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  1. Artikel ; Online: Controlling Parasympathetic Regulation of Heart Rate: A Gatekeeper Role for RGS Proteins in the Sinoatrial Node.

    Mighiu, Alexandra S / Heximer, Scott P

    Frontiers in physiology

    2012  Band 3, Seite(n) 204

    Abstract: Neurotransmitters released from sympathetic and parasympathetic nerve terminals in the sinoatrial node (SAN) exert their effects via G-protein-coupled receptors. Integration of these different G-protein signals within pacemaker cells of the SAN is ... ...

    Abstract Neurotransmitters released from sympathetic and parasympathetic nerve terminals in the sinoatrial node (SAN) exert their effects via G-protein-coupled receptors. Integration of these different G-protein signals within pacemaker cells of the SAN is critical for proper regulation of heart rate and function. For example, excessive parasympathetic signaling can be associated with sinus node dysfunction (SND) and supraventricular arrhythmias. Our previous work has shown that one member of the regulator of G-protein signaling (RGS) protein family, RGS4, is highly and selectively expressed in pacemaker cells of the SAN. Consistent with its role as an inhibitor of parasympathetic signaling, RGS4-knockout mice have reduced basal heart rates and enhanced negative chronotropic responses to parasympathetic agonists. Moreover, RGS4 appears to be an important part of SA nodal myocyte signaling pathways that mediate G-protein-coupled inwardly rectifying potassium channel (GIRK) channel activation/deactivation and desensitization. Since RGS4 acts immediately downstream of M2 muscarinic receptors, it is tempting to speculate that RGS4 functions as a master regulator of parasympathetic signaling upstream of GIRKs, HCNs, and L-type Ca(2+) channels in the SAN. Thus, loss of RGS4 function may lead to increased susceptibility to conditions associated with increased parasympathetic signaling, including bradyarrhythmia, SND, and atrial fibrillation.
    Sprache Englisch
    Erscheinungsdatum 2012-06-13
    Erscheinungsland Switzerland
    Dokumenttyp Journal Article
    ZDB-ID 2564217-0
    ISSN 1664-042X ; 1664-042X
    ISSN (online) 1664-042X
    ISSN 1664-042X
    DOI 10.3389/fphys.2012.00204
    Datenquelle MEDical Literature Analysis and Retrieval System OnLINE

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  2. Artikel ; Online: Inducibility, but not stability, of atrial fibrillation is increased by NOX2 overexpression in mice.

    Mighiu, Alexandra S / Recalde, Alice / Ziberna, Klemen / Carnicer, Ricardo / Tomek, Jakub / Bub, Gil / Brewer, Alison C / Verheule, Sander / Shah, Ajay M / Simon, Jillian N / Casadei, Barbara

    Cardiovascular research

    2021  Band 117, Heft 11, Seite(n) 2354–2364

    Abstract: Aims: Gp91-containing NADPH oxidases (NOX2) are a significant source of myocardial superoxide production. An increase in NOX2 activity accompanies atrial fibrillation (AF) induction and electrical remodelling in animal models and predicts incident AF in ...

