Your search keyword '"Li, Jingxia"' showing total 13 results

1. NF-κB p65 Overexpression Promotes Bladder Cancer Cell Migration via FBW7-Mediated Degradation of RhoGDIα Protein.

Author

Zhu J, Li Y, Chen C, Ma J, Sun W, Tian Z, Li J, Xu J, Liu CS, Zhang D, Huang C, and Huang H

Subjects

Animals, Cell Line, Tumor, Disease Models, Animal, Genes, Reporter, Heterografts, Humans, Mice, Mice, Knockout, Protein Binding, Protein Stability, Transcription Factor RelA metabolism, Urinary Bladder Neoplasms pathology, Cell Movement genetics, F-Box-WD Repeat-Containing Protein 7 metabolism, Gene Expression, Transcription Factor RelA genetics, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms metabolism, rho Guanine Nucleotide Dissociation Inhibitor alpha metabolism

Abstract

Background: Since invasive bladder cancer (BC) is one of the most lethal urological malignant tumors worldwide, understanding the molecular mechanisms that trigger the migration, invasion, and metastasis of BC has great significance in reducing the mortality of this disease. Although RelA/p65, a member of the NF-kappa B transcription factor family, has been reported to be upregulated in human BCs, its regulation of BC motility and mechanisms have not been explored yet., Methods: NF-κBp65 expression was evaluated in N-butyl-N-(4-hydroxybutyl)-nitrosamine (BBN)-induced high invasive BCs by immunohistochemistry staining and in human BC cell lines demonstrated by Western Blot. The effects of NF-κBp65 knockdown on BC cell migration and invasion, as well as its regulated RhoGDIα and FBW7, were also evaluated in T24T cells by using loss- and gain-function approaches. Moreover, the interaction of FBW7 with RhoGDIα was determined with immunoprecipitation assay, while critical role of ubiquitination of RhoGDIα by FBW7 was also demonstrated in the studies., Results: p65 protein was remarkably upregulated in the BBN-induced high invasive BCs and in human BC cell lines. We also observed that p65 overexpression promoted BC cell migration by inhibiting RhoGDIα expression. The regulatory effect of p65 on RhoGDIα expression is mediated by its upregulation of FBW7, which specifically interacted with RhoGDIα and promoted RhoGDIα ubiquitination and degradation. Mechanistic studies revealed that p65 stabilizing the E3 ligase FBW7 protein was mediated by its attenuating pten mRNA transcription., Conclusions: We demonstrate that p65 overexpression inhibits pten mRNA transcription, which stabilizes the protein expression of ubiquitin E3 ligase FBW7, in turn increasing the ubiquitination and degradation of RhoGDIα protein and finally promoting human BC migration. The novel identification of p65/PTEN/FBW7/RhoGDIα axis provides a significant insight into understanding the nature of BC migration, further offering a new theoretical support for cancer therapy., (Copyright © 2017 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2017

2. Molecular mechanisms involved in chemoprevention of black raspberry extracts: from transcription factors to their target genes.

Author

Lu H, Li J, Zhang D, Stoner GD, and Huang C

Subjects

Animals, Benzopyrans pharmacology, Cell Line, Cyclooxygenase 2 genetics, Epoxy Compounds pharmacology, Methanol, Mice, NF-kappa B antagonists & inhibitors, Phytotherapy, Signal Transduction drug effects, Transcription Factor AP-1 antagonists & inhibitors, Vascular Endothelial Growth Factor A genetics, Anticarcinogenic Agents pharmacology, Fruit chemistry, Gene Expression drug effects, Plant Extracts pharmacology, Rosaceae chemistry, Transcription Factors antagonists & inhibitors

Abstract

Berries have attracted attention for their chemopreventive activities in last a few years. Dietary freeze-dried blackberries have been shown to reduce esophagus and colon cancer development induced by chemical carcinogen in rodents. To elucidate molecular mechanisms involved in chemoprevention by berry extracts, we employed mouse epidermal Cl 41 cell line, a well-characterized in vitro model in tumor promotion studies. Pretreatment of Cl 41 cells with methanol-extracted blackberry fraction RO-ME resulted in a dramatical inhibition of B(a)PDE-induced activation of AP-1 and NFkB, and expression of VEGF and COX-2. The inhibitory effects of RO-ME on B(a)PDE-induced activation of AP-1 and NFkappaB appear to be mediated via inhibition of MAPKs and IkappaBalpha phosphorylation, respectively. In view of the important roles of AP-1, NFkappaB, VEGF and COX-2 in tumor promotion/progression, and VEGF and COX-2 are target of AP-1 and NFkappaB, we anticipate that the ability of black raspberries to inhibit tumor development may be mediated by impairing signal transduction pathways leading to activation of AP-1 and NFkappaB, subsequently resulting in down-regulation of VEGF and COX-2 expression. The RO-ME fraction appears to be the major fraction responsible for the inhibitory activity of black raspberries.

