Your search keyword '"Roberta Franks"' showing total 16 results

1. Essential roles of FoxM1 in Ras-induced liver cancer progression and in cancer cells with stem cell features

Author

Dragana Kopanja, Grace Guzman, Pradip Raychaudhuri, Neha Chandan, Megan M. Kiefer, Akshay Pandey, Zebin Wang, Roberta Franks, Janai R. Carr, Dae Yeul Yu, and Ajay V. Maker

Subjects

Male, Carcinoma, Hepatocellular, Carcinogenesis, medicine.disease_cause, Article, Mice, Cell Line, Tumor, medicine, Animals, Humans, neoplasms, Cell Proliferation, Hepatology, biology, Cell growth, Stem Cells, Forkhead Box Protein M1, Liver Neoplasms, CD44, Forkhead Transcription Factors, Prognosis, medicine.disease, Immunohistochemistry, digestive system diseases, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, Cell culture, Cancer cell, Disease Progression, ras Proteins, Cancer research, biology.protein, FOXM1, Stem cell, Liver cancer, Signal Transduction

Abstract

Background & Aims Overexpression of FoxM1 correlates with poor prognosis in hepatocellular carcinoma (HCC). Moreover, the Ras-signaling pathway is found to be ubiquitously activated in HCC through epigenetic silencing of the Ras-regulators. We investigated the roles of FoxM1 in Ras-driven HCC, and on HCC cells with stem-like features. Methods We employed a transgenic mouse model that expresses the oncogenic Ras in the liver. That strain was crossed with a strain that harbor floxed alleles of FoxM1 and the MxCre gene that allows conditional deletion of FoxM1 . FoxM1 alleles were deleted after development of HCC, and the effects on the tumors were analyzed. Also, FoxM1 siRNA was used in human HCC cell lines to determine its role in the survival of the HCC cells with stem cell features. Results Ras-driven tumors overexpress FoxM1. Deletion of FoxM1 inhibits HCC progression. There was increased accumulation of reactive oxygen species (ROS) in the FoxM1 deleted HCC cells. Moreover, FoxM1 deletion caused a disproportionate loss of the CD44+ and EpCAM+ HCC cells in the tumors. We show that FoxM1 directly activates expression of CD44 in human HCC cells. Moreover, the human HCC cells with stem cell features are addicted to FoxM1 for ROS-regulation and survival. Conclusion Our results provide genetic evidence for an essential role of FoxM1 in the progression of Ras-driven HCC. In addition, FoxM1 is required for the expression of CD44 in HCC cells. Moreover, FoxM1 plays a critical role in the survival of the HCC cells with stem cell features by regulating ROS.

Published

2015

2. Expression and function of COOH-terminal myosin heavy chain isoforms in mouse smooth muscle

Author

Roberta Franks, Anne F. Martin, Sunita Bhatti, Vlasios Manaves, Gail J. Pyne-Geithman, Mariam Farjah, Richard J. Paul, Lori A. Walker, and Arthur R. Strauch

Subjects

Gene isoform, Genetically modified mouse, Physiology, Ratón, Urinary Bladder, Gene Expression, Mice, Transgenic, Biology, Potassium Chloride, Mice, Smooth muscle, Myosin, Animals, Protein Isoforms, Muscle Strength, RNA, Messenger, Promoter Regions, Genetic, Aorta, Dose-Response Relationship, Drug, Myosin Heavy Chains, Muscle, Smooth, Smooth Muscle Myosins, Cell Biology, Molecular biology, Actins, Protein Structure, Tertiary, Rats, Cell biology, Kinetics, Phenotype, Terminal (electronics), MYH7, Function (biology), Muscle Contraction

Abstract

Isoforms of the smooth muscle myosin motor, SM1 and SM2, differ in length at the carboxy terminal tail region. Their proportion changes with development, hormonal status and disease, but their function is unknown. We developed mice carrying the myosin heavy chain (MyHC) transgenes SM1, cMyc-tagged SM1, SM2, and V5-tagged SM2, and all transgenes corresponded to the SMa NH2-terminal isoform. Transgene expression was targeted to smooth muscle by the smooth muscle α-actin promoter. Immunoblot analysis showed substantial expression of the cMyc-tagged SM1 and V5-tagged SM2 MyHC protein in aorta and bladder and transgene mRNA was expressed in mice carrying unlabeled SM1 or SM2 transgenes. Despite significant protein expression of tagged MyHCs we found only small changes in the SM1:SM2 protein ratio. Significant changes in functional phenotype were observed in mice carrying unlabeled SM1 or SM2 transgenes. Force in aorta and bladder was increased (72 ± 14%, 92 ± 11%) in SM1 and decreased to 57 ± 1% and 80 ± 3% in SM2 transgenic mice. SM1 transgenic bladders had faster (1.8 ± 0.3 s) and SM2 slower (7.1 ± 0.5 s) rates of force redevelopment following a rapid step shortening. We hypothesize that small changes in the SM1:SM2 ratio could be amplified if they are associated with changes in thick filament assembly and underlie the altered contractility. These data provide evidence indicating an in vivo function for the COOH-terminal isoforms of smooth muscle myosin and suggest that the SM1:SM2 ratio is tightly regulated in smooth muscle tissues.

