Your search keyword '"Ji-hye Paik"' showing total 27 results

1. Rapid and Selective Targeting of Heterogeneous Pancreatic Neuroendocrine Tumors

Author

G. Kate Park, Jeong Heon Lee, Eduardo Soriano, Myunghwan Choi, Kai Bao, Wataru Katagiri, Do-Yeon Kim, Ji-Hye Paik, Seok-Hyun Yun, John V. Frangioni, Thomas E. Clancy, Satoshi Kashiwagi, Maged Henary, and Hak Soo Choi

Subjects

Science

Abstract

Summary: Design of tissue-specific contrast agents to delineate tumors from background tissues is a major unmet clinical need for ultimate surgical interventions. Bioconjugation of fluorophore(s) to a ligand has been mainly used to target overexpressed receptors on tumors. However, the size of the final targeted ligand can be large, >20 kDa, and cannot readily cross the microvasculature to meet the specific tissue, resulting in low targetability with a high background. Here, we report a small and hydrophilic phenoxazine with high targetability and retention to pancreatic neuroendocrine tumor. This bioengineered fluorophore permits sensitive detection of ultrasmall (

Published

2020

2. FoxO1 in dopaminergic neurons regulates energy homeostasis and targets tyrosine hydroxylase

Author

Khanh V. Doan, Ann W. Kinyua, Dong Joo Yang, Chang Mann Ko, Sang Hyun Moh, Ko Eun Shong, Hail Kim, Sang-Kyu Park, Dong-Hoon Kim, Inki Kim, Ji-Hye Paik, Ronald A. DePinho, Seul Gi Yoon, Il Yong Kim, Je Kyung Seong, Yun-Hee Choi, and Ki Woo Kim

Subjects

Science

Abstract

Dopaminergic neurons are important for regulating energy homeostasis. Here, the authors show the transcription factor FoxO1 negatively regulates tyrosine hydroxylase expression in midbrain dopaminergic neurons, and plays an important role in regulation of glucose homeostasis, energy expenditure, and resistance to diet-induced obesity.

Published

2016

3. Transcription factor FoxO1 is essential for enamel biomineralization.

Author

Ross A Poché, Ramaswamy Sharma, Monica D Garcia, Aya M Wada, Mark J Nolte, Ryan S Udan, Ji-Hye Paik, Ronald A DePinho, John D Bartlett, and Mary E Dickinson

Subjects

Medicine, Science

Abstract

The Transforming growth factor β (Tgf-β) pathway, by signaling via the activation of Smad transcription factors, induces the expression of many diverse downstream target genes thereby regulating a vast array of cellular events essential for proper development and homeostasis. In order for a specific cell type to properly interpret the Tgf-β signal and elicit a specific cellular response, cell-specific transcriptional co-factors often cooperate with the Smads to activate a discrete set of genes in the appropriate temporal and spatial manner. Here, via a conditional knockout approach, we show that mice mutant for Forkhead Box O transcription factor FoxO1 exhibit an enamel hypomaturation defect which phenocopies that of the Smad3 mutant mice. Furthermore, we determined that both the FoxO1 and Smad3 mutant teeth exhibit changes in the expression of similar cohort of genes encoding enamel matrix proteins required for proper enamel development. These data raise the possibility that FoxO1 and Smad3 act in concert to regulate a common repertoire of genes necessary for complete enamel maturation. This study is the first to define an essential role for the FoxO family of transcription factors in tooth development and provides a new molecular entry point which will allow researchers to delineate novel genetic pathways regulating the process of biomineralization which may also have significance for studies of human tooth diseases such as amelogenesis imperfecta.

Published

2012

4. Supplementary Tables 1-2, Figures 1-8 from PTEN Is a Major Tumor Suppressor in Pancreatic Ductal Adenocarcinoma and Regulates an NF-κB–Cytokine Network

Author

Ronald A. DePinho, Sarah P. Thayer, Lynda Chin, Y. Alan Wang, Shannon J. Turley, Nabeel Bardeesy, Aram F. Hezel, Yonghong Xiao, Simona Colla, Alexei Protopopov, Brian Malinn, Shan Jiang, Samuel R. Perry, Carol Lim, Ji-hye Paik, Alec C. Kimmelman, Hongwu Zheng, Xiaojia Ren, Wei Wang, Yingchun Liu, Hailei Zhang, Eliot Fletcher-Sananikone, Haiyan Yan, Gerald C. Chu, Stephanie M. Zimmerman, Anant Vinjamoori, Kutlu G. Elpek, and Haoqiang Ying

Abstract

Supplementary Tables 1-2, Figures 1-8 from PTEN Is a Major Tumor Suppressor in Pancreatic Ductal Adenocarcinoma and Regulates an NF-κB–Cytokine Network

Published

2023

5. Supplementary Figure S2 from The G Protein–Coupled Receptor S1P2 Regulates Rho/Rho Kinase Pathway to Inhibit Tumor Cell Migration