Published

2006

3. Transcriptome Analysis Reveals Anti-Cancer Effects of Isorhapontigenin (ISO) on Highly Invasive Human T24 Bladder Cancer Cells.

Author

Li, Alex H., Park, Sun Young, Li, Peiwei, Zhou, Chaoting, Kluz, Thomas, Li, Jingxia, Costa, Max, and Sun, Hong

Subjects

BLADDER cancer, CYTOSKELETON, RNA sequencing, ANTINEOPLASTIC agents, CANCER cells, GENE expression

Abstract

Bladder cancer, the most common malignancy of the urinary tract, has a poor overall survival rate when the tumor becomes muscle invasive. The discovery and evaluation of new alternative medications targeting high-grade muscle invasive bladder cancer (MIBC) are of tremendous importance in reducing bladder cancer mortality. Isorhapontigenin (ISO), a stilbene derivative from the Chinese herb Gnetum cleistostachyum, exhibits a strong anti-cancer effect on MIBCs. Here, we report the whole transcriptome profiling of ISO-treated human bladder cancer T24 cells. A total of 1047 differentially expressed genes (DEGs) were identified, including 596 downregulated and 451 upregulated genes. Functional annotation and pathway analysis revealed that ISO treatment induced massive changes in gene expression associated with cell movement, migration, invasion, metabolism, proliferation, and angiogenesis. Additionally, ISO treatment-activated genes involved in the inflammatory response but repressed genes involved in hypoxia signaling, glycolysis, the actin cytoskeleton, and the tumor microenvironment. In summary, our whole transcriptome analysis demonstrated a shift in metabolism and altered actin cytoskeleton in ISO-treated T24 cells, which subsequently contribute to tumor microenvironment remodeling that suppresses tumor growth and progression. [ABSTRACT FROM AUTHOR]

Published

2024

4. DNMT3A/ miR-129-2-5p /Rac1 Is an Effector Pathway for SNHG1 to Drive Stem-Cell-like and Invasive Behaviors of Advanced Bladder Cancer Cells.

Author

Xu, Jiheng, Yang, Rui, Li, Jingxia, Wang, Lidong, Cohen, Mitchell, Simeone, Diane M., Costa, Max, and Wu, Xue-Ru

Subjects

BLADDER tumors, CANCER cell culture, CANCER invasiveness, MICRORNA, CELLULAR signal transduction, DNA methylation, GENE expression, STEM cells, MESSENGER RNA, CARRIER proteins

Abstract

Simple Summary: Bladder cancer ranks fourth among the most prevalent cancers in men and is the most expensive cancer to treat on a per-patient basis. The muscle-invasive form of bladder cancer is one of the deadliest cancers, with a 5-year survival rate of only 6% in patients with distant metastasis. Effective therapeutic options remain few and far between. SNHG1 is a long non-coding RNA that is over-expressed in 95% of muscle-invasive bladder cancers. However, very little information is available about the role and mechanisms of SNHG1 in bladder tumor formation and progression. Here, we provide experimental evidence establishing that SNHG1 drives bladder cancer cell invasion and stem-cell-like behaviors through a specific signaling pathway. Our results reveal novel biomarkers predictive of the progression of muscle-invasive bladder cancer and potential new targets for therapeutic intervention. The stem-cell-like behavior of cancer cells plays a central role in tumor heterogeneity and invasion and correlates closely with drug resistance and unfavorable clinical outcomes. However, the molecular underpinnings of cancer cell stemness remain incompletely defined. Here, we show that SNHG1, a long non-coding RNA that is over-expressed in ~95% of human muscle-invasive bladder cancers (MIBCs), induces stem-cell-like sphere formation and the invasion of cultured bladder cancer cells by upregulating Rho GTPase, Rac1. We further show that SNHG1 binds to DNA methylation transferase 3A protein (DNMT3A), and tethers DNMT3A to the promoter of miR-129-2, thus hyper-methylating and repressing miR-129-2-5p transcription. The reduced binding of miR-129-2 to the 3′-UTR of Rac1 mRNA leads to the stabilization of Rac1 mRNA and increased levels of Rac1 protein, which then stimulates MIBC cell sphere formation and invasion. Analysis of the Human Protein Atlas shows that a high expression of Rac1 is strongly associated with poor survival in patients with MIBC. Our data strongly suggest that the SNHG1/DNMT3A/miR-129-2-5p/Rac1 effector pathway drives stem-cell-like and invasive behaviors in MIBC, a deadly form of bladder cancer. Targeting this pathway, alone or in combination with platinum-based therapy, may reduce chemoresistance and improve longer-term outcomes in MIBC patients. [ABSTRACT FROM AUTHOR]

