Your search keyword '"L. Revell"' showing total 74 results

1. Pieter Vos, Longing for the Good Life: Virtue Ethics After Protestantism (London: Bloomsbury, 2020), pp. 224. £90.00/$115.00

Author

Roger L. Revell

Subjects

Religious studies

Published

2023

2. Supplementary Table 1 from Modulation of Plasma Metabolite Biomarkers of the MAPK Pathway with MEK Inhibitor RO4987655: Pharmacodynamic and Predictive Potential in Metastatic Melanoma

Author

Florence I. Raynaud, Udai Banerji, Paul Workman, Stanley B. Kaye, Johann S. de Bono, Suzanne A. Eccles, Valerie Meresse, Ruediger Rueger, Miro Venturi, Debra J. Skene, Victoria L. Revell, Alexis de haven Brandon, Gary Box, Melanie Valenti, Alan T. Henley, Yasmin J. Asad, Akos Pal, and Joo Ern Ang

Abstract

Time of day variation in metabolites in healthy volunteers and in patients treated with the MEK inhibitor.

Published

2023

3. Light and melatonin treatment for jet lag

Author

Charmane I. Eastman, Stephanie J. Crowley, and Victoria L. Revell

Published

2023

4. The Reformation and the Right Reading of Scripture, by Iain Provan

Author

Roger L. Revell

Subjects

History of religions, Philosophy, Reading (process), media_common.quotation_subject, Religious studies, Theology, media_common

Published

2020

5. Book Review: Canonical Theology: The Biblical Canon, Sola Scriptura, and Theological Method

Author

Roger L. Revell

Subjects

Philosophy, General Earth and Planetary Sciences, Canon, Theology, General Environmental Science

Published

2019

6. The effect of atmospheric nudging on the stratospheric residual circulation in chemistry–climate models

Author

A. Chrysanthou, A. C. Maycock, M. P. Chipperfield, S. Dhomse, H. Garny, D. Kinnison, H. Akiyoshi, M. Deushi, R. R. Garcia, P. Jöckel, O. Kirner, G. Pitari, D. A. Plummer, L. Revell, E. Rozanov, A. Stenke, T. Y. Tanaka, D. Visioni, and Y. Yamashita

Subjects

Mass flux, Atmospheric Science, 010504 meteorology & atmospheric sciences, Atmospheric physics, DATA processing & computer science, Flux, Magnitude (mathematics), Forcing (mathematics), 010502 geochemistry & geophysics, Residual, 01 natural sciences, lcsh:QC1-999, lcsh:Chemistry, chemistry-climate models Brewer-Dobson circulation Nudging, lcsh:QD1-999, 13. Climate action, Climatology, Erdsystem-Modellierung, Hindcast, Climate model, ddc:004, Stratosphere, lcsh:Physics, 0105 earth and related environmental sciences

Abstract

We perform the first multi-model intercomparison of the impact of nudged meteorology on the stratospheric residual circulation using hindcast simulations from the Chemistry–Climate Model Initiative (CCMI). We examine simulations over the period 1980–2009 from seven models in which the meteorological fields are nudged towards a reanalysis dataset and compare these with their equivalent free-running simulations and the reanalyses themselves. We show that for the current implementations, nudging meteorology does not constrain the mean strength of the stratospheric residual circulation and that the inter-model spread is similar, or even larger, than in the free-running simulations. The nudged models generally show slightly stronger upwelling in the tropical lower stratosphere compared to the free-running versions and exhibit marked differences compared to the directly estimated residual circulation from the reanalysis dataset they are nudged towards. Downward control calculations applied to the nudged simulations reveal substantial differences between the climatological lower-stratospheric tropical upward mass flux (TUMF) computed from the modelled wave forcing and that calculated directly from the residual circulation. This explicitly shows that nudging decouples the wave forcing and the residual circulation so that the divergence of the angular momentum flux due to the mean motion is not balanced by eddy motions, as would typically be expected in the time mean. Overall, nudging meteorological fields leads to increased inter-model spread for most of the measures of the mean climatological stratospheric residual circulation assessed in this study. In contrast, the nudged simulations show a high degree of consistency in the inter-annual variability in the TUMF in the lower stratosphere, which is primarily related to the contribution to variability from the resolved wave forcing. The more consistent inter-annual variability in TUMF in the nudged models also compares more closely with the variability found in the reanalyses, particularly in boreal winter. We apply a multiple linear regression (MLR) model to separate the drivers of inter-annual and long-term variations in the simulated TUMF; this explains up to ∼75 % of the variance in TUMF in the nudged simulations. The MLR model reveals a statistically significant positive trend in TUMF for most models over the period 1980–2009. The TUMF trend magnitude is generally larger in the nudged models compared to their free-running counterparts, but the intermodel range of trends doubles from around a factor of 2 to a factor of 4 due to nudging. Furthermore, the nudged models generally do not match the TUMF trends in the reanalysis they are nudged towards for trends over different periods in the interval 1980–2009. Hence, we conclude that nudging does not strongly constrain long-term trends simulated by the chemistry–climate model (CCM) in the residual circulation. Our findings show that while nudged simulations may, by construction, produce accurate temperatures and realistic representations of fast horizontal transport, this is not typically the case for the slower zonal mean vertical transport in the stratosphere. Consequently, caution is required when using nudged simulations to interpret the behaviour of stratospheric tracers that are affected by the residual circulation.

Published

2019

7. Effect of acute total sleep deprivation on plasma melatonin, cortisol and metabolite rhythms in females

Author

Aya Honma, Debra J. Skene, Sarah K. Davies, Benita Middleton, Florence I. Raynaud, Pippa J. Gunn, and Victoria L. Revell

Subjects

Male, Circadian Rhythms ‐ Special Issue, medicine.medical_specialty, Hydrocortisone, Metabolite, Total sleep deprivation, Melatonin, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Rhythm, Internal medicine, medicine, Humans, Circadian rhythm, Young female, 030304 developmental biology, 0303 health sciences, business.industry, General Neuroscience, sleep biomarkers, Special Issue Article, metabolomics, Circadian Rhythm, Sleep deprivation, Endocrinology, chemistry, circadian rhythms, Sleep Deprivation, Female, Wakefulness, medicine.symptom, Sleep, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Disruption to sleep and circadian rhythms can impact on metabolism. The study aimed to investigate the effect of acute sleep deprivation on plasma melatonin, cortisol and metabolites, to increase understanding of the metabolic pathways involved in sleep/wake regulation processes. Twelve healthy young female participants remained in controlled laboratory conditions for ~92 hr with respect to posture, meals and environmental light (18:00–23:00 hr and 07:00‐09:00 hr, Young females were kept in controlled laboratory conditions comprising baseline sleep, sleep deprivation and recovery sleep and 1–2 hr blood sampling for 70 hr. Night‐time melatonin increased during sleep deprivation, returning to baseline levels during recovery sleep, whilst no significant changes were observed in cortisol. Of 130 plasma metabolites quantified by targeted metabolomics, 41 were altered across the nights (00:00–06:00 hr) and 58 maintained their rhythmicity across the three study days.

Published

2019

8. S‐cone contribution to the acute melatonin suppression response in humans

Author

Debra J. Skene, Josephine Arendt, Timothy M. Brown, Kavita Thapan, and Victoria L. Revell

Subjects

Adult, Male, 0301 basic medicine, Melanopsin, Light, Stimulus (physiology), Melatonin, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, medicine, Humans, Circadian rhythm, Young male, Action spectrum, Physics, Intrinsically photosensitive retinal ganglion cells, Rod Opsins, Circadian Rhythm, 030104 developmental biology, Spectral sensitivity, Retinal Cone Photoreceptor Cells, sense organs, Neuroscience, 030217 neurology & neurosurgery, medicine.drug

Abstract

Light influences diverse aspects of human physiology and behaviour including neuroendocrine function, the circadian system and sleep. A role for melanopsin-expressing intrinsically photosensitive retinal ganglion cells (ipRGCs) in driving such effects is well established. However, rod and/or cone signals routed through ipRGCs could also influence "non-visual" spectral sensitivity. In humans, this has been most extensively studied for acute, light-dependent, suppression of nocturnal melatonin production. Of the published action spectra for melatonin suppression, one demonstrates a spectral sensitivity consistent with that expected for melanopsin while our own (using briefer 30 minute light exposures) displays very high sensitivity to short wavelength light, suggesting a contribution of S-cones. To clarify that possibility, six healthy young male participants were each exposed to 30 minutes of five irradiances of 415 nm monochromatic light (1-40 µW/cm2 ) across different nights. These data were then combined with the original action spectrum. The aggregated data are incompatible with the involvement of any single-opsin and multi-opsin models based on the original action spectrum (including Circadian Stimulus) fail to predict the responses to 415 nm stimuli. Instead, the extended action spectrum can be most simply approximated by an ~2:1 combination of melanopsin and S-cone signals. Such a model also better describes the magnitude of melatonin suppression observed in other studies using an equivalent 30 minute mono- or polychromatic light paradigm but not those using longer (90 minute) light exposures. In sum, these data provide evidence for an initial S-cone contribution to melatonin suppression that rapidly decays under extended light exposure.

Published

2021

9. Effects of the selective orexin-2 receptor antagonist JNJ-48816274 on sleep initiated in the circadian wake maintenance zone: a randomised trial

Author

Derk-Jan Dijk, Hana Hassanin, Ciro della Monica, Sandra R. Chaplan, Robin Halter, Jeewaka Mendis, and Victoria L. Revell

Subjects

Male, medicine.drug_class, Polysomnography, Placebo, Non-rapid eye movement sleep, Article, Double-Blind Method, Orexin Receptors, Sleep Initiation and Maintenance Disorders, Medicine, Humans, Effects of sleep deprivation on cognitive performance, Circadian rhythm, Pharmacology, Orexins, business.industry, Antagonist, Receptor antagonist, Sleep in non-human animals, Psychiatry and Mental health, Anesthesia, Orexin Receptor Antagonists, Sleep onset latency, Circadian rhythms and sleep, business, Sleep

Abstract

The effects of orexinergic peptides are diverse and are mediated by orexin-1 and orexin-2 receptors. Antagonists that target both receptors have been shown to promote sleep initiation and maintenance. Here, we investigated the role of the orexin-2 receptor in sleep regulation in a randomised, double-blind, placebo-controlled, three-period crossover clinical trial using two doses (20 and 50 mg) of a highly selective orexin-2 receptor antagonist (2-SORA) (JNJ-48816274). We used a phase advance model of sleep disruption where sleep initiation is scheduled in the circadian wake maintenance zone. We assessed objective and subjective sleep parameters, pharmacokinetic profiles and residual effects on cognitive performance in 18 healthy male participants without sleep disorders. The phase advance model alone (placebo condition) resulted in disruption of sleep at the beginning of the sleep period compared to baseline sleep (scheduled at habitual time). Compared to placebo, both doses of JNJ-48816274 significantly increased total sleep time, REM sleep duration and sleep efficiency, and reduced latency to persistent sleep, sleep onset latency, and REM latency. All night EEG spectral power density for both NREM and REM sleep were unaffected by either dose. Participants reported significantly better quality of sleep and feeling more refreshed upon awakening following JNJ-48816274 compared to placebo. No significant residual effects on objective performance measures were observed and the compound was well tolerated. In conclusion, the selective orexin-2 receptor antagonist JNJ-48816274 rapidly induced sleep when sleep was scheduled earlier in the circadian cycle and improved self-reported sleep quality without impact on waking performance.