Author

Fernando Ferrer, Timothy Hla, Ji-Hye Paik, and Denise Lepley

Abstract

Supplementary Figure S2 from The G Protein–Coupled Receptor S1P2 Regulates Rho/Rho Kinase Pathway to Inhibit Tumor Cell Migration

Published

2023

6. Legends to Supplementary Figures from The G Protein–Coupled Receptor S1P2 Regulates Rho/Rho Kinase Pathway to Inhibit Tumor Cell Migration

Author

Fernando Ferrer, Timothy Hla, Ji-Hye Paik, and Denise Lepley

Abstract

Legends to Supplementary Figures from The G Protein–Coupled Receptor S1P2 Regulates Rho/Rho Kinase Pathway to Inhibit Tumor Cell Migration

Published

2023

7. Supplementary Figures 1-9 from Development of Resistance to EGFR-Targeted Therapy in Malignant Glioma Can Occur through EGFR-Dependent and -Independent Mechanisms

Author

Hongwu Zheng, Haoqiang Ying, Ji-Hye Paik, Y. Alan Wang, James W. Horner, Peter Canoll, Sida Chen, Angelina V. Vaseva, Ling Zhang, Haiyan Yan, Jun Yao, Baofeng Guo, and Stefan Klingler

Abstract

Supplementary Figures 1-9. Figure S1: Auto-phosphorylation of EGFR-A289V and EGFR-G598V can be inhibited by EGFR TKIs. Figure S2: EGFR* expression is strongly induced in hGFAP-tTA tetO-EGFR* off-Dox mouse brains. Figure S3: Gfap and Nestin protein expression are overlapped in a subpopulation of NPCs. Figure S4: Representative H&E images of a Grade IV malignant glioma. Figure S5: Malignant glioma cells do not express terminally differentiated CNS cell lineage markers. Figure S6: iEIP glioma subcutaneous transplants are sensitive to genetic suppression of EGFR* induction but not to EGFR TKI. Figure S7: iEIP gliomas are sensitive to acute EGFR* ablation. Figure S8: Ingenuity pathway analysis comparing gene expression profiling of untreated control tumors with Dox-treated relapsed tumors. Figure S9: Combined treatment of Dox and Bez-235 inhibits EGFR* induction and Akt activation.

Published

2023

8. Comparative oncogenomics identifies NEDD9 as a melanoma metastasis gene

Author

Minjung Kim, Gans, Joseph D., Nogueira, Cristina, Wang, Audrey, Ji-Hye Paik, Bin Feng, Brennan, Cameron, Hahn, William C., Cordon-Cardo, Carlos, Wagner, Stephan N., Flotte, Thomas J., Duncan, Lyn M., Granter, Scott R., and Chin, Lynda

Subjects

Oncogenes -- Research, Metastasis -- Genetic aspects, Melanoma -- Genetic aspects, Biological sciences

Abstract

Metastatic variants are characterized with an acquired focal chromosomal amplification that corresponds to a much larger amplification in human metastatic melanomas and the analyses has identified Nedd9, an adaptor protein related to p130CAS, as the only gene within the minimal common region that displayed amplification-associated overexpression. The comparative oncogenomics has helped in the identification and has facilitated the validation of a highly relevant cancer gene governing metastatic potential in human melanoma.

Published

2006

9. Role of guanine nucleotide exchange factor P-Rex-2b in sphingosine 1-phosphate-induced Rac1 activation and cell migration in endothelial cells

Author

Zhong, Li, Ji-Hye, Paik, Jie-Hye, Paik, Zhenglong, Wang, Tim, Hla, and Dianqing, Wu

Subjects

rac1 GTP-Binding Protein, Physiology, PDZ domain, RAC1, GTPase, Biology, Biochemistry, Cell Line, Mice, chemistry.chemical_compound, Cell Movement, Sphingosine, Animals, Guanine Nucleotide Exchange Factors, Humans, Immunoprecipitation, Sphingosine-1-phosphate, DNA Primers, Pharmacology, Reporter gene, Base Sequence, GTPase-Activating Proteins, fungi, Wild type, Cell migration, Cell Biology, Molecular biology, chemistry, Guanine nucleotide exchange factor, Lysophospholipids

