Your search keyword '"Michael J. Waters"' showing total 201 results

1. Growth Hormone Stops Excessive Inflammation After Partial Hepatectomy, Allowing Liver Regeneration and Survival Through Induction of H2‐Bl/HLA‐G

Author

Viral Chikani, Shiro Minami, Michael J. Waters, Ken K. Y. Ho, Jamie Rossjohn, Andrew J. Brooks, Grant A. Ramm, Kathryn A. Tunny, Johan Medina, Robert G. Parton, Mayumi Ishikawa, Manuel A. Fernandez-Rojo, Julian P. Vivian, and Yash Chhabra

Subjects

0301 basic medicine, Gene knockdown, medicine.medical_specialty, Hepatology, biology, Inflammation, Original Articles, Growth hormone receptor, Liver regeneration, Transplantation, 03 medical and health sciences, Liver Injury and Regeneration, 030104 developmental biology, 0302 clinical medicine, Endocrinology, Downregulation and upregulation, Apoptosis, Internal medicine, medicine, biology.protein, Original Article, 030211 gastroenterology & hepatology, medicine.symptom, STAT5

Abstract

Background and Aims Growth hormone (GH) is important for liver regeneration after partial hepatectomy (PHx). We investigated this process in C57BL/6 mice that express different forms of the GH receptor (GHR) with deletions in key signaling domains. Approach and Results PHx was performed on C57BL/6 mice lacking GHR (Ghr −/−), disabled for all GH‐dependent Janus kinase 2 signaling (Box1 −/−), or lacking only GH‐dependent signal transducer and activator of transcription 5 (STAT5) signaling (Ghr391 −/−), and wild‐type littermates. C57BL/6 Ghr −/−mice showed striking mortality within 48 hours after PHx, whereas Box1 −/− or Ghr391 −/− mice survived with normal liver regeneration. Ghr −/− mortality was associated with increased apoptosis and elevated natural killer/natural killer T cell and macrophage cell markers. We identified H2‐Bl, a key immunotolerance protein, which is up‐regulated by PHx through a GH‐mediated, Janus kinase 2–independent, SRC family kinase–dependent pathway. GH treatment was confirmed to up‐regulate expression of the human homolog of H2‐Bl (human leukocyte antigen G [HLA‐G]) in primary human hepatocytes and in the serum of GH‐deficient patients. We find that injury‐associated innate immune attack by natural killer/natural killer T cell and macrophage cells are instrumental in the failure of liver regeneration, and this can be overcome in Ghr −/− mice by adenoviral delivery of H2‐Bl or by infusion of HLA‐G protein. Further, H2‐Bl knockdown in wild‐type C57BL/6 mice showed elevated markers of inflammation after PHx, whereas Ghr −/− backcrossed on a strain with high endogenous H2‐Bl expression showed a high rate of survival following PHx. Conclusions GH induction of H2‐Bl expression is crucial for reducing innate immune‐mediated apoptosis and promoting survival after PHx in C57BL/6 mice. Treatment with HLA‐G may lead to improved clinical outcomes following liver surgery or transplantation.

Published

2020

2. Insulin and Growth Hormone Balance: Implications for Obesity

Author

Zhengxiang Huang, Chen Chen, Michael J. Waters, and Lili Huang

Subjects

Blood Glucose, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, 030209 endocrinology & metabolism, Carbohydrate metabolism, Biology, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Internal medicine, medicine, Humans, Insulin, Endocrine system, Obesity, Human Growth Hormone, Lipid metabolism, Metabolism, Lipid Metabolism, medicine.disease, Biomarker (medicine), Energy Metabolism, Hormone

Abstract

Disruption of endocrine hormonal balance (i.e., increased levels of insulin, and reduced levels of growth hormone, GH) often occurs in pre-obesity and obesity. Using distinct intracellular signaling pathways to control cell and body metabolism, GH and insulin also regulate each other's secretion to maintain overall metabolic homeostasis. Therefore, a comprehensive understanding of insulin and GH balance is essential for understanding endocrine hormonal contributions to energy storage and utilization. In this review we summarize the actions of, and interactions between, insulin and GH at the cellular level, and highlight the association between the insulin/GH ratio and energy metabolism, as well as fat accumulation. Use of the [insulin]:[GH] ratio as a biomarker for predicting the development of obesity is proposed.

Published

2020

3. A growth hormone receptor SNP promotes lung cancer by impairment of SOCS2-mediated degradation

Author

Frederic A. Meunier, Andreas Papadopulos, Michael J. Waters, Yash Chhabra, Birthe B. Kragelund, Ho Yi Wong, Helena Steinocher, Louise F. Nikolajsen, Kathryn A. Tunny, Aaron G. Smith, and Andrew J. Brooks

Subjects

Male, Threonine, 0301 basic medicine, Cancer Research, Lung Neoplasms, Magnetic Resonance Spectroscopy, Receptor expression, DNA Mutational Analysis, Suppressor of Cytokine Signaling Proteins, Growth hormone receptor, Cohort Studies, Mice, Phosphorylation, Receptor, Lung, SOCS2, Growth hormone secretion, Cell biology, Gene Expression Regulation, Neoplastic, Disease Progression, Original Article, Female, Protein Binding, Signal Transduction, medicine.medical_specialty, Cell signaling, Epithelial-Mesenchymal Transition, Proline, Ubiquitin-Protein Ligases, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, Protein Domains, Cell Line, Tumor, Internal medicine, Journal Article, Genetics, medicine, Animals, Humans, Autocrine signalling, Molecular Biology, Ubiquitination, Computational Biology, Cancer, medicine.disease, HEK293 Cells, 030104 developmental biology, Endocrinology, Proteolysis, Carrier Proteins

Abstract

Both humans and mice lacking functional growth hormone (GH) receptors are known to be resistant to cancer. Further, autocrine GH has been reported to act as a cancer promoter. Here we present the first example of a variant of the GH receptor (GHR) associated with cancer promotion, in this case lung cancer. We show that the GHRP495T variant located in the receptor intracellular domain is able to prolong the GH signal in vitro using stably expressing mouse pro-B-cell and human lung cell lines. This is relevant because GH secretion is pulsatile, and extending the signal duration makes it resemble autocrine GH action. Signal duration for the activated GHR is primarily controlled by suppressor of cytokine signalling 2 (SOCS2), the substrate recognition component of the E3 protein ligase responsible for ubiquitinylation and degradation of the GHR. SOCS2 is induced by a GH pulse and we show that SOCS2 binding to the GHR is impaired by a threonine substitution at Pro 495. This results in decreased internalisation and degradation of the receptor evident in TIRF microscopy and by measurement of mature (surface) receptor expression. Mutational analysis showed that the residue at position 495 impairs SOCS2 binding only when a threonine is present, consistent with interference with the adjacent Thr494. The latter is key for SOCS2 binding, together with nearby Tyr487, which must be phosphorylated for SOCS2 binding. We also undertook nuclear magnetic resonance spectroscopy approach for structural comparison of the SOCS2 binding scaffold Ile455-Ser588, and concluded that this single substitution has altered the structure of the SOCS2 binding site. Importantly, we find that lung BEAS-2B cells expressing GHRP495T display increased expression of transcripts associated with tumour proliferation, epithelial-mesenchymal transition and metastases (TWIST1, SNAI2, EGFR, MYC and CCND1) at 2 h after a GH pulse. This is consistent with prolonged GH signalling acting to promote cancer progression in lung cancer.Oncogene advance online publication, 2 October 2017; doi:10.1038/onc.2017.352.

Published

2017

4. Refractory myasthenia gravis successfully treated with ofatumumab

Author

Janakan Ravindran, Michael J. Waters, and Deborah Field

Subjects

medicine.medical_specialty, Physiology, medicine.drug_class, medicine.medical_treatment, Monoclonal antibody, Ofatumumab, Antibodies, Monoclonal, Humanized, Gastroenterology, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Refractory, Physiology (medical), Internal medicine, Myasthenia Gravis, medicine, Humans, Immunologic Factors, Treatment Failure, Aged, biology, business.industry, Immunoglobulins, Intravenous, Plasmapheresis, medicine.disease, Thymectomy, Myasthenia gravis, Treatment Outcome, chemistry, Monoclonal, biology.protein, Female, Neurology (clinical), Antibody, business, Immunosuppressive Agents

Published

2019

5. Loss of growth hormone–mediated signal transducer and activator of transcription 5 (STAT5) signaling in mice results in insulin sensitivity with obesity

Author

Salvatore P. Mangiafico, Sof Andrikopoulos, David J. Waxman, Andrew J. Brooks, Monika Plescher, Michael J. Waters, Aaron G. Smith, Johanna L. Barclay, Yash Chhabra, and Caroline N. Nelson

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Growth hormone receptor, Growth hormone, Biochemistry, 03 medical and health sciences, Mice, 0302 clinical medicine, Internal medicine, Genetics, medicine, STAT5 Transcription Factor, Animals, Obesity, Molecular Biology, STAT5, Mice, Knockout, biology, Chemistry, Research, Intracellular Signaling Peptides and Proteins, Metabolism, medicine.disease, Receptor, Insulin, Fatty Liver, 030104 developmental biology, Endocrinology, Glucose, Gluconeogenesis, Liver, biology.protein, STAT protein, Insulin Receptor Substrate Proteins, Phosphoenolpyruvate Carboxykinase (GTP), Insulin Resistance, Carrier Proteins, hormones, hormone substitutes, and hormone antagonists, 030217 neurology & neurosurgery, Function (biology), Glycogen, Biotechnology, Signal Transduction

Abstract

Growth hormone (GH) has an important function as an insulin antagonist with elevated insulin sensitivity evident in humans and mice lacking a functional GH receptor (GHR). We sought the molecular basis for this sensitivity by utilizing a panel of mice possessing specific deletions of GHR signaling pathways. Metabolic clamps and glucose homeostasis tests were undertaken in these obese adult C57BL/6 male mice, which indicated impaired hepatic gluconeogenesis. Insulin sensitivity and glucose disappearance rate were enhanced in muscle and adipose of mice lacking the ability to activate the signal transducer and activator of transcription (STAT)5 via the GHR (Ghr-391(−/−)) as for GHR-null (GHR(−/−)) mice. These changes were associated with a striking inhibition of hepatic glucose output associated with altered glycogen metabolism and elevated hepatic glycogen content during unfed state. The enhanced hepatic insulin sensitivity was associated with increased insulin receptor β and insulin receptor substrate 1 activation along with activated downstream protein kinase B signaling cascades. Although phosphoenolpyruvate carboxykinase (Pck)-1 expression was unchanged, its inhibitory acetylation was elevated because of decreased sirtuin-2 expression, thereby promoting loss of PCK1. Loss of STAT5 signaling to defined chromatin immunoprecipitation targets would further increase lipogenesis, supporting hepatosteatosis while lowering glucose output. Finally, up-regulation of IL-15 expression in muscle, with increased secretion of adiponectin and fibroblast growth factor 1 from adipose tissue, is expected to promote insulin sensitivity.—Chhabra, Y., Nelson, C. N., Plescher, M., Barclay, J. L., Smith, A. G., Andrikopoulos, S., Mangiafico, S., Waxman, D. J., Brooks, A. J., Waters, M. J. Loss of growth hormone–mediated signal transducer and activator of transcription 5 (STAT5) signaling in mice results in insulin sensitivity with obesity.

Published

2019

6. Role of the growth hormone-IGF-1 axis in cancer

Author

Andrew J. Brooks, Michael J. Waters, and Yash Chhabra

Subjects

medicine.medical_specialty, biology, Endocrinology, Diabetes and Metabolism, Cancer, medicine.disease, Prolactin, Prostate cancer, Endocrinology, Tumor progression, Internal medicine, Pegvisomant, biology.protein, medicine, Autocrine signalling, Receptor, STAT5, medicine.drug

Abstract

A substantial body of evidence supports a role for the growth hormone (GH)-IGF-1 axis in cancer incidence and progression. This includes epidemiological evidence relating elevated plasma IGF-1 to cancer incidence as well as a lack of cancers in GH/IGF-1 deficiency. Rodent models lacking GH or its receptor are strikingly resistant to the induction of a wide range of cancers, and treatment with the GH antagonist pegvisomant slows tumor progression. While GH receptor expression is elevated in many cancers, autocrine GH is present in several types, and overexpression of autocrine GH can induce cell transformation. While the mechanism of autocrine action is not clear, it does involve both STAT5 and STAT3 activation, and probably nuclear translocation of the GH receptor. Development of a more potent GH receptor antagonist or secretion inhibitor is warranted for cancer therapy.

Published

2019

7. Activation of the growth hormone receptor

Author

Michael J. Waters and Rebecca A. Pelekanos

Subjects

Antisense therapy, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, government.form_of_government, medicine.medical_treatment, Regulator, Growth hormone receptor, Biology, medicine.disease, Endocrinology, Cytokine, Internal medicine, Acromegaly, Pegvisomant, government, medicine, Signal transduction, Receptor, medicine.drug

Abstract

Growth hormone (GH) is a major regulator of postnatal growth and metabolism. There are extensive clinical applications for GH or its antagonists, including treatments for dwarfism, cancer and metabolic wasting. Owing to this, there is considerable interest in the mechanisms of GH receptor (GHR) activation. It is conventionally thought that GH induces dimerization of two GHR monomers, which initiates intracellular signaling cascades. However, recent studies have provided evidence for a ligand-induced conformational change within constitutively dimerized GHRs being responsible for activating signaling pathways. This review will relate the new model of GHR activation to the activation of related cytokine receptors and discuss the implication of this new model for the design of small GH mimetics and antagonists for therapeutic use.

