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19 results on '"Luke, Thomas"'

4. Sulfidation and Reoxidation of U(VI)-Incorporated Goethite: Implications for U Retention during Sub-Surface Redox Cycling

Author

Stagg, Olwen, Morris, Katherine, Townsend, Luke Thomas, Kvashnina, Kristina O., Baker, Michael L., Dempsey, Ryan L., Abrahamsen-Mills, Liam, and Shaw, Samuel

Abstract

Over 60 years of nuclear activity have resulted in a global legacy of contaminated land and radioactive waste. Uranium (U) is a significant component of this legacy and is present in radioactive wastes and at many contaminated sites. U-incorporated iron (oxyhydr)oxides may provide a long-term barrier to U migration in the environment. However, reductive dissolution of iron (oxyhydr)oxides can occur on reaction with aqueous sulfide (sulfidation), a common environmental species, due to the microbial reduction of sulfate. In this work, U(VI)–goethite was initially reacted with aqueous sulfide, followed by a reoxidation reaction, to further understand the long-term fate of U species under fluctuating environmental conditions. Over the first day of sulfidation, a transient release of aqueous U was observed, likely due to intermediate uranyl(VI)–persulfide species. Despite this, overall U was retained in the solid phase, with the formation of nanocrystalline U(IV)O2in the sulfidized system along with a persistent U(V) component. On reoxidation, U was associated with an iron (oxyhydr)oxide phase either as an adsorbed uranyl (approximately 65%) or an incorporated U (35%) species. These findings support the overarching concept of iron (oxyhydr)oxides acting as a barrier to U migration in the environment, even under fluctuating redox conditions.

Published
2022
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6. Social media influencers, YouTube & performance and image enhancing drugs: A narrative-typology.

Author

Cox, Luke Thomas Joseph and Paoli, Letizia

Abstract

The health and fitness industry has witnessed a rise of influencers on social media promoting a myriad of brands and products, including some promoting anabolic steroids and other performance and image enhancing drugs (PIEDs). It is currently unclear, however, what type of information and advice social media influencers distribute. This study aims to examine the narratives of social media influencers who discuss PIEDs. The study identified 20 influencers specialized in PIEDs and then made a content analysis of the videos they posted on YouTube. While we find several similarities in influencers' narratives, we also categorize them in three distinct categories: (1) narratives primarily relying on scientific literature and discussing 'usual' bodybuilders' products and doses; (2) narratives primarily relying on the influencers' personal experience and discussing 'usual' bodybuilders products and doses; and (3) narratives primarily relying on the influencers' personal experience and discussing experimental products and 'unusual' doses. The narrative-typology should be used as a means of identifying high-risk videos on social media platforms like YouTube. Policy-makers should do more to challenge high-risk and potentially harmful discussions. Conversely, reliable discussions ought to be made more visible to ensure they are not overshadowed by flashier and riskier narratives. [ABSTRACT FROM AUTHOR]

Published
2023
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7. Why size matters; rugby union and doping.

Author

Cox, Luke Thomas Joseph, McNamee, Mike, Petróczi, Andrea, and Bloodworth, Andrew

Abstract

• Welsh Rugby Union players perceive size and muscularity are important. • Perceptions stem from performance related and societal factors. • Some athletes use doping substances to fulfil these perceived demands. • Acknowledgment of these factors should inform future Anti-Doping education. • The health of recreational athletes should be a primary focus. • Traditional understandings of doping ought to be re-evaluated. Rugby Union is a sport where physical attributes such as strength, speed and power, are highly desirable. To this end, there have been suggestions that rugby players might use doping substances to fulfil these said demands. The present study comprises interviews with thirteen doped recreational Welsh Rugby Union players. The study examined: (i) perceived physical demands of rugby; (ii) motivations to lift weights and follow specific diets; and (iii) the motivating factors to use nutritional and doping substances. Participants detail novel insight into doping within recreational Welsh rugby and reaffirm the perception that size matters. Specific factors such as coach reinforcement, age group categories and level of competition, contribute to this perception. Notably, however, participants use/d doping substances for multiple reasons that were context-sensitive, each carrying different weight and influenced by temporal and developmental dimensions. Importantly, most players also referred to factors outside of rugby participation. These findings have important implications for the Welsh Rugby Union and National Anti-Doping Organisations. We recommend that the Welsh Rugby Union target these potentially doping-inducing perceptions, offering more non-elite focused education for both athletes and coaches, with a focus on safe and healthy weight and size gaining practices. [ABSTRACT FROM AUTHOR]