Published

2021

10. Leopoldo A. Sanchez, Sculptor Spirit: Models of Sanctification from Spirit Christology (Downers Grove, IL: IVP Academic, 2019), pp. xxi + 278. $28.00

Author

Roger L. Revell

Subjects

Philosophy, Christology, Religious studies, Sanctification, Theology

Published

2020

11. Efficacy of a Topical Aromatic Rub (Vicks VapoRub®) on Effects on Self-Reported and Actigraphically Assessed Aspects of Sleep in Common Cold Patients

Author

David Hull, Victoria L. Revell, Derk-Jan Dijk, David Ramsey, Gill Phillipson, and Nayantara Santhi

Subjects

Sleep disorder, medicine.medical_specialty, Visual analogue scale, business.industry, Actigraphy, medicine.disease, Placebo, 03 medical and health sciences, 0302 clinical medicine, 030228 respiratory system, Refreshing Sleep, medicine, Physical therapy, Sleep diary, Sleep onset latency, medicine.drug_brand, business, 030217 neurology & neurosurgery, Vicks vaporub

Abstract

Common cold sufferers frequently report sleep disruption during the symptomatic period of infections. We examined the effects of treatment with a topical aromatic pharmaceutical ointment (Vicks VapoRub®), on associated sleep disturbances. The effects of Vicks VapoRub® versus placebo (petrolatum ointment) on subjective and objective measured sleep parameters were assessed in an exploratory study of 100 common cold patients, in a randomized, single blind, controlled, two-arm, parallel design study. The primary efficacy variable was subjective sleep quality measured with the SQSQ (Subjective Quality of Sleep Questionnaire). Additional measures included, ease of falling asleep and depth of sleep (measured with a post-sleep Visual Analog Scale), total sleep time, sleep onset latency, activity score, percentage of sleep, sleep efficiency (measured with actigraphy and SQSQ) and sleep quality index measured with a modified Karolinska Sleep Diary (KSD). The primary endpoint, “How was the quality of your sleep last night?” showed a statistically significant difference in change from baseline in favour of VapoRub treatment (p = 0.0392) versus placebo. Positive effects of VapoRub versus placebo were also observed for “How refreshed did you feel upon waking up?” (p = 0.0122) (SQSQ), “Did you get enough sleep?” (p = 0.0036) (KSD), “How was it to get up?” (p = 0.0120) (KSD) and “Do you feel well-rested?” (p = 0.0125) (KSD). No statistically significant changes from baseline versus placebo were detected in the Actiwatch endpoints. Vicks VapoRub® when applied before retiring to bed can reduce subjective sleep disturbances during a common cold. The results of this exploratory study support the belief among patients that the use of VapoRub improves subjective sleep quality during common cold which was associated with more refreshing sleep.

Published

2017

12. Book Review: The Theological Anthropology of David Kelsey: Responses to Eccentric Existence

Author

Roger L. Revell

Subjects

Philosophy, General Earth and Planetary Sciences, Eccentric, Theology, General Environmental Science

Published

2017

13. Circadian regulation in human white adipose tissue revealed by transcriptome and metabolic network analysis

Author

Jonathan D. Johnston, Victoria L. Revell, Cheryl Isherwood, Huihai Wu, Skevoulla Christou, Carla S. Möller-Levet, Debra J. Skene, Emma Laing, Sophie M T Wehrens, Giselda Bucca, and Simon Archer

Subjects

0301 basic medicine, Adipose Tissue, White, lcsh:Medicine, Adipose tissue, White adipose tissue, Biology, Article, Nucleic acid metabolism, Transcriptome, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Circadian Clocks, Animals, Humans, Circadian rhythm, lcsh:Science, Regulation of gene expression, Multidisciplinary, Gene Expression Profiling, lcsh:R, Computational Biology, Lipid metabolism, Circadian Rhythm, Cell biology, Metabolic pathway, 030104 developmental biology, Gene Expression Regulation, chemistry, lcsh:Q, Energy Metabolism, Metabolic Networks and Pathways, 030217 neurology & neurosurgery

Abstract

Studying circadian rhythms in most human tissues is hampered by difficulty in collecting serial samples. Here we reveal circadian rhythms in the transcriptome and metabolic pathways of human white adipose tissue. Subcutaneous adipose tissue was taken from seven healthy males under highly controlled ‘constant routine’ conditions. Five biopsies per participant were taken at six-hourly intervals for microarray analysis and in silico integrative metabolic modelling. We identified 837 transcripts exhibiting circadian expression profiles (2% of 41619 transcript targeting probes on the array), with clear separation of transcripts peaking in the morning (258 probes) and evening (579 probes). There was only partial overlap of our rhythmic transcripts with published animal adipose and human blood transcriptome data. Morning-peaking transcripts associated with regulation of gene expression, nitrogen compound metabolism, and nucleic acid biology; evening-peaking transcripts associated with organic acid metabolism, cofactor metabolism and redox activity. In silico pathway analysis further indicated circadian regulation of lipid and nucleic acid metabolism; it also predicted circadian variation in key metabolic pathways such as the citric acid cycle and branched chain amino acid degradation. In summary, in vivo circadian rhythms exist in multiple adipose metabolic pathways, including those involved in lipid metabolism, and core aspects of cellular biochemistry.

Published

2019

14. Effect of Single and Combined Monochromatic Light on the Human Pupillary Light Response

Author

Maria A. Bonmati-Carrion, Konstanze Hild, Cheryl M. Isherwood, Stephen J. Sweeney, Victoria L. Revell, Juan A. Madrid, Maria A. Rol, and Debra J. Skene

Subjects

Materials science, Retinal ganglion, lcsh:RC346-429, human melanopic lux, 03 medical and health sciences, 0302 clinical medicine, Optics, ipRGC, Pupillary response, Pupillary light reflex, lcsh:Neurology. Diseases of the nervous system, Original Research, business.industry, pupillometry, Intrinsically photosensitive retinal ganglion cells, pupillary light reflex, Wavelength, Spectral sensitivity, Neurology, 030221 ophthalmology & optometry, Neurology (clinical), Monochromatic color, light, business, melanopsin, 030217 neurology & neurosurgery, Pupillometry

Abstract

The pupillary light reflex (PLR) is a neurological reflex driven by rods, cones, and melanopsin-containing retinal ganglion cells. Our aim was to achieve a more precise picture of the effects of 5-min duration monochromatic light stimuli, alone or in combination, on the human PLR, to determine its spectral sensitivity and to assess the importance of photon flux. Using pupillometry, the PLR was assessed in 13 participants (6 women) aged 27.2 ± 5.41 years (mean ± SD) during 5-min light stimuli of purple (437 nm), blue (479 nm), red (627 nm), and combinations of red+purple or red+blue light. In addition, nine 5-min, photon-matched light stimuli, ranging in 10 nm increments peaking between 420 and 500 nm were tested in 15 participants (8 women) aged 25.7 ± 8.90 years. Maximum pupil constriction, time to achieve this, constriction velocity, area under the curve (AUC) at short (0–60 s), and longer duration (240–300 s) light exposures, and 6-s post-illumination pupillary response (6-s PIPR) were assessed. Photoreceptor activation was estimated by mathematical modeling. The velocity of constriction was significantly faster with blue monochromatic light than with red or purple light. Within the blue light spectrum (between 420 and 500 nm), the velocity of constriction was significantly faster with the 480 nm light stimulus, while the slowest pupil constriction was observed with 430 nm light. Maximum pupil constriction was achieved with 470 nm light, and the greatest AUC0−60 and AUC240−300 was observed with 490 and 460 nm light, respectively. The 6-s PIPR was maximum after 490 nm light stimulus. Both the transient (AUC0−60) and sustained (AUC240−300) response was significantly correlated with melanopic activation. Higher photon fluxes for both purple and blue light produced greater amplitude sustained pupillary constriction. The findings confirm human PLR dependence on wavelength, monochromatic or bichromatic light and photon flux under 5-min duration light stimuli. Since the most rapid and high amplitude PLR occurred within the 460–490 nm light range (alone or combined), our results suggest that color discrimination should be studied under total or partial substitution of this blue light range (460–490 nm) by shorter wavelengths (~440 nm). Thus for nocturnal lighting, replacement of blue light with purple light might be a plausible solution to preserve color discrimination while minimizing melanopic activation.

Published

2018

15. Luther and Calvinism: Image and Reception of Martin Luther in the History and Theology of Calvinism, by Herman Selderhuis and J. Marius J. Lange van Ravenswaay, eds

Author

Roger L. Revell

Subjects

Martin luther, Calvinism, History of religions, Philosophy, Religious studies, Theology

Published

2019

16. Validation of an innovative method, based on tilt sensing, for the assessment of activity and body position

Author

Debra J. Skene, Juan Antonio Madrid, M. A. Rol, Maria-Angeles Bonmati-Carrion, Benita Middleton, and Victoria L. Revell

Subjects

Adult, Male, medicine.medical_specialty, Light, Physiology, Posture, Monitoring, Ambulatory, Wrist, Young Adult, Acceleration, Physical medicine and rehabilitation, Physiology (medical), medicine, Humans, Motor activity, Joint evaluation, Daily routine, Melatonin, business.industry, Body position, Actigraphy, Circadian Rhythm, Surgery, Tilt (optics), medicine.anatomical_structure, Female, Skin Temperature, Sleep, business