Published

2019

8. JAK2 activation by growth hormone and other cytokines

Author

Andrew J. Brooks and Michael J. Waters

Subjects

Models, Molecular, TMD, transmembrane domain, Review Article, Biochemistry, Tropomyosin receptor kinase C, JM, juxtamembrane, Receptor tyrosine kinase, FNIII, fibronectin III-like, Janus kinase 2, biology, Janus kinase 1, class I cytokine receptors, MAb, monoclonal antibody, 3. Good health, Cell biology, CT-1, cardiotropin-1, Srk family kinases, growth hormone receptor, Cytokines, GM-CSF, granulocyte-macrophage colony-stimulating factor, JAK, Janus kinase, Platelet-derived growth factor receptor, Protein Binding, Signal Transduction, Proto-oncogene tyrosine-protein kinase Src, Janus kinase 2 (JAK2), cytokine receptor signalling, TPO, thrombopoietin, Animals, Humans, Protein Interaction Domains and Motifs, Receptors, Cytokine, PK, pseudokinase, CNTF, ciliary neurotropic factor, Molecular Biology, Receptor Cross-Talk, Receptors, Somatotropin, Cell Biology, Janus Kinase 2, ECD, extracellular domain, OSM, oncostatin-M, GH, growth hormone, Enzyme Activation, Gene Expression Regulation, Growth Hormone, ROR1, biology.protein, Protein Multimerization, EPO, erythropoietin, Janus kinase, CRH, cytokine receptor homology

Abstract

Growth hormone (GH) and structurally related cytokines regulate a great number of physiological and pathological processes. They do this by coupling their single transmembrane domain (TMD) receptors to cytoplasmic tyrosine kinases, either as homodimers or heterodimers. Recent studies have revealed that many of these receptors exist as constitutive dimers rather than being dimerized as a consequence of ligand binding, which has necessitated a new paradigm for describing their activation process. In the present study, we describe a model for activation of the tyrosine kinase Janus kinase 2 (JAK2) by the GH receptor homodimer based on biochemical data and molecular dynamics simulations. Binding of the bivalent ligand reorientates and rotates the receptor subunits, resulting in a transition from a form with parallel TMDs to one where the TMDs separate at the point of entry into the cytoplasm. This movement slides the pseudokinase inhibitory domain of one JAK kinase away from the kinase domain of the other JAK within the receptor dimer–JAK complex, allowing the two kinase domains to interact and trans-activate. This results in phosphorylation and activation of STATs and other signalling pathways linked to this receptor which then regulate postnatal growth, metabolism and stem cell activation. We believe that this model will apply to most if not all members of the class I cytokine receptor family, and will be useful in the design of small antagonists and agonists of therapeutic value.

Published

2015

9. Unusual presentation of Epstein-Barr virus encephalitis in an older patient with a dramatic clinical response to intravenous immunoglobulin

Author

Timothy Kleinig, Michael J. Waters, Sarah Borg, and Andrew Tonkin

Subjects

Multimodal imaging, medicine.diagnostic_test, biology, business.industry, medicine.disease_cause, medicine.disease, Epstein–Barr virus, Virology, Biopsy, Immunology, Internal Medicine, medicine, biology.protein, Presentation (obstetrics), Antibody, business, Epstein–Barr virus infection, Encephalitis

Published

2015

10. Caveolin-1 Is Necessary for Hepatic Oxidative Lipid Metabolism: Evidence for Crosstalk between Caveolin-1 and Bile Acid Signaling

Author

Andrew J. Brooks, Christina Restall, Manuel A. Fernandez-Rojo, Susan J. Nixon, Sally Martin, Maria P. Ikonomopoulou, Nick Martel, Harriet P. Lo, Robin L. Anderson, Sean L. McGee, John F. Hancock, Michael J. Waters, Rebecca L. Fitzsimmons, Paul F. Pilch, George E.O. Muscat, Sheree D. Martin, Sean M. Grimmond, Milena Gongora, Charles Ferguson, Stephen Myers, and Robert G. Parton

Subjects

medicine.medical_specialty, medicine.drug_class, Caveolin 1, Peroxisome proliferator-activated receptor, Biology, General Biochemistry, Genetics and Molecular Biology, Bile Acids and Salts, Mice, chemistry.chemical_compound, Caveolae, Internal medicine, medicine, Animals, lcsh:QH301-705.5, chemistry.chemical_classification, Bile acid, Fatty acid metabolism, Lipid metabolism, Lipid Metabolism, Endocrinology, lcsh:Biology (General), Liver, chemistry, Nuclear receptor, Signal transduction, Oxidation-Reduction, Signal Transduction

Abstract

SummaryCaveolae and caveolin-1 (CAV1) have been linked to several cellular functions. However, a model explaining their roles in mammalian tissues in vivo is lacking. Unbiased expression profiling in several tissues and cell types identified lipid metabolism as the main target affected by CAV1 deficiency. CAV1−/− mice exhibited impaired hepatic peroxisome proliferator-activated receptor α (PPARα)-dependent oxidative fatty acid metabolism and ketogenesis. Similar results were recapitulated in CAV1-deficient AML12 hepatocytes, suggesting at least a partial cell-autonomous role of hepatocyte CAV1 in metabolic adaptation to fasting. Finally, our experiments suggest that the hepatic phenotypes observed in CAV1−/− mice involve impaired PPARα ligand signaling and attenuated bile acid and FXRα signaling. These results demonstrate the significance of CAV1 in (1) hepatic lipid homeostasis and (2) nuclear hormone receptor (PPARα, FXRα, and SHP) and bile acid signaling.

Published

2013

11. Increased adiposity and insulin correlates with the progressive suppression of pulsatile GH secretion during weight gain

Author

Lili Huang, Johannes D Veldhuis, Frederik J. Steyn, Shyuan T. Ngo, Chen Chen, T. Y. Xie, and Michael J. Waters

Subjects

Leptin, Male, medicine.medical_specialty, Calorie, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Pulsatile flow, Down-Regulation, Biology, Weight Gain, Mice, Endocrinology, Internal medicine, medicine, Animals, Humans, Insulin, Secretion, Obesity, Adiposity, Growth hormone secretion, Mice, Inbred C57BL, Glucose, Growth Hormone, Lipogenesis, medicine.symptom, Weight gain

Abstract

Pathological changes associated with obesity are thought to contribute to GH deficiency. However, recent observations suggest that impaired GH secretion relative to excess calorie consumption contributes to progressive weight gain and thus may contribute to the development of obesity. To clarify this association between adiposity and GH secretion, we investigated the relationship between pulsatile GH secretion and body weight; epididymal fat mass; and circulating levels of leptin, insulin, non-esterified free fatty acids (NEFAs), and glucose. Data were obtained from male mice maintained on a standard or high-fat diet. We confirm the suppression of pulsatile GH secretion following dietary-induced weight gain. Correlation analyses reveal an inverse relationship between measures of pulsatile GH secretion, body weight, and epididymal fat mass. Moreover, we demonstrate an inverse relationship between measures of pulsatile GH secretion and circulating levels of leptin and insulin. The secretion of GH did not change relative to circulating levels of NEFAs or glucose. We conclude that impaired pulsatile GH secretion in the mouse occurs alongside progressive weight gain and thus precedes the development of obesity. Moreover, data illustrate key interactions between GH secretion and circulating levels of insulin and reflect the potential physiological role of GH in modulation of insulin-induced lipogenesis throughout positive energy balance.

Published

2013

12. Mechanism of JAK2 Activation by the Archetype Class I Cytokine Receptor, the Growth Hormone Receptor

Author

Andrew J. Brooks, Daniel Abankwa, Yash Chhabra, Alan E. Mark, Megan L. O'Mara, Yann Gambin, Wei Dai, Guillermo A. Gomez, Louise F. Nikolajsen, Michael W. Parker, Manolis Doxastakis, Michael J. Waters, Emma Sierecki, Gitte W. Haxholm, and Kathryn A. Tunny

Subjects

Biochemistry, Growth-hormone-releasing hormone receptor, Growth factor receptor, ROR1, Enzyme-linked receptor, Biophysics, 5-HT5A receptor, Growth hormone receptor, Biology, Interleukin-13 receptor, Insulin-like growth factor 1 receptor, Cell biology

Abstract

The growth hormone receptor (GHR) has been the archetype for the class I cytokine receptor family. The original paradigm for how growth hormone (GH) binding to the GHR led to activation of the associated JAK2 was based on biophysical and structural studies over 20 years ago which showed that growth hormone binding to the extracellular domain of the receptor occurred in a sequential fashion, first binding to a high affinity site on a single receptor (site 1) and then binding to a lower affinity site (site 2) on a second receptor. We propose a new model for JAK2 activation by the growth hormone receptor. We utilised multiple approaches to define this model including FRET to monitor positioning of the JAK2 binding motif, leucine-zipper receptor constructs to control receptor transmembrane helix position, atomistic modelling of TM helix interactions and docking of JAK2 kinase and inhibitory pseudokinase crystal structures with an opposing pair in trans. Surprisingly, we identified that receptor activation induces a separation of its JAK2 binding motifs which leads to removal of the pseudokinase domain from the kinase domain of the partner JAK2 and pairing of the two kinase domains, facilitating trans-activation. In addition, we have recently shown that the receptor intracellular domain is intrinsically disordered and has specific interactions with the lipids of the inner membrane. This model of receptor activation may represent a common mechanism to other class I cytokine receptors.

Published

2016

13. GH Does Not Modulate the Early Fasting-Induced Release of Free Fatty Acids in Mice

Author

Colleen C. Nelson, Michael J. Waters, Johannes D. Veldhuis, Jacques Epelbaum, J. W. Leong, Chen Chen, H. Y. Tan, T. Y. Xie, Frederik J. Steyn, and Lili Huang

Subjects

Leptin, Male, medicine.medical_specialty, Time Factors, Hypothalamus, Pulsatile flow, Gene Expression, Adipose tissue, Fatty Acids, Nonesterified, Biology, Mice, Endocrinology, Species Specificity, In vivo, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Receptors, Somatostatin, Circadian rhythm, Insulin-Like Growth Factor I, Mice, Knockout, Fasting, Receptors, Somatotropin, Neuropeptide Y receptor, Ghrelin, Growth hormone secretion, Mice, Inbred C57BL, Growth Hormone, Pituitary Gland, Models, Animal, Knockout mouse, lipids (amino acids, peptides, and proteins), Corticosterone, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

Fasting results in the mobilization of adipose stores and the elevation of levels of free fatty acids (FFA). In humans, this process is driven by a release in GH. Little is known regarding the role of GH in modulating this process during early stages of fasting in the mouse. Confirmation of the role of GH in modulating FFA release in the fasting mouse is of particular importance given the frequent use of mouse models to study metabolic mechanisms. Here, we correlate the initial release of FFA throughout fasting in mice with pulsatile GH secretion. Observations illustrate the rapid release of FFA in response to food withdrawal. This does not correlate with a rise in GH secretion. Rather, we observed a striking loss in pulsatile secretion of GH throughout the first 6 h of fasting, suggesting that GH does not modulate the initial release of FFA in the mouse in response to fasting. This was confirmed in GH receptor knockout mice, in which we observed a robust fasting-induced rise in FFA. We further illustrate the dynamic relationship between the orexigenic and anorexigenic hormones ghrelin and leptin during fasting in the mouse. Our findings show an initial suppression of leptin and the eventual rise in circulating levels of acyl-ghrelin with fasting. However, altered acyl-ghrelin and leptin secretion occurs well after the rise in FFA and the suppression of GH secretion. Consequently, we conclude that although acyl-ghrelin and leptin may modulate the physiological response to drive food intake, these changes do not contribute to the initial loss of pulsatile GH secretion. Rather, it appears that the suppression of GH secretion in fasting may occur in response to an elevation in fasting levels of FFA or physiological stress. Observations highlight a divergent role for GH in modulating FFA release between man and mouse.

Published

2012

14. Inhibitory GH Receptor Extracellular Domain Monoclonal Antibodies: Three-Dimensional Epitope Mapping

Author

Yu Wan, Stuart J. Frank, Jing Jiang, Jie Xu, Kurt R. Zinn, Jonathan M. Harris, Peter E. Lobie, Yu Zhang, Michael J. Waters, and Xiangdong Wang

Subjects

Growth Hormone-Somatostatin-GRH, medicine.drug_class, Growth hormone receptor, Biology, Monoclonal antibody, Epitope, Mice, Endocrinology, Downregulation and upregulation, medicine, Animals, Protein Interaction Domains and Motifs, Receptor, Cell Proliferation, Binding protein, Antibodies, Monoclonal, Receptors, Somatotropin, Molecular biology, Protein Structure, Tertiary, Epitope mapping, Liver, Rabbits, Protein Multimerization, Signal transduction, Epitope Mapping, hormones, hormone substitutes, and hormone antagonists, Peptide Hydrolases, Signal Transduction

Abstract

GH receptor (GHR) mediates the anabolic and metabolic effects of GH. We previously characterized a monoclonal antibody (anti-GHR(ext-mAb)) that reacts with subdomain 2 of the rabbit GHR extracellular domain (ECD) and is a conformation-specific inhibitor of GH signaling in cells bearing rabbit or human GHR. Notably, this antibody has little effect on GH binding and also inhibits inducible metalloproteolysis of the GHR that occurs in the perimembranous ECD stem region. In the current study, we demonstrate that anti-GHR(ext-mAb) inhibits GH-dependent cellular proliferation and also inhibits hepatic GH signaling in vivo in mice that adenovirally express rabbit GHR, as assessed with our noninvasive bioluminescence hepatic signaling assay. A separate monoclonal antibody (anti-GHR(mAb 18.24)) is a sister clone of anti-GHR(ext-mAb). Here, we demonstrate that anti-GHR(mAb 18.24) also inhibits rabbit and human GHR signaling and inducible receptor proteolysis. Further, we use a random PCR-generated mutagenic expression system to map the three-dimensional epitopes in the rabbit GHR ECD for both anti-GHR(ext-mAb) and anti-GHR(mAb 18.24). We find that each of the two antibodies has similar, but nonidentical, discontinuous epitopes that include regions of subdomain 2 encompassing the dimerization interface. These results have fundamental implications for understanding the role of the dimerization interface and subdomain 2 in GHR activation and regulated GHR metalloproteolysis and may inform development of therapeutics that target GHR.

