA editing, *CYTOPLASM, *BREAST cancer treatment

Abstract

Apobec-1 complementation factor (A1CF) is a heterogeneous nuclear ribonuceloprotein (hnRNP) and mediates apolipoprotein-B mRNA editing. A1CF can promote the regeneration of the liver by post-transcriptionally stabilizing Interleukin-6 (IL-6) mRNA. It also contains two transcriptional variants-A1CF64 and A1CF65, distinguished by the appearance of a 24-nucleotide motif which contributes to the corresponding eight-amino acid motif of EIYMNVPV. For the first time, we demonstrated that the EIYMNVPV motif was essential for A1CF nucleus localization, A1CF deficient of the EIYMNVPV motif, A1CF (-8aa) showed cytoplasm distribution. More importantly, we found that A1CF (-8aa), but not its full-length counterpart, can promote proliferation of MDA-MB-231 cells accompanied with increased level of IL-6 mRNA. Furthermore, silencing of IL-6 attenuated A1CF (-8aa)-induced proliferation in MDA-MB-231 cells. In conclusion, notably, these findings suggest that A1CF (-8aa) promoted proliferation of MDA-MB-231 cells in vitro viewing IL-6 as a target. Thus, the EIYMNVPV motif could be developed as a potential target for basal-like breast cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2016

5. Apobec-1 Complementation Factor (A1CF) Inhibits Epithelial-Mesenchymal Transition and Migration of Normal Rat Kidney Proximal Tubular Epithelial Cells.

Author

Liyuan Huang, Honglian Wang, Yuru Zhou, Dongsheng Ni, Yanxia Hu, Yaoshui Long, Jianing Liu, Rui Peng, Li Zhou, Zhicheng Liu, Zhongshi Lyu, Zhaomin Mao, Jin Hao, Yiman Li, and Qin Zhou

Subjects

*EPITHELIAL cells, *MESENCHYMAL stem cells, *APOLIPOPROTEIN B, *SMALL intestine, *NUCLEOPROTEINS, *MESSENGER RNA

Abstract

Apobec-1 complementation factor (A1CF) is a member of the heterogeneous nuclear ribonucleoproteins (hnRNP) family, which participates in site-specific posttranscriptional RNA editing of apolipoprotein B (apoB) transcript. The posttranscriptional editing of apoB mRNA by A1CF in the small intestine is required for lipid absorption. Apart from the intestine, A1CF mRNA is also reported to be highly expressed in the kidneys. However, it is remained unknown about the functions of A1CF in the kidneys. The aim of this paper is to explore the potential functions of A1CF in the kidneys. Our results demonstrated that in C57BL/6 mice A1CF was weakly expressed in embryonic kidneys from E15.5dpc while strongly expressed in mature kidneys after birth, and it mainly existed in the tubules of inner cortex. More importantly, we identified A1CF negatively regulated the process of epithelial-mesenchymal transition (EMT) in kidney tubular epithelial cells. Our results found ectopic expression of A1CF up-regulated the epithelial markers E-cadherin, and down-regulated the mesenchymal markers vimentin and α-smooth muscle actin (α-SMA) in NRK52e cells. In addition, knockdown of A1CF enhanced EMT contrary to the overexpression effect. Notably, the two A1CF variants led to the similar trend in the EMT process. Taken together, these data suggest that A1CF may be an antagonistic factor to the EMT process of kidney tubular epithelial cells. [ABSTRACT FROM AUTHOR]

Published

2016

6. MicroRNA-148b enhances proliferation and apoptosis in human renal cancer cells via directly targeting MAP3K9.

Author

FANG NIE, TIANMING LIU, LIANG ZHONG, XIANGGUI YANG, YUNHONG LIU, HONGWEI XIA, XIAOQIANG LIU, XIAOYAN WANG, ZHICHENG LIU, LI ZHOU, ZHAOMIN MAO, QIN ZHOU, and TINGMEI CHEN

Subjects

*MICRORNA, *APOPTOSIS, *CELL proliferation, *CANCER cells, *GENE expression, *GROWTH factors, *CELL differentiation, *TUMOR suppressor proteins