    Abstract Aims: Gp91-containing NADPH oxidases (NOX2) are a significant source of myocardial superoxide production. An increase in NOX2 activity accompanies atrial fibrillation (AF) induction and electrical remodelling in animal models and predicts incident AF in humans; however, a direct causal role for NOX2 in AF has not been demonstrated. Accordingly, we investigated whether myocardial NOX2 overexpression in mice (NOX2-Tg) is sufficient to generate a favourable substrate for AF and further assessed the effects of atorvastatin, an inhibitor of NOX2, on atrial superoxide production and AF susceptibility.
    Methods and results: NOX2-Tg mice showed a 2- to 2.5-fold higher atrial protein content of NOX2 compared with wild-type (WT) controls, which was associated with a significant (twofold) increase in NADPH-stimulated superoxide production (2-hydroxyethidium by HPLC) in left and right atrial tissue homogenates (P = 0.004 and P = 0.019, respectively). AF susceptibility assessed in vivo by transoesophageal atrial burst stimulation was modestly increased in NOX2-Tg compared with WT (probability of AF induction: 88% vs. 69%, respectively; P = 0.037), in the absence of significant alterations in AF duration, surface ECG parameters, and LV mass or function. Mechanistic studies did not support a role for NOX2 in promoting electrical or structural remodelling, as high-resolution optical mapping of atrial tissues showed no differences in action potential duration and conduction velocity between genotypes. In addition, we did not observe any genotype difference in markers of fibrosis and inflammation, including atrial collagen content and Col1a1, Il-1β, Il-6, and Mcp-1 mRNA. Similarly, NOX2 overexpression did not have consistent effects on RyR2 Ca2+ leak nor did it affect PKA or CaMKII-mediated RyR2 phosphorylation. Finally, treatment with atorvastatin significantly inhibited atrial superoxide production in NOX2-Tg but had no effect on AF induction in either genotype.
    Conclusion: Together, these data indicate that while atrial NOX2 overexpression may contribute to atrial arrhythmogenesis, NOX2-derived superoxide production does not affect the electrical and structural properties of the atrial myocardium.
    Mesh-Begriff(e) Action Potentials ; Animals ; Anti-Arrhythmia Agents/pharmacology ; Atorvastatin/pharmacology ; Atrial Fibrillation/enzymology ; Atrial Fibrillation/genetics ; Atrial Fibrillation/physiopathology ; Atrial Fibrillation/prevention & control ; Disease Models, Animal ; Enzyme Induction ; Enzyme Inhibitors/pharmacology ; Heart Atria/drug effects ; Heart Atria/enzymology ; Heart Atria/physiopathology ; Heart Rate ; Mice, Transgenic ; Myocytes, Cardiac/drug effects ; Myocytes, Cardiac/enzymology ; NADPH Oxidase 2/antagonists & inhibitors ; NADPH Oxidase 2/biosynthesis ; NADPH Oxidase 2/genetics ; Signal Transduction ; Superoxides/metabolism ; Time Factors
    Chemische Substanzen Anti-Arrhythmia Agents ; Enzyme Inhibitors ; Superoxides (11062-77-4) ; Atorvastatin (A0JWA85V8F) ; CYBB protein, human (EC 1.6.3.-) ; NADPH Oxidase 2 (EC 1.6.3.-)
    Sprache Englisch
    Erscheinungsdatum 2021-01-22
    Erscheinungsland England
    Dokumenttyp Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 80340-6
    ISSN 1755-3245 ; 0008-6363
    ISSN (online) 1755-3245
    ISSN 0008-6363
    DOI 10.1093/cvr/cvab019
    Datenquelle MEDical Literature Analysis and Retrieval System OnLINE

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  3. Artikel ; Online: Amino-terminal cysteine residues differentially influence RGS4 protein plasma membrane targeting, intracellular trafficking, and function.

    Bastin, Guillaume / Singh, Kevin / Dissanayake, Kaveesh / Mighiu, Alexandra S / Nurmohamed, Aliya / Heximer, Scott P

    The Journal of biological chemistry

    2012  Band 287, Heft 34, Seite(n) 28966–28974

    Abstract: Regulator of G-protein signaling (RGS) proteins are potent inhibitors of heterotrimeric G-protein signaling. RGS4 attenuates G-protein activity in several tissues. Previous work demonstrated that cysteine palmitoylation on residues in the amino-terminal ( ...