Published

2011

15. Development of a Method for the Determination of Pulsatile Growth Hormone Secretion in Mice

Author

Johannes D. Veldhuis, Michael J. Waters, Shyuan T. Ngo, H. Y. Tan, T. Y. Xie, Frederik J. Steyn, Lili Huang, Albert F. Parlow, Chen Chen, and J. W. Leong

Subjects

Male, Blood Specimen Collection, medicine.medical_specialty, Deconvolution analysis, Period (gene), Pulsatile flow, Enzyme-Linked Immunosorbent Assay, Blood volume, Biology, Growth hormone secretion, Mice, Inbred C57BL, Mice, Endocrinology, Growth Hormone, Internal medicine, medicine, Animals, Secretion, Sample collection, Whole blood

Abstract

Measures of pulsatile GH secretion require frequent collection and analysis of blood samples at regular intervals. Due to blood volume constraints, repeat measures of circulating levels of GH in mice remain challenging. Consequently, few observations exist in which the pulsatile pattern of GH secretion in mice have been characterized. To address this, we developed a technique for the collection and analysis of circulating levels of GH at regular and frequent intervals in freely moving mice. This was achieved through the development of a sensitive assay for the detection of GH in small (2 μl) quantities of whole blood. The specificity and accuracy of this assay was validated following guidelines established for single-laboratory validation as specified by the International Union of Pure and Applied Chemistry. We incorporated an established method for tail-clip blood sample collection to determine circulating levels of GH secretion in 36 whole blood samples collected consecutively over a period of 6 h. Resulting measures were characterized by peak secretion periods and interpulse stable baseline secretion periods. Periods characterized by elevated whole blood GH levels consisted of multicomponent peaks. Deconvolution analysis of resulting measures confirmed key parameters associated with pulsatile GH secretion. We show a striking decrease in pulsatile GH secretion in mice after 12-18 h of fasting. This model is necessary to characterize the pulsatile profile of GH secretion in mice and will significantly contribute to current attempts to clarify mechanisms that contribute to the regulation of GH secretion.

Published

2011

16. GH-Dependent STAT5 Signaling Plays an Important Role in Hepatic Lipid Metabolism

Author

Michael J. Waters, Mayumi Ishikawa, Linda M. Kerr, Elizabeth E. Powell, Timothy R. McPhee, Lauren A. Murray, Johanna L. Barclay, and Caroline N. Nelson

Subjects

Male, medicine.medical_specialty, Normal diet, Protein Array Analysis, Biology, Cell Line, Mice, Endocrinology, Internal medicine, STAT5 Transcription Factor, medicine, Animals, STAT1, STAT3, STAT5, Mice, Knockout, Fatty liver, Receptors, Somatotropin, Lipid Metabolism, medicine.disease, Fatty Liver, STAT1 Transcription Factor, Gene Expression Regulation, Liver, Growth Hormone, Hepatocytes, biology.protein, STAT protein, Steatosis, Signal transduction

Abstract

GH deficiency is known to be clinically associated with a high incidence of nonalcoholic fatty liver disease, and this can be reversed by GH administration. Here we investigated the mechanistic basis for this phenomenon using engineered male mice lacking different signaling elements of the GH receptor, hepatic stat5a/b−/− mice and a mouse hepatoma line. We found deficient GH-dependent signal transducer and activator of transcription (STAT)-5 signaling correlates with steatosis, and through microarray analysis, quantitative PCR, and chromatin immunoprecipitation, identified putative targets of STAT5 signaling responsible for the steatosis seen on a normal diet. These targets were verified with liver-specific stat5a/b deletion in vivo, and in vitro we show that dominant-negative (DN) STAT5 increases lipid uptake in a mouse hepatoma line. Because loss of STAT5 signaling results in elevated STAT1 and STAT3 activity and intracellular lipid accumulation, we have used DN-STAT5a/b, DN-STAT1, constitutively active (CA)-STAT3, or addition of oleate/palmitate in the hepatoma line to assign which of these apply to individual targets in STAT5 signaling deficiency. These findings and published mouse models of steatosis enable us to propose elevated cd36, pparγ, and pgc1α/β expression as primary instigators of the steatosis along with elevated fatty acid synthase, lipoprotein lipase, and very low-density lipoprotein receptor expression. Decreased fgf21 and insig2 expression may also contribute. In conclusion, despite normal plasma free fatty acids and minimal obesity, absent GH activation leads to steatosis because activated STAT5 prevents hepatic steatosis. These results raise the possibility of low-dose GH treatment for nonalcoholic fatty liver disease.

Published

2011

17. Growth Hormone Receptor: Structure Function Relationships

Author

Andrew J. Brooks and Michael J. Waters

Subjects

Janus kinase 2, Endocrinology, Diabetes and Metabolism, Tropomyosin receptor kinase B, Biology, Interleukin-13 receptor, Tropomyosin receptor kinase C, Receptor tyrosine kinase, Cell biology, Endocrinology, Biochemistry, Pediatrics, Perinatology and Child Health, ROR1, Enzyme-linked receptor, biology.protein, Insulin-like growth factor 1 receptor

Abstract

Background: The growth hormone receptor (GHR) was the first class 1 cytokine receptor to be cloned, and it has been studied intensively. The crystal structures of the bound and unbound forms have been solved and the energetic contributions of residues involved in the binding interaction have been quantified. Two receptor subunits bind to opposite sides of the hormone through site 1 and site 2, and a third interaction occurs between receptors in the lower β-sandwich module at site 3. All three interactions are required for receptor activation, which was thought to be a consequence of hormone-induced receptor dimerization. However, substantial data support the existence of a constitutive receptor dimer that interacts via the transmembrane domain (TMD), with receptor activation triggered by a hormone-induced conformational change. Mutagenesis studies and crystal structure data indicate that receptor activation involves a relative rotation and scissor movement of subunits to activate the associated tyrosine kinase, Janus kinase 2 (JAK2). We have recently reported that a second tyrosine kinase, an Src-family kinase, also associates constitutively with the receptor and activates the Ras–extracellular-signal-regulated kinase pathway. Activation of this kinase requires a conformational change in a loop of the lower sandwich module, and a different orientation of the TMDs than needed for JAK2 activation. Conclusions: This structural difference could allow differential activation of these two kinases by GH analogues such as I179M human GH.

Published

2011

18. The growth hormone receptor: mechanism of activation and clinical implications

Author

Andrew J. Brooks and Michael J. Waters

Subjects

Models, Molecular, medicine.medical_specialty, Thyroid hormone receptor, Growth-hormone-releasing hormone receptor, Human Growth Hormone, Endocrinology, Diabetes and Metabolism, Receptors, Somatotropin, Growth hormone receptor, Janus Kinase 2, Biology, Models, Biological, Thyroid hormone receptor beta, Hormone Antagonists, Endocrinology, Growth factor receptor, Hormone receptor, Thyrotropin-releasing hormone receptor, Internal medicine, Mutation, medicine, Animals, Humans, Phosphorylation, Insulin-like growth factor 1 receptor

Abstract

Growth hormone is widely used clinically to promote growth and anabolism and for other purposes. Its actions are mediated via the growth hormone receptor, both directly by tyrosine kinase activation and indirectly by induction of insulin-like growth factor 1 (IGF-1). Insensitivity to growth hormone (Laron syndrome) can result from mutations in the growth hormone receptor and can be treated with IGF-1. This treatment is, however, not fully effective owing to the loss of the direct actions of growth hormone and altered availability of exogenous IGF-1. Excessive activation of the growth hormone receptor by circulating growth hormone results in gigantism and acromegaly, whereas cell transformation and cancer can occur in response to autocrine activation of the receptor. Advances in understanding the mechanism of receptor activation have led to a model in which the growth hormone receptor exists as a constitutive dimer. Binding of the hormone realigns the subunits by rotation and closer apposition, resulting in juxtaposition of the catalytic domains of the associated tyrosine-protein kinase JAK2 below the cell membrane. This change results in activation of JAK2 by transphosphorylation, then phosphorylation of receptor tyrosines in the cytoplasmic domain, which enables binding of adaptor proteins, as well as direct phosphorylation of target proteins. This model is discussed in the light of salient information from closely related class 1 cytokine receptors, such as the erythropoietin, prolactin and thrombopoietin receptors.

Published

2010

19. Growth hormone promotes proliferation of adult neurosphere cultures

Author

M.-G. Lum, Ann M. Turnley, Samuel McLenachan, and Michael J. Waters

Subjects

medicine.medical_specialty, Neurogenesis, Endocrinology, Diabetes and Metabolism, Cellular differentiation, Blotting, Western, Subventricular zone, Biology, Immunoenzyme Techniques, Mice, Endocrinology, Tubulin, Epidermal growth factor, Spheroids, Cellular, Internal medicine, Neurosphere, STAT5 Transcription Factor, medicine, Animals, Immunoprecipitation, Receptors, Growth Factor, Phosphorylation, Progenitor cell, Autocrine signalling, Cells, Cultured, Cell Proliferation, Mice, Knockout, Neurons, Stem Cells, Cell Differentiation, Neural stem cell, Mice, Inbred C57BL, medicine.anatomical_structure, Growth Hormone

Abstract

Objectives Growth hormone (GH) and its receptor (GHR) are widely expressed in the CNS. During development, GH signaling regulates both proliferation of neural progenitor cells as well as their differentiation into neurons and glia. Here we have examined the effect of GH signaling on adult subventricular zone derived neural progenitor cells cultured as neurospheres. Design GH was added to adult wild-type (WT) neurosphere cultures and neurosphere growth measured using the MTT cell proliferation assay. To examine the influence of endogenous GH production on neural progenitors, neurospheres derived from GH receptor knockout (GHRKO) mice were examined by measuring neurosphere sizes and Ki67 and TUNEL immunoreactivity. In addition, neurosphere growth curves were compared following long term culture. Finally, the differentiation of WT vs. GHRKO neurospheres was compared using immunocytochemistry for βIII-tubulin and GFAP. Results While GH alone was insufficient to support neurosphere formation, it enhanced neurosphere growth by 20% in the presence of epidermal growth factor and fibroblast growth factor-2. Compared to wildtype neurospheres, GHRKO neurospheres were smaller, contained fewer proliferating cells and exhibited reduced self-renewal in long term culture. Addition of GH increased STAT5 phosphorylation levels in neurosphere cells. Upon differentiation, GHRKO neurospheres showed accelerated neurogenesis, although over time similar numbers of βIII-tubulin positive neurons were generated by cells of both genotypes. Conclusions GH functions as an autocrine mitogen in adult neurosphere cultures and promotes proliferation of neural progenitor cells as well as self-renewal of neurosphere cultures. In addition, signaling through the GHR appeared to delay neuronal differentiation in adult neurospheres.

Published

2009

20. Exercise Increases Neural Stem Cell Number in a Growth Hormone-Dependent Manner, Augmenting the Regenerative Response in Aged Mice

Author

Michael J. Waters, Beatrice Large, Rodney L. Rietze, Daniel G. Blackmore, and Mohammad Ghasem Golmohammadi

Subjects

Aging, medicine.medical_specialty, Neurogenesis, Hippocampus, Endogeny, Biology, Mice, Lateral Ventricles, Internal medicine, Neurosphere, medicine, Animals, Humans, Cognitive decline, Exercise, Cells, Cultured, Cell Proliferation, Neurons, Stem Cells, Neurodegeneration, Brain, Cell Biology, medicine.disease, Neural stem cell, Nerve Regeneration, Mice, Inbred C57BL, Endocrinology, nervous system, Growth Hormone, Molecular Medicine, Stem cell, Developmental Biology

Abstract

The exercise-induced enhancement of learning and memory, and its ability to slow age-related cognitive decline in humans led us to investigate whether running stimulates periventricular (PVR) neural stem cells (NSCs) in aging mice, thereby augmenting the regenerative capacity of the brain. To establish a benchmark of normal aging on endogenous NSCs, we harvested the PVR from serial vibratome sections through the lateral ventricles of juvenile (6-8 weeks), 6-, 12-, 18-, and 24-month-old mice, culturing the cells in the neural colony-forming cell assay. A significant decline in NSC frequency was apparent by 6 months (∼40%), ultimately resulting in a ∼90% reduction by 24 months. Concurrent with this decline was a progressive loss in regenerative capacity, as reflected by an incomplete repopulation of neurosphere-forming cells following gamma cell irradiation-induced depletion of the PVR. However, voluntary exercise (i.e., 21 days of running) significantly increased NSC frequency in mice ≥ 18 months of age, augmenting the regeneration of irradiation-ablated periventricular cells and restoring NSC numbers to youthful levels. Importantly, and consistent with the demonstrated ability of growth hormone (GH) to increase NSC proliferation, and the elevated secretion of GH during exercise, exercise failed to stimulate NSCs in GH receptor-null mice. These findings now provide a novel basis for understanding the ability of exercise to delay the onset and rate of decline in neurodegenerative conditions not typically associated with the hippocampus and suggest that the GH-dependent activation of endogenous NSCs may be effective in reversing or preventing age-related neurodegeneration in humans. Disclosure of potential conflicts of interest is found at the end of this article.

