Your search keyword '"Melanie K. Miller"' showing total 13 results

1. Flibanserin: From Bench to Bedside

Author

Melanie K. Miller, Anita H. Clayton, and Erin M. Dooley

Subjects

medicine.medical_specialty, Urology, Endocrinology, Diabetes and Metabolism, Female sexual dysfunction, 030232 urology & nephrology, Food and drug administration, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, medicine, Clinical endpoint, Humans, Sexual Dysfunctions, Psychological, Psychiatry, Drug Approval, 030219 obstetrics & reproductive medicine, United States Food and Drug Administration, Obstetrics and Gynecology, Hypoactive sexual desire disorder, medicine.disease, United States, Bench to bedside, Psychiatry and Mental health, Distress, Reproductive Medicine, Female sexual function, Flibanserin, Benzimidazoles, Female, Psychology, medicine.drug

Abstract

Introduction The process of approval for flibanserin (trade name Addyi) has been associated with controversy since before its approval on August 18, 2015. This argument centered on challenges to the validity of the diagnosis of hypoactive sexual desire disorder in women and the safety and efficacy of the drug. Aim To explore the process of Food and Drug Administration (FDA) approval for flibanserin and delve further into the research, concerns, and various roadblocks to its approval. Methods A literature review was undertaken using the terms flibanserin and hypoactive sexual desire disorder and relevant commentary from supporters and critics regarding the medication and difficulties leading up to approval. Main Outcome Measures Review of the process of FDA approval of a medication to treat hypoactive sexual desire disorder and research published exploring the efficacy and safety of flibanserin. Results Before flibanserin, there were no drugs approved to treat hypoactive sexual desire disorder, which has a reported estimated incidence of 10% of women. For studying the effectiveness of flibanserin, the FDA required satisfying sexual events as the primary end point, although this end point does not measure level of desire or the associated distress. The satisfying sexual event measurement was significant across all three flibanserin trials in premenopausal women, as was an increase in desire according to the Female Sexual Function Index desire domain and a decrease in distress as recorded with the Female Sexual Distress Scale–Revised, Item 13. Safety concerns centered on the incidence of sedation, syncope, hypotension, and the interaction of flibanserin with alcohol and CYP3A4 inhibitors. Additional targeted challenge studies were mandated by the FDA. Conclusion The process of approval of flibanserin was lengthy. This was due in part to it being the first drug in its class and one with no clear guidance on study design from the FDA or roadmap for development and approval. Dooley EM, Miller MK, Clayton AH. Flibanserin: From Bench to Bedside. Sex Med Rev 2017;5:461–469.

Published

2017

2. Expert opinion on existing and developing drugs to treat female sexual dysfunction

Author

Anita H. Clayton, Jacqueline J Norman, Melanie K. Miller, and Joshua R Smith

Subjects

medicine.medical_specialty, Female sexual dysfunction, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Ospemifene, medicine, Bremelanotide, Animals, Humans, Pharmacology (medical), 030212 general & internal medicine, Sexual Dysfunctions, Psychological, Intensive care medicine, Drug Approval, Pharmacology, 030219 obstetrics & reproductive medicine, business.industry, United States Food and Drug Administration, Testosterone (patch), Hypoactive sexual desire disorder, Drugs, Investigational, medicine.disease, United States, Clinical trial, Sexual Dysfunction, Physiological, Drug development, chemistry, Drug Design, Flibanserin, Female, business, medicine.drug

Abstract

Female sexual dysfunction (FSD) is a highly prevalent, yet commonly underdiagnosed and undertreated condition. This paper reviews the diagnostic terminology for FSD, and basic sexual physiology in women. The Food and Drug Administration (FDA) approved drugs for FSD are discussed, followed by investigational drugs for FSD currently in phase 2 or 3 clinical trials, reasons for failure of drug development, and potential future drug targets. Areas covered: A literature review was conducted for available treatments for FSD: flibanserin, estrogen, ospemifene and prasterone. Potential treatments are assessed, as was the Pharmaprojects database which includes clinical trial information. Testosterone, bremelanotide, bupropion-trazodone, PDE-5 inhibitors, prostaglandins, tibolone and combination therapies, and the theoretical basis of potential drug targets are discussed. Expert opinion: The lack of established endpoints for phase 3 studies of FSD has impeded approval of new treatments, and required additional studies for validation, resulting in proposed changes to the FDA draft guidance for FSD clinical trials in October 2016. Current DSM-5 diagnostic nosology also fails to capture the full range of symptomology. Several promising compounds have shown no movement for several years limiting women's options. Overcoming socio-cultural bias against women's sexual and reproductive health will be critical in the approval of new treatments for FSD.