    Abstract Regulator of G-protein signaling (RGS) proteins are potent inhibitors of heterotrimeric G-protein signaling. RGS4 attenuates G-protein activity in several tissues. Previous work demonstrated that cysteine palmitoylation on residues in the amino-terminal (Cys-2 and Cys-12) and core domains (Cys-95) of RGS4 is important for protein stability, plasma membrane targeting, and GTPase activating function. To date Cys-2 has been the priority target for RGS4 regulation by palmitoylation based on its putative role in stabilizing the RGS4 protein. Here, we investigate differences in the contribution of Cys-2 and Cys-12 to the intracellular localization and function of RGS4. Inhibition of RGS4 palmitoylation with 2-bromopalmitate dramatically reduced its localization to the plasma membrane. Similarly, mutation of the RGS4 amphipathic helix (L23D) prevented membrane localization and its G(q) inhibitory function. Together, these data suggest that both RGS4 palmitoylation and the amphipathic helix domain are required for optimal plasma membrane targeting and function of RGS4. Mutation of Cys-12 decreased RGS4 membrane targeting to a similar extent as 2-bromopalmitate, resulting in complete loss of its G(q) inhibitory function. Mutation of Cys-2 did not impair plasma membrane targeting but did partially impair its function as a G(q) inhibitor. Comparison of the endosomal distribution pattern of wild type and mutant RGS4 proteins with TGN38 indicated that palmitoylation of these two cysteines contributes differentially to the intracellular trafficking of RGS4. These data show for the first time that Cys-2 and Cys-12 play markedly different roles in the regulation of RGS4 membrane localization, intracellular trafficking, and G(q) inhibitory function via mechanisms that are unrelated to RGS4 protein stabilization.
    Mesh-Begriff(e) Amino Acid Substitution ; Cell Membrane/genetics ; Cell Membrane/metabolism ; Cysteine/genetics ; Cysteine/metabolism ; Endosomes/genetics ; Endosomes/metabolism ; Enzyme Activation/genetics ; GTP-Binding Protein alpha Subunits, Gq-G11/genetics ; GTP-Binding Protein alpha Subunits, Gq-G11/metabolism ; HEK293 Cells ; Humans ; Lipoylation/physiology ; Membrane Glycoproteins/genetics ; Membrane Glycoproteins/metabolism ; Mutation, Missense ; Protein Stability ; Protein Structure, Secondary ; Protein Structure, Tertiary ; Protein Transport/physiology ; RGS Proteins/genetics ; RGS Proteins/metabolism
    Chemische Substanzen Membrane Glycoproteins ; RGS Proteins ; TGOLN2 protein, human ; RGS4 protein (175335-35-0) ; GTP-Binding Protein alpha Subunits, Gq-G11 (EC 3.6.5.1) ; Cysteine (K848JZ4886)
    Sprache Englisch
    Erscheinungsdatum 2012-06-29
    Erscheinungsland United States
    Dokumenttyp Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 2997-x
    ISSN 1083-351X ; 0021-9258
    ISSN (online) 1083-351X
    ISSN 0021-9258
    DOI 10.1074/jbc.M112.345629
    Datenquelle MEDical Literature Analysis and Retrieval System OnLINE

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    Verfügbar in ZB MED Köln/Königswinter

    Uc I Zs.108: Hefte anzeigen Standort:
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  4. Artikel ; Online: The autonomic nervous system and cardiac GLP-1 receptors control heart rate in mice.

    Baggio, Laurie L / Ussher, John R / McLean, Brent A / Cao, Xiemin / Kabir, M Golam / Mulvihill, Erin E / Mighiu, Alexandra S / Zhang, Hangjun / Ludwig, Andreas / Seeley, Randy J / Heximer, Scott P / Drucker, Daniel J

    Molecular metabolism

    2017  Band 6, Heft 11, Seite(n) 1339–1349

    Abstract: Objectives: Glucagon-like peptide-1 (GLP-1) is secreted from enteroendocrine cells and exerts a broad number of metabolic actions through activation of a single GLP-1 receptor (GLP-1R). The cardiovascular actions of GLP-1 have garnered increasing ... ...