Published

2007

3. Reporter Expression, Induced by a Growth Hormone Promoter-Driven Cre Recombinase (rGHp-Cre) Transgene, Questions the Developmental Relationship between Somatotropes and Lactotropes in the Adult Mouse Pituitary Gland

Author

Raúl M. Luque, Roberta Franks, Corrinne G. Lobe, Shinya Ishii, Geraldine Amargo, Hiro Kiyokawa, and Rhonda D Kineman

Subjects

Pituitary gland, medicine.medical_specialty, Somatotropic cell, Lactotrophs, Transgene, Cre recombinase, Mice, Transgenic, Biology, Gonadotropic cell, Mice, Endocrinology, Anterior pituitary, Genes, Reporter, Pituitary Gland, Anterior, Internal medicine, medicine, Animals, Humans, Transgenes, Promoter Regions, Genetic, Integrases, Human Growth Hormone, Age Factors, Gene Expression Regulation, Developmental, Somatotrophs, Growth hormone secretion, Mice, Inbred C57BL, medicine.anatomical_structure, Models, Animal, Endocrine gland

Abstract

This report describes the development and validation of the rGHp-Cre transgenic mouse that allows for selective Cre-mediated recombination of loxP-modified alleles in the GH-producing cells of the anterior pituitary. Initial screening of the rGHp-Cre parental line showed Cre mRNA was specifically expressed in the anterior pituitary gland of adult Cre+/- mice and cephalic extracts of e17 Cre+/- fetuses. Heterozygote rGHp-Cre transgenic mice were crossbred with Z/AP reporter mice to generate Cre+/-,Z/AP+/- offspring. In this model system, the GH promoter-driven, Cre-mediated recombination of the Z/AP reporter leads to human placental alkaline phosphatase (hPLAP) expression that serves to mark cells that currently produce GH, in addition to cells that would have differentiated from GH cells but currently do not express the GH gene. Double immunocytochemistry of adult male and female Cre+/-,Z/AP+/- pituitary cells revealed the majority (approximately 99%) of GH-producing cells of the anterior pituitary also expressed hPLAP, whereas ACTH-, TSH-, and LH-producing cells were negative for hPLAP, confirming previous reports that corticotropes, thyrotropes, and gonadotropes develop independently of the somatotrope lineage. A small subset (approximately 10%) of the prolactin-producing cells was positive for hPLAP, consistent with previous reports showing lactotropes can arise from somatotropes during pituitary development. However, the fact that 90% of prolactin-producing cells were negative for hPLAP suggests that the majority of lactotropes in the adult mouse pituitary gland develop independently of the somatotrope lineage. In addition to developmental studies, the rGHp-Cre transgenic mouse will provide a versatile tool to study the role of a variety of genes in somatotrope function and neoplastic transformation.

Published

2007

4. Deregulated CDC25A Expression Promotes Mammary Tumorigenesis with Genomic Instability

Author

Dipankar Ray, Eleftherios T. Papoutsakis, Francesco J. DeMayo, Zhi Qing Ma, Roberta Franks, Konstantin Christov, Peter G. Fuhrken, Nyla A. Heerema, Sophia Y. Tsai, Yasuhisa Terao, and Hiroaki Kiyokawa

Subjects

Genetically modified mouse, Genome instability, Cancer Research, CDC25A, Transgene, Cell, Mice, Transgenic, Biology, medicine.disease_cause, Genomic Instability, Mice, Mammary Glands, Animal, medicine, Animals, Humans, cdc25 Phosphatases, Hyperplasia, Mammary Neoplasms, Experimental, Genes, erbB-2, Cell cycle, Genes, ras, medicine.anatomical_structure, Oncology, Cancer cell, Cancer research, Female, Carcinogenesis

Abstract

Checkpoint pathways help cells maintain genomic integrity, delaying cell cycle progression in response to various risks of fidelity, such as genotoxic stresses, compromised DNA replication, and impaired spindle control. Cancer cells frequently exhibit genomic instability, and recent studies showed that checkpoint pathways are likely to serve as a tumor-suppressive barrier in vivo. The cell cycle–promoting phosphatase CDC25A is an activator of cyclin-dependent kinases and one of the downstream targets for the CHK1-mediated checkpoint pathway. Whereas CDC25A overexpression is observed in various human cancer tissues, it has not been determined whether deregulated CDC25A expression triggers or promotes tumorigenesis in vivo. Here, we show that transgenic expression of CDC25A cooperates markedly with oncogenic ras or neu in murine mammary tumorigenesis. MMTV-CDC25A transgenic mice exhibit alveolar hyperplasia in the mammary tissue but do not develop spontaneous mammary tumors. The MMTV-CDC25A transgene markedly shortens latency of tumorigenesis in MMTV-ras mice. The MMTV-CDC25A transgene also accelerates tumor growth in MMTV-neu mice with apparent cell cycle miscoordination. CDC25A-overexpressing tumors, which invade more aggressively, exhibit various chromosomal aberrations on fragile regions, including the mouse counterpart of human 1p31-36, according to array-based comparative genomic hybridization and karyotyping. The chromosomal aberrations account for substantial changes in gene expression profile rendered by transgenic expression of CDC25A, including down-regulation of Trp73. These data indicate that deregulated control of cellular CDC25A levels leads to in vivo genomic instability, which cooperates with the neu-ras oncogenic pathway in mammary tumorigenesis. [Cancer Res 2007;67(3):984–91]