Published

2018

3. The sensitive giant: the role of titin-based stretch sensing complexes in the heart

Author

Henk Granzier, Elisabeth Ehler, Melanie K. Miller, and Carol C. Gregorio

Subjects

Cardiomyopathy, Dilated, Sarcomeres, Contraction (grammar), Sarcolemma, Costameres, Muscle Proteins, Heart, Cell Biology, Anatomy, Biology, musculoskeletal system, Models, Biological, Myocardial Contraction, cardiovascular system, Biophysics, Heart beat, biology.protein, Animals, Humans, Myocyte, Connectin, Titin, Cytoskeleton, Myofibril, Protein Kinases

Abstract

Every heart beat is not equal. As physiological demands of the cardiovascular system change, cardiac myocytes modulate contractile parameters including the rate and force of contraction. Adaptive responses require the sensing of biomechanical signals involving the interface between the contractile cytoskeleton (myofibrils) and the sarcolemma at specialized cell–cell junctions (intercalated discs) and cell–substrate adhesion complexes (costameres). Recent studies have shed insight into how protein complexes within cardiac myocytes sense biomechanical signals, processes required for normal adaptive or pathological responses. This new evidence suggests that complexes associated with the giant, myofibrillar protein titin sense myocyte stretch. Here, we discuss evidence supporting titin being an ideal biomechanical sensor.

Published

2004

4. The Muscle Ankyrin Repeat Proteins: CARP, ankrd2/Arpp and DARP as a Family of Titin Filament-based Stress Response Molecules

Author

Christian Witt, Melanie K. Miller, Carol C. Gregorio, Siegfried Labeit, Kaori Watanabe, Charles Trombitas, Abigail S. McElhinny, Dietmar Labeit, Marie Louise Bang, and Henk Granzier

Subjects

ANKRD2, ANKRD1, animal structures, Amino Acid Motifs, Molecular Sequence Data, Muscle Proteins, Muscle hypertrophy, Structural Biology, Humans, Myocyte, Connectin, Amino Acid Sequence, Muscle, Skeletal, Molecular Biology, Conserved Sequence, Base Sequence, biology, Myocardium, Nuclear Proteins, musculoskeletal system, Molecular biology, Repressor Proteins, Actinin, alpha 2, biology.protein, Titin, Ankyrin repeat, Myofibril, Protein Kinases, tissues

Abstract

CARP, ankrd-2/Arpp, and DARP, are three members of a conserved gene family, referred to here as MARPs (muscle ankyrin repeat proteins). The expression of MARPs is induced upon injury and hypertrophy (CARP), stretch or denervation (ankrd2/Arpp), and during recovery following starvation (DARP), suggesting that they are involved in muscle stress response pathways. Here, we show that MARP family members contain within their ankyrin repeat region a binding site for the myofibrillar elastic protein titin. Within the myofibril, MARPs, myopalladin, and the calpain protease p94 appear to be components of a titin N2A-based signaling complex. Ultrastructural studies demonstrated that all three endogenous MARP proteins co-localize with I-band titin N2A epitopes in adult heart muscle tissues. In cultured fetal rat cardiac myocytes, passive stretch induced differential distribution patterns of CARP and DARP: staining for both proteins was increased in the nucleus and at the I-band region of myofibrils, while DARP staining also increased at intercalated discs. We speculate that the myofibrillar MARPs are regulated by stretch, and that this links titin-N2A-based myofibrillar stress/strain signals to a MARP-based regulation of muscle gene expression.

