Results for 'protein denaturation'

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  1.  8
    Heat Shock Proteins in the “Hot” Mitochondrion: Identity and Putative Roles.Mohamed A. Nasr, Galina I. Dovbeshko, Stephen L. Bearne, Nagwa El-Badri & Chérif F. Matta - 2019 - Bioessays 41 (9):1900055.
    The mitochondrion is known as the “powerhouse” of eukaryotic cells since it is the main site of adenosine 5′‐triphosphate (ATP) production. Using a temperature‐sensitive fluorescent probe, it has recently been suggested that the stray free energy, not captured into ATP, is potentially sufficient to sustain mitochondrial temperatures higher than the cellular environment, possibly reaching up to 50 °C. By 50 °C, some DNA and mitochondrial proteins may reach their melting temperatures; how then do these biomolecules maintain their structure and function? (...)
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  2. Section A. membranes.Protein Synthesis as A. Membrane-Oriented & Richard W. Hendler - 1968 - In Peter Koestenbaum (ed.), Proceedings. [San Jose? Calif.,: [San Jose? Calif.. pp. 37.
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  3.  21
    Chaperone discovery.Shu Quan & James Ca Bardwell - 2012 - Bioessays 34 (11):973-981.
    Molecular chaperones assist de novo protein folding and facilitate the refolding of stress‐denatured proteins. The molecular chaperone concept was coined nearly 35 years ago, and since then, tremendous strides have been made in understanding how these factors support protein folding. Here, we focus on how various chaperone proteins were first identified to play roles in protein folding. Examples are used to illustrate traditional routes of chaperone discovery and point out their advantages and limitations. Recent advances, including the (...)
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  4.  16
    The role of conformational change in serpin structure and function.Peter Gettins, Philip A. Patston & Marc Schapira - 1993 - Bioessays 15 (7):461-467.
    Serpins are members of a family of structurally related protein inhibitors of serine proteinases, with molecular masses between 40 and 100kDa. In contrast to other, simpler, proteinase inhibitors, they may interact with proteinases as inhibitors, as substrates, or as both. They undergo conformational interconversions upon complex formation with proteinase, upon binding of some members to heparin, upon proteolytic cleavage at the reactive center, and under mild denaturing conditions. These conformational changes appear to be critical in determining the properties of (...)
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  5.  11
    Electrophoresis today and tomorrow: Helping biologists' dreams come true.Karel Klepárník & Petr Boček - 2010 - Bioessays 32 (3):218-226.
    Intensive research and development of electrophoresis methodology and instrumentation during past decades has resulted in unique methods widely implemented in bioanalysis. While two‐dimensional electrophoresis and denaturing polyacrylamide gel electrophoresis in sodium dodecylsulfate are still the most frequently used electrophoretic methods applied to analyses of proteins, new miniaturized capillary and microfluidic versions of electromigrational methods have been developed. High‐throughput electrophoretic instruments with hundreds of capillaries for parallel separations and laser‐induced fluorescence detection of labeled DNA strands have been of key importance for (...)
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  6.  38
    Denaturalization and denationalization in comparison.Patrick Weil - 2017 - Philosophy and Social Criticism 43 (4-5):417-429.
    Denaturalization and denationalization were once much more common among western democracies. From 1906 till 1968, the United States of America, France and the United Kingdom denationalized their citizens by hundreds and thousands, for fraud or illegality during the process of naturalization, for dual citizenship, or for banal default of loyalty. In a context of a ‘war against terror’ we are now seeing an apparent return to the past – with the resuming of denationalization policies and provisions. However, the previous restriction (...)
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  7. Dénaturation et violence dans la pensée de J.-J. Rousseau.[author unknown] - 1978 - Revue Philosophique de la France Et de l'Etranger 168 (3):357-359.
     
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  8.  17
    Denaturalizing the Environment: Dissensus and the Possibility of Radically Democratizing Discourses of Environmental Sustainability.Charles Barthold & Peter Bloom - 2020 - Journal of Business Ethics 164 (4):671-681.