Abstract

Since there is less movement during sleep than during wake, the recording of body movements by actigraphy has been used to indirectly evaluate the sleep-wake cycle. In general, most actigraphic devices are placed on the wrist and their measures are based on acceleration detection. Here, we propose an alternative way of measuring actigraphy at the level of the arm for joint evaluation of activity and body position. This method analyzes the tilt of three axes, scoring activity as the cumulative change of degrees per minute with respect to the previous sampling, and measuring arm tilt for the body position inference. In this study, subjects (N = 13) went about their daily routine for 7 days, kept daily sleep logs, wore three ambulatory monitoring devices and collected sequential saliva samples during evenings for the measurement of dim light melatonin onset (DLMO). These devices measured motor activity (arm activity, AA) and body position (P) using the tilt sensing of the arm, with acceleration (wrist acceleration, WA) and skin temperature at wrist level (WT). Cosinor, Fourier and non-parametric rhythmic analyses were performed for the different variables, and the results were compared by the ANOVA test. Linear correlations were also performed between actimetry methods (AA and WA) and WT. The AA and WA suitability for circadian phase prediction and for evaluating the sleep-wake cycle was assessed by comparison with the DLMO and sleep logs, respectively. All correlations between rhythmic parameters obtained from AA and WA were highly significant. Only parameters related to activity levels, such as mesor, RA (relative amplitude), VL5 and VM10 (value for the 5 and 10 consecutive hours of minimum and maximum activity, respectively) showed significant differences between AA and WA records. However, when a correlation analysis was performed on the phase markers acrophase, mid-time for the 10 consecutive hours of highest (M10) and mid-time for the five consecutive hours of lowest activity (L5) with DLMO, all of them showed a significant correlation for AA (R = 0.607, p = 0.028; R = 0.582, p = 0.037; R = 0.620, p = 0.031, respectively), while for WA, only acrophase did (R = 0.621, p = 0.031). Regarding sleep detection, WA showed higher specificity than AA (0.95 ± 0.01 versus 0.86 ± 0.02), while the agreement rate and sensitivity were higher for AA (0.76 ± 0.02 versus 0.66 ± 0.02 and 0.71 ± 0.03 versus 0.53 ± 0.03, respectively). Cohen's kappa coefficient also presented the highest values for AA (0.49 ± 0.04) and AP (0.64 ± 0.04), followed by WT (0.45 ± 0.06) and WA (0.37 ± 0.04). The findings demonstrate that this alternative actigraphy method (AA), based on tilt sensing of the arm, can be used to reliably evaluate the activity and sleep-wake rhythm, since it presents a higher agreement rate and sensitivity for detecting sleep, at the same time allows the detection of body position and improves circadian phase assessment compared to the classical actigraphic method based on wrist acceleration.

Published

2015

17. Book Review: The Groaning of Creation: God, Evolution, and the Problem of Evil

Author

Roger L. Revell

Subjects

Philosophy, media_common.quotation_subject, Flourishing, Problem of evil, Metaphysics, Faith, Dilemma, Aesthetics, Intelligent design, Dualism, General Earth and Planetary Sciences, Theology, Creationism, General Environmental Science, media_common

Abstract

The Groaning of Creation: God, Evolution, and the Problem of Evil. By Christopher Southgate. Louisville, Ky.: Westminster John Knox Press, 2008. xii + 196 pp. $27.00 (paper).With care and conviction, Christopher Southgate embarks on a task that daunts but beckons. Several acknowledgments launch his project: the Christian affirmation that creation is good as well as the sobering awareness that violence and death are endemic to it. Can such "grandeur and groaning" be reconciled? Southgate aims to engage creations groaning while yet espousing faith in a God who is "creative, redemptive, and all-loving" (p. 15).This dilemma has elicited various prior approaches. In the first portion, Southgate rejects many. This list includes the path of creationism/intelligent design, which is insufficiently attuned to modern science. Metaphysical dualism is also jettisoned. There is no rival to God; there is no evil within God. Southgate also critiques the so-called "fall narrative" theology of Genesis. This conception attributes all violence and pain in creation to human rebellion against God (Genesis 3). It is an outlook that must be debunked: biological death cannot be regarded as a consequence of any long-past human activity. Support for this indictment draws both from biological science and improved readings of Genesis 1-3.In chapter 3, Thomas Aquinas enters the discussion as Southgate undertakes "good-harm analyses" as a means for situating "evolutionary evil" (that is, that with no human cause) within creations goodness. This mode of reasoning posits that certain creation "values" can only emerge through a process that involves the "disvalues" of evolutionary suffering (pp. 41-42). Evolutionary suffering leads to something higher. This perspective, of course, begs certain questions. Accordingly, Southgate invokes the notion of Gods "co-suffering" with creation, as well as Gods promised eschatological redemption, as an answer to the problem of individual suffering. This lays the groundwork for chapter 4. Here, Southgate speculatively attempts to fuse elements of evolutionary creation with certain core Christian convictions. He ponders anew the objective ramification of the atonement. It is characterized as an event which begins the final phase of creation: the evolutionary process will finally be sublimated to ultimate healing and transformation. Southgate imagines this as redemption for creatures who never knew flourishing because of evolutionary violence. Though suppositional, this rumination is hardly dissonant with the testimony of Colossians 1 and Ephesians 1.On the coattails of this hope, chapter 5 contemplates-in a biblical, creative manner-the eschatological existence of non-human creation. Especially intriguing is an attempt to imagine what non-human eschatological redemption might involve. …

Published

2016

18. Key lessons for incorporating natural infrastructure into regional climate adaptation planning

Author

Kevin O'Connor, Gregory M. Verutes, Chris Coburn, Ross Clark, Anne D. Guerry, Erin Prahler, Sarah Stoner-Duncan, Suzanne Langridge, Mary Ruckelshaus, Katie K. Arkema, Margaret R. Caldwell, Adina Abeles, Eric Hartge, and David L. Revell

Subjects

Process (engineering), business.industry, Flooding (psychology), Environmental resource management, Vulnerability, Management, Monitoring, Policy and Law, Aquatic Science, Oceanography, Natural (archaeology), Coastal erosion, Scale (social sciences), Business, Adaptation (computer science), Coastal flood

Abstract

Sea-level rise, potential changes in the intensity and frequency of storms, and consequent shoreline erosion and flooding will have increasing impacts on the economy and culture of coastal regions. A growing body of evidence suggests that coastal ecosystemsdnatural infrastructuredcan play an important role in reducing the vulnerability of people and property to these impacts. To effectively inform climate adaptation planning, experts often struggle to develop relevant local and regional information at a scale that is appropriate for decision-making. In addition, institutional capacity and resource constraints often limit planners’ ability to incorporate innovative, scientifically based approaches into planning. In this paper, we detail our collaborative process in two coastal California counties to account for the role of natural infrastructure in climate adaptation planning. We used an interdisciplinary team of scientists, economists, engineers, and law and policy experts and planners, and an iterative engagement process to (1) identify natural infrastructure that is geographically relevant to local jurisdictional planning units, (2) refine data and models to reflect regional processes, and (3) develop metrics likely to resonate within the local decision contexts. Using an open source decisionsupport tool, we demonstrated that protecting existing natural infrastructuredincluding coastal dunes and wetlandsdcould reduce the vulnerability of water resource-related structures, coastal populations, and farmland most exposed to coastal flooding and erosion. This information formed part of the rationale for priority climate adaptation projects the county governments are now pursuing. Our collaborative and iterative approach, as well as replicable use of an open source decision-support tool, facilitated inclusion of relevant natural infrastructure information into regional climate adaptation planning processes and products. This approach can be applied in diverse coastal climate adaptation planning contexts to locate and characterize the degree to which specific natural habitats can reduce vulnerability to sea-level rise and storms.

Published

2014

19. Effect of sleep deprivation on the human metabolome

Author

Victoria L. Revell, Alfred E. Thumser, Manfred Kayser, Sarah K. Davies, Anuska Mann, Benita Middleton, Debra J. Skene, F Robertson, Nanyi Cui, Florence I. Raynaud, Ben Holmes, Joo Ern Ang, Katrin Ackermann, Erasmus MC other, and Genetic Identification

Subjects

Male, medicine.medical_specialty, Principal Component Analysis, Multidisciplinary, Circadian clock, Biology, Biological Sciences, Melatonin, Sleep deprivation, Endocrinology, SDG 3 - Good Health and Well-being, Internal medicine, Multivariate Analysis, medicine, Metabolome, Humans, Metabolomics, Sleep Deprivation, Wakefulness, Serotonin, Circadian rhythm, medicine.symptom, medicine.drug, Sleep restriction

Abstract

Sleep restriction and circadian clock disruption are associated with metabolic disorders such as obesity, insulin resistance, and diabetes. The metabolic pathways involved in human sleep, however, have yet to be investigated with the use of a metabolomics approach. Here we have used untargeted and targeted liquid chromatography (LC)/MS metabolomics to examine the effect of acute sleep deprivation on plasma metabolite rhythms. Twelve healthy young male subjects remained in controlled laboratory conditions with respect to environmental light, sleep, meals, and posture during a 24-h wake/sleep cycle, followed by 24 h of wakefulness. Two-hourly plasma samples collected over the 48 h period were analyzed by LC/MS. Principal component analysis revealed a clear time of day variation with a significant cosine fit during the wake/sleep cycle and during 24 h of wakefulness in untargeted and targeted analysis. Of 171 metabolites quantified, daily rhythms were observed in the majority (n = 109), with 78 of these maintaining their rhythmicity during 24 h of wakefulness, most with reduced amplitude (n = 66). During sleep deprivation, 27 metabolites (tryptophan, serotonin, taurine, 8 acylcarnitines, 13 glycerophospholipids, and 3 sphingolipids) exhibited significantly increased levels compared with during sleep. The increased levels of serotonin, tryptophan, and taurine may explain the antidepressive effect of acute sleep deprivation and deserve further study. This report, to our knowledge the first of metabolic profiling during sleep and sleep deprivation and characterization of 24 h rhythms under these conditions, offers a novel view of human sleep/wake regulation.

Published

2014

20. Circadian phase asessment by ambulatory monitoring in humans: Correlation with dim light melatonin onset

Author

Benita Middleton, Juan Antonio Madrid, M. A. Rol, Victoria L. Revell, Maria-Angeles Bonmati-Carrion, and Debra J. Skene

Subjects

Adult, Male, Light therapy, medicine.medical_specialty, Evening, Light, Physiology, medicine.medical_treatment, Radioimmunoassay, Monitoring, Ambulatory, Body Temperature, Correlation, Melatonin, Young Adult, Surveys and Questionnaires, Physiology (medical), Internal medicine, Humans, Medicine, Circadian rhythm, Saliva, business.industry, Chronotherapy (sleep phase), Actigraphy, Circadian Rhythm, Endocrinology, Ambulatory, Cardiology, Female, Sleep, business, medicine.drug

Abstract

The increased prevalence of circadian disruptions due to abnormal coupling between internal and external time makes the detection of circadian phase in humans by ambulatory recordings a compelling need. Here, we propose an accurate practical procedure to estimate circadian phase with the least possible burden for the subject, that is, without the restraints of a constant routine protocol or laboratory techniques such as melatonin quantification, both of which are standard procedures. In this validation study, subjects (N = 13) wore ambulatory monitoring devices, kept daily sleep diaries and went about their daily routine for 10 days. The devices measured skin temperature at wrist level (WT), motor activity and body position on the arm, and light exposure by means of a sensor placed on the chest. Dim light melatonin onset (DLMO) was used to compare and evaluate the accuracy of the ambulatory variables in assessing circadian phase. An evening increase in WT: WTOnset (WTOn) and "WT increase onset" (WTiO) was found to anticipate the evening increase in melatonin, while decreases in motor activity (Activity Offset or AcOff), body position (Position Offset (POff)), integrative TAP (a combination of WT, activity and body position) (TAPOffset or TAPOff) and an increase in declared sleep propensity were phase delayed with respect to DLMO. The phase markers obtained from subjective sleep (R = 0.811), WT (R = 0.756) and the composite variable TAP (R = 0.720) were highly and significantly correlated with DLMO. The findings strongly support a new method to calculate circadian phase based on WT (WTiO) that accurately predicts and shows a temporal association with DLMO. WTiO is especially recommended due to its simplicity and applicability to clinical use under conditions where knowing endogenous circadian phase is important, such as in cancer chronotherapy and light therapy.