    Abstract Objectives: Glucagon-like peptide-1 (GLP-1) is secreted from enteroendocrine cells and exerts a broad number of metabolic actions through activation of a single GLP-1 receptor (GLP-1R). The cardiovascular actions of GLP-1 have garnered increasing attention as GLP-1R agonists are used to treat human subjects with diabetes and obesity that may be at increased risk for development of heart disease. Here we studied mechanisms linking GLP-1R activation to control of heart rate (HR) in mice.
    Methods: The actions of GLP-1R agonists were examined on the control of HR in wild type mice (WT) and in mice with cardiomyocyte-selective disruption of the GLP-1R (Glp1r
    Results: Doses of liraglutide and lixisenatide that were equipotent for acute glucose control rapidly increased HR in WT and Glp1r
    Conclusions: GLP-1R agonists increase HR through multiple mechanisms, including regulation of autonomic nervous system function, and activation of the atrial GLP-1R. Surprisingly, the isolated atrial GLP-1R does not transduce a direct chronotropic effect following exposure to GLP-1R agonists in the intact heart, or isolated atrium, ex vivo. Hence, cardiac GLP-1R circuits controlling HR require neural inputs and do not function in a heart-autonomous manner.
    Mesh-Begriff(e) Animals ; Autonomic Nervous System/physiology ; Glucagon-Like Peptide 1/metabolism ; Glucagon-Like Peptide-1 Receptor/agonists ; Glucagon-Like Peptide-1 Receptor/metabolism ; Glucagon-Like Peptide-1 Receptor/physiology ; Heart Rate/drug effects ; Heart Rate/physiology ; Liraglutide/pharmacology ; Male ; Mice ; Mice, Inbred C57BL ; Peptides/pharmacology
    Chemische Substanzen Glp1r protein, mouse ; Glucagon-Like Peptide-1 Receptor ; Peptides ; lixisenatide (74O62BB01U) ; Liraglutide (839I73S42A) ; Glucagon-Like Peptide 1 (89750-14-1)
    Sprache Englisch
    Erscheinungsdatum 2017-09-01
    Erscheinungsland Germany
    Dokumenttyp Journal Article ; Research Support, Non-U.S. Gov't
    ISSN 2212-8778
    ISSN (online) 2212-8778
    DOI 10.1016/j.molmet.2017.08.010
    Datenquelle MEDical Literature Analysis and Retrieval System OnLINE

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  5. Artikel: Differential occupational risks to healthcare workers from SARS-CoV-2 observed during a prospective observational study

    Eyre, David W / Lumley, Sheila F / O039, / Donnell, Denise / Campbell, Mark / Sims, Elizabeth / Lawson, Elaine / Warren, Fiona / James, Tim / Cox, Stuart / Howarth, Alison / Doherty, George / Hatch, Stephanie B / Kavanagh, James / Chau, Kevin K / Fowler, Philip W / Swann, Jeremy / Volk, Denis / Yang-Turner, Fan /
    Stoesser, Nicole / Matthews, Philippa C / Dudareva, Maria / Davies, Timothy / Shaw, Robert H / Peto, Leon / Downs, Louise O / Vogt, Alexander / Amini, Ali / Young, Bernadette C / Drennan, Philip George / Mentzer, Alexander J / Skelly, Donal T / Karpe, Fredrik / Neville, Matt J / Andersson, Monique / Brent, Andrew J / Jones, Nicola / Martins Ferreira, Lucas / Christott, Thomas / Marsden, Brian D / Hoosdally, Sarah / Cornall, Richard / Crook, Derrick W / Stuart, David I / Screaton, Gavin / Watson, Adam Jr / Taylor, Adan / Chetwynd, Alan / Grassam-Rowe, Alexander / Mighiu, Alexandra S / Livingstone, Angus

    eLife (Cambridge)

    Abstract: We conducted voluntary Covid-19 testing programmes for symptomatic and asymptomatic staff at a UK teaching hospital using naso-/oro-pharyngeal PCR testing and immunoassays for IgG antibodies. 1128/10,034 (11.2%) staff had evidence of Covid-19 at some ... ...