    The aim of this article is to introduce the concept of dissensus as an important perspective for making current organizational discourses of environmental sustainability more radically democratic. It presents the Anthropocene as a force for social naturalization—one that paradoxically acknowledges humanity’s role in negatively impacting the environment while restricting their agency to address this problem to those compatible with a market ideology. Radical democratic theories of agonism help to denaturalize the relation of organizations to the environment yet risk reproducing values (...)
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  9. The Protein Ontology: A structured representation of protein forms and complexes.Darren Natale, Cecilia N. Arighi, Winona C. Barker, Judith A. Blake, Carol J. Bult, Michael Caudy, Harold J. Drabkin, Peter D’Eustachio, Alexei V. Evsikov, Hongzhan Huang, Jules Nchoutmboube, Natalia V. Roberts, Barry Smith, Jian Zhang & Cathy H. Wu - 2011 - Nucleic Acids Research 39 (1):D539-D545.
    The Protein Ontology (PRO) provides a formal, logically-based classification of specific protein classes including structured representations of protein isoforms, variants and modified forms. Initially focused on proteins found in human, mouse and Escherichia coli, PRO now includes representations of protein complexes. The PRO Consortium works in concert with the developers of other biomedical ontologies and protein knowledge bases to provide the ability to formally organize and integrate representations of precise protein forms so as to (...)
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  10. Protein-centric connection of biomedical knowledge: Protein Ontology research and annotation tools.Cecilia N. Arighi, Darren A. Natale, Judith A. Blake, Carol J. Bult, Michael Caudy, Alexander D. Diehl, Harold J. Drabkin, Peter D'Eustachio, Alexei Evsikov, Hongzhan Huang, Barry Smith & Others - 2011 - In Proceedings of the 2nd International Conference on Biomedical Ontology. Buffalo, NY: NCOR. pp. 285-287.
    The Protein Ontology (PRO) web resource provides an integrative framework for protein-centric exploration and enables specific and precise annotation of proteins and protein complexes based on PRO. Functionalities include: browsing, searching and retrieving, terms, displaying selected terms in OBO or OWL format, and supporting URIs. In addition, the PRO website offers multiple ways for the user to request, submit, or modify terms and/or annotation. We will demonstrate the use of these tools for protein research and annotation.
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  11.  19
    La dénaturation de la vérité ou le fondement des idéologies.Chantal Millon-Delsol - 1988 - Laval Théologique et Philosophique 44 (3):339-343.
  12.  21
    Denaturalizing Ecological Politics: Alienation from Nature.Steven Vogel - 2007 - Environmental Ethics 29 (1):103-106.
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  13.  6
    La « dénaturation » de l'homme.Maurice Vanhoutte - 1960 - Atti Del XII Congresso Internazionale di Filosofia 2:451-456.
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  14.  4
    'Denaturalized'mimesis.V. Zuska - 2006 - Estetika: The Central European Journal of Aestetics; Until 2008: Estetika (Aesthetics) 42 (1-3).
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  15. Protein Ontology: A controlled structured network of protein entities.A. Natale Darren, N. Arighi Cecilia, A. Blake Judith, J. Bult Carol, R. Christie Karen, Cowart Julie, D’Eustachio Peter, D. Diehl Alexander, J. Drabkin Harold, Helfer Olivia, Barry Smith & Others - 2013 - Nucleic Acids Research 42 (1):D415-21..
    The Protein Ontology (PRO; http://proconsortium.org) formally defines protein entities and explicitly represents their major forms and interrelations. Protein entities represented in PRO corresponding to single amino acid chains are categorized by level of specificity into family, gene, sequence and modification metaclasses, and there is a separate metaclass for protein complexes. All metaclasses also have organism-specific derivatives. PRO complements established sequence databases such as UniProtKB, and interoperates with other biomedical and biological ontologies such as the Gene Ontology (...)