Published

2013

21. Effect of sleep deprivation on rhythms of clock gene expression and melatonin in humans

Author

Victoria L. Revell, Katrin Ackermann, Benita Middleton, Rosina Plomp, Oscar Lao, Manfred Kayser, Debra J. Skene, and Genetic Identification

Subjects

Adult, Male, endocrine system, medicine.medical_specialty, Time Factors, Hydrocortisone, Light, Physiology, Circadian clock, Radioimmunoassay, Melatonin, Young Adult, Dark therapy, Oscillometry, Physiology (medical), Internal medicine, Leukocytes, medicine, Humans, Free-running sleep, HSP70 Heat-Shock Proteins, Circadian rhythm, business.industry, Gene Expression Profiling, ARNTL Transcription Factors, Period Circadian Proteins, Circadian Rhythm, CLOCK, Oxidative Stress, Sleep deprivation, Endocrinology, Gene Expression Regulation, Light effects on circadian rhythm, Nuclear Receptor Subfamily 1, Group D, Member 1, Sleep Deprivation, medicine.symptom, Sleep, business, medicine.drug

Abstract

This study investigated the impact of sleep deprivation on the human circadian system. Plasma melatonin and cortisol levels and leukocyte expression levels of 12 genes were examined over 48 h (sleep vs. no-sleep nights) in 12 young males (mean ± SD: 23 ± 5 yrs). During one night of total sleep deprivation, BMAL1 expression was suppressed, the heat shock gene HSPA1B expression was induced, and the amplitude of the melatonin rhythm increased, whereas other high-amplitude clock gene rhythms (e.g., PER1-3, REV-ERBα) remained unaffected. These data suggest that the core clock mechanism in peripheral oscillators is compromised during acute sleep deprivation.

Published

2013

22. Modulation of Plasma Metabolite Biomarkers of the MAPK Pathway with MEK Inhibitor RO4987655: Pharmacodynamic and Predictive Potential in Metastatic Melanoma

Author

Joo Ern, Ang, Akos, Pal, Yasmin J, Asad, Alan T, Henley, Melanie, Valenti, Gary, Box, Alexis, de Haven Brandon, Victoria L, Revell, Debra J, Skene, Miro, Venturi, Ruediger, Rueger, Valerie, Meresse, Suzanne A, Eccles, Johann S, de Bono, Stanley B, Kaye, Paul, Workman, Udai, Banerji, and Florence I, Raynaud

Subjects

Mitogen-Activated Protein Kinase Kinases, Proto-Oncogene Proteins B-raf, MAP Kinase Signaling System, Xenograft Model Antitumor Assays, Article, Mice, Cell Line, Tumor, Benzamides, Mutation, Oxazines, Biomarkers, Tumor, Animals, Humans, Neoplasm Metastasis, Melanoma, Protein Kinase Inhibitors

Abstract

MAPK pathway activation is frequently observed in human malignancies, including melanoma, and is associated with sensitivity to MEK inhibition and changes in cellular metabolism. Using quantitative mass spectrometry-based metabolomics, we identified in preclinical models 21 plasma metabolites including amino acids, propionylcarnitine, phosphatidylcholines, and sphingomyelins that were significantly altered in two B-RAF-mutant melanoma xenografts and that were reversed following a single dose of the potent and selective MEK inhibitor RO4987655. Treatment of non-tumor-bearing animals and mice bearing the PTEN-null U87MG human glioblastoma xenograft elicited plasma changes only in amino acids and propionylcarnitine. In patients with advanced melanoma treated with RO4987655, on-treatment changes of amino acids were observed in patients with disease progression and not in responders. In contrast, changes in phosphatidylcholines and sphingomyelins were observed in responders. Furthermore, pretreatment levels of seven lipids identified in the preclinical screen were statistically significantly able to predict objective responses to RO4987655. The RO4987655 treatment-related changes were greater than baseline physiological variability in nontreated individuals. This study provides evidence of a translational exo-metabolomic plasma readout predictive of clinical efficacy together with pharmacodynamic utility following treatment with a signal transduction inhibitor.

Published

2016

23. Human phase response curve to intermittent blue light using a commercially available device

Author

Victoria L. Revell, Thomas A. Molina, and Charmane I. Eastman

Subjects

Physics, Physiology, business.industry, Circadian clock, Melatonin, Before Bedtime, Optics, medicine, Photopigment, Circadian rhythm, business, medicine.drug, Morning, Phase response curve, Ultradian rhythm

Abstract

Light shifts the timing of the circadian clock according to a phase response curve (PRC). To date, all human light PRCs have been to long durations of bright white light. However, melanopsin, the primary photopigment for the circadian system, is most sensitive to short wavelength blue light. Therefore, to optimise light treatment it is important to generate a blue light PRC.We used a small, commercially available blue LED light box, screen size 11.2 × 6.6 cm at ∼50 cm, ∼200 μW cm(−2), ∼185 lux. Subjects participated in two 5 day laboratory sessions 1 week apart. Each session consisted of circadian phase assessments to obtain melatonin profiles before and after 3 days of free-running through an ultradian light–dark cycle (2.5 h wake in dim light, 1.5 h sleep in the dark), forced desynchrony protocol. During one session subjects received intermittent blue light (three 30 min pulses over 2 h) once a day for the 3 days of free-running, and in the other session (control) they remained in dim room light, counterbalanced. The time of blue light was varied among subjects to cover the entire 24 h day. For each individual, the phase shift to blue light was corrected for the free-run determined during the control session. The blue light PRC had a broad advance region starting in the morning and extending through the afternoon. The delay region started a few hours before bedtime and extended through the night. This is the first PRC to be constructed to blue light and to a stimulus that could be used in the real world.

Published

2012

24. A 'Melanopic' Spectral Efficiency Function Predicts the Sensitivity of Melanopsin Photoreceptors to Polychromatic Lights

Author

Luc J. M. Schlangen, Jazi al Enezi, Timothy M. Brown, Jonathan Wynne, Robert J. Lucas, and Victoria L. Revell

Subjects

Melanopsin, Mice, Inbred C3H, Light, genetic structures, Physiology, business.industry, Mammalian retina, Intrinsically photosensitive retinal ganglion cells, Rod Opsins, Biology, Mice, Optics, Physiology (medical), Biophysics, Animals, Photopigment, sense organs, business, Photoreceptor Cells, Vertebrate

Abstract

Photoreception in the mammalian retina is not restricted to rods and cones but extends to a small number of intrinsically photosensitive retinal ganglion cells expressing the photopigment melanopsin. These mRGCs are especially important contributors to circadian entrainment, the pupil light reflex, and other so-called nonimage-forming (NIF) responses. The spectral sensitivity of melanopsin phototransduction has been addressed in several species by comparing responses to a range of monochromatic stimuli. The resultant action spectra match the predicted profile of an opsin:vitamin A–based photopigment (nomogram) with a peak sensitivity (λmax) around 480 nm. It would be most useful to be able to use this spectral sensitivity function to predict melanopsin’s sensitivity to broad-spectrum, including “white,” lights. However, evidence that melanopsin is a bistable pigment with an intrinsic light-dependent bleach recovery mechanism raises the possibility of a more complex relationship between spectral quality and photoreceptor response. Here, we set out to empirically determine whether simply weighting optical power at each wavelength according to the 480-nm nomogram and integrating across the spectrum could predict melanopsin sensitivity to a variety of polychromatic stimuli. We show that pupillomotor and circadian responses of mice relying solely on melanopsin for their photosensitivity ( rd/rd cl) can indeed be accurately predicted using this methodology. Our data therefore suggest that the 480-nm nomogram may be employed as the basis for a new photometric measure of light intensity (which we term “melanopic”) relevant for melanopsin photoreception. They further show that measuring light in these terms predicts the melanopsin response to light of divergent spectral composition much more reliably than other methods for quantifying irradiance or illuminance currently in widespread use.

Published

2011

25. Enhancing the Legislative Process: The Value of the Legislative Drafter

Author

Donald L. Revell

Subjects

Value (economics), Legislature, Business, Drafter, Legislative process, Law, Law and economics

Published

2011

26. Position and motions of the S4 helix during opening of the Shaker potassium channel

Author

Kenton J. Swartz and L. Revell Phillips

Subjects

Patch-Clamp Techniques, Physiology, Plane (geometry), Chemistry, Depolarization, Nanotechnology, CHO Cells, Article, Protein Structure, Secondary, Potassium channel, Crystallography, Cricetulus, Membrane, Position (vector), Cricetinae, Helix, Shaker Superfamily of Potassium Channels, Animals, Humans, Shaker, Patch clamp, Ion Channel Gating, Cells, Cultured

Abstract

The four voltage sensors in voltage-gated potassium (Kv) channels activate upon membrane depolarization and open the pore. The location and motion of the voltage-sensing S4 helix during the early activation steps and the final opening transition are unresolved. We studied Zn2+ bridges between two introduced His residues in Shaker Kv channels: one in the R1 position at the outer end of the S4 helix (R362H), and another in the S5 helix of the pore domain (A419H or F416H). Zn2+ bridges readily form between R362H and A419H in open channels after the S4 helix has undergone its final motion. In contrast, a distinct bridge forms between R362H and F416H after early S4 activation, but before the final S4 motion. Both bridges form rapidly, providing constraints on the average position of S4 relative to the pore. These results demonstrate that the outer ends of S4 and S5 remain in close proximity during the final opening transition, with the S4 helix translating a significant distance normal to the membrane plane.