Published

2007

5. FoxO1 Regulates Multiple Metabolic Pathways in the Liver

Author

Terry G. Unterman, David R. Powell, Roberta Franks, Wenwei Zhang, Robert V. Farese, Donna B. Stolz, Sandip Patil, Seung Hoi Koo, Mini P. Sajan, Angelos Klotsas, Ryan Matika, Jamie Le, Xiangshan Xiao, Patrick Tso, Shaodong Guo, Balwant Chauhan, Kim A. Heidenreich, and Marc Montminy

Subjects

medicine.medical_specialty, Glucokinase, Glycerol transport, FOXO1, Cell Biology, Biology, Pentose phosphate pathway, Biochemistry, Metabolic pathway, Endocrinology, Gluconeogenesis, Internal medicine, Lipogenesis, medicine, Glycolysis, Molecular Biology

Abstract

FoxO transcription factors are important targets of insulin action. To better understand the role of FoxO proteins in the liver, we created transgenic mice expressing constitutively active FoxO1 in the liver using the α1-antitrypsin promoter. Fasting glucose levels are increased, and glucose tolerance is impaired in transgenic (TGN) versus wild type (WT) mice. Interestingly, fasting triglyceride and cholesterol levels are reduced despite hyperinsulinemia, and post-prandial changes in triglyceride levels are markedly suppressed in TGN versus WT mice. Activation of pro-lipogenic signaling pathways (atypical protein kinase C and protein kinase B) and the ability to suppress β-hydroxybutyrate levels are not impaired in TGN. In contrast, de novo lipogenesis measured with 3H2O is suppressed by ∼70% in the liver of TGN versus WT mice after refeeding. Gene-array studies reveal that the expression of genes involved in gluconeogenesis, glycerol transport, and amino acid catabolism is increased, whereas genes involved in glucose utilization by glycolysis, the pentose phosphate shunt, lipogenesis, and sterol synthesis pathways are suppressed in TGN versus WT. Studies with adenoviral vectors in isolated hepatocytes confirm that FoxO1 stimulates expression of gluconeogenic genes and suppresses expression of genes involved in glycolysis, the shunt pathway, and lipogenesis, including glucokinase and SREBP-1c. Together, these results indicate that FoxO proteins promote hepatic glucose production through multiple mechanisms and contribute to the regulation of other metabolic pathways important in the adaptation to fasting and feeding in the liver, including glycolysis, the pentose phosphate shunt, and lipogenic and sterol synthetic pathways.

Published

2006

6. Intact Follicular Maturation and Defective Luteal Function in Mice Deficient for Cyclin- Dependent Kinase-4

Author

Tateki Tsutsui, Roberta Franks, David S. Moons, Albert F. Parlow, Dale B. Hales, Siwanon Jirawatnotai, Geula Gibori, Hiroaki Kiyokawa, and Asgerally T. Fazleabas

Subjects

Male, Ovulation, endocrine system, medicine.medical_specialty, endocrine system diseases, Granulosa cell, media_common.quotation_subject, Blotting, Western, Cyclin B, Estrous Cycle, Luteal phase, Biology, Chorionic Gonadotropin, Mice, Endocrinology, Ovarian Follicle, Cyclin D2, Corpus Luteum, Proto-Oncogene Proteins, Internal medicine, Follicular phase, medicine, Animals, Ovarian follicle, neoplasms, media_common, Mice, Knockout, Granulosa Cells, integumentary system, Reverse Transcriptase Polymerase Chain Reaction, Cyclin-Dependent Kinase 4, Progesterone secretion, Immunohistochemistry, Cyclin-Dependent Kinases, Hormones, medicine.anatomical_structure, Mutation, biology.protein, Female, biological phenomena, cell phenomena, and immunity, Infertility, Female

Abstract

Cell cycle progression of granulosa cells is critical for ovarian function, especially follicular maturation. During follicular maturation, FSH induces cyclin D2, which promotes G1 progression by activating cyclin-dependent kinase-4 (Cdk4). Because cyclin D2-deficient mice exhibit a block in follicular growth, cyclin D2/Cdk4 has been hypothesized to be required for FSH-dependent proliferation of granulosa cells. Here we investigate ovarian function in Cdk4-knockout mice we recently generated. Cdk4(-/-) females were sterile, but the morphology of their ovaries appeared normal before sexual maturation. The number of preovulatory follicles and the ovulation efficiency were modestly reduced in gonadotropin-treated Cdk4(-/-) mice. However, unlike cyclin D2-deficient mice, Cdk4(-/-) mice showed no obvious defect in FSH-induced proliferation of granulosa cells. Cdk4(-/-) ovaries displayed normal preovulatory expression of aromatase, PR, and cyclooxygenase-2. Postovulatory progesterone secretion was markedly impaired in Cdk4(-/-) mice, although granulosa cells initiated luteinization with induction of p450 side-chain cleavage cytochrome and p27(Kip1). Progesterone treatment rescued implantation and restored fertility in Cdk4(-/-) mice. Serum PRL levels after mating were significantly reduced in Cdk4(-/-) mice, suggesting the involvement of perturbed PRL regulation in luteal failure. Thus, Cdk4 is critical for luteal function, and some redundant protein(s) can compensate for the absence of Cdk4 in proliferation of granulosa cells.