Abstract

Endothelial cell (EC) migration has an important role in angiogenesis. Sphingosine-1 phosphate (S1P) stimulates EC migration via activation of Gi proteins. In this study, we characterized a mouse guanine nucleotide exchange factor (GEF) P-Rex2b for its regulation by Gbetagamma and PI3K and its role in S1P-induced Rac1 activation and cell migration in ECs. We found that co-expression of Gbetagamma or an active form of PI3K (PI3K(AC)) with P-Rex2b increased the SRE. Luciferase (SRE.L) reporter gene activity that can be stimulated by the Rho family of small GTPases including Rac1. Co-expression with P-Rex2b of Gbetagamma and PI3K(AC) or wild type PI3Kgamma that can be activated by Gbetagamma led to further increases in the reporter gene activity. Together with the finding that co-expression of Gbetagamma and/or PI3K(AC) increased the levels of active Rac1, we conclude that P-Rex2b is a Rac GEF that can be regulated by Gbetagamma and PI3K. Additionally, we demonstrated that Gbetagamma interacted with P-Rex2b, probably through P-Rex2b sequences at the PH domain and that the DEP and PDZ domains of P-Rex2b exerted an inhibitory effect on P-Rex2b's activity because their deletion increased the SER.L reporter gene activity. Furthermore, we found that P-Rex2b is involved in S1P-induced Rac1 activation and cell migration in ECs because siRNA-mediated suppression of P-Rex2b expression in ECs-diminished Rac1 activation and cell migration in response to S1P. Therefore, P-Rex2b is a physiologically significant Rac1 GEF that has an important role in the regulation of EC migration.

Published

2005

10. Requirement for sphingosine 1-phosphate receptor-1 in tumor angiogenesis demonstrated by in vivo RNA interference

Author

Sung-Suk Chae, Ji-Hye Paik, Henry Furneaux, and Timothy Hla

Subjects

Neovascularization, Pathologic, Transplantation, Heterologous, Endothelial Cells, General Medicine, Article, Gene Expression Regulation, Neoplastic, Drug Combinations, Mice, Receptors, Lysosphingolipid, Cell Movement, Cell Line, Tumor, Neoplasms, Animals, Proteoglycans, RNA Interference, Collagen, Laminin, RNA, Small Interfering, Cells, Cultured, Neoplasm Transplantation

Abstract

Angiogenesis, or new blood vessel formation, is critical for the growth and spread of tumors. Multiple phases of this process, namely, migration, proliferation, morphogenesis, and vascular stabilization, are needed for optimal tumor growth beyond a diffusion-limited size. The sphingosine 1-phosphate (S1P) receptor-1 (S1P(1)) is required for stabilization of nascent blood vessels during embryonic development. Here we show that S1P(1) expression is strongly induced in tumor vessels. We developed a multiplex RNA interference technique to downregulate S1P(1) in mice. The small interfering RNA (siRNA) for S1P(1) specifically silenced the cognate transcript in endothelial cells and inhibited endothelial cell migration in vitro and the growth of neovessels into subcutaneous implants of Matrigel in vivo. Local injection of S1P(1) siRNA, but not a negative control siRNA, into established tumors inhibited the expression of S1P(1) polypeptide on neovessels while concomitantly suppressing vascular stabilization and angiogenesis, which resulted in dramatic suppression of tumor growth in vivo. These data suggest that S1P(1) is a critical component of the tumor angiogenic response and argue for the utility of siRNA technology in antiangiogenic therapeutics.

Published

2004

11. Regulation of limb development by the sphingosine 1-phosphate receptor S1p1/EDG-1 occurs via the hypoxia/VEGF axis

Author

Sung-Suk, Chae, Ji-Hye, Paik, Maria L, Allende, Richard L, Proia, and Timothy, Hla

Subjects

Vascular Endothelial Growth Factor A, Mice, Receptors, Lysophospholipid, Animals, Gene Expression Regulation, Developmental, Extremities, Hypoxia, Receptors, G-Protein-Coupled

Abstract

Angiogenesis, also known as new blood vessel formation, is regulated coordinately with other tissue differentiation events during limb development. Although vascular endothelial cell growth factor (VEGF) is important in the regulation of angiogenesis, chondrogenesis and osteogenesis during limb development, the role of other angiogenic factors is not well understood. Sphingosine 1-phosphate, a platelet-derived lipid mediator, regulates angiogenesis and vascular maturation via its action on the G-protein-coupled receptor S1P(1) (also known as EDG-1). In addition to vascular defects, abnormal limb development was also observed in S1p(1)(-/-) mice. Here we show that strong induction of S1P(1) expression is observed in the blood vessels and the interdigital mesenchymal cells during limb development. Deletion of S1P(1) results in aberrant chondrocyte condensation and defective digit morphogenesis. Interestingly, the vasculature in the S1p(1)(-/-) limbs was hyperplastic and morphologically altered. In addition, the hypoxia inducible factor (HIF)-1 alpha and its response gene VEGF were induced in S1p(1)(-/-) limbs. However, aberrant regulation of HIF-1 alpha and VEGF were not observed in embryonic fibroblasts derived from S1p(1)(-/-) mice, suggesting a non-cell autonomous effect of S1P(1) on VEGF expression. Indeed, similar limb defects were observed in endothelium-specific S1P(1) null mice in vivo. These data suggest that the function of S1P(1) in the developing vasculature is essential for proper limb development.