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  16.  17
    The Protein‐Coding Human Genome: Annotating High‐Hanging Fruits.Klas Hatje, Stefanie Mühlhausen, Dominic Simm & Martin Kollmar - 2019 - Bioessays 41 (11):1900066.
    The major transcript variants of human protein‐coding genes are annotated to a certain degree of accuracy combining manual curation, transcript data, and proteomics evidence. However, there is considerable disagreement on the annotation of about 2000 genes—they can be protein‐coding, noncoding, or pseudogenes—and on the annotation of most of the predicted alternative transcripts. Pure transcriptome mapping approaches seem to be limited in discriminating functional expression from noise. These limitations have partially been overcome by dedicated algorithms to detect alternative spliced (...)
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  17.  1
    This Denatured Ape.Dardo Scavino - 2018 - In Gert Melville (ed.), Nature and Human: An Intricate Mutuality. Boston: De Gruyter. pp. 41-46.
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  18.  28
    LRRC8 proteins share a common ancestor with pannexins, and may form hexameric channels involved in cell-cell communication.Federico Abascal & Rafael Zardoya - 2012 - Bioessays 34 (7):551-560.
  19.  64
    Denaturalizing disaster: A social autopsy of the 1995 Chicago heat wave. [REVIEW]Eric Klinenberg - 1999 - Theory and Society 28 (2):239-295.
  20. Angiomotin family proteins in the Hippo signaling pathway.Yu Wang & Fa-Xing Yu - forthcoming - Bioessays.
    The Motin family proteins (Motins) are a class of scaffolding proteins consisting of Angiomotin (AMOT), AMOT‐like protein 1 (AMOTL1), and AMOT‐like protein 2 (AMOTL2). Motins play a pivotal role in angiogenesis, tumorigenesis, and neurogenesis by modulating multiple cellular signaling pathways. Recent findings indicate that Motins are components of the Hippo pathway, a signaling cascade involved in development and cancer. This review discusses how Motins are integrated into the Hippo signaling network, as either upstream regulators or downstream effectors, to (...)
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  21.  8
    Ribosomal protein autoantibodies in systemic lupus erythematosus.Keith Elkon, Eloisa Bonfa, Susan Skelly, Herbert Weissbach & Nathan Brot - 1987 - Bioessays 7 (6):258-261.
    Autoantibodies to three eukaryotic 60S ribosomal phosphoproteins P0, P1 and P2 have been found in the sera of 10–20% of patients with systemic lupus erythematosus (SLE). These three proteins share a common epitope contained within the carboxy terminal 22 amino acids of each protein. Because central nervous system disturbances, with major behavioural disorders, occur in a significant fraction of SLE patients, the antiribosomal autoantibodies were measured in this subset of SLE individuals to determine whether or not there was an (...)
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  22. Protein Analysis Meets Visual Word Recognition: A Case for String Kernels in the Brain.Thomas Hannagan & Jonathan Grainger - 2012 - Cognitive Science 36 (4):575-606.
    It has been recently argued that some machine learning techniques known as Kernel methods could be relevant for capturing cognitive and neural mechanisms (Jäkel, Schölkopf, & Wichmann, 2009). We point out that ‘‘String kernels,’’ initially designed for protein function prediction and spam detection, are virtually identical to one contending proposal for how the brain encodes orthographic information during reading. We suggest some reasons for this connection and we derive new ideas for visual word recognition that are successfully put to (...)
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  23.  51
    Fluorescent proteins for FRET microscopy: Monitoring protein interactions in living cells.Richard N. Day & Michael W. Davidson - 2012 - Bioessays 34 (5):341-350.
    The discovery and engineering of novel fluorescent proteins (FPs) from diverse organisms is yielding fluorophores with exceptional characteristics for live‐cell imaging. In particular, the development of FPs for fluorescence (or Förster) resonance energy transfer (FRET) microscopy is providing important tools for monitoring dynamic protein interactions inside living cells. The increased interest in FRET microscopy has driven the development of many different methods to measure FRET. However, the interpretation of FRET measurements is complicated by several factors including the high fluorescence (...)