Published

2010

27. PREDICTING HUMAN NOCTURNAL NONVISUAL RESPONSES TO MONOCHROMATIC AND POLYCHROMATIC LIGHT WITH A MELANOPSIN PHOTOSENSITIVITY FUNCTION

Author

Daniel C G Barrett, Luc J. M. Schlangen, Victoria L. Revell, and Debra J. Skene

Subjects

Adult, Male, Melanopsin, medicine.medical_specialty, Adolescent, Light, Physiology, Photic Stimulation, Posture, Stimulus (physiology), Nocturnal, Audiology, Melatonin, Young Adult, Physiology (medical), medicine, Humans, Circadian rhythm, Wakefulness, Lighting, Cross-Over Studies, Light sensitivity, Circadian Rhythm, Affect, Alertness, Psychology, medicine.drug

Abstract

The short-wavelength (blue) light sensitivity of human circadian, neurobehavioral, neuroendocrine, and neurophysiological responses is attributed to melanopsin. Whether melanopsin is the sole factor in determining the efficacy of a polychromatic light source in driving nonvisual responses, however, remains to be established. Monochromatic (λ(max) 437, 479, and 532 nm administered singly and in combination with 479 nm light) and polychromatic (color temperature: 4000 K and 17000 K) light stimuli were photon matched for their predicted ability to stimulate melanopsin, and their capacity to affect nocturnal melatonin levels, auditory reaction time, and subjective alertness and mood was assessed. Young, healthy male participants aged 18-35 yrs (23.6 ± 3.6 yrs [mean ± SD]; n=12) participated in 12 overnight sessions that included an individually timed 30-min nocturnal light stimulus on the rising limb of the melatonin profile. At regular intervals before, during, and after the light stimulus, subjective mood and alertness were verbally assessed, blood samples were taken for analysis of plasma melatonin levels, and an auditory reaction time task (psychomotor vigilance task; PVT) was performed. Proc GLM (general linear model) repeated-measures ANOVA (analysis of variance) revealed significantly lower melatonin suppression with the polychromatic light conditions (4000 and 17000 K) compared to the "melanopsin photon-matched" monochromatic light conditions (p .05). In contrast, subjective alertness was significantly lower under the 479 nm monochromatic light condition compared to the 437 and 532 nm monochromatic and both polychromatic light conditions. The alerting responses more reflected the total photon content of the light stimulus. The demonstration that the melatonin suppression response to polychromatic light was significantly lower than predicted by the melanopsin photosensitivity function suggests this function is not the sole consideration when trying to predict the efficacy of broadband lighting. The different spectral sensitivity of subjective alertness and melatonin suppression responses may imply a differential involvement of the cone photopigments. An analysis of the photon densities in specific wavelength bands for the polychromatic lights used in this and the authors' previous study suggests the spectral composition of a polychromatic light source, and particularly the very short-wavelength content, may be critical in determining response magnitude for the neuroendocrine and neurobehavioral effects of nocturnal light.

Published

2010

28. Impact of age on human non-visual responses to light

Author

Debra J. Skene and Victoria L. Revell

Subjects

medicine.medical_specialty, Neurology, Homeostat, genetic structures, Physiology, Circadian clock, Audiology, Sleep in non-human animals, Developmental psychology, Neuropsychology and Physiological Psychology, Ageing, Physiology (medical), medicine, Free-running sleep, sense organs, Circadian rhythm, Psychology, Blue light

Abstract

Ageing is associated with increased disturbances in the timing, duration, and quality of sleep. These disruptions may reflect changes in the circadian timing system and/or the sleep homeostat which are both necessary to produce consolidated sleep at an appropriate time. In addition, it is possible that age-related alterations in the detection and transmission of the photic signal responsible for synchronizing the circadian clock may play a role. Ageing is accompanied by many changes within the eye including alterations in pupil size, lens transmission, and number of photoreceptors. The observed increase in ocular lens density with age will diminish the transmission of short wavelength blue light to which the circadian system has been shown to be most sensitive, and may contribute, in part, to the observed increase in sleep disturbances in older people. We were the first group to test the hypothesis that non-visual responses to blue light would be impaired in older individuals. Our research has demonstrated that whilst acute non-visual effects of blue light are impaired with age, the light resetting effect appears unaltered. Future research should work towards optimizing the light environment for older people to promote good quality sleep and daytime functioning.

Published

2010

29. AGE-DEPENDENT ALTERATIONS IN HUMANPER2LEVELS AFTER EARLY MORNING BLUE LIGHT EXPOSURE

Author

Sylvie Chappuis, Dirk-Jan Saaltink, Tracey L. Sletten, Urs Albrecht, Christian Cajochen, Debra J. Skene, Victoria L. Revell, and Corinne Jud

Subjects

Adult, Male, Aging, endocrine system, medicine.medical_specialty, Physiology, Photoperiod, Gene Expression, Age dependent, Biology, Young Adult, Rhythm, Circadian regulation, Physiology (medical), Internal medicine, medicine, Humans, Circadian rhythm, Aged, Blue light, Morning, Artificial light, Mouth Mucosa, Period Circadian Proteins, Middle Aged, Circadian Rhythm, PER2, Cheek, Endocrinology, Photic Stimulation

Abstract

In our modern society, we are exposed to different artificial light sources that could potentially lead to disturbances of circadian rhythms and, hence, represent a risk for health and welfare. Investigating the acute impact of light on clock-gene expression may thus help us to better understand the mechanisms underlying disorders rooted in the circadian system. Here, we show an overall significant reduction in PER2 expression in oral mucosa with aging in the morning, noon, and afternoon. In the afternoon, 10 h after exposure to early morning blue light, PER2 was significantly elevated in the young compared to green light exposure and to older participants. Our findings demonstrate that human buccal samples are a valuable tool for studying clock-gene rhythms and the response of PER2 to light. Additionally, our results indicate that the influence of light on clock-gene expression in humans is altered with age.

Published

2009

30. Blue-Light Phase ShiftsPER3Gene Expression in Human Leukocytes

Author

Katrin Ackermann, Tracey L. Sletten, Victoria L. Revell, Simon N. Archer, and Debra J. Skene

Subjects

Adult, Male, medicine.medical_specialty, Light, Physiology, Phase (waves), Stimulus (physiology), Biology, Melatonin, Young Adult, Rhythm, Physiology (medical), Internal medicine, Gene expression, Leukocytes, medicine, Humans, Aged, Blue light, Age Factors, Nuclear Proteins, Period Circadian Proteins, Middle Aged, CLOCK, Kinetics, PER3, Endocrinology, Gene Expression Regulation, Transcription Factors, medicine.drug

Abstract

The timing of clock gene expression in human leukocytes was investigated following a phase-advancing light stimulus to determine whether the response is wavelength- and/or age-dependent. PERIOD3 (PER3) clock gene expression in leukocytes and plasma melatonin were analyzed before and after monochromatic blue and green light exposure. Significant phase advances were observed in the peak timing of both PER3 expression and melatonin following blue but not green light. The amplitude of the PER3 rhythm at baseline was significantly reduced with age. However, age did not affect the response of the PER3 rhythm to light. (Author correspondence: d.skene@surrey.ac.uk)

Published

2009

31. Ecological effects of coastal armoring on sandy beaches

Author

David L. Revell, Iván F. Rodil, Jenifer E. Dugan, David M. Hubbard, and Stephen C. Schroeter

Subjects

Biomass (ecology), Ecology, Intertidal zone, Aquatic Science, Biology, Coastal erosion, Fishery, Seawall, Habitat destruction, Habitat, Abundance (ecology), Species richness, Ecology, Evolution, Behavior and Systematics

Abstract

Use of coastal armoring is expected to escalate in response to the combination of expanding human populations, beach erosion, and sea level rise along the coasts. To provide a conceptual framework, we developed hypotheses concerning the ecological effects of beach habitat loss associated with coastal armoring. As beaches narrow in response to armoring, dry upper intertidal zones should be lost disproportionately, reducing the habitat types available and the diversity and abundance of macroinvertebrates. Predators, such as shorebirds, could respond to a combination of (i) habitat loss; (ii) decreased accessibility at high tides; and (iii) reduced prey availability on armored beaches. To examine those predictions, zone widths and the distribution and abundance of macroinvertebrates and birds were compared on paired armored and unarmored segments of narrow bluff-backed beaches in southern California. Our results supported the predictions and revealed some unexpected effects of armoring on birds. Dry upper beach zones were lacking and mid-beach zones were narrower (>2 times) year-round on armored segments compared to adjacent unarmored segments. The abundance, biomass and size of upper intertidal macroinvertebrates were also significantly lower on armored segments. Shorebirds, most of which were foraging, responded predictably with significantly lower species richness (two times) and abundance (>3 times) on armored segments. Gulls and other birds (including seabirds), which use beaches primarily for roosting, were also significantly lower in abundance (>4 times and >7 times respectively) on armored segments, an important unexpected result. Given the accelerating pressures on sandy beaches from coastal development, erosion and rising sea levels, our results indicate that further investigation of ecological responses to coastal armoring is needed for the management and conservation of these ecosystems.

Published

2008

32. A three pulse phase response curve to three milligrams of melatonin in humans

Author

Charmane I. Eastman, Helen J. Burgess, and Victoria L. Revell

Subjects

photoperiodism, medicine.medical_specialty, Physiology, Pulse (signal processing), business.industry, Placebo, Melatonin, Endocrinology, Internal medicine, medicine, Circadian rhythm, business, Phase response curve, medicine.drug, Morning, Ultradian rhythm

Abstract

Exogenous melatonin is increasingly used for its phase shifting and soporific effects. We generated a three pulse phase response curve (PRC) to exogenous melatonin (3 mg) by administering it to free-running subjects. Young healthy subjects (n = 27) participated in two 5 day laboratory sessions, each preceded by at least a week of habitual, but fixed sleep. Each 5 day laboratory session started and ended with a phase assessment to measure the circadian rhythm of endogenous melatonin in dim light using 30 min saliva samples. In between were three days in an ultradian dim light (< 150 lux)‐dark cycle (LD 2.5 : 1.5) during which each subject took one pill per day at the same clock time (3 mg melatonin or placebo, double blind, counterbalanced). Each individual’s phase shift to exogenous melatonin was corrected by subtracting their phase shift to placebo (a free-run). The resulting PRC has a phase advance portion peaking about 5 h before the dim light melatonin onset, in the afternoon. The phase delay portion peaks about 11 h after the dim light melatonin onset, shortly after the usual time of morning awakening. A dead zone of minimal phase shifts occurred around the first half of habitual sleep. The fitted maximum advance and delay shifts were 1.8 h and 1.3 h, respectively. This new PRC will aid in determining the optimal time to administer exogenous melatonin to achieve desired phase shifts and demonstrates that using exogenous melatonin as a sleep aid at night has minimal phase shifting effects.

