Your search keyword '"Kevin Christopher Knower"' showing total 4 results

1. Hepatic glucose intolerance precedes hepatic steatosis in the male aromatase knockout (ArKO) mouse

Author

Kerrie A. Herridge, Kevin Christopher Knower, Michelle Van Sinderen, Jane Honeyman, Colin Clyne, Wah Chin Boon, Jenny D. Y. Chow, Sebastian Beck Jørgensen, Margaret E. E. Jones, Sarah Quynh Giao To, Evan R. Simpson, and Gregory R. Steinberg

Subjects

Blood Glucose, Leptin, Male, Anatomy and Physiology, Mouse, medicine.medical_treatment, Glucose uptake, Adipose tissue, lcsh:Medicine, Biochemistry, Mice, Endocrinology, 0302 clinical medicine, Pyruvic Acid, Hyperinsulinemia, Insulin, Phosphorylation, lcsh:Science, Mice, Knockout, 2. Zero hunger, 0303 health sciences, Multidisciplinary, Muscles, Fatty liver, Organ Size, Animal Models, Adipose Tissue, Liver, Medicine, Adiponectin, Signal Transduction, Research Article, medicine.medical_specialty, Endocrine System, 030209 endocrinology & metabolism, Carbohydrate metabolism, Biology, Real-Time Polymerase Chain Reaction, 03 medical and health sciences, Aromatase, Model Organisms, Insulin resistance, Internal medicine, Glucose Intolerance, medicine, Animals, Reproductive Endocrinology, RNA, Messenger, Triglycerides, 030304 developmental biology, Diabetic Endocrinology, Endocrine Physiology, Body Weight, lcsh:R, Gluconeogenesis, Estrogens, medicine.disease, Hormones, Mice, Inbred C57BL, lcsh:Q, Insulin Resistance, Steatosis

Abstract

Estrogens are known to play a role in modulating metabolic processes within the body. The Aromatase knockout (ArKO) mice have been shown to harbor factors of Metabolic syndrome with central adiposity, hyperinsulinemia and male-specific hepatic steatosis. To determine the effects of estrogen ablation and subsequent replacement in males on whole body glucose metabolism, three- and six-month-old male ArKO mice were subjected to whole body glucose, insulin and pyruvate tolerance tests and analyzed for ensuing metabolic changes in liver, adipose tissue, and skeletal muscle. Estrogen-deficient male ArKO mice showed increased gonadal adiposity which was significantly reduced upon 17β-estradiol (E2) treatment. Concurrently, elevated ArKO serum leptin levels were significantly reduced upon E2 treatment and lowered serum adiponectin levels were restored to wild type levels. Three-month-old male ArKO mice were hyperglycemic, and both glucose and pyruvate intolerant. These phenotypes continued through to 6 months of age, highlighting a loss of glycemic control. ArKO livers displayed changes in gluconeogenic enzyme expression, and in insulin signaling pathways upon E2 treatment. Liver triglycerides were increased in the ArKO males only after 6 months of age, which could be reversed by E2 treatment. No differences were observed in insulin-stimulated ex vivo muscle glucose uptake nor changes in ArKO adipose tissue and muscle insulin signaling pathways. Therefore, we conclude that male ArKO mice develop hepatic glucose intolerance by the age of 3 months which precedes the sex-specific development of hepatic steatosis. This can be reversed upon the administration of exogenous E2.

Published

2014

2. The orphan nuclear receptor LRH-1 and ERα activate GREB1 expression to induce breast cancer cell proliferation

Author

Tamara L. Howard, Kerrie A. Herridge, Ashwini L. Chand, Kevin Christopher Knower, Colin Clyne, Kyren A. Lazarus, and Dhilushi D. Wijayakumara

Subjects

medicine.medical_specialty, Transcription, Genetic, Science, Cancer Treatment, Receptors, Cytoplasmic and Nuclear, Estrogen receptor, Breast Neoplasms, Biology, Response Elements, Biochemistry, Breast cancer, Cell Line, Tumor, Internal medicine, Molecular Cell Biology, medicine, Humans, Membrane Receptor Signaling, Promoter Regions, Genetic, Estrogen receptor beta, Cell Proliferation, Multidisciplinary, Cancer Risk Factors, Liver receptor homolog-1, Estrogen Receptor alpha, GATA3, Obstetrics and Gynecology, Orphan Nuclear Receptors, medicine.disease, Neoplasm Proteins, Neuron-derived orphan receptor 1, Gene Expression Regulation, Neoplastic, GREB1, Endocrinology, Oncology, Cancer research, Medicine, Female, Estrogen receptor alpha, Research Article, Signal Transduction

