321 results on '"Samuel, MS"'
Search Results
2. Long-term persistence of SARS-CoV-2 neutralizing antibody responses after infection and estimates of the duration of protection
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Eric HY Lau, David SC Hui, Owen TY Tsang, Wai-Hung Chan, Mike YW Kwan, Susan S Chiu, Samuel MS Cheng, Ronald LW Ko, John KC Li, Sara Chaothai, Chi H Tsang, Leo LM Poon, and Malik Peiris
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COVID-19 ,SARS-CoV-2 ,Coronavirus ,Neutralizing antibody ,Kinetics ,Protection ,Medicine (General) ,R5-920 - Abstract
Background: The duration of immunity in SARS-CoV-2 infected people remains unclear. Neutralizing antibody responses are the best available correlate of protection against re-infection. Recent studies estimated that the correlate of 50% protection from re-infection was 20% of the mean convalescent neutralizing antibody titre. Methods: We collected sera from a cohort of 124 individuals with RT-PCR confirmed SARS-CoV-2 infections from Prince of Wales Hospital, Princess Margaret Hospital, Queen Elizabeth Hospital and Queen Mary Hospitals of the Hospital Authority of Hong Kong, for periods up to 386 days after symptom onset and tested these for antibody to SARS-CoV-2 using 50% virus plaque reduction neutralization tests (PRNT50), surrogate neutralization tests and spike receptor binding domain (RBD) binding antibody. Patients were recruited from 21 January 2020 to 16 February 2021 and follow-up samples were collected until 9th March 2021. Findings: Because the rate of antibody waning slows with time, we fitted lines of decay to 115 sera from 62 patients collected beyond 90 days after symptom onset and estimate that PRNT50 antibody will remain detectable for around 1,717 days after symptom onset and that levels conferring 50% protection will be maintained for around 990 days post-symptom onset, in symptomatic patients. This would potentially be affected by emerging virus variants. PRNT titres wane faster in children. There was a high level of correlation between PRNT50 antibody titers and the % of inhibition in surrogate virus neutralization tests. Interpretation: The data suggest that symptomatic COVID-19 disease is followed by relatively long-lived protection from re-infection by antigenically similar viruses. Funding: Health and Medical Research Fund, Commissioned research on Novel Coronavirus Disease (COVID-19) (Reference Nos. COVID190126 and COVID1903003) from the Food and Health Bureau and the Theme-based Research Scheme project no. T11–712/19-N, the University Grants Committee of the Hong Kong SAR Government.
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- 2021
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3. Longitudinal study of Middle East Respiratory Syndrome coronavirus infection in dromedary camel herds in Saudi Arabia, 2014–2015
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Maged Gomaa Hemida, Abdulmohsen Alnaeem, Daniel KW Chu, Ranawaka APM Perera, Samuel MS Chan, Faisal Almathen, Emily Yau, Brian CY Ng, Richard J Webby, Leo LM Poon, and Malik Peiris
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camel ,cohort ,coronavirus ,dromedary ,immunity ,MERS coronavirus ,Infectious and parasitic diseases ,RC109-216 ,Microbiology ,QR1-502 - Abstract
Two herds of dromedary camels were longitudinally sampled with nasal and rectal swabs and serum, between September 2014 and May 2015, and the samples were tested for Middle East Respiratory Syndrome (MERS) coronavirus RNA and antibodies. Evidence of MERS-CoV infection was confirmed in one herd on the basis of detection of virus RNA in nasal swabs from three camels and significant increases in the antibody titers from three others. The three viruses were genetically identical, thus indicating introduction of a single virus into this herd. There was evidence of reinfection of camels that were previously seropositive, thus suggesting that prior infection does not provide complete immunity from reinfection, a finding that is relevant to camel vaccination strategies as a means to prevent zoonotic transmission.Emerging Microbes & Infections (2017) 6, e56; doi:10.1038/emi.2017.44; published online 21 June 2017
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- 2017
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4. Low Prevalence of SARS-CoV-2 Antibodies in Canine and Feline Serum Samples Collected during the Covid-19 Pandemic in Hong Kong and Korea
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Go, Yun Young, primary, Carrai, Maura, additional, Choi, Yan Ru, additional, Brackman, Christopher J., additional, Tam, Karina W.S., additional, Law, Pierra Y.T., additional, Woodhouse, Fiona, additional, Gray, Jane, additional, Kim, Ji Hun, additional, Park, Joohyung, additional, Jeon, Chae Won, additional, Jang, Hyomi, additional, Magouras, Ioannis, additional, Decaro, Nicola, additional, Cheng, Samuel MS, additional, Peiris, Malik, additional, Beatty, Julia A., additional, and Barrs, Vanessa R., additional
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- 2023
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5. Population-based sero-epidemiological estimates of real-world vaccine effectiveness against Omicron infection in an infection-naive population, Hong Kong, January to July 2022
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Jonathan J Lau, Samuel MS Cheng, Kathy Leung, Cheuk Kwong Lee, Asmaa Hachim, Leo CH Tsang, Kenny WH Yam, Sara Chaothai, Kelvin KH Kwan, Zacary YH Chai, Tiffany HK Lo, Masashi Mori, Chao Wu, Sophie Valkenburg, Gaya K Amarasinghe, Eric HY Lau, David S Hui, Gabriel M Leung, Malik Peiris, and Joseph T Wu
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The SARS-CoV-2 Omicron variant has demonstrated enhanced transmissibility and escape of vaccine-derived immunity. While current vaccines remain effective against severe disease and death, robust evidence on vaccine effectiveness (VE) against all Omicron infections (i.e. irrespective of symptoms) remains sparse. We addressed this knowledge-gap using a community-wide serosurvey with 5,310 subjects by estimating how vaccination histories modulated risk of infection in Hong Kong (which was largely infection naïve) during a large wave of Omicron epidemic during January-July 2022. We estimated that Omicron infected 45% (41-48%) of the Hong Kong population. Three and four doses of BNT162b2 or CoronaVac were effective against Omicron infection (VE of 47% (95% credible interval 34-68%) and 70% (43-99%) for three and four doses of BNT162b2 respectively; VE of 31% (1-73%) and 59% (10-99%) for three and four doses of CoronaVac respectively) seven days after vaccination, but protection waned with half-lives of 15 (3-47) weeks for BNT162b2 and 5 (1-37) weeks for CoronaVac. Our findings suggest that booster vaccination can temporarily enhance population immunity ahead of anticipated waves of infections.