Published

2009

21. Growth hormone receptor; mechanism of action

Author

Jong Wei Wooh, Michael J. Waters, Kathryn A. Tunny, and Andrew J. Brooks

Subjects

Cell Nucleus, Thyroid hormone receptor, Growth-hormone-releasing hormone receptor, Receptors, Somatotropin, Cell Biology, Biology, Biochemistry, Thyroid hormone receptor beta, Protein Transport, Thyrotropin-releasing hormone receptor, Interleukin-21 receptor, Cancer research, Animals, Humans, Estrogen-related receptor gamma, Nuclear receptor co-repressor 1, Insulin-like growth factor 1 receptor

Abstract

The growth hormone receptor has been an archetype for ligand-induced receptor dimerisation in cytokine receptor signalling. However, we now know that it exists as a constitutive dimer and is activated by a reorganisation of receptor subunits as a result of asymmetric placement of two receptor binding sites on the hormone monomer. This review highlights several topics including: current models of receptor activation; recent advances in the understanding of GH signalling demonstrating that ligand-induced signalling activates Src/ERK pathway in parallel to the classical JAK2-STAT5 signalling; and the nuclear localised growth hormone receptor correlates with high proliferation status and carcinogenesis.

Published

2008

22. How growth hormone controls growth, obesity and sexual dimorphism

Author

Agnieszka M. Lichanska and Michael J. Waters

Subjects

Sex Characteristics, medicine.medical_specialty, Cell signaling, Janus kinase 2, biology, Microarray analysis techniques, STAT5B, Endocrinology, Liver, Growth Hormone, Internal medicine, STAT5 Transcription Factor, Genetics, biology.protein, medicine, Animals, Humans, Obesity, Signal transduction, Cytokine receptor, Transcription factor, Proto-oncogene tyrosine-protein kinase Src

Abstract

Understanding the molecular basis for the many actions of growth hormone (GH) has been challenging because many of these actions are only evident in vivo. Recently, STAT5b has emerged as a key GH signaling intermediate in the regulation of postnatal growth, adiposity and sexual dimorphism of hepatic gene expression. This realization is based on targeted disruption or mutation of the GH receptor and its signaling components, together with clinical studies of GH-insensitive mutants. Microarray analysis of liver from GH receptor and signal transducer and activation of transcription 5b (STAT5b)-deleted mice have identified a range of relevant transcripts regulated by the Janus kinase 2/STAT5b signaling pathway. In addition, many transcripts are regulated independently of STAT5b, presumably as a result of PtdIns 3-kinase, extracellular-regulated kinase and Src signaling by this pleiotropic cytokine receptor.

Published

2008

23. New Insights into Growth Hormone Receptor Function and Clinical Implications

Author

Michael J. Waters and Agnieszka M. Lichanska

Subjects

medicine.medical_specialty, Hormone Replacement Therapy, Endocrinology, Diabetes and Metabolism, Growth hormone receptor, Growth hormone, Bioinformatics, Models, Biological, Short stature, Endocrinology, Neoplasms, Internal medicine, STAT5 Transcription Factor, medicine, Animals, Humans, Diabetic Nephropathies, Obesity, Hormone replacement therapy, Receptor, Growth Disorders, STAT5, Regulation of gene expression, biology, Receptors, Somatotropin, Gene Expression Regulation, Pediatrics, Perinatology and Child Health, biology.protein, medicine.symptom, Metabolic Networks and Pathways, Function (biology), Signal Transduction

Abstract

Although used as a therapeutic for 50 years, it is only recently that the application of molecular techniques has provided a basis for understanding growth hormone’s (GH) clinical actions. This article reviews progress in our current knowledge of the molecular mechanism of growth hormone (GH) receptor activation based on a number of physicochemical techniques, and documents insights gained into the means used by the activated GH receptor to control the expression of genes regulating growth and metabolism. These findings are related to disorders of short stature, and the therapeutic consequences are summarized.

Published

2008

24. Characterization of the SOCS3 Promoter Response to Prostaglandin E2 in T47D Cells

Author

Stephen T. Anderson, Michael J. Waters, Johanna L. Barclay, and Jon D. Curlewis

Subjects

Lipopolysaccharides, STAT3 Transcription Factor, Sp1 Transcription Factor, Molecular Sequence Data, Suppressor of Cytokine Signaling Proteins, Biology, Response Elements, Dinoprostone, chemistry.chemical_compound, Endocrinology, Cell Line, Tumor, Serine, Humans, Immunoprecipitation, SOCS3, Phosphorylation, Cyclic AMP Response Element-Binding Protein, Luciferases, Promoter Regions, Genetic, STAT3, Molecular Biology, Base Sequence, Suppressor of cytokine signaling 1, digestive, oral, and skin physiology, Tyrosine phosphorylation, General Medicine, Cyclic AMP-Dependent Protein Kinases, GC Rich Sequence, Up-Regulation, chemistry, Suppressor of Cytokine Signaling 3 Protein, STAT protein, Cancer research, biology.protein, Signal transduction, Janus kinase

Abstract

Suppressor of cytokine signaling 3 (SOCS3), a negative regulator of cytokine signaling, is expressed in breast cancer cells where it can modify sensitivity and responsiveness to cytokine signaling through the Janus kinase/signal transducer and activator of transcription (JAK/STAT) pathways. Although it is widely accepted that SOCS3 expression is in itself regulated by STATs, we and others have shown that prostaglandins can also up-regulate SOCS3 expression. Here we used T47D breast cancer cells treated with prostaglandin E2 (PGE2) to examine this pathway. T47D cells responded to PGE2 stimulation with a significant increase in SOCS3 mRNA that was independent of de novo protein synthesis. PGE2 stimulation resulted in STAT3 serine and tyrosine phosphorylation, although mutation of either of the two previously characterized STAT response elements on the SOCS3 promoter did not affect SOCS3 promoter activation by PGE2. In addition, overexpression of STAT3 wild-type, constitutively active or dominant-negative constructs did not affect PGE2-induced SOCS3 promoter activation, indicating that STATs are unlikely mediators of this pathway in these cells. PGE2 is a known activator of the cAMP/protein kinase A (PKA) pathway, and in T47D cells, up-regulation of SOCS3 mRNA by PGE2 was abolished by pretreatment with H89, a PKA inhibitor and increased by cAMP and forskolin treatment. Consistent with this, PGE2 treatment increased cAMP response element (CRE)-binding protein serine phosphorylation. However, mutation of the activator protein 1/CRE on the promoter did not affect basal or PGE2-stimulated activation, suggesting a role for cAMP/PKA that is independent of CRE-binding protein binding. Mutation of the GC-rich region of the SOCS3 promoter, a putative Sp1/Sp3 binding site, abolished both basal and PGE2-stimulated activation. Gel-shift assays showed increased complex formation after treatment, and this was inhibited by the addition of an Sp1 antibody or pretreatment with PKA inhibitor. Chromatin immunoprecipitation assay verified Sp1 binding to the promoter in response to PGE2. Sp1 overexpression increased SOCS3 promoter activation, and both basal and PGE2-induced SOCS3 mRNA expression was prevented by mithramycin, an inhibitor of Sp1 DNA binding. Finally, a physiological role for PGE2 was demonstrated with PGE2 pretreatment reducing lipopolysaccharide-induced STAT3 activation. Collectively, this study details a novel mechanism of SOCS3 up-regulation by PGE2 in breast cancer cells that appears to be STAT independent and involve Sp1 binding to the promoter. This process has possible implications for cytokine responsiveness and tumor progression.

Published

2007

25. The growth hormone receptor

Author

Michael J. Waters

Subjects

0301 basic medicine, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Growth hormone receptor, Tropomyosin receptor kinase C, Receptor tyrosine kinase, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Downregulation and upregulation, Enzyme-linked receptor, STAT5 Transcription Factor, Animals, Humans, Receptor, Gene, Binding selectivity, STAT5, 030304 developmental biology, Insulin-like growth factor 1 receptor, 0303 health sciences, biology, Prolactin receptor, Alternative splicing, Receptors, Somatotropin, Janus Kinase 2, Interleukin-13 receptor, Cell biology, 030104 developmental biology, src-Family Kinases, JAK2, Biochemistry, Growth Hormone, ROR1, biology.protein, Estrogen-related receptor gamma, Mechanism, Receptor structure, Hormone, Src, Proto-oncogene tyrosine-protein kinase Src

Abstract

Once thought to be present only in liver, muscle and adipose tissue, the GH receptor is now known to be ubiquitously distributed, in accord with the many pleiotropic actions of GH. These include the regulation of metabolism, postnatal growth, cognition, immune, cardiac and renal systems and gut function. GH exerts these actions primarily through alterations in gene expression, initiated by activation of its membrane receptor and the resultant activation of the associated JAK2 (Janus kinase 2) and Src family kinases. Receptor activation involves hormone initiated movements within a receptor homodimer, rather than simple receptor dimerization. We have shown that binding of the hormone realigns the orientation of the two receptors both by relative rotation and by closer apposition just above the cell membrane. This is a consequence of the asymmetric placement of the binding sites on the hormone. Binding results in a conversion of parallel receptor transmembrane domains into a rotated crossover orientation, which produces separation of the lower part of the transmembrane helices. Because the JAK2 is bound to the Box1 motif proximal to the inner membrane, receptor activation results in separation of the two associated JAK2s, and in particular the removal of the inhibitory pseudokinase domain from the kinase domain of the other JAK2 (and vice versa). This brings the two kinase domains into position for trans-activation and initiates tyrosine phosphorylation of the receptor cytoplasmic domain and other substrates such as STAT5, the key transcription factor mediating most genomic actions of GH.There are a limited number of genomic actions initiated by the Src kinase family member which also associates with the upper cytoplasmic domain of the receptor, including important immune regulatory actions to dampen exuberant innate immune activation of cells involved in transplant rejection. These findings offer insights for developing specific receptor antagonists which may be valuable in cancer therapy.

Published

2015

26. Effect of Deletion of Ghrelin-O-Acyltransferase on the Pulsatile Release of Growth Hormone in Mice

Author

Shyuan T. Ngo, Lisa K. Chopin, T. Y. Xie, Frederik J. Steyn, Johannes D. Veldhuis, Matthias H. Tschöp, Michael J. Waters, Penelope L. Jeffery, Chen Chen, Virginie Tolle, and Jacques Epelbaum

Subjects

Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Growth hormone secretagogue receptor, Hypothalamus, Biology, Growth Hormone-Releasing Hormone, Cellular and Molecular Neuroscience, Mice, Endocrinology, Internal medicine, medicine, Animals, Neuropeptide Y, Insulin-Like Growth Factor I, Receptor, Receptors, Ghrelin, Mice, Knockout, Endocrine and Autonomic Systems, Growth factor, Membrane Proteins, Growth hormone–releasing hormone, Ghrelin O-acyltransferase, Somatostatin, Growth Hormone, Ghrelin, Acyltransferases

Abstract

Ghrelin, a gut hormone originating from the post-translational cleavage of preproghrelin, is the endogenous ligand of growth hormone secretagogue receptor 1a (GHS-R1a). Within the growth hormone (GH) axis, the biological activity of ghrelin requires octanoylation by ghrelin-O-acyltransferase (GOAT), conferring selective binding to the GHS-R1a receptor via acylated ghrelin. Complete loss of preproghrelin-derived signalling (through deletion of the Ghrl gene) contributes to a decline in peak GH release; however, the selective contribution of endogenous acyl-ghrelin to pulsatile GH release remains to be established. We assessed the pulsatile release of GH in ad lib. fed male germline goat(-/-) mice, extending measures to include mRNA for key hypothalamic regulators of GH release, and peripheral factors that are modulated relative to GH release. The amount of GH released was reduced in young goat(-/-) mice compared to age-matched wild-type mice, whereas pulse frequency and irregularity increased. Altered GH release did not coincide with alterations in hypothalamic Ghrh, Srif, Npy or Ghsr mRNA expression, or pituitary GH content, suggesting that loss of Goat does not compromise canonical mechanisms that contribute to pituitary GH production and release. Although loss of Goat resulted in an irregular pattern of GH release (characterised by an increase in the number of GH pulses observed during extended secretory events), this did not contribute to a change in the expression of sexually dimorphic GH-dependent liver genes. Of interest, circulating levels of insulin-like growth factor (IGF)-1 were elevated in goat(-/-) mice. This rise in circulating levels of IGF-1 was correlated with an increase in GH pulse frequency, suggesting that sustained or increased IGF-1 release in goat(-/-) mice may occur in response to altered GH release patterning. Our observations demonstrate that germline loss of Goat alters GH release and patterning. Although the biological relevance of altered GH secretory patterning remains unclear, we propose that this may contribute to sustained IGF-1 release and growth in goat(-/-) mice.