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  24.  10
    Ribosomal protein uS3 in cell biology and human disease: Latest insights and prospects.Dmitri Graifer & Galina Karpova - 2020 - Bioessays 42 (12):2000124.
    The conserved ribosomal protein uS3 in eukaryotes has long been known as one of the essential components of the small (40S) ribosomal subunit, which is involved in the structure of the 40S mRNA entry pore, ensuring the functioning of the 40S subunit during translation initiation. Besides, uS3, being outside the ribosome, is engaged in various cellular processes related to DNA repair, NF‐kB signaling pathway and regulation of apoptosis. This review is devoted to recent data opening new horizons in understanding (...)
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  25.  20
    The Protein Side of the Central Dogma: Permanence and Change.Michel Morange - 2006 - History and Philosophy of the Life Sciences 28 (4):513 - 524.
    There are two facets to the central dogma proposed by Francis Crick in 1957. One concerns the relation between the sequence of nucleotides and the sequence of amino acids, the second is devoted to the relation between the sequence of amino acids and the native three-dimensional structure of proteins. 'Folding is simply a function of the order of the amino acids,' i.e. no information is required for the proper folding of a protein other than the information contained in its (...)
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  26. The representation of protein complexes in the Protein Ontology.Carol Bult, Harold Drabkin, Alexei Evsikov, Darren Natale, Cecilia Arighi, Natalia Roberts, Alan Ruttenberg, Peter D’Eustachio, Barry Smith, Judith Blake & Cathy Wu - 2011 - BMC Bioinformatics 12 (371):1-11.
    Representing species-specific proteins and protein complexes in ontologies that are both human and machine-readable facilitates the retrieval, analysis, and interpretation of genome-scale data sets. Although existing protin-centric informatics resources provide the biomedical research community with well-curated compendia of protein sequence and structure, these resources lack formal ontological representations of the relationships among the proteins themselves. The Protein Ontology (PRO) Consortium is filling this informatics resource gap by developing ontological representations and relationships among proteins and their variants and (...)
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  27.  8
    Protein splicing: Excision of intervening sequences at the protein level.Antony A. Cooper & To M. H. Stevens - 1993 - Bioessays 15 (10):667-674.
    Protein splicing is an extraordinary post‐translational reaction that removes an intact central “spacer” domain (Sp) from precursor proteins (N‐Sp‐C) while splicing together the N‐ and C‐domains of the precursor, via a peptide bond, to produce a new protein (N‐C). All of the available data on protein splicing fit a model in which these intervening sequences excise at the protein level via a self‐splicing mechanism. Several proteins have recently been discovered that undergo protein splicing, and in (...)
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  28. TGF-beta signaling proteins and the Protein Ontology.Arighi Cecilia, Liu Hongfang, Natale Darren, Barker Winona, Drabkin Harold, Blake Judith, Barry Smith & Wu Cathy - 2009 - BMC Bioinformatics 10 (Suppl 5):S3.
    The Protein Ontology (PRO) is designed as a formal and principled Open Biomedical Ontologies (OBO) Foundry ontology for proteins. The components of PRO extend from a classification of proteins on the basis of evolutionary relationships at the homeomorphic level to the representation of the multiple protein forms of a gene, including those resulting from alternative splicing, cleavage and/or posttranslational modifications. Focusing specifically on the TGF-beta signaling proteins, we describe the building, curation, usage and dissemination of PRO. PRO provides (...)
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  29.  15
    Peptidylprolylisomerases, Protein Folders, or Scaffolders? The Example of FKBP51 and FKBP52.Theo Rein - 2020 - Bioessays 42 (7):1900250.
    Peptidylprolyl‐isomerases (PPIases) comprise of the protein families of FK506 binding proteins (FKBPs), cyclophilins, and parvulins. Their common feature is their ability to expedite the transition of peptidylprolyl bonds between the cis and the trans conformation. Thus, it seemed highly plausible that PPIase enzymatic activity is crucial for protein folding. However, this has been difficult to prove over the decades since their discovery. In parallel, more and more studies have discovered scaffolding functions of PPIases. This essay discusses the hypothesis (...)