Published

2003

12. Aesthetics of 'Nostalgia' in Yoon Dae nyoung's novel : with a Focus on the A silver fishhooking communications

Author

Ji-Hye Paik

Subjects

Aesthetics, media_common.quotation_subject, Art, media_common

Abstract

본고는 윤대녕의 『은어낚시통신』 에 나타난 노스탤지어의 의미를 구명하고자 한다. 윤대녕의 노스탤지어는 단순히 한 개인의 추억을 서술한 것으로, 밀레니엄을 앞둔 90년대 문학의 경향으로 논의되어 왔다. 이 글에서는 윤대녕이 부여한 ‘노스탤지어’를 과거의 기억들을 활용하여, 그의 사고 속에 자유롭게 편집하고 통합하여 현재의 ‘나’를 만드는 의미있는 정체성의 기체로 파악하였다. 윤대녕의 유년기에는 아버지와 삼촌이 큰 영향을 미쳤다. 이들은 작가의 개인적인 트라우마를 넘어서 작품 전반에 창작의 아이디어를 주는 모체이다. 윤대녕 소설에서는 “공동체”에서 빠져나와 ‘집단’으로부터 탈주하는 주인공들이 등장한다. 윤대녕 소설에 등장하는 남자주인공은 몰개성적인 존재가 아니라, 삶에 적응하지 못하고 ‘언더’의 모습을 감춘 존재들이다. 이들은 문화적 향수감을 인위적으로 기억하는 과정을 공유함으로써, 사회적 마이너리티의 공간을 재창조한다. 한 세기 전에 유행한 대중문화, 익숙한 시인의 이름 나열, 지방 변두리 공간의 소재화는 과거의 잊혀진 기억을 부르는 노스탤지어로 작동한다. 그러나 리얼리티가 떨어지는 이 소재들은 윤대녕의 허무 의식을 극대화하는 장치로 연결된다. 특히 ‘은어’는 회귀성이 강한 동물로, 이는 되돌릴 수 없는 과거에 대한 동경을 넘어서, 치유할 수 없었던 작가의 상처를 극복하는 연장선에 있다. 윤대녕은 한 인간에게 닥친 가장 처절한 순간을 복원하는 길이, 오히려 생의 가장 큰 버팀목이 될 수 있는 길임을 깨달았던 것이다.

Published

2012

13. ZNF365 promotes stalled replication forks recovery to maintain genome stability.

Author

Yuqing Zhang, Eunmi Park, Christopher S. Kim, and Ji-hye Paik

Published

2013

14. FoxO family members in cancer.

Author

Yuqing Zhang, Gan, Boyi, Liu, Debra, and Ji-hye Paik

Published

2011

15. Foxo proteins cooperatively control the differentiation of Foxp3+ regulatory T cells.

Author

Weiming Ouyang, Beckett, Omar, Qian Ma, Ji-hye Paik, DePinho, Ronald A., and Li, Ming O.

Subjects

T cells, PROTEINS, IMMUNOLOGY, TRANSCRIPTION factors, MICE

Abstract

CD4+ regulatory T cells (Treg cells) characterized by expression of the transcription factor Foxp3 have a pivotal role in maintaining immunological tolerance. Here we show that mice with T cell–specific deletion of both the Foxo1 and Foxo3 transcription factors (collectively called 'Foxo proteins' here) developed a fatal multifocal inflammatory disorder due in part to Treg cell defects. Foxo proteins functioned in a Treg cell–intrinsic manner to regulate thymic and transforming growth factor-β (TGF-β)-induced Foxp3 expression, in line with the ability of Foxo proteins to bind to Foxp3 locus and control Foxp3 promoter activity. Transcriptome analyses showed that Foxo proteins regulated the expression of additional Treg cell–associated genes and were essential for inhibiting the acquisition of effector T cell characteristics by Treg cells. Thus, Foxo proteins have crucial roles in specifying the Treg cell lineage. [ABSTRACT FROM AUTHOR]

Published

2010

16. Mig-6 controls EGFR trafficking and suppresses gliomagenesis.

Author

Haoqiang Ying, Hongwu Zheng, Scott, Kenneth, Wiedemeyer, Ruprecht, Haiyan Yan, Lim, Carol, Huang, Joseph, Dhakal, Sabin, Ivanova, Elena, Yonghong Xiao, Hailei Zhang, Jian Hu, Stommel, Jayne M., Lee, Michelle A., Chen, An-Jou, Ji-Hye Paik, Segatto, Oreste, Brennan, Cameron, Elferink, Lisa A., and Wang, Y. Alan

Subjects

GLIOBLASTOMA multiforme, BRAIN cancer, ECTOPIC tissue, GROWTH factors, EPIDERMAL growth factor