Published
2023
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8. Immune plasma for the treatment of severe influenza: an open-label, multicentre, phase 2 randomised study

Author

Beigel, John H, Tebas, Pablo, Elie-Turenne, Marie-Carmelle, Bajwa, Ednan, Bell, Todd E, Cairns, Charles B, Shoham, Shmuel, Deville, Jaime G, Feucht, Eric, Feinberg, Judith, Luke, Thomas, Raviprakash, Kanakatte, Danko, Janine, O'Neil, Dorothy, Metcalf, Julia A, King, Karen, Burgess, Timothy H, Aga, Evgenia, Lane, H Clifford, Hughes, Michael D, Davey, Richard T, Tebas, Pablo, Quinn, Joseph, Jiang, Yan, Elie-Turenne, Marie-Carmelle, Hoelle, Robyn, Iovine, Nicole, Wills, Robert Shawn, Pata, Socorro, Huggins, Monique, Manukian, Belinda, Bajwa, Ednan, Holland, Carrie, Brait, Kelsey, Hunt, Taylor, Stowell, Christopher, Slater, Amy, Bell, Todd E, Townsends, Mary, Cairns, Charles B, Quackenbush, Eugenia B, Park, Yara A, Jordan, Paul Gaither, Blanchet, Cherie, Chronowski, Kevin, Alvarez, Kathleen, Shoham, Shmuel, Ostrander, Darin, Woessner, Terry, Thoman, Sandra, Deville, Jaime G, Lin, James, Ziman, Alyssa, Shankar, Kavita, Feucht, Eric, Blok, Tom, Batts, Don, Beck, Bob, Massey, Gail, Bradley, Carol, Feinberg, Judith, Carey, Patricia, Baer, Jenifer, Whitehead, Eva Moore, Kohrs, Sharon, Giulitto, Robert, Schofield, Christina, Fairchok, Mary, Chambers, Susan, Baker, Cindy, RN, Parker, Michelle, Harshbarger, Marta, Nguyen, M Hong, Carey, Mary Ellen, Paronish, Julie, Cornell, Frank, Cramer, Jim, Pakstis, Diana Lynn, Ison, Michael G, Wunderink, Richard, Glesby, Marshall, Ham, Kirsis, Hughes, Valery, Cushing, Melissa, Goss, Cheryl, Grenade, Joanne, Park, Pauline K, Napolitano, Lena M, Raghavendran, Krishnan, Hyzy, Robert C, Davenport, Robertson, Brierley, Kristin, Downs, Theresa, Gong, Michelle Ng, Uehlinger, Joan, Lin, Michael, Fritsche, Janice, Green, Tondria, McLeod, Bruce, Patel, Deena, Bavaro, Mary F, Deiss, Robert, Brandt, Carolyn, Cammarata, Stephanie, Kremp, Allan, Hollis-Perry, Karine, Lalani, Tahaniyat, Banks, Susan, Johnson, Jacqueline, Maguire, Jason, McNiff, Janet, Rigg, Leslie E, Ganesan, Anuradha, Barahona, Irma, Danko, Janine, Spencer, Steven, Stagliano, David, Burgess, Timothy, Talmor, Daniel, Mohammed, Monique, Banner-Goodspeed, Valerie, Salata, Robert, Finberg, Robert, Wang, Jennifer, Longtine, Karen, Longtine, Jaclyn, O'Neil, Mellissa, Bauer, Philippe R, Gajic, Ognjen, Weist, Suanne M, Sevransky, Jonathan, Brown, Mona, Roback, John, Oropello, John, Twohig, Bridget, Jhang, Jeffrey, Seethala, Rahgu, Chen, Wilbur H, Fontaine, Magali, Saharia, Kapil, Husson, Jennifer, DeBiasi, Roberta, Wilson, Jurran L, Criss, Valli Ree, Voell, Jocelyn, Leitman, Susan, Atkins, James Wade, Patel, Hemaxi, Paige, Traci, Cantilena, Cathy, Siegel, Donald, DeMuth, Faye, Fletcher, Craig H, Pelletier, J Peter R, Alnuaimat, Hassan, and Pourde, Michelle

Abstract

Influenza causes substantial morbidity and mortality despite available treatments. Anecdotal reports suggest that plasma with high antibody titres to influenza might be of benefit in the treatment of severe influenza.

Published
2017
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9. Doping in recreational Welsh Rugby Union; Athletes' beliefs and perceptions related to Anti-Doping policy and practice.