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  30. Ferritin-like protein in bovine retina inhibits the activity of cyclic nucleotide phosphodiesterase in rod outer segments.M. G. Yefimova, I. S. Shcherbakova & N. D. Shushakova - 1996 - In Enrique Villanueva (ed.), Perception. Ridgeview. pp. 114-114.
     
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  31. Proteins, Enzymes, Genes: The Interplay of Chemistry and Biology.Joseph S. Fruton - 2001 - Journal of the History of Biology 34 (2):413-415.
     
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  32.  28
    Studying protein‐reconstituted proteoliposome fusion with content indicators in vitro.Jiajie Diao, Minglei Zhao, Yunxiang Zhang, Minjoung Kyoung & Axel T. Brunger - 2013 - Bioessays 35 (7):658-665.
    In vitro reconstitution assays are commonly used to study biological membrane fusion. However, to date, most ensemble and single‐vesicle experiments involving SNARE proteins have been performed only with lipid‐mixing, but not content‐mixing indicators. Through simultaneous detection of lipid and small content‐mixing indicators, we found that lipid mixing often occurs seconds prior to content mixing, or without any content mixing at all, during a 50‐seconds observation period, for Ca2+‐triggered fusion with SNAREs, full‐length synaptotagmin‐1, and complexin. Our results illustrate the caveats of (...)
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  33.  27
    Dénaturation et Violence dans la Pensée de J.-J. Rousseau. Par Michèle Ansart-Dourlen. Coll. Critères. Paris. Klincksieck, 1975, 302 pp. [REVIEW]Jean Roy - 1977 - Dialogue 16 (1):176-180.
  34.  3
    Denaturalizing Ecological Politics. [REVIEW]Steven Vogel - 2007 - Environmental Ethics 29 (1):103-106.
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  35.  16
    Protein‐interaction mapping in search of effective drug targets.Amitabha Chaudhuri & John Chant - 2005 - Bioessays 27 (9):958-969.
    Signaling complexes and networks are being intensely studied in an attempt to discover pathways that are amenable to therapeutic intervention. A challenge in this search is to understand the effect that the modulation of a target will have on the overall function of a cell and its surrounding neighbors. Protein‐interaction mapping reveals relationships between proteins and their impact on cellular processes and is being used more widely in our understanding of disease mechanisms and their treatment. The review discusses challenges (...)
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  36.  14
    Protein trafficking along the exocytotic pathway.Wanjin Hong & Bor Luen Tang - 1993 - Bioessays 15 (4):231-238.
    Proteins of the exocytotic (secretory) pathway are initially targeted to the endoplasmic reticulum (ER) and then translocated across and/or inserted into the membrane of the ER. During their anterograde transport with the bulk of the membrane flow along the exocytotic pathway, some proteins are selectively retained in various intracellular compartments, while others are sorted to different branches of the pathway. The signals or structural motifs that are involved in these selective targeting processes are being revealed and investigations into the mechanistic (...)
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  37.  33
    Protein partners of KCTD proteins provide insights about their functional roles in cell differentiation and vertebrate development.Mikhail Skoblov, Andrey Marakhonov, Ekaterina Marakasova, Anna Guskova, Vikas Chandhoke, Aybike Birerdinc & Ancha Baranova - 2013 - Bioessays 35 (7):586-596.
    The KCTD family includes tetramerization (T1) domain containing proteins with diverse biological effects. We identified a novel member of the KCTD family, BTBD10. A comprehensive analysis of proteinprotein interactions (PPIs) allowed us to put forth a number of testable hypotheses concerning the biological functions for individual KCTD proteins. In particular, we predict that KCTD20 participates in the AKT‐mTOR‐p70 S6k signaling cascade, KCTD5 plays a role in cytokinesis in a NEK6 and ch‐TOG‐dependent manner, KCTD10 regulates the RhoA/RhoB pathway. Developmental (...)