Published

2002

7. Elevated Levels of Hepatocyte Nuclear Factor 3β in Mouse Hepatocytes Influence Expression of Genes Involved in Bile Acid and Glucose Homeostasis

Author

Robert H. Costa, Yongjun Tan, Simon C. Watkins, Donna B. Stolz, Roberta Franks, Heping Zhou, Terry G. Unterman, Francisco M. Rausa, and Kyung W. Yoo

Subjects

Time Factors, Transcription, Genetic, Ligands, Mice, chemistry.chemical_compound, Hepatocyte Nuclear Factor 6, Prealbumin, Protein Isoforms, Glucose homeostasis, Promoter Regions, Genetic, Cell Growth and Development, Glutathione Transferase, Symporters, Bile acid, Glycogen, biology, Nuclear Proteins, Immunohistochemistry, Recombinant Proteins, Cell biology, DNA-Binding Proteins, Hepatocyte nuclear factors, Phenotype, medicine.anatomical_structure, Liver, Hepatocyte, Hepatocyte Nuclear Factor 3-beta, ATP Binding Cassette Transporter, Subfamily B, medicine.drug_class, Blotting, Western, Molecular Sequence Data, Organic Anion Transporters, Sodium-Dependent, Mice, Transgenic, digestive system, Cell Line, Bile Acids and Salts, medicine, Animals, Glycogen synthase, Molecular Biology, Homeodomain Proteins, Base Sequence, Models, Genetic, Membrane Transport Proteins, Cell Biology, DNA Methylation, Molecular biology, Insulin-Like Growth Factor Binding Protein 1, Microscopy, Electron, Glucose, chemistry, Trans-Activators, biology.protein, ATP-Binding Cassette Transporters, Liver function, Carrier Proteins, Transcription Factors

Abstract

The winged helix transcription factor, hepatocyte nuclear factor-3beta (HNF-3beta), mediates the hepatocyte-specific transcription of numerous genes important for liver function. However, the in vivo role of HNF-3beta in regulating these genes remains unknown because homozygous null HNF3beta mouse embryos die in utero prior to liver formation. In order to examine the regulatory function of HNF-3beta, we created transgenic mice in which the -3-kb transthyretin promoter functions to increase hepatocyte expression of the rat HNF-3beta protein. Postnatal transgenic mice exhibit growth retardation, depletion of hepatocyte glycogen storage, and elevated levels of bile acids in serum. The retarded growth phenotype is likely due to a 20-fold increase in hepatic expression of insulin-like growth factor binding protein 1 (IGFBP-1), which results in elevated levels in serum of IGFBP-1 and limits the biological availability of IGFs required for postnatal growth. The defects in glycogen storage and serum bile acids coincide with diminished postnatal expression of hepatocyte genes involved in gluconeogenesis (phosphoenolpyruvate carboxykinase and glycogen synthase) and sinusoidal bile acid uptake (Ntcp), respectively. These changes in gene transcription may result from the disruptive effect of HNF-3beta on the hepatic expression of the endogenous mouse HNF-3alpha,-3beta, -3gamma, and -6 transcription factors. Furthermore, adult transgenic livers lack expression of the canalicular phospholipid transporter, mdr2, which is consistent with ultrastructure evidence of damage to transgenic hepatocytes and bile canaliculi. These transgenic studies represent the first in vivo demonstration that the HNF-3beta transcriptional network regulates expression of hepatocyte-specific genes required for bile acid and glucose homeostasis, as well as postnatal growth.

Published

2000

8. Premature Expression of the Winged Helix Transcription Factor HFH-11B in Regenerating Mouse Liver Accelerates Hepatocyte Entry into S Phase

Author

Ai Xuan Holterman, Roberta Franks, Kyung W. Yoo, Honggang Ye, and Robert H. Costa

Subjects

DNA Replication, Male, Time Factors, Liver cytology, Recombinant Fusion Proteins, Transgene, Mitosis, Mice, Transgenic, Biology, S Phase, Mice, Cyclins, medicine, Animals, Humans, Cyclin B1, Cell Growth and Development, Molecular Biology, Cell Nucleus, Ccaat-enhancer-binding proteins, Forkhead Box Protein M1, DNA replication, Nuclear Proteins, Forkhead Transcription Factors, Cell Biology, Phosphoproteins, Molecular biology, Liver regeneration, Liver Regeneration, DNA-Binding Proteins, X-ray Repair Cross Complementing Protein 1, medicine.anatomical_structure, Liver, Hepatocyte nuclear factor 4, Hepatocyte, CCAAT-Enhancer-Binding Proteins, Signal Transduction, Transcription Factors