Author

Cox, Luke Thomas Joseph, Bloodworth, Andrew, and McNamee, Mike

Abstract

Understanding the attitudes and dispositions of athletes towards doping has been the subject of increasing research. Few studies, however, manage to capture these attitudes and dispositions from athletes who have committed anti-doping rule violations. According to UK Anti-Doping (2020) data, 10% of all sanctioned athletes came from recreational levels of Welsh rugby union. Although there are significant doping concerns within Welsh rugby, no research investigations exist that examine this specific population. Uniquely, the present research sheds light on "doped" athletes within recreational Welsh rugby union. Semi-structured interviews were conducted with (n = 13) "doped" recreational Welsh rugby players. Interviews revealed a wide range of factors, including motivations for doping, drug use patterns, perceived harms and athletes' experiences and perceptions of Anti-Doping Policy and practice. This study focuses on interviews where participants reveal a substantial disregard of Anti-Doping policy and practice and concerns surface across three main themes: (1) perceived lack of frequency related to doping control tests; (2) perceived lack of testing efficacy; and (3) advanced warning of doping controls by coaches. Not only does this data raise serious concerns for the integrity of sport at recreational levels, but it also challenges the discourses around perceived legitimacy of anti-doping therein. • Welsh rugby players perceived there to be a lack of doping control tests;. • Welsh rugby players perceived doping controls to lack efficacy;. • Welsh rugby players received advanced notice of doping controls by coaches. • This data raises serious concerns for the integrity of sport. [ABSTRACT FROM AUTHOR]

Published
2022
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11. Dengue virus photo-inactivated in presence of 1,5-iodonaphthylazide (INA) or AMT, a psoralen compound (4′-aminomethyl-trioxsalen) is highly immunogenic in mice

Author

Raviprakash, Kanakatte, Sun, Peifang, Raviv, Yossef, Luke, Thomas, Martin, Nicholas, and Kochel, Tadeusz

Abstract

Two novel methods of dengue virus inactivation using iodonaphthyl azide (INA) and aminomethyl trioxsalen (AMT) were compared with traditional virus inactivation by formaldehyde. The AMT inactivated dengue-2 virus retained its binding to a panel of 5 monoclonal antibodies specific for dengue-2 envelope protein, whereas inactivation by formaldehyde and INA led to 30–50% decrease in binding. All three inactivated viruses elicited high level virus neutralizing antibodies in vaccinated mice. However, only mice vaccinated with AMT inactivated virus mounted T cell responses similar to live, uninactivated virus.

Published
2013
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12. A dengue DNA vaccine formulated with Vaxfectin®is well tolerated, and elicits strong neutralizing antibody responses to all four dengue serotypes in New Zealand white rabbits

Author

Raviprakash, Kanakatte, Luke, Thomas, Doukas, John, Danko, Janine, Porter, Kevin, Burgess, Timothy, and Kochel, Tadeusz

Abstract

A tetravalent DNA vaccine formulated with Vaxfectin adjuvant was shown to elicit high levels of neutralizing antibody against all four dengue virus serotypes (Porter et al.,16), warranting further testing in humans. In preparation for a phase 1 clinical testing, the vaccine and the adjuvant were manufactured under current good manufacturing practice guidelines. The formulated vaccine and the adjuvant were tested for safety and/or immunogenicity in New Zealand white rabbits using a repeat dose toxicology study. The formulated vaccine and the adjuvant were found to be well tolerated by the animals. Animals injected with formulated vaccine produced strong neutralizing antibody response to all four dengue serotypes.

Published
2012
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13. Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparumDNA vaccine combined with escalating dose human GM-CSF DNA

Author

Richie, Thomas L., Charoenvit, Yupin, Wang, Ruobing, Epstein, Judith E., Hedstrom, Richard C., Kumar, Sanjai, Luke, Thomas C., Freilich, Daniel A., Aguiar, Joao C., Sacci, John B., Sedegah, Martha, Nosek, Ronald A., De La Vega, Patricia, Berzins, Mara P., Majam, Victoria F., Abot, Esteban N., Ganeshan, Harini, Richie, Nancy O., Banania, Jo Glenna, Baraceros, Maria Fe B., Geter, Tanya G., Mere, Robin, Bebris, Lolita, Limbach, Keith, Hickey, Bradley W., Lanar, David E., Ng, Jennifer, Shi, Meng, Hobart, Peter M., Norman, Jon A., Soisson, Lorraine A., Hollingdale, Michael R., Rogers, William O., Doolan, Denise L., and Hoffman, Stephen L.