Published

2008

33. Sex differences in the circadian profiles of melatonin and cortisol in plasma and urine matrices under constant routine conditions

Author

Pippa J, Gunn, Benita, Middleton, Sarah K, Davies, Victoria L, Revell, and Debra J, Skene

Subjects

Adult, Male, endocrine system, Sex Characteristics, Hydrocortisone, melatonin, Original Articles, cortisol, 6-sulfatoxymelatonin, constant routine, Circadian Rhythm, Young Adult, circadian rhythms, Report, Sex differences, Humans, Female, human, hormones, hormone substitutes, and hormone antagonists

Abstract

Conflicting evidence exists as to whether there are differences between males and females in circadian timing. The aim of the current study was to assess whether sex differences are present in the circadian regulation of melatonin and cortisol in plasma and urine matrices during a constant routine protocol. Thirty-two healthy individuals (16 females taking the oral contraceptive pill (OCP)), aged 23.8 ± 3.7 (mean ± SD) years, participated. Blood (hourly) and urine (4-hourly) samples were collected for measurement of plasma melatonin and cortisol, and urinary 6-sulfatoxymelatonin (aMT6s) and cortisol, respectively. Data from 28 individuals (14 females) showed no significant differences in the timing of plasma and urinary circadian phase markers between sexes. Females, however, exhibited significantly greater levels of plasma melatonin and cortisol than males (AUC melatonin: 937 ± 104 (mean ± SEM) vs. 642 ± 47 pg/ml.h; AUC cortisol: 13581 ± 1313 vs. 7340 ± 368 mmol/L.h). Females also exhibited a significantly higher amplitude rhythm in both hormones (melatonin: 43.8 ± 5.8 vs. 29.9 ± 2.3 pg/ml; cortisol: 241.7 ± 23.1 vs. 161.8 ± 15.9 mmol/L). Males excreted significantly more urinary cortisol than females during the CR (519.5 ± 63.8 vs. 349.2 ± 39.3 mol) but aMT6s levels did not differ between sexes. It was not possible to distinguish whether the elevated plasma melatonin and cortisol levels observed in females resulted from innate sex differences or the OCP affecting the synthetic and metabolic pathways of these hormones. The fact that the sex differences observed in total plasma concentrations for melatonin and cortisol were not reproduced in the urinary markers challenges their use as a proxy for plasma levels in circadian research, especially in OCP users.

Published

2016

34. Dissecting Daily and Circadian Expression Rhythms of Clock-Controlled Genes in Human Blood

Author

Oscar Lao, Debra J. Skene, Karolina Lech, Manfred Kayser, Victoria L. Revell, Katrin Ackermann, Genetic Identification, and University of St Andrews. School of Chemistry

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Physiology, Circadian clock, NDAS, CLOCK Proteins, Endogeny, QH426 Genetics, Biology, Protein Serine-Threonine Kinases, Real-Time Polymerase Chain Reaction, Melatonin, Human blood, 03 medical and health sciences, Young Adult, Internal medicine, Circadian Clocks, Physiology (medical), medicine, Humans, QD, Circadian rhythm, RNA, Messenger, QH426, Clock-controlled genes, Intracellular Signaling Peptides and Proteins, Fasting, Period Circadian Proteins, QD Chemistry, Circadian Rhythm, Sleep deprivation, PER3, 030104 developmental biology, Endocrinology, Constant routine, Gene Expression Regulation, Sleep Deprivation, Female, Gene expression, medicine.symptom, Sleep, medicine.drug, PER1

Abstract

This study was supported in part by the Netherlands Organization for Scientific Research (NWO) Forensic Science Program Grant 27.011.001, the European Union 6th Framework project EUCLOCK (018741), the UK Biotechnology and Biological Sciences Research Council (BBSRC) grant BB/I019405/1, and Erasmus MC University Medical Center Rotterdam. D.J.S. is a Royal Society Wolfson Research Merit Award holder. The identification and investigation of novel clock-controlled genes (CCGs) has been conducted thus far mainly in model organisms such as nocturnal rodents, with limited information in humans. Here, we aimed to characterize daily and circadian expression rhythms of CCGs in human peripheral blood during a sleep/sleep deprivation (S/SD) study and a constant routine (CR) study. Blood expression levels of 9 candidate CCGs (SREBF1, TRIB1, USF1, THRA1, SIRT1, STAT3, CAPRIN1, MKNK2, and ROCK2), were measured across 48 h in 12 participants in the S/SD study and across 33 h in 12 participants in the CR study. Statistically significant rhythms in expression were observed for STAT3, SREBF1, TRIB1, and THRA1 in samples from both the S/SD and the CR studies, indicating that their rhythmicity is driven by the endogenous clock. The MKNK2 gene was significantly rhythmic in the S/SD but not the CR study, which implies its exogenously driven rhythmic expression. In addition, we confirmed the circadian expression of PER1, PER3, and REV-ERBα in the CR study samples, while BMAL1 and HSPA1B were not significantly rhythmic in the CR samples; all 5 genes previously showed significant expression in the S/SD study samples. Overall, our results demonstrate that rhythmic expression patterns of clock and selected clock-controlled genes in human blood cells are in part determined by exogenous factors (sleep and fasting state) and in part by the endogenous circadian timing system. Knowledge of the exogenous and endogenous regulation of gene expression rhythms is needed prior to the selection of potential candidate marker genes for future applications in medical and forensic settings. Postprint

Published

2016

35. A prospective audit of paediatric colonoscopy under general anaesthesia

Author

MD Stringer, A Pinfield, L Revell, P McClean, and JWL Puntis

Subjects

medicine.medical_specialty, medicine.diagnostic_test, business.industry, Prospective audit, General surgery, medicine.medical_treatment, Intravenous sedation, Colonoscopy, General Medicine, Polypectomy, Surgery, Endoscopy, Pediatrics, Perinatology and Child Health, Medicine, General anaesthesia, Complication, business

Abstract

Colonoscopy in children is frequently performed using intravenous sedation. Traditionally, there have been few advocates of general anaesthesia and some have regarded colonoscopy conducted in this way as potentially more hazardous. The aim of this study was to undertake a prospective audit of paediatric colonoscopy carried out under general anaesthesia. The details of all children referred for colonoscopy during a 3.5-y period were collected prospectively and the safety and efficacy of performing colonoscopy under general anaesthesia were analysed. A total of 250 colonoscopies was performed in 215 children of median age 10.7 y (range 5 months to 16y) and ileoscopy was carried out in 164 of these cases. An increasing proportion of patients was investigated as day-cases, including most of the 56 who had additional procedures carried out under the same anaesthetic. There were no complications from the colonoscopy (including the 18 patients who underwent polypectomy). Only one procedure-related complication occurred and this was avoidable. These results confirm the safety of paediatric colonoscopy under general anaesthesia and demonstrate the advantages and feasibility of such an approach.

Published

2007

36. Alerting effects of light are sensitive to very short wavelengths

Author

Josephine Arendt, Debra J. Skene, Louis Fogg, and Victoria L. Revell

Subjects

Adult, Male, Materials science, Light, business.industry, General Neuroscience, Short wavelength sensitive, Acute effect, Melatonin, Affect, Wavelength, Alertness, Spectral sensitivity, Optics, medicine, Humans, Arousal, business, medicine.drug

Abstract

In humans a range of non-image-forming (NIF) light responses (melatonin suppression, phase shifting and alertness) are short wavelength sensitive (440-480 nm). The aim of the current study was to assess the acute effect of three different short wavelength light pulses (420, 440 and 470 nm) and 600 nm light on subjective alertness. Healthy male subjects (n = 12, aged 27 +/- 4 years, mean +/- S.D.) were studied in 39, 4-day laboratory study sessions. The subjects were maintained in dim light (8 lx) and on day 3 they were exposed to a single 4-h light pulse (07:15-11:15 h). Four monochromatic wavelengths were administered at two photon densities: 420 and 440 nm at 2.3 x 10(13)photons/cm(2)/s and 440, 470 and 600 nm at 6.2 x 10(13)photons/cm(2)/s. Subjective mood and alertness were assessed at 30 min intervals during the light exposure, using four 9-point VAS scales. Mixed model regression analysis was used to compare alertness and mood ratings during the 470 nm light to those recorded with the other four light conditions. There was a significant effect of duration of light exposure (p0.001) on alertness but no significant effect of subject. Compared to 470 nm light, alertness levels were significantly higher in 420 nm light and significantly lower in the 600 nm light (p0.05). These data (420 nm470 nm600 nm) suggest that subjective alertness may be maximally sensitive to very short wavelength light.

Published

2006

37. Advancing Human Circadian Rhythms with Afternoon Melatonin and Morning Intermittent Bright Light

Author

Victoria L. Revell, Charmane I. Eastman, Helen J. Burgess, Louis Fogg, Mark R. Smith, and Clifford J. Gazda

Subjects

Adult, Male, medicine.medical_specialty, Light, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Circadian clock, Context (language use), Biochemistry, Antioxidants, Article, Melatonin, Endocrinology, Circadian regulation, Surveys and Questionnaires, Internal medicine, medicine, Humans, Circadian rhythm, Morning, Jet Lag Syndrome, business.industry, Biochemistry (medical), Wake time, Middle Aged, Circadian Rhythm, Patient Compliance, Female, Sleep, business, Bright light, medicine.drug

Abstract

Both light and melatonin can be used to phase shift the human circadian clock, but the phase-advancing effect of the combination has not been extensively investigated.The objective of the study was to determine whether phase advances induced by morning intermittent bright light and a gradually advancing sleep schedule could be increased with afternoon melatonin.Healthy adults (25 males, 19 females, between the ages of 19 and 45 yr) participated in the study.There were 3 d of a gradually advancing sleep/dark period (wake time 1 h earlier each morning), bright light on awakening [four 30-min bright-light pulses (approximately 5000 lux) alternating with 30 min room light60 lux] and afternoon melatonin, either 0.5 or 3.0 mg melatonin timed to induce maximal phase advances, or matching placebo. The dim light melatonin onset was measured before and after the treatment to determine the phase advance.There were significantly larger phase advances with 0.5 mg (2.5 h, n = 16) and 3.0 mg melatonin (2.6 h, n = 13), compared with placebo (1.7 h, n = 15), but there was no difference between the two melatonin doses. Subjects did not experience jet lag-type symptoms during the 3-d treatmentAfternoon melatonin, morning intermittent bright light, and a gradually advancing sleep schedule advanced circadian rhythms almost 1 h/d and thus produced very little circadian misalignment. This treatment could be used in any situation in which people need to phase advance their circadian clock, such as before eastward jet travel or for delayed sleep phase syndrome.