Abstract

Two-thirds partial hepatectomy (PH) induces differentiated cells in the liver remnant to proliferate and regenerate to its original size. The proliferation-specific HNF-3/fork head homolog-11B protein (HFH-11B; also known as Trident and Win) is a family member of the winged helix/fork head transcription factors and in regenerating liver its expression is reactivated prior to hepatocyte entry into DNA replication (S phase). To examine whether HFH-11B regulates hepatocyte proliferation during liver regeneration, we used the -3-kb transthyretin (TTR) promoter to create transgenic mice that displayed ectopic hepatocyte expression of HFH-11B. Liver regeneration studies with the TTR-HFH-11B mice demonstrate that its premature expression resulted in an 8-h acceleration in the onset of hepatocyte DNA replication and mitosis. This liver regeneration phenotype is associated with protracted expression of cyclin D1 and C/EBPbeta, which are involved in stimulating DNA replication and premature expression of M phase promoting cyclin B1 and cdc2. Consistent with the early hepatocyte entry into S phase, regenerating transgenic livers exhibited earlier expression of DNA repair genes (XRCC1, mHR21spA, and mHR23B). Furthermore, in nonregenerating transgenic livers, ectopic HFH-11B expression did not elicit abnormal hepatocyte proliferation, a finding consistent with the retention of the HFH-11B transgene protein in the cytoplasm. We found that nuclear translocation of the HFH-11B transgene protein requires mitogenic signalling induced by PH and that its premature availability in regenerating transgenic liver allowed nuclear translocation to occur 8 h earlier than in wild type.

Published

1999

9. Abstract 312: Selective Inhibition of Myocardial NADPH Oxidase Significantly Decreases Heart Size in Transgenic (Tg) Mice with Cardiac-Specific Overexpression of a Dominant-Negative (DN) Mutant of p67 phox

Author

Kristopher McGee, John W. Christman, Lei Xiao, Magdalena Ornatowska, Qiong Zhao, R J Solaro, Roberta Franks, and Dalia Urboniene

Subjects

NADPH oxidase, biology, business.industry, Protein subunit, Transgene, Mutant, Molecular biology, Muscle hypertrophy, Cytosol, Heart size, Physiology (medical), biology.protein, Medicine, Cardiology and Cardiovascular Medicine, business, NOx

Abstract

The role of NADPH oxidase (NOX) was recently suggested in cardiac diseases including hypertrophy. Overexpression of a DN mutant of p67 phox , a cytosolic subunit of NOX, DN-p67 with a V204A point mutation completely inhibited NOX enzymatic function of superoxide generation. We found that overexpression of DN-p67 in cultured adult rat cardiac myocytes attenuated α 1 -adrenoceptor-induced hypertrophy , we thus hypothesized that NOX/p67 phox plays a critical role in cardiac hypertrophy and remodeling in vivo . Accordingly, we recently generated a Tg mouse model in C57BL/6 strain with cardiac-specific overexpression of this DN-p67 mutant along with an IRES-initiated EGFP tag protein using the cardiac-specific α-MHC promoter. Hearts from 1.5-, 3- and 6-month (M) old heterozygous Tg mice and their Non-Tg (NTg) littermates were harvested and compared. The heart weight/body weight (HW/BW) ratio in Tg group was significantly smaller (overall: 14%↓; 1.5-M: 10%↓; 3-M: 16%↓; 6-M: 12%↓) vs. the NTg group ( p < 0.01, n=23). This result was confirmed by 2D echocardiography (2D-echo) measuring the left ventricular myocardial area (LVMA) determined by subtracting endocardial area from epicardial area in short axis view at the end diastole. The LVMA (mm 2 ) in 3-M and 6-M mice was significantly ( p < 0.05, n=21) smaller in Tg (0.44±0.02) than the NTg (0.50±0.02) with equal average BW in both groups. LV internal dimensions and systolic function were preserved without difference in Tg vs. NTg. The LV wall thickness is smaller in Tg vs. NTg by both 2D-echo and hematoxylin/eosin staining of LV cross-sections, but no change in fibrosis was detected in both groups by trichrome staining (n=4). Interestingly, the expression of NOX catalytic subunit gp91 phox in Tg hearts was significantly decreased (~3-fold↓, n=5) vs. NTg by Western blot, whereas the cardiac expression of other NOX subunits p47 phox and p22 phox remained the same in both groups. In summary, we have generated a viable Tg mouse model with cardiac-specific overexpression of a DN p67 phox , which shows significant reduction in both myocardial mass/size and gp91 phox expression with normal cardiac function and development. Our results first show the novel and critical role of NOX/p67 phox in normal cardiac growth and heart development. This research has received full or partial funding support from the American Heart Association, AHA National Center.

Published

2008

10. Hemizygous disruption of Cdc25A inhibits cellular transformation and mammary tumorigenesis in mice

Author

Hiroaki Kiyokawa, Dipali Nimbalkar, Hiroyuki Hirai, Xianghong Zou, Evan C. Osmundson, Roberta Franks, Konstantin Christov, Dipankar Ray, and Yasuhisa Terao

Subjects

G2 Phase, Cancer Research, CDC25A, Time Factors, Mammary Neoplasms, Animal, Mice, Transgenic, Tumor initiation, medicine.disease_cause, Malignant transformation, S Phase, Mice, Cyclin-dependent kinase, medicine, Animals, cdc25 Phosphatases, Cells, Cultured, Cyclin-dependent kinase 1, biology, Kinase, Cell Cycle, Cell cycle, Fibroblasts, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, Cell Transformation, Neoplastic, Oncology, biology.protein, Cancer research, ras Proteins, Carcinogenesis