    Abstract We conducted voluntary Covid-19 testing programmes for symptomatic and asymptomatic staff at a UK teaching hospital using naso-/oro-pharyngeal PCR testing and immunoassays for IgG antibodies. 1128/10,034 (11.2%) staff had evidence of Covid-19 at some time. Using questionnaire data provided on potential risk-factors, staff with a confirmed household contact were at greatest risk (adjusted odds ratio [aOR] 4.82 [95%CI 3.45-6.72]). Higher rates of Covid-19 were seen in staff working in Covid-19-facing areas (22.6% vs. 8.6% elsewhere) (aOR 2.47 [1.99-3.08]). Controlling for Covid-19-facing status, risks were heterogenous across the hospital, with higher rates in acute medicine (1.52 [1.07-2.16]) and sporadic outbreaks in areas with few or no Covid-19 patients. Covid-19 intensive care unit staff were relatively protected (0.44 [0.28-0.69]), likely by a bundle of PPE-related measures. Positive results were more likely in Black (1.66 [1.25-2.21]) and Asian (1.51 [1.28-1.77]) staff, independent of role or working location, and in porters and cleaners (2.06 [1.34-3.15]).
    Schlagwörter covid19
    Verlag WHO
    Dokumenttyp Artikel
    Anmerkung WHO #Covidence: #727516
    Datenquelle COVID19

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  6. Artikel ; Online: Differential occupational risks to healthcare workers from SARS-CoV-2 observed during a prospective observational study

    Eyre, David W / Lumley, Sheila F / O'Donnell, Denise / Campbell, Mark / Sims, Elizabeth / Lawson, Elaine / Warren, Fiona / James, Tim / Cox, Stuart / Howarth, Alison / Doherty, George / Hatch, Stephanie B / Kavanagh, James / Chau, Kevin K / Fowler, Philip W / Swann, Jeremy / Volk, Denis / Yang-Turner, Fan / Stoesser, Nicole /
    Matthews, Philippa C / Dudareva, Maria / Davies, Timothy / Shaw, Robert H / Peto, Leon / Downs, Louise O / Vogt, Alexander / Amini, Ali / Young, Bernadette C / Drennan, Philip George / Mentzer, Alexander J / Skelly, Donal T / Karpe, Fredrik / Neville, Matt J / Andersson, Monique / Brent, Andrew J / Jones, Nicola / Martins Ferreira, Lucas / Christott, Thomas / Marsden, Brian D / Hoosdally, Sarah / Cornall, Richard / Crook, Derrick W / Stuart, David I / Screaton, Gavin / Watson, Adam JR / Taylor, Adan / Chetwynd, Alan / Grassam-Rowe, Alexander / Mighiu, Alexandra S / Livingstone, Angus / Killen, Annabel / Rigler, Caitlin / Harries, Callum / East, Cameron / Lee, Charlotte / Mason, Chris JB / Holland, Christian / Thompson, Connor / Hennesey, Conor / Savva, Constantinos / Kim, David S / Harris, Edward WA / McGivern, Euan J / Qian, Evelyn / Rothwell, Evie / Back, Francesca / Kelly, Gabriella / Watson, Gareth / Howgego, Gregory / Chase, Hannah / Danbury, Hannah / Laurenson-Schafer, Hannah / Ward, Harry L / Hendron, Holly / Vorley, Imogen C / Tol, Isabel / Gunnell, James / Ward, Jocelyn LF / Drake, Jonathan / Wilson, Joseph D / Morton, Joshua / Dequaire, Julie / O'Byrne, Katherine / Motohashi, Kenzo / Harper, Kirsty / Ravi, Krupa / Millar, Lancelot J / Peck, Liam J / Oliver, Madeleine / English, Marcus Rex / Kumarendran, Mary / Wedlich, Matthew / Ambler, Olivia / Deal, Oscar T / Sweeney, Owen / Cowie, Philip / Naudé, Rebecca te Water / Young, Rebecca / Freer, Rosie / Scott, Samuel / Sussmes, Samuel / Peters, Sarah / Pattenden, Saxon / Waite, Seren / Johnson, Síle Ann / Kourdov, Stefan / Santos-Paulo, Stephanie / Dimitrov, Stoyan / Kerneis, Sven / Ahmed-Firani, Tariq / King, Thomas B / Ritter, Thomas G / Foord, Thomas H / De Toledo, Zoe / Christie, Thomas / Gergely, Bernadett / Axten, David / Simons, Emma-Jane / Nevard, Heather / Philips, Jane / Szczurkowska, Justyna / Patel, Kaisha / Smit, Kyla / Warren, Laura / Morgan, Lisa / Smith, Lucianne / Robles, Maria / McKnight, Mary / Luciw, Michael / Gates, Michelle / Sande, Nellia / Turford, Rachel / Ray, Roshni / Rughani, Sonam / Mitchell, Tracey / Bellinger, Trisha / Wharton, Vicki / Justice, Anita / Jesuthasan, Gerald / Wareing, Susan / Huda Mohamad Fadzillah, Nurul / Cann, Kathryn / Kirton, Richard / Sutton, Claire / Salvagno, Claudia / DAmato, Gabriella / Pill, Gemma / Butcher, Lisa / Rylance-Knight, Lydia / Tabirao, Merline / Moroney, Ruth / Wright, Sarah / Peto, Timothy EA / Holthof, Bruno / O'Donnell, Anne-Marie / Ebner, Daniel / Conlon, Christopher P / Jeffery, Katie / Walker, Timothy M