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  38.  16
    Protein structure determination by nuclear magnetic resonance.Robert M. Cooke & Iain D. Campbell - 1988 - Bioessays 8 (2‐3):52-56.
    The solution structures of several small proteins have recently been determined from high‐resolution nuclear magnetic resonance data. The principal features of the methods available to do this are outlined here, together with the advantages, limitations and future prospects of the technique.
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  39.  9
    A protein‐lipid complex that detoxifies free fatty acids.Shaojie Cui & Jin Ye - 2023 - Bioessays 45 (3):2200210.
    Fatty acids (FAs) are well known to serve as substrates for reactions that provide cells with membranes and energy. In contrast to these metabolic reactions, the physiological importance of FAs themselves known as free FAs (FFAs) in cells remains obscure. Since accumulation of FFAs in cells is toxic, cells must develop mechanisms to detoxify FFAs. One such mechanism is to sequester free polyunsaturated FAs (PUFAs) into a droplet‐like structure assembled by Fas‐Associated Factor 1 (FAF1), a cytosolic protein. This sequestration (...)
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  40.  12
    Protein translocation across mitochondrial membranes.Ulla Wienhues & Walter Neupert - 1992 - Bioessays 14 (1):17-23.
    Protein translocation across biological membranes is of fundamental importance for the biogenesis of organelles and in protein secretion. We will give an overview of the recent achievements in the understanding of protein translocation across mitochondrial membranes(1‐5). In particular we will focus on recently identified components of the mitochondrial import apparatus.
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  41.  13
    Motor protein control of ion flux is an early step in embryonic left–right asymmetry.Michael Levin - 2003 - Bioessays 25 (10):1002-1010.
    The invariant left–right asymmetry of animal body plans raises fascinating questions in cell, developmental, evolutionary, and neuro‐biology. While intermediate mechanisms (e.g., asymmetric gene expression) have been well‐characterized, very early steps remain elusive. Recent studies suggested a candidate for the origins of asymmetry: rotary movement of extracellular morphogens by cilia during gastrulation. This model is intellectually satisfying, because it bootstraps asymmetry from the intrinsic biochemical chirality of cilia. However, conceptual and practical problems remain with this hypothesis, and the genetic data is (...)
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  42.  21
    Motor protein control of ion flux is an early step in embryonic left–right asymmetry.Michael Levin - 2003 - Bioessays 25 (10):1002-1010.
    The invariant left–right asymmetry of animal body plans raises fascinating questions in cell, developmental, evolutionary, and neuro‐biology. While intermediate mechanisms (e.g., asymmetric gene expression) have been well‐characterized, very early steps remain elusive. Recent studies suggested a candidate for the origins of asymmetry: rotary movement of extracellular morphogens by cilia during gastrulation. This model is intellectually satisfying, because it bootstraps asymmetry from the intrinsic biochemical chirality of cilia. However, conceptual and practical problems remain with this hypothesis, and the genetic data is (...)
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  43.  6
    PAQR proteins and the evolution of a superpower: Eating all kinds of fats.Marc Pilon & Mario Ruiz - 2023 - Bioessays 45 (9):2300079.
    Recently published work showed that members of the PAQR protein family are activated by cell membrane rigidity and contribute to our ability to eat a wide variety of diets. Cell membranes are primarily composed of phospholipids containing dietarily obtained fatty acids, which poses a challenge to membrane properties because diets can vary greatly in their fatty acid composition and could impart opposite properties to the cellular membranes. In particular, saturated fatty acids (SFAs) can pack tightly and form rigid membranes (...)
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  44.  9
    Computational protein design as an optimization problem.David Allouche, Isabelle André, Sophie Barbe, Jessica Davies, Simon de Givry, George Katsirelos, Barry O'Sullivan, Steve Prestwich, Thomas Schiex & Seydou Traoré - 2014 - Artificial Intelligence 212 (C):59-79.