Abstract

BackgroundLiver Receptor Homolog 1 (LRH-1, NR5A2) is an orphan nuclear receptor that is over-expressed in cancers in tissues such as the breast, colon and pancreas. LRH-1 plays important roles in embryonic development, steroidogenesis and cholesterol homeostasis. In tumor cells, LRH-1 induces proliferation and cell cycle progression. High LRH-1 expression is demonstrated in breast cancers, positively correlating with ERα status and aromatase activity. LRH-1 dependent cellular mechanisms in breast cancer epithelial cells are poorly defined. Hence in the present study we investigated the actions of LRH-1 in estrogen receptor α (ERα) positive breast cancer cells.ResultsThe study aimed to investigate LRH-1 dependent mechanisms that promote breast cancer proliferation. We identified that LRH-1 regulated the expression of Growth Regulation by Estrogen in Breast Cancer 1 (GREB1) in MCF-7 and MDA-MB-231 cells. Over-expression of LRH-1 increased GREB1 mRNA levels while knockdown of LRH-1 reduced its expression. GREB1 is a well characterised ERα target gene, with three estrogen response elements (ERE) located on its promoter. Chromatin immunoprecipitation studies provided evidence of the co-localisation of LRH-1 and ERα at all three EREs. With electrophoretic mobility shift assays, we demonstrated direct binding of LRH-1 to EREs located on GREB1 and Trefoil Factor 1 (TFF1, pS2) promoters. LRH-1 and ERα co-operatively activated transcription of ERE luciferase reporter constructs suggesting an overlap in regulation of target genes in breast cancer cells. Over-expression of LRH-1 resulted in an increase in cell proliferation. This effect was more pronounced with estradiol treatment. In the presence of ICI 182,780, an ERα antagonist, LRH-1 still induced proliferation.ConclusionsWe conclude that in ER-positive breast cancer cells, LRH-1 promotes cell proliferation by enhancing ERα mediated transcription of target genes such as GREB-1. Collectively these findings indicate the importance of LRH-1 in the progression of hormone-dependent breast cancer and implicate LRH-1 as a potential avenue for drug development.

Published

2012

3. Aromatase is a direct target of FOXL2: C134W in granulosa cell tumors via a single highly conserved binding site in the ovarian specific promoter

Author

Colin Clyne, Kyren A. Lazarus, Nicholas I. Fleming, Evan R. Simpson, Peter J. Fuller, and Kevin Christopher Knower

Subjects

Steroidogenic factor 1, Forkhead Box Protein L2, Regulator, Regulatory Sequences, Nucleic Acid, medicine.disease_cause, 0302 clinical medicine, Pathology, Aromatase, Promoter Regions, Genetic, Genetics and Genomics/Genetics of Disease, Granulosa Cell Tumor, Regulation of gene expression, Ovarian Neoplasms, 0303 health sciences, Mutation, Multidisciplinary, Forkhead Transcription Factors, Pathology/Molecular Pathology, Gene Expression Regulation, Neoplastic, Biochemistry/Bioinformatics, Women's Health/Gynecological Cancers, 030220 oncology & carcinogenesis, Oncology/Gynecological Cancers, Medicine, Female, Research Article, endocrine system, medicine.drug_class, Science, Women's Health/Female Subfertility and Gynecological Endocrinology, Biology, 03 medical and health sciences, Cell Line, Tumor, medicine, Humans, Point Mutation, Transcription factor, Genetics and Genomics/Cancer Genetics, 030304 developmental biology, Binding Sites, Phosphoproteins, Molecular biology, Estrogen, Cell culture, Cancer research, biology.protein, Mutagenesis, Site-Directed