Abstract

When introduced in the 1990s, immunization with DNA plasmids was considered potentially revolutionary for vaccine development, particularly for vaccines intended to induce protective CD8 T cell responses against multiple antigens. We conducted, in 1997−1998, the first clinical trial in healthy humans of a DNA vaccine, a single plasmid encoding Plasmodium falciparumcircumsporozoite protein (PfCSP), as an initial step toward developing a multi-antigen malaria vaccine targeting the liver stages of the parasite. As the next step, we conducted in 2000–2001 a clinical trial of a five-plasmid mixture called MuStDO5 encoding pre-erythrocytic antigens PfCSP, PfSSP2/TRAP, PfEXP1, PfLSA1 and PfLSA3. Thirty-two, malaria-naïve, adult volunteers were enrolled sequentially into four cohorts receiving a mixture of 500 μg of each plasmid plus escalating doses (0, 20, 100 or 500 μg) of a sixth plasmid encoding human granulocyte macrophage-colony stimulating factor (hGM-CSF). Three doses of each formulation were administered intramuscularly by needle-less jet injection at 0, 4 and 8 weeks, and each cohort had controlled human malaria infection administered by five mosquito bites 18 d later. The vaccine was safe and well-tolerated, inducing moderate antigen-specific, MHC-restricted T cell interferon-γ responses but no antibodies. Although no volunteers were protected, T cell responses were boosted post malaria challenge. This trial demonstrated the MuStDO5 DNA and hGM-CSF plasmids to be safe and modestly immunogenic for T cell responses. It also laid the foundation for priming with DNA plasmids and boosting with recombinant viruses, an approach known for nearly 15 y to enhance the immunogenicity and protective efficacy of DNA vaccines.

Published
2012
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14. Human immunoglobulin from transchromosomic bovines hyperimmunized with SARS-CoV-2 spike antigen efficiently neutralizes viral variants

Author

Liu, Zhuoming, Wu, Hua, Egland, Kristi A., Gilliland, Theron C., Dunn, Matthew D., Luke, Thomas C., Sullivan, Eddie J., Klimstra, William B., Bausch, Christoph L., and Whelan, Sean P. J.

Abstract

ABSTRACTSevere acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants with amino-acid substitutions and deletions in spike protein (S) can reduce the effectiveness of monoclonal antibodies (mAbs) and may compromise immunity induced by vaccines. We report a polyclonal, fully human, anti-SARS-CoV-2 immunoglobulin produced in transchromosomic bovines (Tc-hIgG-SARS-CoV-2) hyperimmunized with two doses of plasmid DNA encoding the SARS-CoV-2 Wuhan strain S gene, followed by repeated immunization with S protein purified from insect cells. The resulting Tc-hIgG-SARS-CoV-2, termed SAB-185, efficiently neutralizes SARS-CoV-2, and vesicular stomatitis virus (VSV) SARS-CoV-2 chimeras in vitro. Neutralization potency was retained for S variants including S477N, E484K, and N501Y, substitutions present in recent variants of concern. In contrast to the ease of selection of escape variants with mAbs and convalescent human plasma, we were unable to isolate VSV-SARS-CoV-2 mutants resistant to Tc-hIgG-SARS-CoV-2 neutralization. This fully human immunoglobulin that potently inhibits SARS-CoV-2 infection may provide an effective therapeutic to combat COVID-19.

Published
2022
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15. Boosting of DNA Vaccine-Elicited Gamma Interferon Responses in Humans by Exposure to Malaria Parasites

Author

Wang, Ruobing, Richie, Thomas L., Baraceros, Maria Fe, Rahardjo, Nancy, Gay, Tanya, Banania, Jo-Glenna, Charoenvit, Yupin, Epstein, Judith E., Luke, Thomas, Freilich, Daniel A., Norman, Jon, and Hoffman, Stephen L.