Abstract

CDC25A phosphatase activates multiple cyclin-dependent kinases (CDK) during cell cycle progression. Inactivation of CDC25A by ubiquitin-mediated degradation is a major mechanism of DNA damage-induced S-G2 checkpoint. Although increased CDC25A expression has been reported in various human cancer tissues, it remains unclear whether CDC25A activation is a critical rate-limiting step of carcinogenesis. To assess the role for CDC25A in cell cycle control and carcinogenesis, we used a Cdc25A-null mouse strain we recently generated. Whereas Cdc25A−/− mice exhibit early embryonic lethality, Cdc25A+/− mice show no appreciable developmental defect. Cdc25A+/− mouse embryonic fibroblasts (MEF) exhibit normal kinetics of cell cycle progression at early passages, modestly enhanced G2 checkpoint response to DNA damage, and shortened proliferative life span, compared with wild-type MEFs. Importantly, Cdc25A+/− MEFs are significantly resistant to malignant transformation induced by coexpression of H-rasV12 and a dominant negative p53 mutant. The rate-limiting role for CDC25A in transformation is further supported by decreased transformation efficiency in MCF-10A human mammary epithelial cells stably expressing CDC25A small interfering RNA. Consistently, Cdc25A+/− mice show substantially prolonged latency in mammary tumorigenesis induced by MMTV-H-ras or MMTV-neu transgene, whereas MMTV-myc–induced tumorigenesis is not significantly affected by Cdc25A heterozygosity. Mammary tissues of Cdc25A+/−;MMTV-neu mice before tumor development display less proliferative response to the oncogene with increased tyrosine phosphorylation of CDK1/2, but show no significant change in apoptosis. These results suggest that Cdc25A plays a rate-limiting role in transformation and tumor initiation mediated by ras activation. [Cancer Res 2007;67(14):6605–11]

Published

2007

11. Tumor-prone phenotype of the DDB2-deficient mice

Author

Roberta Franks, Hiroaki Kiyokawa, Amit Chakrabortty, Taewon Yoon, Ted Valli, and Pradip Raychaudhuri

Subjects

Cancer Research, Xeroderma pigmentosum, Neoplasms, Radiation-Induced, Skin Neoplasms, Ratón, DNA repair, Pyrimidine dimer, Biology, medicine.disease_cause, Article, DDB1, Mice, Coactivator, Genetics, medicine, Animals, Genetic Predisposition to Disease, Molecular Biology, Mice, Knockout, Xeroderma Pigmentosum, medicine.disease, Molecular biology, Phenotype, DNA-Binding Proteins, Cancer research, Carcinogenesis

Abstract

DDB2 is an essential subunit of the damaged-DNA recognition factor DDB, which is involved in global genomic repair in human cells. Moreover, DDB2 is mutated in the repair-deficiency disease xeroderma pigmentosum (Group E). Expression of DDB2 in human cells is induced by P53, BRCA1 and by ionizing radiation. The DDB2 protein associates with transcriptional activator and coactivator proteins. In addition, DDB2 in conjunction with DDB1 associates with cullin 4A and the Cop9/signalosome. We generated a mouse strain deficient for DDB2 (DDB2-/-). Consistent with the human disease (XP-E), the DDB2-/- mice were susceptible to UV-induced skin carcinogenesis. We observed a significant difference in the initial rate of cyclobutane pyrimidine dimer (CPD)-removal from the skin following UV irradiation. Also, the DDB2-deficient mice exhibited a significantly reduced life span compared to their wild-type littermates. Moreover, unlike other XP-deficient mice, the DDB2-deficient mice developed spontaneous malignant tumors at a high rate between the ages of 20 and 25 months. The observations suggest that, in addition to DNA repair, the other interactions of DDB2 are significant in its tumor suppression function.

Published

2004

12. The cyclin-dependent kinase inhibitors p27Kip1 and p21Cip1 cooperate to restrict proliferative life span in differentiating ovarian cells

Author

Hiroaki Kiyokawa, Dale B. Hales, David S. Moons, Siwanon Jirawatnotai, Roberta Franks, Geula Gibori, and Carlos Stocco

Subjects

Cyclin-Dependent Kinase Inhibitor p21, endocrine system, Cell type, medicine.drug_class, Cell, Cell Cycle Proteins, Biology, Biochemistry, chemistry.chemical_compound, Mice, Cyclin-dependent kinase, Cyclins, medicine, Animals, Receptor, Molecular Biology, Cells, Cultured, Cellular Senescence, Granulosa Cells, urogenital system, Tumor Suppressor Proteins, Cell Cycle, Ovary, Cell Differentiation, Cell Biology, Cell cycle, Cyclin-Dependent Kinases, Cell biology, medicine.anatomical_structure, chemistry, biology.protein, Female, Gonadotropin, Luteinizing hormone, Bromodeoxyuridine, Cell Division, Cyclin-Dependent Kinase Inhibitor p27