Published

2006

38. How to Trick Mother Nature into Letting You Fly Around or Stay Up All Night

Author

Victoria L. Revell and Charmane I. Eastman

Subjects

0301 basic medicine, Light, Physiology, Article, Shift work, Melatonin, 03 medical and health sciences, 0302 clinical medicine, Optics, Work Schedule Tolerance, Physiology (medical), medicine, Zeitgeber, Animals, Humans, Circadian rhythm, Phase response curve, Jet Lag Syndrome, business.industry, Darkness, Circadian Rhythm, 030104 developmental biology, Aviation, Entrainment (chronobiology), Psychology, business, 030217 neurology & neurosurgery, medicine.drug, Cognitive psychology

Abstract

Night shift work and rapid transmeridian travel result in a misalignment between circadian rhythms and the new times for sleep, wake, and work, which has health and safety implications for both the individual involved and the general public. Entrainment to the new sleep/wake schedule requires circadian rhythms to be phase-shifted, but this is often slow or impeded. The authors show superimposed light and melatonin PRCs to explain how to appropriately time these zeitgebers to promote circadian adaptation. They review studies in which bright light and melatonin were administered to try to counteract jet lag or to produce circadian adaptation to night work. They demonstrate how jet lag could be prevented entirely if rhythms are shifted before the flight using their preflight plan and discuss the combination of interventions that they now recommend for night shift workers.

Published

2005

39. Voltage-sensor activation with a tarantula toxin as cargo

Author

Jae I. I. Kim, Joseph A. Mindell, Kenton J. Swartz, Yingying Li-Smerin, Mirela Milescu, and L. Revell Phillips

Subjects

Tarantula, Multidisciplinary, biology, Stereochemistry, Chemistry, Toxin, Bilayer, Lipid Bilayers, Kinetics, Spider Venoms, Spiders, biology.organism_classification, medicine.disease_cause, Membrane, Amino Acid Substitution, Potassium Channels, Voltage-Gated, Voltage sensor, medicine, Biophysics, Animals, Hanatoxin, Peptides, Lipid bilayer, Ion Channel Gating

Abstract

The opening and closing of voltage-activated Na+, Ca2+ and K+ (Kv) channels underlies electrical and chemical signalling throughout biology, yet the structural basis of voltage sensing is unknown. Hanatoxin is a tarantula toxin that inhibits Kv channels by binding to voltage-sensor paddles, crucial helix-turn-helix motifs within the voltage-sensing domains that are composed of S3b and S4 helices. The active surface of the toxin is amphipathic, and related toxins have been shown to partition into membranes, raising the possibility that the toxin is concentrated in the membrane and interacts only weakly and transiently with the voltage sensors. Here we examine the kinetics and state dependence of the toxin-channel interaction and the physical location of the toxin in the membrane. We find that hanatoxin forms a strong and stable complex with the voltage sensors, far outlasting fluctuations of the voltage sensors between resting (closed) conformations at negative voltages and activated (open) conformations at positive voltages. Toxin affinity is reduced by voltage-sensor activation, explaining why the toxin stabilizes the resting conformation. We also find that when hanatoxin partitions into membranes it is localized to an interfacial region, with Trp 30 positioned about 8.5 A from the centre of the bilayer. These results demonstrate that voltage-sensor paddles activate with a toxin as cargo, and suggest that the paddles traverse no more than the outer half of the bilayer during activation.

Published

2005

40. Circadian phase determined from melatonin profiles is reproducible after 1 wk in subjects who sleep later on weekends

Author

Christine Y. Tseng, Victoria L. Revell, Hyungsoo Kim, Charmane I. Eastman, and Stephanie J. Crowley

Subjects

medicine.medical_specialty, Circadian phase, business.industry, Nap, Melatonin, Endocrinology, Anesthesia, Internal medicine, Medicine, Absolute Change, Sleep (system call), Circadian rhythm, business, Salivary melatonin, Morning, medicine.drug

Abstract

The aim of this study was to determine whether circadian phase from salivary melatonin profiles is the same when measured in phase assessments 1 wk apart. Eleven healthy young men and women maintained a fixed, home sleep-wake schedule, in bed, in the dark 23:00-07:00 hr on weekdays. On Friday and Saturday nights they were permitted to wake up and go to bed up to 1 hr later, and on Saturdays and Sundays they could nap between 13:30 and 16:30 hr. The study was run in the summer. Subjects wore sunglasses when outside during the day, and went outside for at least 15 min between 08:00 and 09:00 hr each morning. They maintained this schedule for 15 days before the first assessment and the 6 days in between the two assessments. During the assessments subjects remained awake overnight in

Published

2005

41. Molecular Basis of Inward Rectification

Author

Harley T. Kurata, Hariolf Fritzenschaft, Thierry Rose, Decha Enkvetchakul, Thomas Baukrowitz, L. Revell Phillips, Gildas Loussouarn, Stefan Herlitze, and Colin G. Nichols

Subjects

Membrane potential, 0303 health sciences, Physiology, Chemistry, Stereochemistry, Ligand, Mutagenesis, Spermine, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Rectification, Cytoplasm, Biophysics, Structure–activity relationship, Polyamine, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Polyamines cause inward rectification of (Kir) K+ channels, but the mechanism is controversial. We employed scanning mutagenesis of Kir6.2, and a structural series of blocking diamines, to combinatorially examine the role of both channel and blocker charges. We find that introduced glutamates at any pore-facing residue in the inner cavity, up to and including the entrance to the selectivity filter, can confer strong rectification. As these negative charges are moved higher (toward the selectivity filter), or lower (toward the cytoplasm), they preferentially enhance the potency of block by shorter, or longer, diamines, respectively. MTSEA+ modification of engineered cysteines in the inner cavity reduces rectification, but modification below the inner cavity slows spermine entry and exit, without changing steady-state rectification. The data provide a coherent explanation of classical strong rectification as the result of polyamine block in the inner cavity and selectivity filter.

Published

2004

42. Ligand-induced Closure of Inward Rectifier Kir6.2 Channels Traps Spermine in the Pore

Author

Colin G. Nichols and L. Revell Phillips

Subjects

Helix bundle, spermine, Voltage-gated ion channel, Physiology, Inward-rectifier potassium ion channel, Stereochemistry, Chemistry, Kinetics, Spermine, Cardiac action potential, Gating, Kir6.2, Ligands, inward rectifier, Article, ATP, chemistry.chemical_compound, K channel, COS Cells, Chlorocebus aethiops, gating, Biophysics, Animals, Potassium Channels, Inwardly Rectifying, Ion Channel Gating

Abstract

Small organic amines block open voltage-gated K+ channels and can be trapped by subsequent closure. Such studies provide strong evidence for voltage gating occurring at the intracellular end of the channel. We engineered the necessary properties (long block times with unblock kinetics comparable to, or slower than, the kinetics of gating) into spermine-blocked, ATP-gated (N160D,L157C) mutant KATP channels, in order to test the possibility of “blocker trapping” in ligand-gated Kir channels. Spermine block of these channels is very strongly voltage dependent, such that, at positive voltages, the off-rate of spermine is very low. A brief pulse to negative voltages rapidly relieves the block, but no such relief is observed in ATP-closed channels. The results are well fit by a simple kinetic model that assumes no spermine exit from closed channels. The results incontrovertibly demonstrate that spermine is trapped in channels that are closed by ATP, and implicate the M2 helix bundle crossing, or somewhere lower, as the probable location of the gate.

Published

2003

43. Erratum to: investigation of metabolites for estimating blood deposition time

Author

Roelof A. Hut, Joo Ern Ang, Benita Middleton, Sarah K. Davies, Debra J. Skene, Victoria L. Revell, Karolina Lech, Manfred Kayser, Katrin Ackermann, Florence I. Raynaud, I. Hoveijn, and Fan Liu

Subjects

Male, Time Factors, Published Erratum, Hydrocortisone, Intracellular Signaling Peptides and Proteins, Forensic Medicine, Protein Serine-Threonine Kinases, Pathology and Forensic Medicine, Blood, Logistic Models, Environmental chemistry, Metabolome, Humans, Metabolomics, Environmental science, RNA, Messenger, Erratum, Deposition (chemistry), Biomarkers, Melatonin

Abstract

Trace deposition timing reflects a novel concept in forensic molecular biology involving the use of rhythmic biomarkers for estimating the time within a 24-h day/night cycle a human biological sample was left at the crime scene, which in principle allows verifying a sample donor's alibi. Previously, we introduced two circadian hormones for trace deposition timing and recently demonstrated that messenger RNA (mRNA) biomarkers significantly improve time prediction accuracy. Here, we investigate the suitability of metabolites measured using a targeted metabolomics approach, for trace deposition timing. Analysis of 171 plasma metabolites collected around the clock at 2-h intervals for 36 h from 12 male participants under controlled laboratory conditions identified 56 metabolites showing statistically significant oscillations, with peak times falling into three day/night time categories: morning/noon, afternoon/evening and night/early morning. Time prediction modelling identified 10 independently contributing metabolite biomarkers, which together achieved prediction accuracies expressed as AUC of 0.81, 0.86 and 0.90 for these three time categories respectively. Combining metabolites with previously established hormone and mRNA biomarkers in time prediction modelling resulted in an improved prediction accuracy reaching AUCs of 0.85, 0.89 and 0.96 respectively. The additional impact of metabolite biomarkers, however, was rather minor as the previously established model with melatonin, cortisol and three mRNA biomarkers achieved AUC values of 0.88, 0.88 and 0.95 for the same three time categories respectively. Nevertheless, the selected metabolites could become practically useful in scenarios where RNA marker information is unavailable such as due to RNA degradation. This is the first metabolomics study investigating circulating metabolites for trace deposition timing, and more work is needed to fully establish their usefulness for this forensic purpose.