Abstract

A mixture of DNA plasmids expressing five Plasmodium falciparum pre-erythrocyte-stage antigens was administered with or without a DNA plasmid encoding human granulocyte-macrophage colony-stimulating factor (hGM-CSF) as an immune enhancer. After DNA immunization, antigen-specific gamma interferon (IFN-γ) responses were detected by ELISPOT in 15/31 volunteers to multiple class I- and/or class II-restricted T-cell epitopes derived from all five antigens. Responses to multiple epitopes (≤7) were detected simultaneously in some volunteers. By 4 weeks after challenge with P. falciparum parasites, 23/31 volunteers had positive IFN-γ responses and the magnitude of responses was increased from 2- to 143-fold. Nonetheless, none was protected against malaria. Volunteers who received hGM-CSF had a reduced frequency of IFN-γ responses to class I peptides compared to those who only received plasmids expressing P. falciparum proteins before challenge (3/23 versus 3/8; P = 0.15) or after parasite challenge (4/23 versus 5/8; P = 0.015) but not to class II peptides before or after challenge. The responses to one antigen (P. falciparum circumsporozoite protein [PfCSP]) were similar among volunteers who received the five-gene mixture compared to volunteers who only received the PfCSP DNA plasmid in a previous study. In summary, DNA-primed IFN-γ responses were boosted in humans by exposure to native antigen on parasites, coadministration of a plasmid expressing hGM-CSF had a negative effect on boosting of class I-restricted IFN-γ responses, and there was no evidence that immunization with PfCSP DNA in the mixture reduced T-cell responses to PfCSP compared to when it was administered alone.

Published
2005

16. Boosting of DNA Vaccine-Elicited Gamma Interferon Responses in Humans by Exposure to Malaria Parasites

Author

Wang, Ruobing, Richie, Thomas L., Baraceros, Maria Fe, Rahardjo, Nancy, Gay, Tanya, Banania, Jo-Glenna, Charoenvit, Yupin, Epstein, Judith E., Luke, Thomas, Freilich, Daniel A., Norman, Jon, and Hoffman, Stephen L.

Abstract

ABSTRACTA mixture of DNA plasmids expressing five Plasmodium falciparumpre-erythrocyte-stage antigens was administered with or without a DNA plasmid encoding human granulocyte-macrophage colony-stimulating factor (hGM-CSF) as an immune enhancer. After DNA immunization, antigen-specific gamma interferon (IFN-γ) responses were detected by ELISPOT in 15/31 volunteers to multiple class I- and/or class II-restricted T-cell epitopes derived from all five antigens. Responses to multiple epitopes (≤7) were detected simultaneously in some volunteers. By 4 weeks after challenge with P. falciparumparasites, 23/31 volunteers had positive IFN-γ responses and the magnitude of responses was increased from 2- to 143-fold. Nonetheless, none was protected against malaria. Volunteers who received hGM-CSF had a reduced frequency of IFN-γ responses to class I peptides compared to those who only received plasmids expressing P. falciparumproteins before challenge (3/23 versus 3/8; P= 0.15) or after parasite challenge (4/23 versus 5/8; P= 0.015) but not to class II peptides before or after challenge. The responses to one antigen (P. falciparumcircumsporozoite protein [PfCSP]) were similar among volunteers who received the five-gene mixture compared to volunteers who only received the PfCSP DNA plasmid in a previous study. In summary, DNA-primed IFN-γ responses were boosted in humans by exposure to native antigen on parasites, coadministration of a plasmid expressing hGM-CSF had a negative effect on boosting of class I-restricted IFN-γ responses, and there was no evidence that immunization with PfCSP DNA in the mixture reduced T-cell responses to PfCSP compared to when it was administered alone.

Published
2005
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17. Human polyclonal immunoglobulin G from transchromosomic bovines inhibits MERS-CoV in vivo

Author

Luke, Thomas, Wu, Hua, Zhao, Jincun, Channappanavar, Rudragouda, Coleman, Christopher M., Jiao, Jin-An, Matsushita, Hiroaki, Liu, Ye, Postnikova, Elena N., Ork, Britini L., Glenn, Gregory, Flyer, David, Defang, Gabriel, Raviprakash, Kanakatte, Kochel, Tadeusz, Wang, Jonathan, Nie, Wensheng, Smith, Gale, Hensley, Lisa E., Olinger, Gene G., Kuhn, Jens H., Holbrook, Michael R., Johnson, Reed F., Perlman, Stanley, Sullivan, Eddie, and Frieman, Matthew B.

Abstract

Anti–MERS-CoV human IgG produced from transchromosomic bovines neutralizes MERS-CoV in vitro and in vivo.

Published
2016
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19. THERAPEUTIC USE OF MUD.

Author

Luke, Thomas D.

Subjects
MUD, PEAT soils, HEAT, RHEUMATOID arthritis, ARTHRITIS, THERAPEUTICS
Abstract

The article presents an extract from the 1912 issue of "The Practitioner" on the therapeutic use of mud. A background is provided involving the sources of mud, the various names of peat baths which are based on different varieties, and a brief history. Its mechanism of action is discussed by way of the uniformly continuous and extensive supply of heat derived from a fango pack. The rheumatic affections of the joints are presented along with its contra-indications.

Published
2012

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