Published

2015

27. Rewriting the mechanism of JAK2 activation

Author

Andrew J. Brooks and Michael J. Waters

Subjects

B-cell receptor, Cell Biology, Receptors, Somatotropin, Biology, Janus Kinase 2, Editorials: Cell Cycle Features, Interleukin-13 receptor, Glycoprotein 130, Models, Biological, Cell biology, Enzyme Activation, Biochemistry, Small heterodimer partner, Enzyme-linked receptor, Fluorescence Resonance Energy Transfer, Animals, Humans, 5-HT5A receptor, Protein Multimerization, Receptors, Cytokine, Receptor, Molecular Biology, Developmental Biology, G protein-coupled receptor

Abstract

Class I cytokine receptors regulate a wide range of clinically relevant cellular processes. This family of receptors contains around 30 members including receptors for erythropoietin (EPO), prolactin (PRL), growth hormone (GH), thrombopoietin (TPO), granulocyte-macrophage colony-stimulating factor (GM-CSF), leukemia inhibitory factor (LIF), interleukin-3 (IL-3), IL-5, and IL-6.1 The growth hormone receptor has been the archetype for the class I cytokine receptor family, as it was the first to be both cloned and have its extracellular domain crystal structure solved. The original paradigm for the mechanism of activation was based on biophysical and structural studies over 20 y ago showing that growth hormone binding to the extracellular domain of the receptor occurred in a sequential fashion, first binding to a high affinity site on a single receptor (site 1) and then binding to a lower affinity site (site 2) on a second receptor.2 The subsequent publication of the crystal structure showed a single hormone bound to 2 receptor domains at the site 1 and site 2 positions, and also revealed the lower fibronectin III domain of the receptor locked together (site 3 or dimerization domain).3 The conclusion from these studies was that hormone binding induced dimerization of the receptor and that this would bring the intracellular signaling domains together to allow association and activation of the associated janus kinases (JAKs). However, despite great progress in elucidating the structural details of ligand binding to the extracellular domain of receptors for several members of this family, the means by which these receptors activate their associated JAKs to initiate signaling had remained elusive. The original ligand-mediated activation model was undermined by several lines of evidence, particularly by studies showing that the GH receptor and other related receptors such as the PRL, EPO, and TPO receptors exist predominantly as dimers prior to ligand binding.4 The question remained as to how ligand binding was able to transmit its signal through the transmembrane domain and to the intracellular domain of the pre-dimerized receptors to activate the associated kinases. Our group embarked on studies to unravel this mechanism, and recently were able to present the first complete mechanistic model of JAK2 activation by an archetypal class I cytokine receptor, the growth hormone receptor.5 We confirmed that the GH receptor exists as a preformed dimer in vivo by using confocal microscopy anisotropy analysis at the surface of live mammalian cells. We then utilized a model system where we could lock receptors in different activation states. We did this by removing the extracellular domain of the receptor and replacing it with the dimerizing leucine zipper from the JUN transcription factor which results in a constitutively active receptor. We interrogated the role of the 12 residue linker that joins the transmembrane domain to the extracellular domain and found that as the zipper was brought closer to the membrane, the activation signal strength increased. We then monitored the relative positioning of the JAK2 binding region of the intracellular domains of the receptor by placing FRET reporters 37 amino acids below the Box1 motif in order to retain JAK2 binding to the receptor. By comparing the FRET signal from the leucine zipper construct with the weakest activation signal (containing the full 12 amino acid linker) to the construct with the strongest signal (no linker) we found that an increase in receptor signaling correlated with an increased distance between the JAK2 binding regions of the receptor, i.e., the intracellular domains were separating upon activation. We then confirmed that GH addition to its receptor induced a separation of the JAK2 binding regions by using a GH receptor construct with FRET reporters placed at the same intracellular position as before. Since the activation of a pre-dimerized receptor must be transmitting a signal through the transmembrane domain, we identified the interaction face of the transmembrane domains of the receptor in the absence of GH by cysteine crosslinking analysis and molecular modeling. Further in silico modeling showed that the transmembrane domains are in a parallel interaction in the inactive state and that transition to the active state involves a rotation resulting in a left-handed crossover dimer. This brings the residues at the extracellular juxtamembrane in close proximity, while C-termini of the transmembrane domains separate, explaining the repositioning of the intracellular domains that we observed with FRET upon activation. Previous models of JAK2 activation did not identify a separation of the JAK2 binding Box1 motifs, therefore we proposed a new model of JAK2 activation where in the inactive state of the predimerized receptor the pseudokinase domain from a JAK2 molecule that is bound to one receptor, interacts with and inhibits the kinase domain of the JAK2 bound to the other receptor. Upon activation, the intracellular domains of the receptor where the JAK2 FERM domain is bound separate, which brings the kinase domains together, facilitating trans-activation (Fig. 1). We were able to use FRET, molecular modeling as well as interaction and JAK2 activation assays to support this model.5 The key remaining question is: does such a mechanism generalize to other class I cytokine receptors? Figure 1. Activation model of homodimeric class I cytokine receptors shown for the archetypal GH receptor. Adapted from Brooks et al.5

Published

2015

28. Expression of Histocompatibility 2 Blastocyst (H2-Bl) in Embryonic Stem Cells Inhibits CD8+ T-Cell Activation but is not Sufficient to Facilitate Graft Tolerance

Author

Martin F. Lavin, Andrew J. Brooks, Steven Dingwall, Ernst J. Wolvetang, Michael J. Waters, and Simon H. Apte

Subjects

Endothelial stem cell, Induced stem cells, Cancer stem cell, Immunology, Biology, Stem cell, Induced pluripotent stem cell, Embryonic stem cell, Stem cell transplantation for articular cartilage repair, Cell biology, Adult stem cell

Abstract

Universal embryonic stem cell donor lines would greatly facilitate stem cell based regenerative medicine and permit facile testing of human pluripotent stem cell derived grafts in xenogeneic settings. Because HLA-G overcomes immune cell mediated attack of foetal tissues during pregnancy and inhibits T-cell responses and dendritic cell antigen maturation in vitro and in vivo, it is an attractive candidate molecule for achieving this goal. Here we investigated whether enforced expression of either the soluble or the membrane bound form of the HLA-G mouse homologue, H2- Bl, in human and mouse ES cell lines would allow engraftment in immunocompetent mice. Despite evidence for robust expression of soluble or membrane bound H2-Bl molecules and effective inhibition of CD8+ T-cell proliferation by all H2-Bl engineered ES cell lines, all failed to generate teratomas in immunocompetent mice, despite doing so in NODSCID mice. We conclude that expression of H2-Bl in human and mouse embryonic stem cells alone is insufficient to overcome xenogeneic rejection.

Published

2015

29. Prolactin and the expression of suppressor of cytokine signaling-3 in the sheep adrenal gland before birth

Author

Michael J. Waters, Sheridan Gentili, Jeffrey Schwartz, Isabella Caroline McMillen, Gentili, Sheridan, Schwartz, J, Waters, M, and McMillen, Isabella Caroline

Subjects

medicine.medical_specialty, Physiology, Adipose tissue, Suppressor of Cytokine Signaling Proteins, Biology, Fetus, Hormone Antagonists, Pregnancy, Physiology (medical), Internal medicine, Adrenal Glands, medicine, Animals, RNA, Messenger, SOCS3, Biological sciences, Bromocriptine, Cells, Cultured, Fetal Growth Retardation, Sheep, Adrenal gland, medicine.disease, Angiotensin II, Prolactin, Endocrinology, medicine.anatomical_structure, Gene Expression Regulation, Adrenal Cortex, Female

Abstract

The fetal pituitary-adrenal axis plays a key role in the fetal response to intrauterine stress and in the timing of parturition. The fetal sheep adrenal gland is relatively refractory to stimulation in midgestation (90–120 days) before the prepartum activation, which occurs around 135 days gestation (term = 147 ± 3 days). The mechanisms underlying the switch from adrenal quiescence to activation are unclear. Therefore, we have investigated the expression of suppressor of cytokine signaling-3 (SOCS-3), a putative inhibitor of tissue growth in the fetal sheep adrenal between 50 and 145 days gestation and in the adrenal of the growth-restricted fetal sheep in late gestation. SOCS-3 is activated by a range of cytokines, including prolactin (PRL), and we have, therefore, determined whether PRL administered in vivo or in vitro stimulates SOCS-3 mRNA expression in the fetal adrenal in late gestation. There was a decrease ( P < 0.005) in SOCS-3 expression in the fetal adrenal between 54 and 133 days and between 141 and 144 days gestation. Infusion of the dopaminergic agonist, bromocriptine, which suppressed fetal PRL concentrations but did not decrease adrenal SOCS-3 mRNA expression. PRL administration, however, significantly increased adrenal SOCS-3 mRNA expression ( P < 0.05). Similarly, there was an increase ( P < 0.05) in SOCS-3 mRNA expression in adrenocortical cells in vitro after exposure to PRL (50 ng/ml). Placental and fetal growth restriction had no effect on SOCS-3 expression in the adrenal during late gestation. In summary, the decrease in the expression of the inhibitor SOCS-3 after 133 days gestation may be permissive for a subsequent increase in fetal adrenal growth before birth. We conclude that factors other than PRL act to maintain adrenal SOCS-3 mRNA expression before 133 days gestation but that acute elevations of PRL can act to upregulate adrenal SOCS-3 expression in the sheep fetus during late gestation.

Published

2006

30. Differential regulation of suppressor of cytokine signaling-3 in the liver and adipose tissue of the sheep fetus in late gestation

Author

Michael J. Waters, I. Caroline McMillen, Sheridan Gentili, Gentili, Sheridan, Waters, M, and McMillen, Isabella Caroline

Subjects

prolactin, medicine.medical_specialty, Physiology, Placenta, growth, medicine.medical_treatment, Adipose tissue, Gestational Age, Suppressor of Cytokine Signaling Proteins, 111401 [FOR], Growth hormone receptor, Biology, stat, Physiology (medical), Internal medicine, STAT5 Transcription Factor, medicine, Animals, Animal Physiology - Cell, RNA, Messenger, SOCS3, development, Bromocriptine, Fetus, Sheep, Prolactin receptor, Foetal Development and Medicine, Gene Expression Regulation, Developmental, Prolactin, Cell biology, Endocrinology, Cytokine, Adipose Tissue, Liver, Suppressor of Cytokine Signaling 3 Protein, Systems Physiology, pregnancy, Signal transduction, Signal Transduction, Media Studies

Abstract

It is unknown whether the JAK/STAT/suppressor of cytokine signaling-3 (SOCS-3) intracellular signaling pathway plays a role in tissue growth and metabolism during fetal life. We investigated whether there is a differential profile of SOCS-3 expression in the liver and perirenal adipose tissue during the period of increased fetal growth in late gestation and the impact of fetal growth restriction on SOCS-3 expression in the fetal liver. We also determined whether basal SOCS-3 expression in the fetal liver and perirenal adipose tissue is regulated by endogenous fetal prolactin (PRL). SOCS-3 mRNA abundance was higher in the liver than in the pancreas, spleen, and kidney of the sheep fetus during late gestation. In the liver, SOCS-3 mRNA expression was increased ( P < 0.05) between 125 ( n = 4) and 145 days ( n = 7) gestation and lower ( P < 0.05) in growth-restricted compared with normally grown fetal sheep in late gestation. The relative expression of SOCS-3 mRNA in the fetal liver was directly related to the mean plasma PRL concentrations during a 48-h infusion of either a dopaminergic agonist, bromocriptine ( n = 7), or saline ( n = 5), such that SOCS-3 mRNA expression was lower when plasma PRL concentrations decreased below ∼20 ng/ml [ y = 0.99 − (2.47/ x) + (4.96/ x2); r2 = 0.91, P < 0.0001, n = 12]. No relationship was shown between the abundance of phospho-STAT5 in the fetal liver and circulating PRL. SOCS-3 expression in perirenal adipose tissue decreased ( P < 0001) between 90–91 ( n = 6) and 140–145 days ( n = 9) gestation and was not related to endogenous PRL concentrations. Thus SOCS-3 is differentially expressed and regulated in key fetal tissues and may play an important and tissue-specific role in the regulation of cellular proliferation and differentiation before birth.