  45.  6
    Membrane protein insertion into the endoplasmic reticulum ‐ another channel tunnel?Stephen High - 1992 - Bioessays 14 (8):535-540.
    The synthesis of biological membranes requires the insertion of proteins into a lipid bilayer. The rough endoplasmic reticulum of eukaryotic cells is a principal site of membrane biogenesis. The insertion of proteins into the membrane of the endoplasmic reticulum is mediated by a resident proteinaceous machinery. Over the last five years several different experimental approaches have provided information about the components of the machinery and how it may function.
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  46.  11
    Protein Topology Prediction Algorithms Systematically Investigated in the Yeast Saccharomyces cerevisiae.Uri Weill, Nir Cohen, Amir Fadel, Shifra Ben-Dor & Maya Schuldiner - 2019 - Bioessays 41 (8):1800252.
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  47.  17
    Quinary protein structure and the consequences of crowding in living cells: Leaving the test‐tube behind.Anna Jean Wirth & Martin Gruebele - 2013 - Bioessays 35 (11):984-993.
    Although the importance of weak proteinprotein interactions has been understood since the 1980s, scant attention has been paid to this “quinary structure”. The transient nature of quinary structure facilitates dynamic sub‐cellular organization through loose grouping of proteins with multiple binding partners. Despite our growing appreciation of the quinary structure paradigm in cell biology, we do not yet understand how the many forces inside the cell – the excluded volume effect, the “stickiness” of the cytoplasm, and hydrodynamic interactions – (...)
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  48. Framework for a protein ontology.Darren A. Natale, Cecilia N. Arighi, Winona Barker, Judith Blake, Ti-Cheng Chang, Zhangzhi Hu, Hongfang Liu, Barry Smith & Cathy H. Wu - 2007 - BMC Bioinformatics 8 (Suppl 9):S1.
    Biomedical ontologies are emerging as critical tools in genomic and proteomic research where complex data in disparate resources need to be integrated. A number of ontologies exist that describe the properties that can be attributed to proteins; for example, protein functions are described by Gene Ontology, while human diseases are described by Disease Ontology. There is, however, a gap in the current set of ontologies—one that describes the protein entities themselves and their relationships. We have designed a (...) Ontology (PRO) to facilitate protein annotation and to guide new experiments. The components of PRO extend from the classification of proteins on the basis of evolutionary relationships to the representation of the multiple protein forms of a gene (products generated by genetic variation, alternative splicing, proteolytic cleavage, and other post-translational modification). PRO will allow the specification of relationships between PRO, GO and other OBO Foundry ontologies. Here we describe the initial development of PRO, illustrated using human proteins from the TGF-beta signaling pathway. (shrink)
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  49.  29
    G protein‐coupled receptors: the inside story.Kees Jalink & Wouter H. Moolenaar - 2010 - Bioessays 32 (1):13-16.
    Recent findings necessitate revision of the traditional view of G protein‐coupled receptor (GPCR) signaling and expand the diversity of mechanisms by which receptor signaling influences cell behavior in general. GPCRs elicit signals at the plasma membrane and are then rapidly removed from the cell surface by endocytosis. Internalization of GPCRs has long been thought to serve as a mechanism to terminate the production of second messengers such as cAMP. However, recent studies show that internalized GPCRs can continue to either (...)
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  50.  13
    G proteins, chemosensory perception, and the C. elegans genome project: An attractive story.Thomas M. Wilkie - 1999 - Bioessays 21 (9):713-717.
    Heterotrimeric G proteins, consisting of α, β, and γ subunits, couple ligand-bound seven transmembrane domain receptors to the regulation of effector proteins and production of intracellular second messengers. G protein signaling mediates the perception of environmental cues in all higher eukaryotic organisms, including yeast, Dictyostelium, plants, and animals. The nematode Caenorhabditis elegans is the first animal to have complete descriptions of its cellular anatomy, cell lineage, neuronal wiring diagram, and genomic sequence. In a recent paper, Jansen et al.(1) used (...)
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