Abstract

Glioblastoma multiforme (GBM) is the most common and lethal primary brain cancer that is driven by aberrant signaling of growth factor receptors, particularly the epidermal growth factor receptor (EGFR). EGFR signaling is tightly regulated by receptor endocytosis and lysosome-mediated degradation, although the molecular mechanisms governing such regulation, particularly in the context of cancer, remain poorly delineated. Here, high-resolution genomic profiles of GBM identified a highly recurrent focal 1p36 deletion encompassing the putative tumor suppressor gene, Mig-6. We show that Mig-6 quells the malignant potential of GBM cells and dampens EGFR signaling by driving EGFR into late endosomes and lysosome-mediated degradation upon ligand stimulation. Mechanistically, this effect is mediated by the binding of Mig-6 to a SNARE protein STX8, a protein known to be required for late endosome trafficking. Thus, Mig-6 functions to ensure recruitment of internalized receptor to late endosomes and subsequently the lysosomal degradation compartment through its ability to specifically link EGFR and STX8 during ligand-stimulated EGFR trafficking. In GBM, the highly frequent loss of Mig-6 would therefore serve to sustain aberrant EGFR-mediated oncogenic signaling. Together, these data uncover a unique tumor suppression mechanism involving the regulation of receptor trafficking. [ABSTRACT FROM AUTHOR]

Published

2010

17. FoxOs Cooperatively Regulate Diverse Pathways Governing Neural Stem Cell Homeostasis.

Author

Ji-hye Paik, Zhihu Ding, Narurkar, Rujuta, Ramkissoon, Shakti, Muller, Florian, Kamoun, Walid S., Sung-Suk Chae, Hongwu Zheng, Haoqiang Ying, Mahoney, Jed, Hiller, David, Shan Jiang, Protopopov, Alexei, Wong, Wing H., Chin, Lynda, Ligon, Keith L., and DePinhol, Ronald A.

Subjects

FORKHEAD transcription factors, NEURAL stem cells, TRANSCRIPTION factors, NERVOUS system, MOLECULAR biology, HOMEOSTASIS, CELL proliferation

Abstract

The PI3K-AKT-FoxO pathway is integral to lifespan regulation in lower organisms and essential for the stability of long-lived cells in mammals. Here, we report the impact of combined FoxO1, 3, and 4 deficiencies on mammalian brain physiology with a particular emphasis on the study of the neural stem/ progenitor cell (NSC) pool. We show that the FoxO family plays a prominent role in NSC proliferation and renewal. FoxO-deficient mice show initial increased brain size and proliferation of neural progenitor cells during early postnatal life, followed by precocious significant decline in the NSC pool and accompanying neurogenesis in adult brains. Mechanistically, integrated transcriptomic, promoter, and functional analyses of FoxO-deficient NSC cultures identified direct gene targets with known links to the regulation of human brain size and the control of cellular proliferation, differentiation, and oxidative defense. Thus, the FoxO family coordinately regulates diverse genes and pathways to govern key aspects of NSC homeostasis in the mammalian brain. [ABSTRACT FROM AUTHOR]

Published

2009

18. Genomic alterations link Rho family of GTPases to the highly invasive phenotype of pancreas cancer.

Author

Kimmelman, Alec C., Hezel, Aram F., Aguirre, Andrew J., Zheng, Hongwu, Ji-hye Paik, Haoqiang Ying, Chu, Gerald C., Zhang, Jean X., Sahin, Ergun, Yeo, Giminna, Ponugoti, Aditya, Nabioullin, Roustem, Deroo, Scott, Yang, Shenghong, Wang, Xiaoxu, McGrath, John P., Protopopova, Marina, Ivanova, Elena, Jianhua Zhang, and Bin Feng

Subjects

PANCREATIC duct, ADENOCARCINOMA, GUANOSINE triphosphatase, RHO GTPases, G proteins, CANCER invasiveness, GENE amplification, CANCER

Abstract

Pancreas ductal adenocarcinoma (PDAC) is a highly lethal cancer that typically presents as advanced. unresectable disease. This invasive tendency, coupled with intrinsic resistance to standard therapies and genome instability, are major contributors to poor long-term survival. The genetic elements governing the invasive propensity of PDAC have not been well elucidated. Here, in the course of validating resident genes in highly recurrent and focal amplifications in PDAC, we have identified Rio Kinase 3 (RIOK3) as an amplified gene that alters cytoskeletal architecture as well as promotes pancreatic ductal cell migration and invasion. We determined that RIOK3 promotes its invasive activities through activation of the small G protein, Rac. This genomic and functional link to Rac signaling prompted a genome wide survey of other components of the Rho family network, revealing p21 Activated Kinase 4 (PAK4) as another amplified gene in PDAC tumors and cell lines. Like RIOK3, PAK4 promotes pancreas ductal cell motility and invasion. Together, the genomic and functional profiles establish the Rho family GTP-binding proteins as integral to the hallmark invasive nature of this lethal disease. [ABSTRACT FROM AUTHOR]

Published

2008

19. Ink4a/Arf tumor suppressor does not modulate the degenerative conditions or tumor spectrum of the telomerase-deficient mouse.

Author

Khoo, Christine M., Carrasco, Daniel R., Bosenberg, Marcus W., Ji-Hye Paik, and Depinho, Ronald A.