Published

2006

31. Mechanisms Underlying the Diminished Sensitivity to Prolactin Negative Feedback during Lactation: Reduced STAT5 Signaling and Up-Regulation of Cytokine-Inducible SH2 Domain-Containing Protein (CIS) Expression in Tuberoinfundibular Dopaminergic Neurons

Author

Michael J. Waters, Stephen T. Anderson, Jon D. Curlewis, Daphne H. L. Kusters, Kent Fanning, and Johanna L. Barclay

Subjects

medicine.medical_specialty, Suppressor of cytokine signaling 1, Dopaminergic, Biology, Prolactin, Endocrinology, medicine.anatomical_structure, Hypothalamus, Internal medicine, Lactation, medicine, biology.protein, SOCS3, Signal transduction, STAT5

Abstract

Hyperprolactinaemia during lactation is a consequence of the sucking stimulus and in part due to reduced prolactin (PRL) negative feedback. To date, the mechanisms involved in this diminished sensitivity to PRL feedback are unknown but may involve changes in PRL signal transduction within tuberoinfundibular dopaminergic (TIDA) neurons. Therefore, we investigated signal transducers and activators of transcription (STAT) 5 signaling in the TIDA neurons of lactating rats. Dual-label confocal immunofluorescence studies were used to determine the intracellular distribution of STAT5 within TIDA neurons in the dorsomedial arcuate nucleus. In lactating rats with pups removed for 16 h, injection of ovine PRL significantly (P < 0.05) increased the STAT5 nuclear/cytoplasmic ratio compared with vehicle-treated mothers. In contrast, ovine PRL injection did not increase the STAT5 nuclear/cytoplasmic ratio in lactating mothers with pups, demonstrating that PRL signal transduction through STAT5 is reduced in TIDA neurons in the presence of pups. To investigate possible mechanisms involved in reduced PRL signaling, we examined the expression of suppressors of cytokine signaling (SOCS) proteins. Northern analysis on whole hypothalamus showed that CIS (cytokine-inducible SH2 domain-containing protein), but not SOCS1 or SOCS3, mRNA expression was significantly (P < 0.01) up-regulated in suckled lactating rats. Semiquantitative RT-PCR on arcuate nucleus micropunches also showed up-regulation of CIS transcripts. Immunofluorescence studies demonstrated that CIS is expressed in all TIDA neurons in the dorsomedial arcuate nucleus, and the intensity of CIS staining in these neurons is significantly (P < 0.05) increased in lactating rats with sucking pups. Together, these results support the hypothesis that loss of sensitivity to PRL-negative feedback during lactation is a result of increased CIS expression in TIDA neurons.

Published

2006

32. Chemical Effects in Biological Systems—Data Dictionary (CEBS-DD): A Compendium of Terms for the Capture and Integration of Biological Study Design Description, Conventional Phenotypes, and ‘Omics Data

Author

Rick Irwin, Assunta-Susanna Sansone, Michael J. Waters, Michael L. Cunningham, Wenjun Bao, Weida Tong, Jennifer H. Madenspacher, Ann M. Richard, Atif Hasan, Danielle Choi, Norman Morrison, B. Alex Merrick, William Eastin, Roger Brown, Asif Rashid, Jennifer Fostel, Richard S. Paules, Pierre R. Bushel, Chihae Yang, Philippe Rocca-Serra, Thomas Papoian, Alex Garcia, James L. Stevens, Maribel Bruno, David J. Dix, Carlos Frade, Kenneth B. Tomer, Craig Zwickl, and Alexandra N. Heinloth

Subjects

Proteomics, Research design, Biomedical Research, Databases, Factual, Dose-Response Relationship, Drug, Systems Biology, Toxicogenetics, Administration, Oral, Context (language use), Data dictionary, Biology, Toxicology, Bioinformatics, Data science, Compendium, Variety (cybernetics), Research Design, Terminology as Topic, Component (UML), Toxicity Tests, Animals, Database Management Systems, Toxicogenomics, Acetaminophen

Abstract

A critical component in the design of the Chemical Effects in Biological Systems (CEBS) Knowledgebase is a strategy to capture toxicogenomics study protocols and the toxicity endpoint data (clinical pathology and histopathology). A Study is generally an experiment carried out during a period of time for the purpose of obtaining data, and the Study Design Description captures the methods, timing, and organization of the Study. The CEBS Data Dictionary (CEBS-DD) has been designed to define and organize terms in an attempt to standardize nomenclature needed to describe a toxicogenomics Study in a structured yet intuitive format and provide a flexible means to describe a Study as conceptualized by the investigator. The CEBS-DD will organize and annotate information from a variety of sources, thereby facilitating the capture and display of toxicogenomics data in biological context in CEBS, i.e., associating molecular events detected in highly-parallel data with the toxicology/pathology phenotype as observed in the individual Study Subjects and linked to the experimental treatments. The CEBS-DD has been developed with a focus on acute toxicity studies, but with a design that will permit it to be extended to other areas of toxicology and biology with the addition of domain-specific terms. To illustrate the utility of the CEBS-DD, we present an example of integrating data from two proteomics and transcriptomics studies of the response to acute acetaminophen toxicity (A. N. Heinloth et al., 2004, Toxicol. Sci. 80, 193-202).

Published

2005

33. In Vivo Analysis of Growth Hormone Receptor Signaling Domains and Their Associated Transcripts

Author

Agnieszka M. Lichanska, Elisabetta M. d’Aniello, Jennifer E. Rowland, Michael J. Waters, Sheryl L. Maher, Rohan D. Teasdale, Mary White, Linda M. Kerr, Peter G. Noakes, and Richard J. C. Brown

Subjects

Cytoplasm, Time Factors, Genotype, Transgene, Blotting, Western, Immunoblotting, Mutant, Mice, Transgenic, Growth hormone receptor, Biology, Mice, Downregulation and upregulation, STAT5 Transcription Factor, Animals, Immunoprecipitation, Obesity, RNA, Messenger, Insulin-Like Growth Factor I, Receptor, Molecular Biology, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Mitogen-Activated Protein Kinase 3, Models, Genetic, Stem Cells, Homozygote, Exons, Organ Size, Receptors, Somatotropin, Cell Biology, Blotting, Northern, Milk Proteins, Molecular biology, Protein Structure, Tertiary, Up-Regulation, DNA-Binding Proteins, Phenotype, Gene Expression Regulation, Mutation, Trans-Activators, RNA, Phosphorylation, Erratum, Signal transduction, hormones, hormone substitutes, and hormone antagonists, Densitometry, Signal Transduction

Abstract

The growth hormone receptor (GHR) is a critical regulator of postnatal growth and metabolism. However, the GHR signaling domains and pathways that regulate these processes in vivo are not defined. We report the first knock-in mouse models with deletions of specific domains of the receptor that are required for its in vivo actions. Mice expressing truncations at residue m569 (plus Y539/545-F) and at residue m391 displayed a progressive impairment of postnatal growth with receptor truncation. Moreover, after 4 months of age, marked male obesity was observed in both mutant 569 and mutant 391 and was associated with hyperglycemia. Both mutants activated hepatic JAK2 and ERK2, whereas STAT5 phosphorylation was substantially decreased for mutant 569 and absent from mutant 391, correlating with loss of IGF-1 expression and reduction in growth. Microarray analysis of these and GHR(-/-) mice demonstrated that particular signaling domains are responsible for the regulation of different target genes and revealed novel actions of growth hormone. These mice represent the first step in delineating the domains of the GHR regulating body growth and composition and the transcripts associated with these domains.

Published

2005

34. Increased Site 1 Affinity Improves Biopotency of Porcine Growth Hormone

Author

Andrew McDevitt, Yu Wan, Bojiang Shen, Mark L. Smythe, and Michael J. Waters

Subjects

Phage display, Protein subunit, Cell Biology, Plasma protein binding, Biology, Biochemistry, Cell biology, Binding site, Signal transduction, Receptor, Molecular Biology, Ternary complex, Hormone

Abstract

Based on phage display optimization studies with human growth hormone (GH), it is thought that the biopotency of GH cannot be increased. This is proposed to be a result of the affinity of the first receptor for hormone far exceeding that which is required to trap the hormone long enough to allow diffusion of the second receptor to form the ternary complex, which initiates signaling. We report here that despite similar site 1 kinetics to the hGH/hGH receptor interaction, the potency of porcine GH for its receptor can be increased up to 5-fold by substituting hGH residues involved in site 1 binding into pGH. Based on extensive mutations and BIAcore studies, we show that the higher potency and site 1 affinity of hGH for the pGHR is primarily a result of a decreased off-rate associated with residues in the extended loop between helices 1 and 2 that interact with the two key tryptophans Trp104 and Trp169 in the receptor binding hot spot. Our mutagenic analysis has also identified a second determinant (Lys165), which in addition to His169, restricts the ability of non-primate hormones to activate hGH receptor. The increased biopotency of GH that we observe can be explained by a model for GH receptor activation where subunit alignment is critical for effective signaling.

Published

2004

35. Comparative analysis of CNS populations in knockout mice with altered growth hormone responsiveness

Author

Ann M. Turnley, Yona Goldshmit, Perry F. Bartlett, Mark I. Ransome, and Michael J. Waters

Subjects

Central Nervous System, Male, medicine.medical_specialty, Interneuron, Cell Count, Suppressor of Cytokine Signaling Proteins, Calbindin, Mice, Internal medicine, medicine, Animals, Cholinergic neuron, Mice, Knockout, Neurons, Glial fibrillary acidic protein, biology, General Neuroscience, Cell Differentiation, DNA-Binding Proteins, Mice, Inbred C57BL, Repressor Proteins, medicine.anatomical_structure, Endocrinology, nervous system, Growth Hormone, Trans-Activators, biology.protein, Neuron, NeuN, Calretinin, Neuroscience, hormones, hormone substitutes, and hormone antagonists, Parvalbumin

Abstract

Recently we have shown that growth hormone (GH) inhibits neuronal differentiation and that this process is blocked by suppressor of cytokine signalling-2 (SOCS2). Here we examine several cortical and subcortical neuronal populations in GH hyper-responsive SOCS2 null (-/-) mice and GH non-responsive GH receptor null (GHR-/-) mice. While SOCS2-/- mice showed a 30% decrease in density of NeuN positive neurons in cortex compared to wildtype, GHR-/- mice showed a 25% increase even though brain size was decreased. Interneuron sub-populations were variably affected, with a slight decrease in cortical parvalbumin expressing interneurons in SOCS2-/- mice and an increase in cortical calbindin and calretinin and striatal cholinergic neuron density in GHR-/- mice. Analysis of glial cell numbers in cresyl violet or glial fibrillary acidic protein (GFAP) stained sections of cortex showed that the neuron : glia ratio was increased in GHR-/- mice and decreased in SOCS2-/- mice. The astrocytes in GHR-/- mice appeared smaller, while they were larger in SOCS2-/- mice. Neuronal soma size also varied in the different genotypes, with smaller striatal cholinergic neurons in GHR-/- mice. While the size of layer 5 pyramidal neurons was not significantly different from wildtype, SOCS2-/- neurons were larger than GHR-/- neurons. In addition, primary dendritic length was similar in all genotypes but dendritic branching of pyramidal neurons in the cortex appeared sparser in GHR-/- and SOCS2-/- mice. These results suggest that GH, possibly regulated by SOCS2, has multiple effects on central nervous system (CNS) development and maturation, regulating the number and size of multiple neuronal and glial cell types.

Published

2004

36. Epitope Map for a Growth Hormone Receptor Agonist Monoclonal Antibody, MAb 263

Author

Michael J. Waters, Yu Wan, Richard J. C. Brown, Jonathan M. Harris, and Yuan Zhi Zheng

Subjects

Models, Molecular, Agonist, genetic structures, Protein Conformation, medicine.drug_class, Molecular Sequence Data, Growth hormone receptor, Crystallography, X-Ray, Monoclonal antibody, Epitope, Immunoglobulin Fab Fragments, Mice, Endocrinology, Antibody Specificity, medicine, Animals, Humans, Amino Acid Sequence, Disulfides, Receptor, Molecular Biology, Cellular localization, biology, Tryptophan, Antibodies, Monoclonal, Receptors, Somatotropin, General Medicine, Molecular biology, Epitope mapping, Immunoglobulin G, Mutation, biology.protein, Rabbits, Antibody, Sequence Alignment, Epitope Mapping

Abstract

Monoclonal antibody (MAb) 263 is a widely used monoclonal antibody that recognizes the extracellular domain (ECD) of the GH receptor. It has been shown to act as a GH agonist both in vitro and in vivo, and we report here that it must be divalent to exert its effect on the full-length receptor. To understand the mechanism of its agonist action, we have determined the precise epitope for this antibody using a novel random PCR mutagenesis approach together with expression screening in yeast. A library of 5200 clones of rabbit GH receptor ECD mutants were screened both with MAb 263 and with an anticarboxy-tag antibody to verify complete ECD expression. Sequencing for clones that expressed complete ECD but were not MAb 263 positive identified 20 epitope residues distributed in a discontinuous manner throughout the ECD. The major part of the epitope, as revealed after mapping onto the crystal structure model of the ECD molecule, was located on the side and upper portion of domain 1, particularly within the D–E strand disulfide loop 79–96. Molecular dynamics docking of an antibody of the same isotype as MAb 263 was used to dock the bivalent antibody to the 1528-A 2 epitope and to visualize the likely consequences of MAb binding. The minimized model enables the antibody to grasp two receptors in a pincer-like movement from opposite sides, facilitating alignment of the receptor dimerization domains in a manner similar to, but not identical with, GH. (Molecular Endocrinology 17: 2240–2250, 2003)

Published

2003

37. Suppressor of cytokine signalling gene expression is elevated in breast carcinoma

Author

H Li, Michael J. Waters, Gérard Morel, Michael A. McGuckin, Mireille Raccurt, Tomás García-Caballero, Patrick Lau, S P Tam, Anne Lambert, Hichem C. Mertani, and Richard J. C. Brown

Subjects

prolactin, Cancer Research, medicine.medical_treatment, Breast Neoplasms, Suppressor of Cytokine Signaling Proteins, carcinoma, Biology, Suppressor of cytokine signalling, Immediate-Early Proteins, src Homology Domains, Suppressor of Cytokine Signaling 1 Protein, Breast cancer, Tumor Cells, Cultured, cytokine, medicine, Humans, Autocrine signalling, In Situ Hybridization, breast, Regulation of gene expression, Human Growth Hormone, Kinase, Carcinoma, Ductal, Breast, Intracellular Signaling Peptides and Proteins, Molecular and Cellular Pathology, Proteins, Cancer, medicine.disease, SOCS, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Repressor Proteins, Carcinoma, Intraductal, Noninfiltrating, Cytokine, Oncology, Suppressor of Cytokine Signaling 3 Protein, Protein Biosynthesis, growth hormone, Trans-Activators, Cancer research, Cytokines, Female, Signal transduction, Carrier Proteins, Signal Transduction, Transcription Factors

Abstract

Cytokines are important for breast cell function, both as trophic hormones and as mediators of host defense mechanisms against breast cancer. Recently, inducible feedback suppressors of cytokine signalling (SOCS/JAB/SSI) have been identified, which decrease cell sensitivity to cytokines. We examined the expression of SOCS genes in 17 breast carcinomas and 10 breast cancer lines, in comparison with normal tissue and breast lines. We report elevated expression of SOCS-1-3 and CIS immunoreactive proteins within in situ ductal carcinomas and infiltrating ductal carcinomas relative to normal breast tissue. Significantly increased expression of SOCS-1-3 and CIS transcripts was also shown by quantitative in situ hybridisation within both tumour tissue and reactive stroma. CIS transcript expression was elevated in all 10 cancer lines, but not in control lines. However, there was no consistent elevation of other SOCS transcripts. CIS protein was shown by immunoblot to be present in all cancer lines at increased levels, mainly as the 47 kDa ubiquitinylated form. A potential proliferative role for CIS overexpression is supported by reports that CIS activates ERK kinases, and by strong induction in transient reporter assays with an ERK-responsive promoter. The in vivo elevation of SOCS gene expression may be part of the host/tumour response or a response to autocrine/paracrine GH and prolactin. However, increased CIS expression in breast cancer lines appears to be a specific lesion, and could simultaneously shut down STAT 5 signalling by trophic hormones, confer resistance to host cytokines and increase proliferation through ERK kinases.