Published

2017

44. Assessing the suitability of miRNA-142-5p and miRNA-541 for bloodstain deposition timing

Author

Karolina Lech, Manfred Kayser, Debra J. Skene, Katrin Ackermann, Andreas Wollstein, Victoria L. Revell, and Genetic Identification

Subjects

Forensic Genetics, Genetic Markers, Future studies, Reverse Transcriptase Polymerase Chain Reaction, Physiology, Venous blood, Biology, Pathology and Forensic Medicine, Time of death, MicroRNAs, Expression pattern, microRNA, Genetics, Analysis of variance, Circadian rhythm, Deposition (chemistry)

Abstract

A recent proof-of-concept pilot study proposed using microRNA (miRNA) markers for time of death determination. The markers - miRNA-142-5p and miRNA-541, were reported to show considerable expression differences in vitreous humor between individuals who died during the day or night. Here, we investigated whether these miRNA markers show the same diurnal expression pattern in blood, which would make them useful for estimating bloodstain deposition time to allow molecular alibi testing for forensic casework. We analyzed venous blood samples collected from 12 healthy individuals every 4 h during the 24 h day/night period under controlled sleep-laboratory conditions. MiRNA-142-5p normalized against miRNA-222 showed no statistically significant expression differences between blood samples collected during daytime and nighttime (one-way ANOVA p = 0.81), and also no statistically significant rhythmicity during the 24 h day/night period (cosine fit for all individuals p > 0.05, averaged data p = 0.932). MicroRNA-541 amplification in blood was above the 34-cycle threshold applied in the study, indicating too low quantities for obtaining reliable data. Overall, we conclude that the two miRNA markers previously suggested for time of death determination in vitreous humor are not suitable for estimating the deposition time of forensic bloodstains. Future studies may find out if miRNA markers with significant diurnal expression patterns can be identified and how useful they would be for forensic trace deposition timing. (C) 2014 Elsevier Ireland Ltd. All rights reserved.

Published

2014

45. Flexibility of the Kir6.2 inward rectifier K + channel pore

Author

Colin G. Nichols, Ricard Masia, Thierry Rose, L. Revell Phillips, and Gildas Loussouarn

Subjects

Models, Molecular, Potassium Channels, Protein Conformation, Stereochemistry, Dimer, Molecular Sequence Data, KcsA potassium channel, Crystal structure, Models, Biological, chemistry.chemical_compound, Protein structure, Potassium Channel Blockers, Animals, Point Mutation, Amino Acid Sequence, Cysteine, Potassium Channels, Inwardly Rectifying, Pliability, Mesylates, Multidisciplinary, Sequence Homology, Amino Acid, Chemistry, Inward-rectifier potassium ion channel, Kir6.2, Biological Sciences, Methyl Methanesulfonate, Potassium channel, Quaternary Ammonium Compounds, Ethyl Methanesulfonate, COS Cells, Helix, Indicators and Reagents, Dimerization, Cadmium

Abstract

Interactions of sulfhydryl reagents with introduced cysteines in the pore-forming (Kir6.2) subunits of the K ATP channel were examined. 2-Aminoethyl methanethiosulfonate (MTSEA + ) failed to modify Cd 2+ -insensitive control-Kir6.2 channels, but rapidly and irreversibly modified Kir6.2[L164C] (L164C) channels. Although a single Cd 2+ ion is coordinated by L164C, four MTSEA + “hits” can occur, each sequentially reducing the single-channel current. A dimeric fusion of control-Kir6.2 and L164C subunits generates Cd 2+ -insensitive channels, confirming that at least three cysteines are required for coordination, but MTSEA + modification of the dimer occurs in two hits. L164C channels were not modified by bromotrimethyl ammoniumbimane (qBBr + ), even though qBBr + caused voltage-dependent block (as opposed to modification) that was comparable to that of MTSEA + or 3-(triethylammonium)propyl methanethiosulfonate (MTSPTrEA + ), implying that qBBr + can also enter the inner cavity but does not modify L164C residues. The Kir channel pore structure was modeled by homology with the KcsA crystal structure. A stable conformation optimally places the four L164C side chains for coordination of a single Cd 2+ ion. Modification of these cysteines by up to four MTSEA + (or three MTSPTrEA + , or two qBBr + ) does not require widening of the cavity to accommodate the derivatives within it. However, like the KcsA crystal structure, the energy-minimized model shows a narrowing at the inner entrance, and in the Kir6.2 model this narrowing excludes all ions. To allow entry of ions as large as MTSPTrEA + or qBBr + , the entrance must widen to >8 Å, but this widening is readily accomplished by minimal M2 helix motion and side-chain rearrangement.

Published

2001

46. Book Review: The Acts of Paul: A New Translation with Introduction and Commentary

Author

Roger L. Revell

Subjects

Literature, business.industry, Philosophy, SAINT, Christianity, Romance, Apostle, General Earth and Planetary Sciences, Narrative, Erudition, business, Gnosticism, Value (semiotics), General Environmental Science

Abstract

The Acts of Paul: A New Translation with Introduction and Commentary. By Richard I. Pervo. Eugene, Ore.: Cascade Books, 2014. xvii + 376 pp. $45.00 (paper).With his characteristic erudition, Richard Pervo's fresh translation and commentary on the pseudoepigraphic Acts of Paul offers an engaging and well-examined treatment of this apocryphal text. His project is accessible not only to seasoned students of the Apocryphal Acts of the Apostles (ApocActs), but also to those who are novices. Within this collection, the Acts of Paul is one of five surviving narratives that traces the ministry and martyrdom of the apostolic missionaries.The project begins with a complete translation-some surviving segments are quite fragmentary!-of the Acts. The text dates to the latter part of the second century. Paul's Acts, on account of its doctrinal outlook, was more widely accepted in early catholic circles than other texts from the ApocActs.Following the translation, Pervo provides an illuminating survey of the Acts' usage in Christian histoiy. He indexes its secondary attestations and reception in a variety of ancient sources. While some, like Tertullian, condemned the Acts, others, such as Eusebius, maintained a higher estimation of this non-canonical account. A list of reconstructive sources, a discussion of genre, and a survey of editorial theories is also provided. Of particular interest is Pervo s discussion of the book's theology. Here, he highlights both its non-Nicene tenor and its polemical interface with Gnosticism. Further to this, he stresses the text's value as a window into "ordinary Christianity in Asia" (p. 71) during the closing decades of the second century. Major themes of Christianity surface time and again, but not in a systematic manner.The ensuing commentary amply substantiates all of these broad observations. As Pervo strolls through the text, a series of insights on its history, canonical echoes, and cultural influences are published. Consider two representative examples.Chapters 3 and 4 introduce the Thecla narrative. Drawing on a freestanding account, the author incorporates this vignette into Paul's Acts so as to link this beloved female saint with the apostle. Amid this rendition, Pervo discerns a parallel with the popular Greek "romantic novels" (p. 94) extant at this moment in history. These stories relished love at first sight. In like manner, from the moment she hears his voice, Thecla is transfixed with Paul. Her devotion is not romantic, but it is rapt. …

Published

2015

47. Bilingual Legislation: The Ontario Experience

Author

Donald L. Revell

Subjects

Law, Political science, Media studies, Legislation

Published

1998

48. Short-Wavelength Sensitivity of the Human Circadian System to Phase-Advancing Light

Author

Josephine Arendt, Victoria L. Revell, Debra J. Skene, and Michael Terman

Subjects

Adult, Male, 0301 basic medicine, Photons, Light, Physiology, Extramural, Phase (waves), Biology, Circadian Rhythm, Melatonin, 03 medical and health sciences, Wavelength, 030104 developmental biology, 0302 clinical medicine, Physiology (medical), Biophysics, medicine, Humans, Circadian rhythm, Sensitivity (control systems), 030217 neurology & neurosurgery, medicine.drug

Published

2005

49. Human phase response curve to intermittent blue light using a commercially available device

Author

Victoria L, Revell, Thomas A, Molina, and Charmane I, Eastman

Subjects

Adult, Male, Young Adult, Adolescent, Light, Circadian Clocks, Humans, Neuroscience: Behavioural/Systems/Cognitive, Female, Saliva, Melatonin

Abstract

Light shifts the timing of the circadian clock according to a phase response curve (PRC). To date, all human light PRCs have been to long durations of bright white light. However, melanopsin, the primary photopigment for the circadian system, is most sensitive to short wavelength blue light. Therefore, to optimise light treatment it is important to generate a blue light PRC.We used a small, commercially available blue LED light box, screen size 11.2 × 6.6 cm at ∼50 cm, ∼200 μW cm(−2), ∼185 lux. Subjects participated in two 5 day laboratory sessions 1 week apart. Each session consisted of circadian phase assessments to obtain melatonin profiles before and after 3 days of free-running through an ultradian light–dark cycle (2.5 h wake in dim light, 1.5 h sleep in the dark), forced desynchrony protocol. During one session subjects received intermittent blue light (three 30 min pulses over 2 h) once a day for the 3 days of free-running, and in the other session (control) they remained in dim room light, counterbalanced. The time of blue light was varied among subjects to cover the entire 24 h day. For each individual, the phase shift to blue light was corrected for the free-run determined during the control session. The blue light PRC had a broad advance region starting in the morning and extending through the afternoon. The delay region started a few hours before bedtime and extended through the night. This is the first PRC to be constructed to blue light and to a stimulus that could be used in the real world.

Published

2012

50. Diurnal rhythms in blood cell populations and the effect of acute sleep deprivation in healthy young men

Author

Elwin J. C. Rombouts, Manfred Kayser, Debra J. Skene, Victoria L. Revell, Katrin Ackermann, Oscar Lao, and Genetic Identification

Subjects

Adult, Male, medicine.medical_specialty, Blood cell, Leukocyte Count, Young Adult, Rhythm, Immune system, Physiology (medical), Internal medicine, medicine, Leukocytes, Humans, Circadian rhythm, Lymphocyte Count, Young adult, business.industry, biochemical phenomena, metabolism, and nutrition, Flow Cytometry, Sleep in non-human animals, Diurnal rhythms, CD4 Lymphocyte Count, Circadian Rhythm, Sleep deprivation, Endocrinology, medicine.anatomical_structure, Commentary, Sleep Deprivation, Neurology (clinical), medicine.symptom, business, Granulocytes

Abstract

The sleep/wake cycle is accompanied by changes in circulating numbers of immune cells. The goal of this study was to provide an in-depth characterization of diurnal rhythms in different blood cell populations and to investigate the effect of acute sleep deprivation on the immune system, as an indicator of the body's acute stress response.Observational within-subject design.Home environment and Clinical Research Centre.15 healthy male participants aged 23.7 ± 5.4 (standard deviation) yr.Total sleep deprivation.Diurnal rhythms of several blood cell populations were assessed under a normal sleep/wake cycle followed by 29 hr of extended wakefulness. The effect of condition (sleep versus sleep deprivation) on peak time and amplitude was investigated. Interindividual variation of, and the level of correlation between, the different cell populations was assessed. Comprehensive nonlinear curve fitting showed significant diurnal rhythms for all blood cell types investigated, with CD4 (naïve) cells exhibiting the most robust rhythms independent of condition. For those participants exhibiting significant diurnal rhythms in blood cell populations, only the amplitude of the granulocyte rhythm was significantly reduced by sleep deprivation. Granulocytes were the most diverse population, being most strongly affected by condition, and showed the lowest correlations with any other given cell type while exhibiting the largest interindividual variation in abundance.Granulocyte levels and diurnal rhythmicity are directly affected by acute sleep deprivation; these changes mirror the body's immediate immune response upon exposure to stress.

Published

2012