Subjects

TUMOR suppressor genes, CANCER genes, TELOMERES, DNA damage, LABORATORY mice, GENETIC research

Abstract

The Rb/p16Ink4a and p53/p19Arf tumor suppressor pathways have been linked to diverse cancer-relevant processes, including those governing the cellular responses to telomere dysfunction. In this study, we sought to provide direct genetic evidence of a role for the Ink4a/Arf tumor suppressor gene, encoding both p16Ink4a and p19Arf, in modulating the cellular and tissue phenotypes associated with telomere dysfunction by using the mTerc Ink4a/Arf mouse model. In contrast to the rescue associated with p53 deficiency, Ink4a/Arf deficiency did not attenuate the degenerative phenotypes elicited by telomere dysfunction in the late-generation mTerc-/- mice. Furthermore, in contrast to accelerated cancer onset and increased epithelial cancers of late-generation mTerc-/- p53 mutant mice, late-generation mTerc-/- Ink4a/Arf mutant mice experienced a delayed tumor onset and maintained the lymphoma and sarcoma spectrum. Consistent with the negligible role of Ink4a/Arf in the telomere checkpoint response in vivo, late-generation mTerc-/- Ink4a/Arf-/- tissues show activated p53, and derivative tumor cell lines sustain frequent loss of p53 function, whereas all early generation mTerc Ink4a/Arf-/- tumor cell lines remain intact for p53. In addition, the late-generation mTerc-/- Ink4a/Arf-/- tumors showed activation of the alternative lengthening of telomere mechanism, underscoring the need for adaptation to the presence of telomere dysfunction in the absence of p16Ink4a and p19Arf. These observations highlight the importance of genetic context in dictating whether telomere dysfunction promotes or suppresses age-related degenerative conditions as well as the rate of initiation and type of spontaneous cancers. [ABSTRACT FROM AUTHOR]

Published

2007

20. Sphingosine 1-phosphate receptor regulation of N-cadherin mediates vascular stabilization.

Author

Ji-Hye Paik, Skoura, Athanasia, Sung-Suk Chae, Cowan, Ann E., Han, David K., Proia, Richard L., and Hla, Timothy

Subjects

*CELLS, *NEOVASCULARIZATION, *LIPIDS, *CELL adhesion, *CELL communication

Abstract

Vascular stabilization, a process by which nascent vessels are invested with mural cells, is important in angiogenesis. Here we describe the molecular basis of vascular stabilization regulated by sphingosine 1-phosphate (S1P), a platelet-derived lipid mediator. S1P1 receptor-dependent cell-surface trafficking and activation of the cell-cell adhesion molecule N-cadherin is essential for interactions between endothelial and mural cells. Endothelial cell S1P1/Gi/Rac pathway induces microtubule polymerization, resulting in trafficking of N-cadherin to polarized plasma membrane domains. S1P treatment modulated the phosphorylation of N-cadherin as well as p120-catenin and induced the formation of cadherin/catenin/actin complexes containing novel regulatory and trafficking factors. The net result of endothelial cell S1P1 receptor activation is the proper trafficking and strengthening of N-cadherin-dependent cell-cell adhesion with mural cells. Perturbation of N-cadherin expression with small interfering RNA profoundly attenuated vascular stabilization in vitro and in vivo. S1P-induced trafficking and activation of N-cadherin provides a novel mechanism for the stabilization of nascent blood vessels by mural cells and may be exploited to control angiogenesis and vascular diseases. [ABSTRACT FROM AUTHOR]

Published

2004

21. STAR RNA-binding protein Quaking suppresses cancer via stabilization of specific miRNA.

Author

An-Jou Chen, Ji-Hye Paik, Hailei Zhang, Shukla, Sachet A., Mortensen, Richard, Jian Hu, Haoqiang Ying, Baoli Hu, Hurt, Jessica, Farny, Natalie, Dong, Caroline, Yonghong Xiao, Wang, Y. Alan, Silver, Pamela A., Chin, Lynda, Vasudevan, Shobha, and DePinho, Ronald A.

Subjects

*CANCER, *GENOMES, *GLIOBLASTOMA multiforme, *PROTEINS, *GENETIC regulation

Abstract

Multidimensional cancer genome analysis and validation has defined Quaking (QKI), a member of the signal transduction and activation of RNA (STAR) family of RNA-binding proteins, as a novel glioblastoma multiforme (GBM) tumor suppressor. Here, we establish that p53 directly regulates QKI gene expression, and QKI protein associates with and leads to the stabilization of miR-20a; miR-20a, in turn, regulates TGFβR2 and the TGFβ signaling network. This pathway circuitry is substantiated by in silico epistasis analysis of its components in the human GBM TCGA (The Cancer Genome Atlas Project) collection and by their gain- and loss-of-function interactions in in vitro and in vivo complementation studies. This p53–QKI–miR-20a–TGFβ pathway expands our understanding of the p53 tumor suppression network in cancer and reveals a novel tumor suppression mechanism involving regulation of specific cancer-relevant microRNAs. [ABSTRACT FROM AUTHOR]