Abstract

BackgroundGranulosa cell tumors (GCT) of the ovary often express aromatase and synthesize estrogen, which in turn may influence their progression. Recently a specific point mutation (C134W) in the FOXL2 protein was identified in >94% of adult-type GCT and it is likely to contribute to their development. A number of genes are known to be regulated by FOXL2, including aromatase/CYP19A1, but it is unclear which are direct targets and whether the C134W mutation alters their regulation. Recently, it has been reported that FOXL2 forms a complex with steroidogenic factor 1 (SF-1) which is a known regulator of aromatase in granulosa cells.Methodology/principal findingsIn this work, the human GCT-derived cell lines KGN and COV434 were heterozygous and wildtype for the FOXL2:C134W mutation, respectively. KGN had abundant FOXL2 mRNA expression but it was not expressed in COV434. Expression of exogenous FOXL2:C134W in COV434 cells induced higher expression of a luciferase reporter for the ovarian specific aromatase promoter, promoter II (PII) (-516bp) than expression of wildtype FOXL2, but did not alter induction of a similar reporter for the steroidogenic acute regulatory protein (StAR) promoter (-1300bp). Co-immunoprecipitation confirmed that FOXL2 bound SF-1 and that it also bound its homologue, liver receptor homologue 1 (LRH-1), however, the C134W mutation did not alter these interactions or induce a selective binding of the proteins. A highly conserved putative binding site for FOXL2 was identified in PII. FOXL2 was demonstrated to bind the site by electrophoretic mobility shift assays (EMSA) and site-directed mutagenesis of this element blocked its differential induction by wildtype FOXL2 and FOXL2:C134W.Conclusions/significanceThese findings suggest that aromatase is a direct target of FOXL2:C134W in adult-type GCT via a single distinctive and highly conserved binding site in PII and therefore provide insight into the pathogenic mechanism of this mutation.

Published

2010

4. Failure of SOX9 Regulation in 46XY Disorders of Sex Development with SRY, SOX9 and SF1 Mutations

Author

Robin Lovell-Badge, Kevin Christopher Knower, Stefan Bagheri-Fam, Helena Yin Yee Sim, Pascal Bernard, Louisa M. Ludbrook, Sabine Kelly, Vincent R. Harley, and Ryohei Sekido

Subjects

Male, Steroidogenic factor 1, Steroidogenic Factor 1, medicine.disease_cause, Biochemistry, Molecular cell biology, 0302 clinical medicine, Testis, Morphogenesis, Transcriptional regulation, Disorders of sex development, SOX9 Transcription Factor, Genetics, 0303 health sciences, Mutation, Sexual Differentiation, Multidisciplinary, Sexual differentiation in humans, musculoskeletal system, Up-Regulation, Enhancer Elements, Genetic, Testis determining factor, Organ Specificity, embryonic structures, Medicine, Research Article, endocrine system, animal structures, Science, DNA transcription, SOX9, Biology, Cell Line, 03 medical and health sciences, stomatognathic system, Genetic Mutation, medicine, Humans, Gene Networks, 030304 developmental biology, Disorder of Sex Development, 46,XY, Cofactors, Sex Determination, medicine.disease, Sex-Determining Region Y Protein, Genetics of Disease, Trans-Activators, Mutant Proteins, Gene expression, Gene Function, 030217 neurology & neurosurgery, Developmental Biology

Abstract

BackgroundIn human embryogenesis, loss of SRY (sex determining region on Y), SOX9 (SRY-related HMG box 9) or SF1 (steroidogenic factor 1) function causes disorders of sex development (DSD). A defining event of vertebrate sex determination is male-specific upregulation and maintenance of SOX9 expression in gonadal pre-Sertoli cells, which is preceded by transient SRY expression in mammals. In mice, Sox9 regulation is under the transcriptional control of SRY, SF1 and SOX9 via a conserved testis-specific enhancer of Sox9 (TES). Regulation of SOX9 in human sex determination is however poorly understood.Methodology/principal findingsWe show that a human embryonal carcinoma cell line (NT2/D1) can model events in presumptive Sertoli cells that initiate human sex determination. SRY associates with transcriptionally active chromatin in NT2/D1 cells and over-expression increases endogenous SOX9 expression. SRY and SF1 co-operate to activate the human SOX9 homologous TES (hTES), a process dependent on phosphorylated SF1. SOX9 also activates hTES, augmented by SF1, suggesting a mechanism for maintenance of SOX9 expression by auto-regulation. Analysis of mutant SRY, SF1 and SOX9 proteins encoded by thirteen separate 46,XY DSD gonadal dysgenesis individuals reveals a reduced ability to activate hTES.Conclusions/significanceWe demonstrate how three human sex-determining factors are likely to function during gonadal development around SOX9 as a hub gene, with different genetic causes of 46,XY DSD due a common failure to upregulate SOX9 transcription.

Published

2011