    eLife

    2020  Band 9

    Abstract: We conducted voluntary Covid-19 testing programmes for symptomatic and asymptomatic staff at a UK teaching hospital using naso-/oro-pharyngeal PCR testing and immunoassays for IgG antibodies. 1128/10,034 (11.2%) staff had evidence of Covid-19 at some ... ...

    Abstract We conducted voluntary Covid-19 testing programmes for symptomatic and asymptomatic staff at a UK teaching hospital using naso-/oro-pharyngeal PCR testing and immunoassays for IgG antibodies. 1128/10,034 (11.2%) staff had evidence of Covid-19 at some time. Using questionnaire data provided on potential risk-factors, staff with a confirmed household contact were at greatest risk (adjusted odds ratio [aOR] 4.82 [95%CI 3.45–6.72]). Higher rates of Covid-19 were seen in staff working in Covid-19-facing areas (22.6% vs. 8.6% elsewhere) (aOR 2.47 [1.99–3.08]). Controlling for Covid-19-facing status, risks were heterogenous across the hospital, with higher rates in acute medicine (1.52 [1.07–2.16]) and sporadic outbreaks in areas with few or no Covid-19 patients. Covid-19 intensive care unit staff were relatively protected (0.44 [0.28–0.69]), likely by a bundle of PPE-related measures. Positive results were more likely in Black (1.66 [1.25–2.21]) and Asian (1.51 [1.28–1.77]) staff, independent of role or working location, and in porters and cleaners (2.06 [1.34–3.15]).
    Schlagwörter General Biochemistry, Genetics and Molecular Biology ; General Immunology and Microbiology ; General Neuroscience ; General Medicine ; covid19
    Sprache Englisch
    Verlag eLife Sciences Publications, Ltd
    Erscheinungsland uk
    Dokumenttyp Artikel ; Online
    ZDB-ID 2687154-3
    ISSN 2050-084X
    ISSN 2050-084X
    DOI 10.7554/elife.60675
    Datenquelle BASE - Bielefeld Academic Search Engine (Lebenswissenschaftliche Auswahl)

    Volltext online

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  7. Buch ; Online: Author response