Published

2012

22. Intracellular Role for Sphingosine Kinase 1 in Intestinal Adenoma Cell Proliferation.

Author

Kohno, Masataka, Momoi, Michiko, Myat Lin Oo, Ji-Hye Paik, Yong-Moon Lee, Venkataraman, Krishnan, Youxi Ai, Ristimaki, Ari P., Fyrst, Henrik, Sano, Hajime, Rosenberg, Daniel, Saba, Julie D., Proia, Richard L., and Hla, Timothy

Subjects

SPHINGOSINE, PROTEIN kinases, SPHINGOLIPIDS, CELL proliferation, CELL growth, CANCER cells

Abstract

Sphingosine kinase (Sphk) enzymes are important in intracellular sphingolipid metabolism as well as in the biosynthesis of sphingosine 1-phosphate (S1P), an extracellular lipid mediator. Here, we show that Sphk1 is expressed and is required for small intestinal tumor cell proliferation in ApcMin/+ mice. Adenoma size but not incidence was dramatically reduced in ApcMin/+ Sphk-/- mice. Concomitantly, epithelial cell proliferation in the polyps was significantly attenuated, suggesting that Sphk1 regulates adenoma progression. Although the S1P receptors (S1P1R, S1P2R, and S1P3R) are expressed, polyp incidence or size was unaltered in ApcMin/+ S1p2r-/-, ApcMin/+ S1p3r-/-, and ApcMin/+ S1p1r+/- bigenic mice. These data suggest that extracellular S1P signaling via its receptors is not involved in adenoma cell proliferation. Interestingly, tissue sphingosine content was elevated in the adenomas of ApcMin/+ Sphk1-/- mice, whereas S1P levels were not significantly altered. Concomitantly, epithelial cell proliferation and the expression of the G1/S cell cycle regulator CDK4 and c-myc were diminished in the polyps of ApcMin/+ Sphk1-/- mice. In rat intestinal epithelial (RIE) cells in vitro, Sphk1 overexpression enhanced cell cycle traverse at the G¹/S boundary. In addition, RIE cells treated with sphingosine but not C6-ceramide exhibited reduced cell proliferation, reduced retinoblastoma protein phosphorylation, and cyclin-dependent kinase 4 (Cdk4) expression. Our findings suggest that Sphk1 plays a critical role in intestinal tumor cell proliferation and that inhibitors of Sphk1 may be useful in the control of intestinal cancer. [ABSTRACT FROM AUTHOR]

Published

2006

23. Phosphorylation and Action of the Immunomodulator FTY720 Inhibits Vascular Endothelial Cell Growth Factor-induced Vascular Permeability.

Author

Sanchez, Teresa, Estrada-Hernandez, Tatiana, Ji-Hye Paik, Ming-Tao Wu, Venkataraman, Krishnan, Brinkmann, Volker, Claffey, Kevin, and Hla, Timothy

Subjects

*IMMUNOLOGICAL adjuvants, *PHOSPHORYLATION, *VASCULAR endothelium, *GROWTH factors

Abstract

FTY720, a potent immunosuppressive agent, is phosphorylated in vivo into FTY720-P, a high affinity agonist for sphingosine 1-phosphate (SIP) receptors. The effects of FTY720 on vascular cells, a major target of SIP action, have not been addressed. We now report the metabolic activation of FTY720 by sphingosine kinase-2 and potent activation of vascular endothelial cell functions in vitro and in vivo by phosphorylated FTY720 (FTY720-P). Incubation of endothelial cells with FTY720 resulted in phosphorylation by sphingosine kinase activity and formation of FTY720-P. Sphingosine kinase-2 effectively phosphorylated FTY720 in the human embryonic kidney 293T heterologous expression system. FTY720-P treatment of endothelial cells stimulated extracellular signal-activated kinase and Akt phosphorylation and adherens junction assembly and promoted cell survival. The effects of FTY720-P were inhibited by pertussis toxin, suggesting the requirement for G[sub i]-coupled SIP receptors. Indeed, transmonolayer permeability induced by vascular endothelial cell growth factor was potently reversed by FTY720-P. Furthermore, oral FTY720 administration in mice potently blocked VEGF-induced vascular permeability in vivo. These findings suggest that FTY720 or its analogs may find utility in the therapeutic regulation of vascular permeability, an important process in angiogenesis, inflammation, and pathological conditions such as sepsis, hypoxia, and solid tumor growth. [ABSTRACT FROM AUTHOR]

Published

2003

24. Leptomycin B, an Inhibitor of the Nuclear Export receptor CRM, Inhibits COX-2 Expression.

Author

Byeong-Churl Jang, Munoz-Najar, Ursula, Ji-Hye Paik, Claffey, Kevin, Yoshida, Minoru, and Hla, Timothy

Subjects

*CYCLOOXYGENASE 2, *ENZYME inhibitors, *CANCER cells

Abstract

Reports that leptomycin B, a specific inhibitor of the nuclear export factor CRM1, potentially inhibits the stabilization of cyclooxygenase (COX)-2 mRNA in MDA-MB-231 human mammary cancer cells. Over-expression of the inducible prostaglandin synthase COX-2 in cancer and chronic inflammatory diseases; Analysis of pertinent topics and relevant issues; Implications on biological chemistry.