Published

2003

5. Translational Control by an Upstream Open Reading Frame in the HER-2/neu Transcript

Author

Adam P. Geballe, Melanie K. Miller, and Stephanie J. Child

Subjects

Genetics, Base Sequence, Five prime untranslated region, Receptor, ErbB-2, Molecular Sequence Data, Leaky scanning, Translation (biology), Cell Biology, Biology, Biochemistry, Open Reading Frames, Open reading frame, Cistron, Start codon, Protein Biosynthesis, COS Cells, Upstream open reading frame, Protein biosynthesis, Animals, Humans, RNA, Messenger, Codon, Molecular Biology

Abstract

Overexpression of the HER-2 (neu, erb B-2) receptor results in cellular transformation and is associated with a variety of human cancers. Multiple mechanisms, including gene amplification and transcriptional, post-transcriptional, and translational controls contribute to the regulation of HER-2 expression. One of the components of these regulatory mechanisms is a short upstream open reading frame (uORF) in the HER-2 mRNA that represses downstream translation in a variety of cell types. Here we explore the mechanism by which this uORF exerts its inhibitory effect. As judged by comparisons of protein and mRNA abundance and by polysomal distribution analyses, the uORF represses translation of the HER-2 cistron or of a heterologous reporter gene. Despite its conservation among mammalian species, the peptide sequence of the uORF is not required for this inhibitory effect. Rather, the majority of ribosomes that load on the HER-2 mRNA most likely translate the uORF and are then unable to reinitiate at the downstream AUG codon, in part due to the short intercistronic spacing. A minority of ribosomes gain access to the HER-2 initiation codon either by leaky scanning past the upstream AUG codon or by reinitiating after having translated the uORF despite the short intercistronic region. These results suggest that the HER-2 uORF controls synthesis of this oncoprotein by limiting ribosomal access to downstream initiation sites.

Published

1999

6. Climate change. Preserving Montreal Protocol climate benefits by limiting HFCs

Author

Guus J M, Velders, A R, Ravishankara, Melanie K, Miller, Mario J, Molina, Joseph, Alcamo, John S, Daniel, David W, Fahey, Stephen A, Montzka, and Stefan, Reimann

Published

2012

7. Developmental expression and cardiac transcriptional regulation of Myh7b, a third myosin heavy chain in the vertebrate heart

Author

Melanie K. Miller, Andrew S. Warkman, Catherine Schwach, Robert J. Garriock, Paul A. Krieg, Samantha A. Whitman, and Carol C. Gregorio

Subjects

Mef2, Adult, Transcriptional Activation, Transcription, Genetic, Blotting, Western, Molecular Sequence Data, Cardiomegaly, Chick Embryo, Biology, Real-Time Polymerase Chain Reaction, Sarcomere, Article, Immunoenzyme Techniques, Mice, Xenopus laevis, Structural Biology, Sequence Homology, Nucleic Acid, Myosin, medicine, Transcriptional regulation, Animals, Humans, Amino Acid Sequence, RNA, Messenger, Luciferases, Muscle, Skeletal, Promoter Regions, Genetic, Cells, Cultured, In Situ Hybridization, Cell Nucleus, Binding Sites, Base Sequence, Myosin Heavy Chains, Sequence Homology, Amino Acid, Reverse Transcriptase Polymerase Chain Reaction, Myocardium, Skeletal muscle, Gene Expression Regulation, Developmental, Promoter, Heart, Cell Biology, Molecular biology, Rats, DNA-Binding Proteins, medicine.anatomical_structure, MYH7, MYH6, Transcription Factors

Abstract

The mammalian heart expresses two myosin heavy chain (MYH) genes (Myh6 and Myh7), which are major components of the thick filaments of the sarcomere. We have determined that a third MYH, MYH7B, is also expressed in the myocardium. Developmental analysis shows Myh7b expression in cardiac and skeletal muscle of Xenopus, chick and mouse embryos, and in smooth muscle tissues during later stages of mouse embryogenesis. Myh7b is also expressed in the adult human heart. The promoter region of the Myh7b gene shows remarkable similarity between diverse species, suggesting that transcriptional control mechanisms have been conserved. Using luciferase reporter analysis in rat cardiomyocytes, it can be shown that MEF2, GATA, and E-box regulatory elements are essential for efficient expression of the Myh7b gene. In addition two conserved elements that do not correspond to consensus binding sites for known transcription factors are also essential for full transcriptional activity of the Myh7b reporter. Finally, the Myh7b gene shows a transcriptional response similar to Myh6 in response to cardiac hypertrophy. © 2012 Wiley Periodicals, Inc

Published

2011

8. Expression of the fast twitch troponin complex, fTnT, fTnI and fTnC, in vascular smooth muscle

Author

Paul A. Krieg, Carlos M. Moran, Melanie K. Miller, Robert J. Garriock, Carol C. Gregorio, and Ronald L. Heimark