Published

2022

5. Identification of Ubiquitin-Related Gene-Pair Signatures for Predicting Tumor Microenvironment Infiltration and Drug Sensitivity of Lung Adenocarcinoma.

Author

Li, Yumei, An, Lanfen, Jia, Zhe, Li, Jingxia, Zhou, E, Wu, Feng, Yin, Zhengrong, Geng, Wei, Liao, Tingting, Xiao, Wenjing, Deng, Jingjing, Chen, Wenjuan, Li, Minglei, and Jin, Yang

Subjects

LUNG cancer diagnosis, ADENOCARCINOMA, LUNG cancer, PROTEINS, CELL physiology, GENE expression, CANCER patients, GENES, GENOMES, DRUG resistance in cancer cells

Abstract

Simple Summary: Lung adenocarcinoma (LUAD) has a high mortality and incidence rate. The therapeutic efficacy of LUAD varies with the individual heterogeneity of the tumor microenvironment (TME). It is necessary to explore more biomarkers and targets to improve the prognosis of patients. Ubiquitination pathways are involved in the biological process of regulating the anti-tumor immunity of immune cells and immunosuppression of tumor cells in the TME of patients. In this study, we clarified the characteristics of ubiquitin-related gene pairs (UbRGPs) and identified the relationship between the status of the TME and UbRGPs of patients with LUAD. A prognostic signature based on six UbRGPs was established, which performed well in predicting the immune infiltration and tumor mutation burden (TMB) in the TME and the response of LUAD to immuno-, chemo-, and targeted therapy. In conclusion, the UbRGPs signature is an independent prognostic indicator and has great potential in assisting the clinical therapy for patients with LUAD. Lung adenocarcinoma (LUAD) is a common pathological type of lung cancer worldwide, and new biomarkers are urgently required to guide more effective individualized therapy for patients. Ubiquitin-related genes (UbRGs) partially participate in the initiation and progression of lung cancer. In this study, we used ubiquitin-related gene pairs (UbRGPs) in tumor tissues to access the function of UbRGs in overall survival, immunocyte infiltration, and tumor mutation burden (TMB) of patients with LUAD from The Cancer Genome Atlas (TCGA) database. In addition, we constructed a prognostic signature based on six UbRGPs and evaluated its performance in an internal (TCGA testing set) and an external validation set (GSE13213). The prognostic signature revealed that risk scores were negatively correlated with the overall survival, immunocyte infiltration, and expression of immune checkpoint inhibitor-related genes and positively correlated with the TMB. Patients in the high-risk group showed higher sensitivity to partially targeted and chemotherapeutic drugs than those in the low-risk group. This study contributes to the understanding of the characteristics of UbRGPs in LUAD and provides guidance for effective immuno-, chemo-, and targeted therapy. [ABSTRACT FROM AUTHOR]

Published

2022

6. Isorhapontigenin (ISO) inhibits malignant cell transformation, migration, and invasion through MEG3/NEDD9 signaling in Cr(VI)-transformed cells.

Author

Shi, Sophia, Li, Jingxia, Zhang, Zhuo, Tu, Huailu, and Max, Costa

Subjects

*CELL transformation, *CANCER cells, *LINCRNA, *WNT proteins, *GENE expression, *WNT signal transduction, *CELL cycle regulation, *CELL cycle