Abstract

Increasing evidence revealed that miRNAs, the vital regulators of gene expression, are involved in various cellular processes, including cell growth, differentiation, apoptosis and progression. In addition, miRNAs act as oncogenes and/or tumor suppressors. The present study aimed to verify the potential roles of miR148b in human renal cancer cells. miR-148b was found to be downregulated in human renal cancel tissues and human renal cancer cell lines. Functional studies demonstrated that plasmid-mediated overexpression of miR-148b promoted cell proliferation, increased the S-phase population of the cell cycle and enhanced apoptosis in the 786-O and OS-RC-2 renal cancer cell lines, while it did not appear to affect the total number of viable cells according to a Cell Counting Kit-8 assay. Subsequently, a luciferase reporter assay verified that miR148b directly targeted mitogen-activated protein kinase (MAPK) kinase kinase 9 (MAP3K9), an upstream activator of MAPK kinase/c-Jun N-terminal kinase (JNK) signaling, suppressing the protein but not the mRNA levels. Furthermore, western blot analysis indicated that overexpression of miR148b in renal cancer cells inhibited MAPK/JNK signaling by decreasing the expression of phosphorylated (p)JNK. In addition, overexpression of MAP3K9 and pJNK was detected in clinical renal cell carcinoma specimens compared with that in their normal adjacent tissues. The present study therefore suggested that miR-148b exerts an oncogenic function by enhancing the proliferation and apoptosis of renal cancer cells by inhibiting the MAPK/JNK pathway. [ABSTRACT FROM AUTHOR]

Published

2016

7. MiR542-3p Regulates the Epithelial-Mesenchymal Transition by Directly Targeting BMP7 in NRK52e.

Author

Zhicheng Liu, Yuru Zhou, Yue Yuan, Fang Nie, Rui Peng, Qianyin Li, Zhongshi Lyu, Zhaomin Mao, Liyuan Huang, Li Zhou, Yiman Li, Jing Hao, Dongsheng Ni, Qianni Jin, Yaoshui Long, Pan Ju, Wen Yu, Jianing Liu, Yanxia Hu, and Qin Zhou

Subjects

*MICRORNA, *EPITHELIAL cells, *MESENCHYMAL stem cells, *RENAL fibrosis, *BONE morphogenetic proteins

Abstract

Accumulating evidence demonstrated that miRNAs are highly involved in kidney fibrosis and Epithelial-Eesenchymal Transition (EMT), however, the mechanisms of miRNAs in kidney fibrosis are poorly understood. In this work, we identified that miR542-3p could promote EMT through down-regulating bone morphogenetic protein 7 (BMP7) expression by targeting BMP7 31UTR. Firstly, real-time PCR results showed that miR542-3p was significantly up-regulated in kidney fibrosis in vitro and in vivo. Moreover, Western blot results demonstrated that miR542-3p may promote EMT in the NRK52e cell line. In addition, we confirmed that BMP7, which played a crucial role in anti-kidney fibrosis and suppressed the progression of EMT, was a target of miR542-3p through Dual-Luciferase reporter assay, as did Western blot analysis. The effects of miR542-3p on regulating EMT could also be suppressed by transiently overexpressing BMP7 in NRK52e cells. Taken together, miR542-3p may be a critical mediator of the induction of EMT via directly targeting BMP7. [ABSTRACT FROM AUTHOR]

Published

2015

8. MiR-30a Inhibits the Epithelial--Mesenchymal Transition of Podocytes through Downregulation of NFATc3.

Author

Rui Peng, Li Zhou, Yuru Zhou, Ya Zhao, Qianyin Li, Dongsheng Ni, Yanxia Hu, Yaoshui Long, Jianing Liu, Zhongshi Lyu, Zhaomin Mao, Yue Yuan, Liyuan Huang, Hui Zhao, Ge Li, and Qin Zhou

Subjects

*MICRORNA, *KIDNEY diseases, *BIOMARKERS, *TRANSCRIPTION factors, *FIBRONECTINS, *COLLAGEN

Abstract

MicroRNAs (miRNAs) possess an important regulating effect among numerous renal diseases, while their functions in the process of epithelial-to-mesenchymal transition (EMT) after podocyte injury remain unclear. The purpose of our study is to identify the potential functions of mi-30a in EMT of podocytes and explore the underlying mechanisms of mi-30a in the impaired podocytes. The results revealed that downregulation of mi-30a in podocyte injury animal models and patients, highly induced the mesenchymal markers of EMT including Collagen I, Fibronectin and Snail. Furthermore, overexpression of mi-30a enhances epithelial markers (E-cadherin) but diminished mesenchymal markers (Collagen I, Fibronectin and Snail) in podocytes. In addition, we established mi-30a target NFATc3, an important transcription factor of Non-canonical Wnt signaling pathway. More importantly, our findings demonstrated that the augmentation of mi-30a level in podocytes inhibits the nuclear translocation of NFATc3 to protect cytoskeleton disorder or rearrangement. In summary, we uncovered the protective function of miR30a targeting NFATc3 in the regulation of podocyte injury response to EMT. [ABSTRACT FROM AUTHOR]

Published

2015