Abstract

The timing of cellular exit from the cell cycle during differentiation is specific for each cell type or lineage. Granulosa cells in the ovary establish quiescence within several hours after the ovulation-inducing luteinizing hormone surge, whereas they undergo differentiation into corpora lutea. The expression of Cdk inhibitors p21(Cip1/Waf1) and p27(Kip1) is up-regulated during this process, suggesting that these cell cycle inhibitors are involved in restricting proliferative capacity of differentiating granulosa cells. Here we demonstrate that the lack of p27(Kip1) and p21(Cip1) synergistically renders granulosa cells extended an proliferative life span. Immunohistochemical analyses demonstrated that corpora lutea of p27(Kip1), p21(Cip1) double-null mice showed large numbers of cells with bromodeoxyuridine incorporation and high proliferative cell nuclear antigen expression, which were more remarkable than those in p27(Kip1) single-deficient mice showing modest hyperproliferation. In contrast, differentiating granulosa cells in p21(Cip1)-deficient mice ceased proliferation similarly to those in wild-type mice. Interestingly, granulosa cells isolated from p27(Kip1), p21(Cip1) double-null mice exhibited markedly prolonged proliferative life span in culture, unlike cells with other genotypes. Cultured p27(Kip1), p21(Cip1) double-null granulosa cells maintained expression of steroidogenic enzymes and gonadotropin receptors through 8-10 passages and could undergo further differentiation in responses to cAMP accumulation. Thus, the cooperation of p27(Kip1) and p21(Cip1) is critical for withdrawal of granulosa cells from the cell cycle, in concert with luteal differentiation and possibly culture-induced senescence.

Published

2003

13. Human ubiquitous JCV(CY) T-antigen gene induces brain tumors in experimental animals

Author

Roberta Franks, Barbara Krynska, Kamel Khalili, Sidney Croul, and Jessica Otte

Subjects

Male, Cancer Research, Pathology, medicine.medical_specialty, Genes, Viral, viruses, Antigens, Polyomavirus Transforming, Population, Molecular Sequence Data, JC virus, Neuroectodermal Tumors, Mice, Transgenic, medicine.disease_cause, Mice, Genetics, medicine, Demyelinating disease, Animals, Humans, education, Molecular Biology, Tropism, Medulloblastoma, education.field_of_study, biology, Base Sequence, Brain Neoplasms, Progressive multifocal leukoencephalopathy, virus diseases, Brain, biology.organism_classification, medicine.disease, Virology, JC Virus, Disease Models, Animal, Primitive neuroectodermal tumor, DNA, Viral, Female, Papovavirus

Abstract

JCV is a papovavirus which is widespread in the human population. The prototype Mad-1 variant of JCV induces a fatal demyelinating disease of the central nervous system (CNS) called Progressive Multifocal Leukoencephalopathy (PML) in immunosuppressed individuals. The unique tropism of JCV (Mad-1) to the CNS is attributed to the tissue-specific regulation of the viral early promoter which is responsible for the production of the viral regulatory protein, T-antigen. The archetype form of this virus, JCV(CY), which has been repeatedly isolated from the urine of PML and non-PML individuals, is distinct from JCV(Mad-1) in the structural organization of the regulatory sequence. To characterize the tissue specific expression of JCV(CY) and to investigate its potential in inducing disease, transgenic mice containing the early region of JCV(CY) were generated. Some of these mice between 9 – 13 months of age exhibited signs of illness as manifested by paralysis of rear limbs, hunched posture, and poor grooming. Neuropathological examination indicated no sign of hypomyelination of the brain, but surprisingly, revealed the presence of primitive tumors originating from the cerebellum and the surrounding brain stem. The tumor masses also infiltrated the surrounding tissue. Results from RNA and protein studies revealed a high level of T-antigen mRNA expression in hindbrains of clinically normal and affected transgenic mice. However, higher levels of T-antigen RNA and protein were detected in brains of the animals exhibiting severe illness. The close resemblance of JCV(CY) induced tumor in transgenic mice to the human medulloblastoma/primitive neuroectodermal tumor (PNETs) in location, histologic appearance, and expression of marker proteins strongly suggests the utility of this novel animal model for the study of human brain tumors.

Published

1999

14. Modifications in protein binding to upstream sequences of the sea urchin cytoplasmic actin gene CyIIa in comparison to its linked neighbors, CyI and CyIIb

Author

R.Lynn Dukes, Hyacinth Paul, Karen S. Katula, and Roberta Franks

Subjects

Cytoplasm, Molecular Sequence Data, DNA Footprinting, Biology, Regulatory Sequences, Nucleic Acid, Sequence Homology, Nucleic Acid, Consensus Sequence, Genetics, Gene family, Animals, Histone octamer, Binding site, Promoter Regions, Genetic, Gene, Base Sequence, DNase-I Footprinting, General Medicine, biology.organism_classification, Serum Response Element, Strongylocentrotus purpuratus, Actins, Gene Expression Regulation, Genes, Sea Urchins, DNase I hypersensitive site, Protein Binding

Abstract

The sequences corresponding to regions upstream of the ATG and transcription start site of the CyIIa cytoplasmic actin gene of the sea urchin Strongylocentrotus purpuratus were determined and compared to the genomically linked CyI and CyIIb actin genes. Sites of protein–DNA interaction in the CyIIa upstream sequences were identified by DNase I footprinting. The similarity between CyIIa and CyI (and CyIIb) upstream sequences was limited and included a consensus octamer sequence, serum response element (SRE) and some short sequences within the proximal promoter region. The octamer sequence was found to bind protein. A single DNase I hypersensitive site was detected within the SRE and to two flanking nucleotides, but otherwise, the SRE did not appear to be protected. This is in contrast to strong protein binding to the CyIIb SRE. A region in the CyIIa gene with limited identity to the functionally significant protein binding site D in CyI also did not bind protein. Four additional sites of protein–DNA interaction were identified in CyIIa upstream sequences. One of these is similar to a protein binding site previously located in the CyI upstream sequences, whereas the others appear to be unique. These data indicate that the CyIIa upstream sequences differ extensively from those of CyI. The pattern of CyIIa expression is likely a consequence of these alternations in DNA sequence and protein–DNA interactions.