Published

2003

25. Development of Resistance to EGFR-Targeted Therapy in Malignant Glioma Can Occur through EGFR-Dependent and -Independent Mechanisms.

Author

Klingler, Stefan, Baofeng Guo, Jun Yao, Haiyan Yan, Ling Zhang, Vaseva, Angelina V., Sida Chen, Canoll, Peter, Horner, James W., Wang, Y. Alan, Ji-Hye Paik, Haoqiang Ying, and Hongwu Zheng

Subjects

*EPIDERMAL growth factor receptors, *CELLULAR signal transduction, *GLIOMAS, *NEOPLASTIC cell transformation, *PROTEIN-tyrosine kinase inhibitors

Abstract

Epidermal growth factor receptor (EGFR) is highly amplified, mutated, and overexpressed in human malignant gliomas. Despite its prevalence and growth-promoting functions, therapeutic strategies to inhibit EGFR kinase activity have not been translated into profound beneficial effects in glioma clinical trials. To determine the roles of oncogenic EGFR signaling in gliomagenesis and tumor maintenance, we generated a novel glioma mouse model driven by inducible expression of a mutant EGFR (EGFR*). Using combined genetic and pharmacologic interventions, we revealed that EGFR*-driven gliomas were insensitive to EGFR tyrosine kinase inhibitors, although they could efficiently inhibit EGFR_ autophosphorylation in vitro and in vivo. This is in contrast with the genetic suppression of EGFR_ induction that led to significant tumor regression and prolonged animal survival. However, despite their initial response to genetic EGFR* extinction, all tumors would relapse and propagate independent of EGFR*. We further showed that EGFR*-independent tumor cells existed prior to treatment and were responsible for relapse following genetic EGFR* suppression. And, the addition of a PI3K/ mTOR inhibitor could significantly delay relapse and prolong animal survival. Our findings shed mechanistic insight into EGFR drug resistance in glioma and provide a platform to test therapies targeting aberrant EGFR signaling in this setting. [ABSTRACT FROM AUTHOR]

Published

2015

26. FoxO1 expression in osteoblasts regulates glucose homeostasis through regulation of osteocalcin in mice.

Author

Rached, Marie-Therese, Kode, Aruna, Silva, Barbara C., Dae Young Jung, Gray, Susan, Ong, Helena, Ji-Hye Paik, DePinho, Ronald A., Kim, Jason K., Karsenty, Gerard, Kousteni, Stavroula, Jung, Dae Young, and Paik, Ji-Hye

Subjects

*PHYSIOLOGICAL effects of glucose, *GLYCOGENOLYSIS, *HOMEOSTASIS, *GENE expression, *TRANSCRIPTION factors, *NUCLEAR receptors (Biochemistry)

Abstract

Osteoblasts have recently been found to play a role in regulating glucose metabolism through secretion of osteocalcin. It is unknown, however, how this osteoblast function is regulated transcriptionally. As FoxO1 is a forkhead family transcription factor known to regulate several key aspects of glucose homeostasis, we investigated whether its expression in osteoblasts may contribute to its metabolic functions. Here we show that mice lacking Foxo1 only in osteoblasts had increased pancreatic beta cell proliferation, insulin secretion, and insulin sensitivity. The ability of osteoblast-specific FoxO1 deficiency to affect metabolic homeostasis was due to increased osteocalcin expression and decreased expression of Esp, a gene that encodes a protein responsible for decreasing the bioactivity of osteocalcin. These results indicate that FoxO1 expression in osteoblasts contributes to FoxO1 control of glucose homeostasis and identify FoxO1 as a key modulator of the ability of the skeleton to function as an endocrine organ regulating glucose metabolism. [ABSTRACT FROM AUTHOR]

Published

2010

27. The RNA-binding Protein HuR Regulates the Expression of Cyclooxygenase-2.

Author

Sengupta, Sibani, Byeong-Churl Jang, Ming-Tao Wu, Ji-Hye Paik, Furneaux, Henry, and Hla, Timothy

Subjects

*CYCLOOXYGENASE 2, *RNA-protein interactions, *GENE expression

Abstract

Discusses the role of RNA-binding protein HuR in regulating the expression of cyclooxygenase-2 (COX-2). Identification of HuR binding sites; Correlation between the cellular levels of HuR and COX-2; Effect of suppression of HuR expression on COX-2 induction.

Published

2003