Abstract

Cr(VI) compounds are confirmed human carcinogens. Maternally expression 3 (MEG3) is the first long non-coding RNA to be identified as a tumor suppressor. MEG3 is frequently downregulated or lost in various primary human tumor tissues and cancer cell lines. Downregulation of MEG3 is associated with cancer initiation, progression, and metastasis. Our previous study has revealed that MEG3 was lost and NEDD9 was upregulated in Cr(VI)-transformed cells compared to those in passage-matched normal BEAS-2B cells. Overexpression of MEG3 reduced NEDD9. β-Catenin was activated in Cr(VI)-transformed cells, overexpression of MEG3 or knockdown of NEDD9 inhibited the activation of β-Catenin. The results from the present study showed that isorhapontigenin (ISO) treatment is able to suppress cell proliferation, migration, and invasion of Cr(VI)-transformed cells. Further study showed that ISO treatment in Cr(VI)-transformed cells decreases the levels of Ki67, a biomarker for cell proliferation, and of cyclin D1, a regulator for the cell cycle. ISO elevated the MEG3 expression level in Cr(VI)-transformed cells. The DNA methylation transferases DNMT3a, DNMT3b, and DNMT1 levels were reduced upon ISO treatment. ISO treatment decreased both mRNA and protein levels of NEDD9. In addition, ISO treatment reduced the activation of β-catenin. Slug was upregulated and E -Cadherin was downregulated in Cr(VI)-transformed cells, treatment with ISO decreased Slug and increased E -Cadherin. This study demonstrated that ISO is a potent therapeutical agent against lung cancer induced by Cr(VI). • Cr(VI) is a confirmed human carcinogen. • ISO is an orally bioavailable dietary polyphenol. • ISO inhibits proliferation of Cr(VI)-transformed cells. • ISO inhibits of migration and invasion of Cr(VI)-transformed cells. [ABSTRACT FROM AUTHOR]

Published

2023

7. GADD45α Induction by Nickel Negatively Regulates JNKs/p38 Activation via Promoting PP2Cα Expression.

Author

Yu, Yonghui, Li, Jingxia, Wan, Yu, Lu, Jianyi, Gao, Jimin, and Huang, Chuanshu

Subjects

*GADD45 proteins, *JNK mitogen-activated protein kinases, *DNA damage, *OXIDATIVE stress, *PHOSPHORYLATION, *TRANSCRIPTION factors, *CELLULAR signal transduction, *MOLECULAR biology

Abstract

Growth arrest and DNA damage (GADD) 45α is a member of GADD inducible gene family, and is inducible in cell response to oxidative stress. GADD45α upregulation induces MKK4/JNK activation in some published experimental systems. However, we found here that the depletion of GADD45α (GADD45α−/−) in mouse embryonic fibroblasts (MEFs) resulted in an increase in the phosphorylation of MKK4/7, MKK3/6 and consequently specific up-regulated the activation of JNK/p38 and their downstream transcription factors, such as c-Jun and ATF2, in comparison to those in GADD45α+/+ MEFs cell following nickel exposure. This up-regulation of MKK-JNK/p38 pathway in GADD45α−/− cell could be rescued by the reconstitutional expression of HA-GADD45α in GADD45α−/− MEFs, GADD45α−/−(HA-GADD45α). Subsequent studies indicated that GADD45α deletion repressed expression of PP2Cα, the phosphotase of MKK3/6 and MKK4/7, whereas ectopic expression of HA-PP2Cα in GADD45α−/− cells attenuated activation of MKK3/6-p38 and MKK4/7-JNK pathways. Collectively, our results demonstrate a novel function and mechanism responsible for GADD45α regulation of MKK/MAPK pathway, further provides insight into understanding the big picture of GADD45α in the regulation of cellular responses to oxidative stress and environmental carcinogens. [ABSTRACT FROM AUTHOR]

Published

2013

8. Arsenite stabilizes HIF-1α protein through p85α-mediated up-regulation of inducible Hsp70 protein expression.

Author

Guo, Wei, Yang, Zhuo, Xia, Qing, Liu, Jinyi, Yu, Yonghui, Li, Jingxia, Zuo, Zhenghong, Zhang, Dongyun, Li, Xueyong, Shi, Xianglin, and Huang, Chuanshu

Subjects

ARSENIC, HYPOXEMIA, HEAT shock proteins, GENE expression, TRANSCRIPTION factors, BIOACCUMULATION, BIOLOGICAL assay, PROTEIN kinases