Published

1998

15. Transgenic mice with p53-responsive lacZ: p53 activity varies dramatically during normal development and determines radiation and drug sensitivity in vivo

Author

George R. Stark, Roberta Franks, Andrei V. Gudkov, Carolyn R. Zelnick, Sarah S. Bacus, Kaihua Wang, Elena A. Komarova, Dot Chin, Gabriella Armin, and Mikhail V. Chernov

Subjects

Genetically modified mouse, Male, Transcriptional Activation, DNA damage, Transgene, Drug Resistance, Spleen, Apoptosis, Mice, Transgenic, Biology, Transfection, Radiation Tolerance, General Biochemistry, Genetics and Molecular Biology, Mice, In vivo, Genes, Reporter, Pregnancy, medicine, Animals, Tissue Distribution, RNA, Messenger, Molecular Biology, DNA Primers, Regulation of gene expression, Mice, Knockout, General Immunology and Microbiology, Base Sequence, General Neuroscience, Gene Expression Regulation, Developmental, 3T3 Cells, Genes, p53, Molecular biology, medicine.anatomical_structure, Lac Operon, Doxorubicin, Female, Tumor Suppressor Protein p53, DNA Damage, Research Article

Abstract

To analyze the involvement of p53-dependent transcriptional activation in normal development and in response to DNA damage in vivo, we created transgenic mice with a lacZ reporter gene under the control of a p53-responsive promoter. Five independent strains showed similar patterns of transgene expression. In untreated animals, lacZ expression was limited to the developing nervous system of embryos and newborn mice and was strongly decreased in the adult brain. gamma-irradiation or adriamycin treatment induced lacZ expression in the majority of cells of early embryos and in the spleen, thymus and small intestine in adult mice. Transgene expression was p53 dependent and coincided with the sites of strong p53 accumulation. The lacZ-expressing tissues and early embryos, unlike other adult tissues and late embryos, are characterized by high levels of p53 mRNA expression and respond to DNA damage by massive apoptotic cell death. Analysis of p53-null mice showed that this apoptosis is p53 dependent. These data suggest that p53 activity, monitored by the reporter lacZ transgene, is the determinant of radiation and drug sensitivity in vivo and indicate the importance of tissue and stage specificity of p53 regulation at the level of mRNA expression.

Published

1997

16. Role of cell cycle regulators in tumor formation in transgenic mice expressing the human neurotropic virus, JCV, early protein

Author

Jessica Otte, Barbara Krynska, Roberta Franks, Antonio DeLuca, Kamel Khalili, Antonio Giordano, R.L. Knobler, Jennifer Gordon, Krynska, B., Gordon, J., Otte, J., Franks, R., Knobler, R., DE LUCA, Antonio, Giordano, A., and Khalili, K.

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Antigens, Polyomavirus Transforming, Cyclin A, Neoplasms, Nerve Tissue, Gene Expression, Mice, Transgenic, Protein Serine-Threonine Kinases, Biochemistry, Retinoblastoma Protein, Mice, Cyclin D1, Cyclin-dependent kinase, Cyclins, Proliferating Cell Nuclear Antigen, Proto-Oncogene Proteins, Cyclin E, CDC2-CDC28 Kinases, Animals, Humans, Kinase activity, Phosphorylation, Molecular Biology, biology, Kinase, Cyclin-dependent kinase 2, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinase 4, Cell Biology, Cell cycle, Molecular biology, JC Virus, Cyclin-Dependent Kinases, Cell biology, biology.protein, Cyclin-dependent kinase 6, Tumor Suppressor Protein p53

Abstract

Transgenic mice harboring the early genome from the human neurotropic JC virus, JCV, develop massive abdominal tumors of neural crest origin during 6–8 months after birth and succumb to death a few weeks later. The viral early protein, T-antigen, which possesses the ability to transform cells of neural origin, is highly expressed in the tumor cells. Immunoblot analysis of protein extract from tumor tissue shows high level expression of the tumor suppressor protein, p53, in complex with T-antigen. Expression of p21, a downstream target for p53, which controls cell cycle progression by regulating the activity of cyclins and their associated kinases during the G1 phase, is extremely low in the tumor cells. Whereas the level of expression and activity of cyclin D1 and its associated kinase, cdk6, was modest in tumor cells, both cyclin A and E, and their kinase partners, cdk2 and cdk4, were highly expressed and exhibited significant kinase activity. The retinoblastoma gene product, pRb, which upon phosphorylation by cyclins:cdk induces rapid cell proliferation, was found in the phosphorylated state in tumor cell extracts, and was detected in association with JCV T-antigen. The transcription factor, E2F-1, which dissociates from the pRb–E2F-1 complex and stimulates S phase-specific genes upon phosphorylation of pRb and/or complexation of pRb with the viral transforming protein, was highly expressed in tumor cells. Accordingly, high level expression of the E2F-1-responsive gene, proliferating cell nuclear antigen (PCNA), was detected in the tumor cells. These observations suggest a potential regulating pathway that, upon expression of JCV T-antigen, induces formation and progression of tumors of neural origin in a whole animal system. J Cell. Biochem. 67:223–230, 1997. © 1997 Wiley-Liss, Inc.

Published

1997