Published

2003

38. Growth hormone regulates osteogenic marker mRNA expression in human periodontal fibroblasts and alveolar bone-derived cells

Author

Michael J. Waters, Saso Ivanovski, H. R. Haase, and P. M. Bartold

Subjects

Bone sialoprotein, medicine.medical_specialty, biology, Cellular differentiation, Osteoblast, Molecular biology, Bone morphogenetic protein 2, Bone morphogenetic protein 7, medicine.anatomical_structure, Endocrinology, Cell culture, Internal medicine, medicine, Osteocalcin, biology.protein, Periodontics, Osteopontin

Abstract

Background: Growth hormone (GH) is a potent regulator of bone formation. The proposed mechanism of GH action is through the stimulation of osteogenic precursor Cell proliferation and, following clonal expansion of these cells. promotion of differentiation along the osteogenic lineage. Objectives: We tested this hypothesis by studying the effects of GH on primary cell populations of human periodontal ligament cells (PLC) and alveolar bone cells (ABC), which contain a spectrum of osteogenic precursors. Method: The cell populations were assessed for mineralization potential after long-term culture in media containing beta-glycerophosphate and ascorbic acid, by the demonstration of mineral deposition by Von Kossa staining. The proliferative response of the cells to GH was determined over a 48-h period using a crystal violet dye-binding assay. The profile of the cells in terms of osteogcnic marker expression was established using quantitative reverse transcriptase polymerase chain reaction (RT-PCR) for alkaline phosphatase (ALP), osteopontin. osteocalcin, bone sialoprotein (BSP), as well as the bone morphogenetic proteins BMP-2, BMP-4 and BMP-7. Results: As expected, a variety of responses were observed ranging from no mineralization in the PLC populations to dense mineralized deposition observed in one GH-treated ABC population. Over a 48-h period GH was found to be non-mitogenic for all cell populations. Quantitative reverse transcriptase polymerase chain reaction (RT-PCR) BSP mRNA expression correlated well with mineralizing potential of the cells. The change in the mRNA expression of the osteogenic markers was determined following GH treatment of the cells over a 48-h period. GH caused an increase in ALP in most cell populations, and also in BMP expression in some cell populations. However a decrease in BSP. osteocalcin and osteopontin expression in the more highly differentiated cell populations was observed in response to GH. Conclusion: The response of the cells indicates that while long-term treatment with GH may promote mineralization, short-term treatment does not promote proliferation of osteoblast precursors nor induce expression of late osteogenic markers.

Published

2003

39. Genetic disruption of the growth hormone receptor does not influence motoneuron survival in the developing mouse

Author

John J. Kopchick, Michael J. Waters, Glen B. Banks, Karen T. Coschigano, Jenny A Rowland, Sean A Parsons, and Peter G. Noakes

Subjects

Male, Nervous system, Embryology, Programmed cell death, medicine.medical_specialty, Cell Survival, Immunoblotting, Central nervous system, Apoptosis, Growth hormone receptor, Biology, Immunoenzyme Techniques, Mice, Internal medicine, medicine, Animals, Muscle, Skeletal, Mice, Knockout, Motor Neurons, Mice, Inbred BALB C, Lumbar Vertebrae, Receptors, Somatotropin, Spinal cord, Mice, Inbred C57BL, medicine.anatomical_structure, Endocrinology, Spinal Cord, Growth Hormone, Knockout mouse, biology.protein, Female, Neuron death, Signal Transduction, Developmental Biology, Neurotrophin

Abstract

In the rodent central nervous system (CNS) during the five days prior to birth, both growth hormone (GH) and its receptor (GHR) undergo transient increases in expression to levels considerably higher than those found postnatally. This increase in expression coincides with the period of neuronal programmed cell death (PCD) in the developing CNS. To evaluate the involvement of growth hormone in the process of PCD, we have quantified the number of motoneurons in the spinal cord and brain stem of wild type and littermate GHR-deficient mice at the beginning and end of the neuronal PCD period. We found no change in motoneuron survival in either the brachial or lumbar lateral motor columns of the spinal cord or in the trochlear, trigeminal, facial or hypoglossal nuclei in the brain stem. We also found no significant differences in spinal cord volume, muscle fiber diameter, or body weight of GHR-deficient fetal mice when compared to their littermate controls. Therefore, despite considerable in vitro evidence for GH action on neurons and glia, genetic disruption of GHR signalling has no effect on prenatal motoneuron number in the mouse, under normal physiological conditions. This may be a result of compensation by the signalling of other neurotrophic cytokines.

Published

2003

40. The role of growth hormone in fetal development

Author

P.L Kaye and Michael J. Waters

Subjects

Ovulation, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Embryonic Development, Mice, Transgenic, Biology, Embryonic and Fetal Development, Mice, Endocrinology, Pregnancy, Internal medicine, medicine, Animals, Humans, Placental lactogen, Maternal-Fetal Exchange, Cellular localization, media_common, Fetus, Prolactin receptor, Embryo, Receptors, Somatotropin, Prolactin, Rats, Growth Hormone, embryonic structures, Female, Hormone

Abstract

Studies across several species, particularly the mouse, show that growth hormone (GH, somatotrophin) is an important determinant of litter size, and to a lesser extent, of birth length. GH acts at all stages of development, from ovulation through preimplantation development to the late fetus, with actions on both embryo/fetus and mother contributing to successful fetal development. The fact that these are not more obvious in vivo is likely a result of redundancy of cytokine hormone action, particularly in relation to prolactin, which shares common actions and receptor locations with GH.

Published

2002

41. Plasma growth hormone and growth hormone-binding protein during development in the marsupial brushtail possum (Trichosurus vulpecula)

Author

Robert T. Gemmell, J. D. Curlewis, Michael J. Waters, and M. C. Saunders

Subjects

Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Endocrinology, Pregnancy, Growth hormone-binding protein, Cell surface receptor, Internal medicine, medicine, Animals, Marsupial, biology, Molecular mass, Binding protein, Opossums, Phalangeridae, Ligand (biochemistry), biology.organism_classification, Precipitin Tests, Molecular Weight, Milk, Growth Hormone, Chromatography, Gel, Brushtail possum, Female, Carrier Proteins, Half-Life, Protein Binding

Abstract

Plasma concentrations of growth hormone (GH) were measured in the brushtail possum (Trichosurus vulpecula) pouch young from 25 through to 198 days post-partum (n=71). GH concentrations were highest early in pouch life (around 100 ng/ml), and thereafter declined in an exponential fashion to reach adult concentrations (10.8+/-1.8 ng/ml; n=21) by approximately 121-145 days post-partum, one to two months before the young is weaned. Growth hormone-binding protein (GHBP), which has been shown to modify the cellular actions of GH in eutherian mammals, was identified for the first time in a marsupial. Based on size exclusion gel filtration, possum GHBP had an estimated molecular mass of approximately 65 kDa, similar to that identified in other mammalian species, and binding of (125)I-labelled human GH (hGH) was displaced by excess hGH (20 microg). An immunoprecipitation method, in which plasma GHBP was rendered polyethylene glycol precipitable with a monoclonal antibody to the rabbit GHBP/GH receptor (MAb 43) and labelled with (125)I-hGH, was used to quantitate plasma GHBP by Scatchard analysis in the developing (pooled plasma samples) and adult (individual animals) possums. Binding affinity (K(a)) values in pouch young aged between 45 and 54 and 144 and 153 days post-partum varied between 1.0 and 2.4 x 10(9)/M, which was slightly higher than that in adult plasma (0.96+/-0.2 x 10(9)/M, n=6). Binding capacity (B(max)) values increased from non-detectable levels in animals aged 25-38 days post-partum to reach concentrations around half that seen in the adult (1.4+/-0.2 x 10(-9) M) by about 117 days post-partum and remained at this level until 153 days post-partum. Therefore, in early pouch life when plasma GH concentrations are highest, the very low concentrations of GHBP are unlikely to be important in terms of competing with GH-receptor for ligand or altering the half-life of circulating GH.

Published

2002

42. A novel bioassay for human somatogenic activity in serum samples supports the clinical reliability of immunoassays

Author

Michael J. Waters, Andrew Cotterill, S. W. Rowlinson, Kin Chuen Leung, N. J. Marshall, Jennifer E. Rowland, and Ken K. Y. Ho

Subjects

medicine.medical_specialty, medicine.diagnostic_test, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Biology, Monoclonal antibody, medicine.disease, Idiopathic short stature, Endocrinology, Growth hormone-binding protein, Immunoassay, Internal medicine, Blood plasma, Pegvisomant, medicine, Bioassay, Receptor, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

OBJECTIVE Because there is discordance between different immunoassay values for serum hGH, and because clinical state may not correlate with immunoreactive hGH, we have developed an assay to accurately measure serum hGH somatogenic bioactivity. The results of this assay were compared with the Elegance two-site ELISA assay across 135 patient samples in a variety of clinical states. DESIGN The somatogenic assay was based on stable expression of hGH receptor in the murine BaF line, allowing these cells to proliferate in response to hGH. To eliminate interference by other growth factors in serum, we created a specific antagonist of the hGH receptor (similar to Trovert or Pegvisomant) which allowed us to obtain a true measure of hGH somatogenic activity by subtraction of the activity in the presence of the antagonist. The assay was carried out in microtiter plates over 24 h, with oxidation of a chromogenic tetrazolium salt (MTT) as the endpoint. PATIENTS These encompassed a number of different clinical conditions related to short stature, including idiopathic short stature, neurosecretory dysfunction and renal failure, as well as obese patients on dietary restriction and normal volunteers. MEASUREMENTS In addition to the colourimetric (MTT) response to hGH, we measured free hGH by stripping out GHBP-bound hGH using beads coupled to a monoclonal antibody to the GHBP (GH binding protein). All samples were measured in both bioassay and ELISA assay. RESULTS This bioassay was sensitive (5 mU/l or 2 mug/l) and precise, and not subject to interference by the GHBP. There was a good correlation (r = 0.95) between bioactivity and immunoactivity across clinical states. There was, however, an increased bioactivity during secretory peaks (over 25 mU/l), which has been reported previously for the Nb2 bioassay. Free hGH did not correlate with clinical state. CONCLUSIONS Because the results of the Elegance ELISA and the bioassay correlate well, even though there is greater bioactivity at higher hormone concentrations, it is evident that an appropriate immunoassay is able to act as a reliable indicator for clinical assessment. In those rare cases where bio-inactive GH exists, our bioassay should provide an appropriate means to demonstrate this.

Published

2002

43. A new mechanism for growth hormone receptor activation of JAK2, and implications for related cytokine receptors

Author

Yash Chhabra, Andrew J. Brooks, and Michael J. Waters

Subjects

Janus kinase 1, transmembrane helix, General Medicine, Review, Biology, Interleukin-13 receptor, Tropomyosin receptor kinase C, molecular dynamics, Cell biology, conformational change, Interleukin-21 receptor, receptor dimer, Immunology, FRET, Estrogen-related receptor gamma, Cytokine receptor, Box1, Common gamma chain, Insulin-like growth factor 1 receptor

Abstract

The growth hormone receptor was the first cytokine receptor to be cloned and crystallized, and provides a valuable exemplar for activation of its cognate kinase, JAK2. We review progress in understanding its activation mechanism, in particular the molecular movements made by this constitutively dimerized receptor in response to ligand binding, and how these lead to a separation of JAK-binding Box1 motifs. Such a separation leads to removal of the pseudokinase inhibitory domain from the kinase domain of a partner JAK2 bound to the receptor, and vice versa, leading to apposition of the kinase domains and transactivation. This may be a general mechanism for class I cytokine receptor action.