    Eyre, David W / Lumley, Sheila F / O'Donnell, Denise / Campbell, Mark / Sims, Elizabeth / Lawson, Elaine / Warren, Fiona / James, Tim / Cox, Stuart / Howarth, Alison / Doherty, George / Hatch, Stephanie B / Kavanagh, James / Chau, Kevin K / Fowler, Philip W / Swann, Jeremy / Volk, Denis / Yang-Turner, Fan / Stoesser, Nicole /
    Matthews, Philippa C / Dudareva, Maria / Davies, Timothy / Shaw, Robert H / Peto, Leon / Downs, Louise O / Vogt, Alexander / Amini, Ali / Young, Bernadette C / Drennan, Philip George / Mentzer, Alexander J / Skelly, Donal T / Karpe, Fredrik / Neville, Matt J / Andersson, Monique / Brent, Andrew J / Jones, Nicola / Martins Ferreira, Lucas / Christott, Thomas / Marsden, Brian D / Hoosdally, Sarah / Cornall, Richard / Crook, Derrick W / Stuart, David I / Screaton, Gavin / Watson, Adam JR / Taylor, Adan / Chetwynd, Alan / Grassam-Rowe, Alexander / Mighiu, Alexandra S / Livingstone, Angus / Killen, Annabel / Rigler, Caitlin / Harries, Callum / East, Cameron / Lee, Charlotte / Mason, Chris JB / Holland, Christian / Thompson, Connor / Hennesey, Conor / Savva, Constantinos / Kim, David S / Harris, Edward WA / McGivern, Euan J / Qian, Evelyn / Rothwell, Evie / Back, Francesca / Kelly, Gabriella / Watson, Gareth / Howgego, Gregory / Chase, Hannah / Danbury, Hannah / Laurenson-Schafer, Hannah / Ward, Harry L / Hendron, Holly / Vorley, Imogen C / Tol, Isabel / Gunnell, James / Ward, Jocelyn LF / Drake, Jonathan / Wilson, Joseph D / Morton, Joshua / Dequaire, Julie / O'Byrne, Katherine / Motohashi, Kenzo / Harper, Kirsty / Ravi, Krupa / Millar, Lancelot J / Peck, Liam J / Oliver, Madeleine / English, Marcus Rex / Kumarendran, Mary / Wedlich, Matthew / Ambler, Olivia / Deal, Oscar T / Sweeney, Owen / Cowie, Philip / Naudé, Rebecca te Water / Young, Rebecca / Freer, Rosie / Scott, Samuel / Sussmes, Samuel / Peters, Sarah / Pattenden, Saxon / Waite, Seren / Johnson, Síle Ann / Kourdov, Stefan / Santos-Paulo, Stephanie / Dimitrov, Stoyan / Kerneis, Sven / Ahmed-Firani, Tariq / King, Thomas B / Ritter, Thomas G / Foord, Thomas H / De Toledo, Zoe / Christie, Thomas / Gergely, Bernadett / Axten, David / Simons, Emma-Jane / Nevard, Heather / Philips, Jane / Szczurkowska, Justyna / Patel, Kaisha / Smit, Kyla / Warren, Laura / Morgan, Lisa / Smith, Lucianne / Robles, Maria / McKnight, Mary / Luciw, Michael / Gates, Michelle / Sande, Nellia / Turford, Rachel / Ray, Roshni / Rughani, Sonam / Mitchell, Tracey / Bellinger, Trisha / Wharton, Vicki / Justice, Anita / Jesuthasan, Gerald / Wareing, Susan / Huda Mohamad Fadzillah, Nurul / Cann, Kathryn / Kirton, Richard / Sutton, Claire / Salvagno, Claudia / DAmato, Gabriella / Pill, Gemma / Butcher, Lisa / Rylance-Knight, Lydia / Tabirao, Merline / Moroney, Ruth / Wright, Sarah / Peto, Timothy EA / Holthof, Bruno / O'Donnell, Anne-Marie / Ebner, Daniel / Conlon, Christopher P / Jeffery, Katie / Walker, Timothy M

    Differential occupational risks to healthcare workers from SARS-CoV-2 observed during a prospective observational study

    2020  

    Schlagwörter covid19
    Verlag eLife Sciences Publications, Ltd
    Erscheinungsland uk
    Dokumenttyp Buch ; Online
    DOI 10.7554/elife.60675.sa2
    Datenquelle BASE - Bielefeld Academic Search Engine (Lebenswissenschaftliche Auswahl)

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