Abstract

Hypoxia-inducible factor-1α (HIF-1α) has been reported to regulate over 100 gene expressions in response to hypoxia and other stress conditions. In the present study, we found that arsenite could induce HIF-1α protein accumulation in both mouse epidermal Cl41 cells and mouse embryonic fibroblasts (MEFs). Knockout of p85α, a regulatory subunit of PI-3K, in MEFs (p85α) dramatically decreased the arsenite-induced HIF-1α accumulation, indicating that p85α is crucial for arsenite effects on the stabilization of HIF-1α protein. Our further studies suggest that arsenite could induce inducible Hsp70 expression, and transfection of inducible Hsp70 into p85α MEFs could restore HIF-1α protein accumulation. Moreover, the results using EMSA and Supershift assays indicate that p85α is crucial for arsenite-induced activation of the heat-shock transcription factor 1 (HSF-1), which is responsible for transcription of inducible Hsp70. Taken together, p85α-mediated HIF-1α stabilization upon arsenite exposure is specifically through HSF-1 activation and subsequent up-regulation of the inducible Hsp70 expression. [ABSTRACT FROM AUTHOR]

Published

2011

9. A Feedback Loop Formed by ATG7/Autophagy, FOXO3a/miR-145 and PD-L1 Regulates Stem-Like Properties and Invasion in Human Bladder Cancer.

Author

Zhu, Junlan, Li, Yang, Luo, Yisi, Xu, Jiheng, Liufu, Huating, Tian, Zhongxian, Huang, Chao, Li, Jingxia, and Huang, Chuanshu

Subjects

AUTOPHAGY, BLADDER tumors, CANCER invasiveness, CELL lines, ENZYME inhibitors, GENE expression, GROWTH factors, MESSENGER RNA, PROTEINS, STEM cells, TRANSCRIPTION factors, MICRORNA, PHARMACODYNAMICS

Abstract

Programmed cell death protein 1 (PD-1) and its ligand PD-L1 blockade have been identified to target immune checkpoints to treat human cancers with durable clinical benefit. Several studies reveal that the response to PD-1-PD-L1 blockade might correlate with PD-L1 expression levels in tumor cells. However, the mechanistic pathways that regulate PD-L1 protein expression are not understood. Here, we reported that PD-L1 protein is regulated by ATG7-autophagy with an ATG7-initiated positive feedback loop in bladder cancer (BC). Mechanistic studies revealed that ATG7 overexpression elevates PD-L1 protein level mainly through promoting autophagy-mediated degradation of FOXO3a, thereby inhibiting its initiated miR-145 transcription. The lower expression of miR-145 increases pd-l1 mRNA stability due to the reduction of its direct binding to 3′-UTR of pd-l1 mRNA, in turn leading to increasing in pd-l1 mRNA stability and expression, and finally enhancing stem-like property and invasion of BC cells. Notably, overexpression of PD-L1 in ATG7 knockdown cells can reverse the defect of autophagy activation, FOXO3A degradation, and miR-145 transcription attenuation. Collectively, our results revealed a positive feedback loop to promoting PD-L1 expression in human BC cells. Our study uncovers a novel molecular mechanism for regulating pd-l1 mRNA stability and expression via ATG7/autophagy/FOXO3A/miR-145 axis and reveals the potential for using combination treatment with autophagy inhibitors and PD-1/PD-L1 immune checkpoint blockade to enhance therapeutic efficacy for human BCs. [ABSTRACT FROM AUTHOR]

Published

2019

10. MP49-06 STAT3 ACTIVATION STATUS CONTRIBUTES TO THE DIFFERENTIAL RESPONSES OF METASTATIC AND NO-METASTATIC HUMAN BLADDER CANCER CELLS TO MIR-145 INHIBITION OF ANCHORAGE-INDEPENDENT GROWTH THROUGH REGULATION OF FOXO1 EXPRESSION.

Author

Jiang, Guosong, Li, Jingxia, Tang, Moon-Shong, Wu, Xue-Ru, and Huang, Chuanshu

Subjects

BLADDER cancer patients, MICRORNA, FORKHEAD transcription factors, TUMOR growth, GENE expression, GENETIC regulation

Published

2015

11. Lead induces COX-2 expression in glial cells in a NFAT-dependent, AP-1/NFκB-independent manner.

Author

Wei, Jinlong, Du, Kejun, Cai, Qinzhen, Ma, Lisha, Jiao, Zhenzhen, Tan, Jinrong, Xu, Zhou, Li, Jingxia, Luo, Wenjin, Chen, Jingyuan, Gao, Jimin, Zhang, Dongyun, and Huang, Chuanshu

Subjects

*CYCLOOXYGENASE 2, *GENE expression, *NEUROGLIA, *NFAT5 protein, *EPIDEMIOLOGICAL research, *NEUROTOXICOLOGY