Subjects

Vascular smooth muscle, Blotting, Western, Myocytes, Smooth Muscle, Gene Expression, Aorta, Thoracic, macromolecular substances, Biology, Muscle, Smooth, Vascular, Article, Troponin C, Rats, Sprague-Dawley, Mice, Troponin complex, Troponin T, Structural Biology, Tandem Mass Spectrometry, Troponin I, medicine, Myocyte, Animals, Immunoprecipitation, Intestinal Mucosa, In Situ Hybridization, Reverse Transcriptase Polymerase Chain Reaction, Smooth muscle layer, Skeletal muscle, Cell Biology, Anatomy, musculoskeletal system, Actins, Cell biology, Rats, Intestines, medicine.anatomical_structure, Microscopy, Fluorescence, Muscle Fibers, Fast-Twitch, Blood Vessels, Chromatography, Liquid

Abstract

It is generally believed that proteins of the troponin complex are not expressed in smooth muscle. We have directly assayed for expression of troponin transcripts in mouse vascular smooth muscle and found that troponin sequences normally associated with fast twitch skeletal muscle (fTnT, fTnI, fTnC) were present at significant levels in the thoracic aorta. In situ hybridization experiments demonstrated that fTnT, fTnI and fTnC transcripts were expressed in the smooth muscle layer of mouse blood vessels of all sizes. Protein blot analysis using rat tissue showed that at least two members of the troponin complex, Troponin T and Troponin I, were translated in vascular smooth muscle of the aorta. Finally, immuno-fluorescence microscopy of rat aortic smooth muscle revealed that TnT and TnI are localized in a unique pattern, coincident with the distribution of tropomyosin. It seems likely therefore, that a complete troponin complex is expressed in vascular smooth muscle and is associated with the contractile machinery of the cell. These observations raise the possibility that troponins play a role in regulation of smooth muscle function.

Published

2008

9. Apelin, the ligand for the endothelial G-protein-coupled receptor, APJ, is a potent angiogenic factor required for normal vascular development of the frog embryo

Author

Ronald L. Heimark, Christopher M. Cox, Susan L. D'Agostino, Paul A. Krieg, and Melanie K. Miller

Subjects

medicine.medical_specialty, Embryo, Nonmammalian, Endothelium, Angiogenesis, medicine.medical_treatment, Xenopus, Molecular Sequence Data, Neovascularization, Physiologic, Biology, Xenopus Proteins, Receptors, G-Protein-Coupled, Internal medicine, medicine, Animals, Amino Acid Sequence, Receptor, Hypoxia, Molecular Biology, Apelin receptor, G protein-coupled receptor, Growth factor, Gene Expression Profiling, Cell Biology, Apelin, Cell biology, CAM assay, Chorioallantoic membrane, Endocrinology, medicine.anatomical_structure, APJ, Intercellular Signaling Peptides and Proteins, Angiogenesis Inducing Agents, Endothelial mitogen, Endothelium, Vascular, Developmental Biology

Abstract

The peptide growth factor apelin is the high affinity ligand for the G-protein-coupled receptor APJ. During embryonic development of mouse and frog, APJ receptor is expressed at high levels in endothelial precursor cells and in nascent vascular structures. Characterization of Xenopus apelin shows that the sequence of the bioactive region of the peptide is perfectly conserved between frogs and mammals. Embryonic expression studies indicate that apelin is expressed in, or immediately adjacent to, a subset of the developing vascular structures, particularly the intersegmental vessels. Experimental inhibition of either apelin or APJ expression, using antisense morpholino oligos, results in elimination or disruption of intersegmental vessels in a majority of embryos. In gain of function experiments, apelin peptide is a potent angiogenic factor when tested using two in vivo angiogenesis assays, the frog embryo and the chicken chorioallantoic membrane. Furthermore, studies using the mouse brain microvascular cell line bEnd.3 show that apelin acts as a mitogenic, chemotactic and anti-apoptotic agent for endothelial cells in culture. Finally, we show that, similar to a number of other angiogenic factors, expression of the apelin gene is increased under conditions of hypoxia. Taken together, these studies indicate that apelin is required for normal vascular development in the frog embryo and has properties consistent with a role during normal and pathological angiogenesis.