Published

2014

44. Growth Hormone (GH)/GH Receptor Expression and GH-Mediated Effects During Early Bovine Embryogenesis1

Author

Sabine Kölle, Michael J. Waters, Katja Prelle, Fred Sinowatz, Miodrag Stojkovic, and Eckhard Wolf

Subjects

medicine.medical_specialty, Embryogenesis, Embryo, Cell Biology, General Medicine, Growth hormone receptor, Biology, medicine.anatomical_structure, Endocrinology, Reproductive Medicine, Internal medicine, embryonic structures, medicine, Conceptus, Inner cell mass, Blastocyst, Receptor, Developmental biology, hormones, hormone substitutes, and hormone antagonists

Abstract

Pituitary growth hormone (GH) stimulates postnatal growth and metabolism. The role of GH and its receptor (GHR) during prenatal development, however, is still controversial. As shown by reverse transcription polymerase chain reaction (RT-PCR), bovine in vitro fertilization embryos synthesized the transcript of GHR from Day 2 of embryonic life onwards. Real time RT-PCR revealed that synthesis of GHR mRNA was increased 5.9-fold in 6-day-old embryos compared with 2-day-old embryos. Using in situ hybridization, the mRNA encoding GHR was predominantly localized to the inner cell mass of blastocysts. The GHR protein was first visualized 3 days after fertilization. GH-specific transcripts were first detected in embryos on Day 8 of in vitro culture. As shown by transmission electron microscopy, GH treatment resulted in elimination of glycogen storage in 6- to 8-dayold embryos and an increase in exocytosis of lipid vesicles. These results suggest that a functional GHR able to modulate carbohydrate and lipid metabolism is synthesized during preimplantation development of the bovine embryo and that this GHR may be subject to activation by embryonic GH after Day 8. conceptus, developmental biology, early development, growth hormone, IVF/ART

Published

2001

45. Binding and Functional Studies with the Growth Hormone Receptor Antagonist, B2036-PEG (Pegvisomant), Reveal Effects of Pegylation and Evidence That It Binds to a Receptor Dimer1

Author

Kin-Chuen Leung, W. Bennett, Ken K. Y. Ho, Nathan Doyle, Michael J. Waters, Richard J. Ross, and M. Maamra

Subjects

medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Biochemistry (medical), Clinical Biochemistry, Biology, Biochemistry, Erythropoietin receptor, Endocrinology, Competitive antagonist, Growth hormone-binding protein, Cell surface receptor, Internal medicine, Pegvisomant, medicine, PEGylation, Receptor, Growth Hormone Receptor Antagonist, medicine.drug

Abstract

GH actions are dependent on receptor dimerization. The GH receptor antagonist, B2036-PEG, has been developed for treating acromegaly. B2036 has mutations in site 1 to enhance receptor binding and in site 2 to block receptor dimerization. Pegylation (B2036-PEG) increases half-life and lowers immunogenicity, but high concentrations are required to control insulin-like growth factor-I levels. We examined antagonist structure and function and the impact of pegylation on biological efficacy. Unpegylated B2036 had a 4.5-fold greater affinity for GH binding protein (GHBP) than GH but similar affinity for membrane receptor. Pegylation substantially reduced membrane binding affinity and receptor antagonism, as assessed by a transcription assay, by 39- and 20-fold, respectively. GHBP reduced antagonist activity of unpegylated B2036 but did not effect antagonism by B2036-PEG. B2036 down-regulated receptors, and membrane binding sites doubled in the presence of dimerization-blocking antibodies, suggesting that B2036 binds to a receptor dimer. It is concluded that the high concentration requirement of B2036-PEG for clinical efficacy relates to pegylation, which decreases binding to membrane receptor but has the advantages of reduced clearance, immunogenicity, and interactions with GHBP. Our studies suggest that B2036 binds to a receptor dimer and induces internalization but not signaling.

Published

2001

46. Insulin Regulation of Human Hepatic Growth Hormone Receptors: Divergent Effects on Biosynthesis and Surface Translocation1

Author

Michael J. Waters, Nathan Doyle, Kin Chuen Leung, Ken K. Y. Ho, and Mercedes Ballesteros

Subjects

medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Insulin, medicine.medical_treatment, media_common.quotation_subject, Biochemistry (medical), Clinical Biochemistry, Growth hormone receptor, Biology, Biochemistry, Endocrinology, Internal medicine, Insulin receptor substrate, medicine, Phosphorylation, Receptor, Internalization, Pancreatic hormone, Intracellular, media_common

Abstract

Insulin modulates the biological actions of GH, but little is known about its effect on human hepatic GH receptors (GHRs). Using the human hepatoma cell line HuH7 as a model, we investigated insulin regulation of total, intracellular, and cell surface GHRs and receptor biosynthesis and turnover. Insulin up-regulated total and intracellular GHRs in a concentration-dependent manner. It increased surface GHRs in a biphasic manner, with a peak response at 10 nmol/L, and modulated GH-induced Janus kinase-2 phosphorylation in parallel with expression of surface GHRs. The abundance of GHR messenger ribonucleic acid and protein, as assessed by RT-PCR and Western analysis, respectively, markedly increased with insulin treatment. To examine whether insulin regulates GHRs at the posttranslational level, its effects on receptor surface translocation and internalization were investigated. Insulin suppressed surface translocation in a concentration-dependent manner, whereas internalization was unaffected. Moreover, insulin actions on total GHRs and surface translocation were inhibited by PD98059 and wortmannin, respectively. In conclusion, insulin regulates hepatic GHR biosynthesis and surface translocation in a reciprocal manner, with surface receptor availability the net result of the divergent effects. The divergent actions of insulin appear to be mediated by the mitogen-activated protein kinase and phosphatidylinositol 3-kinase pathways, respectively.

Published

2000

47. Identification of Genes Induced by Growth Hormone in Rat Liver Using cDNA Arrays

Author

Michael J. Waters, Catherine A. Shang, and Barry J. L. Thompson

Subjects

Monocarboxylic Acid Transporters, STAT3 Transcription Factor, medicine.medical_specialty, DNA, Complementary, DNA Repair, Matrix Metalloproteinases, Membrane-Associated, medicine.medical_treatment, Carbon-Oxygen Lyases, Gene Expression, p38 Mitogen-Activated Protein Kinases, Rats, Mutant Strains, Endocrinology, Internal medicine, Complementary DNA, Gene expression, DNA-(Apurinic or Apyrimidinic Site) Lyase, medicine, Animals, RNA, Messenger, STAT3, biology, Gadd45, Growth factor, Intracellular Signaling Peptides and Proteins, Fibrinogen, Metalloendopeptidases, Proteins, Glycoprotein 130, Receptors, Interleukin-6, Molecular biology, Deoxyribonuclease IV (Phage T4-Induced), Rats, DNA-Binding Proteins, Kinetics, Somatropin, Liver, Growth Hormone, Trans-Activators, biology.protein, Mitogen-Activated Protein Kinases, Signal transduction, Carrier Proteins, DNA Damage, Signal Transduction

Abstract

Growth hormone (GH) is a pleiotropic cytokine that acts upon its target cells to regulate their growth, differentiation and metabolism. GH is thought to act by altering gene expression in target cells, but few GH-regulated genes are known. In this study, we used cDNA array analysis to identify genes rapidly induced in the liver of GH-deficient dwarf rats following a single systemic injection of GH. Eight genes were found to upregulate their mRNA expression within 1-3 hours of GH administration, results which were confirmed by northern analysis. The identity of these genes suggests GH may influence a diversity of cellular processes. A role for GH in regulating cytokine and growth factor signalling is suggested by upregulation of mRNAs encoding three signal transducers: a subunit of the receptor for IL-6-type cytokines (gp130), STAT3 (signal transducer and activator of transcription) and p38MAPK (mitogen activated protein kinase). Two genes involved in DNA repair and cell cycle control, APEN (apurinic endonuclease) and GADD45 (growth arrest and DNA damage 45) were upregulated. Other induced genes include those encoding a lactate transporter (MCT-1), an extracellular matrix remodelling enzyme, MTI-MMP (membrane type 1 matrix metalloproteinase) and an acute phase protein (fibrinogen beta). In summary, this work is the first to apply cDNA arrays to the study of peptide hormone action in vivo and has identified 8 novel GH target genes.

Published

2000

48. Molecular recognition events involved in the activation of the growth hormone receptor by growth hormone

Author

Michael J. Waters and Stuart N. Behncken

Subjects

Growth-hormone-releasing hormone receptor, Biochemistry, Thyroid hormone receptor alpha, Structural Biology, Hormone receptor, Prolactin receptor, Enzyme-linked receptor, Growth hormone receptor, Biology, Ligand (biochemistry), Receptor, Molecular Biology

Abstract

Binding of growth hormone (GH) to its receptor (GHR) is a well-studied example of molecular recognition between a cytokine and its receptor. Extensive mutagenesis studies and several crystal structures have defined the key interactive amino acid residues that are involved in binding and subsequent receptor dimerization. This review encompasses each of the three molecular recognition events involved in GHR activation, namely binding of GH to its two receptors and the interactions that occur between these receptors, Particular attention is given to species and ligand specificity of hormone binding and to the molecular recognition events involved in receptor activation, including the possibility that a conformational change in the receptor is required. Copyright (C) 1999 John Wiley & Sons, Ltd.

Published

1999

49. GROWTH HORMONE AS A CYTOKINE

Author

S. P. Tam, Peter E. Lobie, H. Li, Bojiang Shen, C. A. Shang, Stuart N. Behncken, and Michael J. Waters

Subjects

Pharmacology, medicine.medical_specialty, Janus kinase 2, biology, Physiology, medicine.medical_treatment, Growth hormone receptor, medicine.disease, Paracrine signalling, Endocrinology, Cytokine, Growth hormone-binding protein, Growth Hormone, Physiology (medical), Internal medicine, Laron syndrome, medicine, biology.protein, Animals, Cytokines, Humans, Receptor, Transcription factor

Abstract

1. The growth hormone (GH) receptor was the first of the class 1 cytokine receptors to be cloned. It shares a number of structural characteristics with other family members and common signalling mechanisms based on common usage of the Janus kinase 2 (JAK2). 2. Growth hormone receptor activation is initiated by GH-induced homodimerization of receptor molecules. This has enabled the creation of specific hormone antagonists that block receptor dimerization. 3. The details of the transcription factors used by the activated receptor are being revealed as a result of promoter analyses and electrophoretic mobility gelshift analysis. 4. Growth hormone receptors are widespread and their discovery in certain tissues has led to the assignment of new physiological roles for GH, Some of these involve local or paracrine roles for GH, as befits its cytokine status. 5. Four examples of such novel roles are discussed, These are: (i) the brain GH axis; (ii) GH and the vitamin B-12 axis; (iii) GH in early pre-implantation development; and (iv) GH in development of the tooth. 6. We propose that the view that GH acts through the intermediacy of insulin-like growth factor-1 is simplistic; rather, GH acts to induce an array of growth factors and their receptors and the composition of this array varies with tissue type and, probably, stage of development.

Published

1999

50. Alterations in the neural growth hormone axis following hypoxic–ischemic brain injury

Author

Erica Beilharz, Michael J. Waters, Arjan Scheepens, Chris E. Williams, Bernhard H. Breier, Peter D. Gluckman, and E. Sirimanne

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Central nervous system, Ischemia, Apoptosis, Growth hormone receptor, Biology, Neuroprotection, Brain Ischemia, Necrosis, Cellular and Molecular Neuroscience, Cerebrospinal fluid, Internal medicine, medicine, Animals, Insulin-Like Growth Factor I, Rats, Wistar, Hypoxia, Brain, Molecular Biology, Microglia, Growth factor, Cerebral Infarction, Organ Size, medicine.disease, Immunohistochemistry, Rats, Endocrinology, medicine.anatomical_structure, Blood-Brain Barrier, Growth Hormone, Female, Hormone

Abstract

Recently, there has been considerable interest in determining the role of the growth hormone receptor (GHR) in the central nervous system (CNS). The aim of this study was to investigate the role of circulating growth hormone (GH) and the neural GHR after hypoxic-ischemic (HI) brain injury in the 21-day old rat. We observed growth hormone receptor/binding protein (GHR/BP) immunoreactivity to be rapidly upregulated following a severe unilateral HI injury. There was a biphasic increase with an initial rise occurring in blood vessels within a few hours after injury followed by a secondary rise evident by 3 days post-hypoxia in microglia/macrophages, some of which are destined to express insulin-like growth factor-I (IGF-I). There was also an increased immunoreactivity in reactive astrocytes, some of which were in the process of dividing. Subsequently, we attempted to activate the endothelial GHR/BP which was found to be increased after injury by treating with 15 microgram g-1 day-1 s.c. bGH for 7 days. Circulating concentrations of IGF-I fell after injury and were restored with GH treatment (P=0.001), whereas treatment of normal animals had no effect on serum IGF-I. Peripheral GH treatment increased the cerebrospinal fluid (CSF) concentration of immunoreactive IGF-I in the injured rats (P=0.017). GH treatment also reversed the systemic catabolism caused by the injury but had no significant neuroprotective effects. These results indicate that GH therapy can be used to reverse the systemic catabolism that occurs after CNS injury. In addition, these data suggest a role for the neural GHR during the recovery from brain injury, both in terms of the induction of IGF-I and in terms of glial proliferation.

Published

1999