Abstract

Epidemiologic studies have provided solid evidence for the neurotoxic effect of lead for decades of years. In view of the fact that children are more vulnerable to the neurotoxicity of lead, lead exposure has been an urgent public health concern. The modes of action of lead neurotoxic effects include disturbance of neurotransmitter storage and release, damage of mitochondria, as well as induction of apoptosis in neurons, cerebrovascular endothelial cells, astroglia and oligodendroglia. Our studies here, from a novel point of view, demonstrates that lead specifically caused induction of COX-2, a well known inflammatory mediator in neurons and glia cells. Furthermore, we revealed that COX-2 was induced by lead in a transcription-dependent manner, which relayed on transcription factor NFAT, rather than AP-1 and NFκB, in glial cells. Considering the important functions of COX-2 in mediation of inflammation reaction and oxidative stress, our studies here provide a mechanistic insight into the understanding of lead-associated inflammatory neurotoxicity effect via activation of pro-inflammatory NFAT3/COX-2 axis. [ABSTRACT FROM AUTHOR]

Published

2014

12. p27 suppresses cyclooxygenase-2 expression by inhibiting p38β and p38δ-mediated CREB phosphorylation upon arsenite exposure.

Author

Che, Xun, Liu, Jinyi, Huang, Haishan, Mi, Xiaoyi, Xia, Qing, Li, Jingxia, Zhang, Dongyun, Ke, Qingdong, Gao, Jimin, and Huang, Chuanshu

Subjects

*CYCLOOXYGENASE 2, *GENE expression, *CREB protein, *PHOSPHORYLATION, *ARSENITES, *CYCLIN-dependent kinase inhibitors

Abstract

Abstract: p27 is a cyclin-dependent kinase (CDK) inhibitor that suppresses a cell's transition from G0 to S phase, therefore acting as a tumor suppressor. Our most recent studies demonstrate that upon arsenite exposure, p27 suppresses Hsp27 and Hsp70 expressions through the JNK2/c-Jun- and HSF-1-dependent pathways, suggesting a novel molecular mechanism underlying the tumor suppressive function of p27 in a CDK-independent manner. We found that p27-deficiency (p27−/−) resulted in the elevation of cyclooxygenase-2 (COX-2) expression at transcriptional level, whereas the introduction of p27 brought back COX-2 expression to a level similar to that of p27+/+ cells, suggesting that p27 exhibits an inhibitory effect on COX-2 expression. Further studies identified that p27 inhibition of COX-2 expression was specifically due to phosphorylation of transcription factor cAMP response element binding (CREB) phosphorylation mediated by p38β and p38δ. These results demonstrate a novel mechanism underlying tumor suppression effect of p27 and will contribute to the understanding of the overall mechanism of p27 tumor suppression in a CDK-independent manner. [Copyright &y& Elsevier]

Published

2013

13. A novel role of IKKα in the mediation of UVB-induced G0/G1 cell cycle arrest response by suppressing Cyclin D1 expression

Author

Song, Lun, Dong, Wen, Gao, Ming, Li, Jingxia, Hu, Meiru, Guo, Ning, and Huang, Chuanshu

Subjects

*CELL cycle regulation, *GENE expression, *IMMUNOSUPPRESSION, *SUNBURN, *SKIN cancer, *PHYSIOLOGICAL effects of ultraviolet radiation, *GENETIC regulation, *PROTEIN kinases

Abstract

Abstract: Exposure to ultraviolet B (UVB) irradiation (290–320nm wavelength) from sunlight induces a variety of medical problems, including sunburn, immunosuppression and skin cancers. However, the molecular mechanisms related to UVB-induced cell damage and/or mutagenic effects have not been fully defined. Here, we demonstrate that one of the catalytic subunits of the IκB kinase complex (IKK), IKKα, plays a critical role in mediation of the UVB-induced G0/G1 cell cycle arrest response by suppressing Cyclin D1 expression. Notably, IKKa-dependent Cyclin D1 regulation is unrelated to IKKβ/NF-κB activity. We further show that IKKα-dependent downregulation of Cyclin D1 expression in the UVB response results from the reduction of ERK1/2-dependent Cyclin D1 transcription coupled with an increase of p38 kinase-dependent Cyclin D1 proteolysis. Thus, our results have identified the novel role of IKKα in regulating cell cycle progression during the cellular UVB response. Targeting IKKα might be promising for the prevention of UVB-induced cell damage and tumorigenic effects. [Copyright &y& Elsevier]

Published

2010