Published

2005

10. Preserving Montreal Protocol Climate Benefits by Limiting HFCs

Author

Stefan Reimann, Stephen A. Montzka, A. R. Ravishankara, Mario J. Molina, John S. Daniel, Joseph Alcamo, Melanie K. Miller, Guus J. M. Velders, and David W. Fahey

Subjects

Multidisciplinary, Environmental protection, Greenhouse gas, Ozone layer, Montreal Protocol, Environmental science, Kyoto Protocol, Limiting, Treaty, Environmental economics

Abstract

The Montreal Protocol is perhaps the most successful international environmental treaty, responsible for global phaseout of the consumption and production of ozone-depleting substances (ODSs), e.g., chlorofluorocarbons (CFCs) and hydrochlorofluorocarbons (HCFCs). Hydrofluorocarbons (HFCs), which do not destroy stratospheric ozone, were considered long-term substitutes for ODSs and are not controlled by the Montreal Protocol. Because most HFCs are potent greenhouse gases (GHGs), they are included in the Kyoto Protocol. But climate benefits provided by this protocol are limited as they apply only to developed countries and over a short time (2008–2012). As we describe below, with no impending global controls on HFCs, inclusion of HFCs under the Montreal Protocol offers a path, starting in the short term, to preserve the climate benefits already achieved by this protocol.

Published

2012

11. Cell type-dependent and -independent control of HER-2/neu translation

Author

Stephanie J. Child, Melanie K. Miller, and Adam P. Geballe

Subjects

Messenger RNA, Cell type, Translational efficiency, Base Sequence, Transcription, Genetic, Receptor, ErbB-2, Molecular Sequence Data, Cell Biology, Biology, Fibroblasts, Biochemistry, Molecular biology, Cell culture, Polysome, Protein Biosynthesis, Translational regulation, Upstream open reading frame, COS Cells, Chlorocebus aethiops, Protein biosynthesis, Animals, Humans, Cell Line, Transformed

Abstract

Overexpression of the HER-2 oncogene occurs in a variety of human tumors, including 25-30% of breast carcinomas, and has been associated with an adverse prognosis. Amplification of the HER-2 gene is frequently detected in tumors, but by itself may not fully account for HER-2 overexpression since transcriptional and post-transcriptional mechanisms also regulate HER-2 protein synthesis. Our studies reveal that the efficiency of HER-2 translation differs between primary and transformed cells. In primary human fibroblasts and human mammary epithelial cells, the HER-2 mRNA is associated with monosome and small polysome fractions. In contrast, in BT474 and MCF-7 human breast cancer cell lines and in COS-7 cells the mRNA co-sedimented with larger polysomes, indicating that it is more efficiently translated in these transformed cells. Northern analysis revealed no detectable mRNA size difference, and nuclease S1 protection and sequence analyses showed no differences between the HER-2 transcript leader in primary cells compared to transformed human cells. The transcript leader in all cell types contains a short upstream open reading frame that is also conserved in other mammalian species. Transient transfection assays revealed that the HER-2 transcript leader repressed downstream translation approximately five-fold in both primary and transformed cells and mutation of the upstream initiation codon alleviated most of the inhibitory effect. These results indicate that HER2 expression is translationally controlled both by a short upstream open reading frame that represses HER-2 translation in a cell type-independent manner, and by a distinct cell type-dependent mechanism that increases translational efficiency of HER-2 in transformed cells.

Published

1999

12. Correction: Developmental expression and cardiac transcriptional regulation ofMyh7b, a third myosin heavy chain in the vertebrate heart

Author

Andrew S. Warkman, Samantha A. Whitman, Melanie K. Miller, Robert J. Garriock, Catherine M. Schwach, Carol C. Gregorio, and Paul A. Krieg

Subjects

Structural Biology, Cell Biology

Published

2012

13. Transcriptional regulation of MyH-7b, a novel myosin heavy chain expressed in the vertebrate heart

Author

Andrew S. Warkman, Paul A. Krieg, Melanie K. Miller, Robert J. Garriock, and Susan L. D'Agostino

Subjects

Myosin light-chain kinase, animal structures, biology, MUTYH, biology.animal, Myosin, embryonic structures, Transcriptional regulation, Vertebrate, Cell Biology, Molecular Biology, Cell biology, Developmental Biology