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- 2022
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6. Population-based sero-epidemiological estimates of real-world vaccine effectiveness against Omicron infection in an infection-naive population, Hong Kong, January to July 2022
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Lau, Jonathan J, primary, Cheng, Samuel MS, additional, Leung, Kathy, additional, Lee, Cheuk Kwong, additional, Hachim, Asmaa, additional, Tsang, Leo CH, additional, Yam, Kenny WH, additional, Chaothai, Sara, additional, Kwan, Kelvin KH, additional, Chai, Zacary YH, additional, Lo, Tiffany HK, additional, Mori, Masashi, additional, Wu, Chao, additional, Valkenburg, Sophie, additional, Amarasinghe, Gaya K, additional, Lau, Eric HY, additional, Hui, David S, additional, Leung, Gabriel M, additional, Peiris, Malik, additional, and Wu, Joseph T, additional
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- 2022
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7. Humoral and Cellular Immunogenicity and Safety of 3 Doses of CoronaVac and BNT162b2 in Young Children and Adolescents with Kidney Diseases
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Daniel Leung, Eugene Yu-hin Chan, Xiaofeng Mu, Jaime S Rosa Duque, Samuel MS Cheng, Fanny Tsz-wai Ho, Pak-chiu Tong, Wai-ming Lai, Matthew HL Lee, Stella Chim, Issan YS Tam, Leo CH Tsang, Kelvin KH Kwan, Yuet Chung, Howard HW Wong, Amos MT Lee, Wing Yan Li, Summer TK Sze, Jennifer HY Lam, Derek HL Lee, Sau Man Chan, Wenwei Tu, Malik Peiris, Alison Lap-tak Ma, and Yu Lung Lau
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BackgroundPatients with kidney diseases are at risk of severe complications from COVID-19, yet little is known about the effectiveness of COVID-19 vaccines in children and adolescents with kidney diseases.MethodsWe investigated the immunogenicity and safety of an accelerated, 3-dose primary series of COVID-19 vaccines among 64 pediatric chronic kidney disease patients (mean age 12.2; 32 male) with or without immunosuppression, dialysis, or kidney transplant. CoronaVac was given to those aged ResultsAntibody responses including S-RBD IgG (90.9-100% seropositive) and surrogate virus neutralization (geometric mean sVNT% level, 78.6-94.0%) were significantly elicited by 3 doses of any vaccine. T cell responses were also elicited. Weaker neutralization responses were observed among kidney transplant recipients and non-dialysis children receiving rituximab for glomerular diseases. Neutralization was reduced against Omicron BA.1 compared to wild-type (post-dose 3 sVNT% level; 84% vs 27.2%; pConclusionsOur findings support that an accelerated 3-dose primary series with CoronaVac and BNT162b2 is safe and immunogenic in young children and adolescents with kidney diseases.TRIAL REGISTRATIONClinicaltrials.govNCT04800133SIGNIFICANCE STATEMENTLittle is known about the effectiveness of COVID-19 vaccines in children and adolescents with kidney diseases. This paper describes the antibody and T cell responses of 3 doses of CoronaVac or BNT162b2, the top 2 COVID-19 vaccines distributed worldwide, by an accelerated regimen in patients with kidney diseases aged 1-18 years. Antibody and T cell responses were significantly elicited by either vaccine. Neutralization was reduced against Omicron while T cell response was preserved, which likely confer protection against severe COVID-19. Rate of severe adverse reactions was low in the study. Results confirm that accelerated 3-dose primary series with CoronaVac and BNT162b2 is safe and immunogenic in young children and adolescents with kidney diseases.
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- 2022
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8. Antibody and T cell responses against wild-type and Omicron SARS-CoV-2 after the third dose of BNT162b2 in healthy adolescents
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Yu Lung Lau, Xiaofeng Mu, Carolyn A Cohen, Daniel Leung, Jaime S Rosa Duque, Samuel MS Cheng, Yuet Chung, Howard HW Wong, Amos MT Lee, Wing Yan Li, Issan Tam, Jennifer HY Lam, Derek HL Lee, Sau Man Chan, Leo CH Tsang, Karl CK Chan, John KC Li, Leo LH Luk, Sara Chaothai, Kelvin KH Kwan, Nym Coco Chu, Masashi Mori, Trushar Jeevan, Ahmed Kandeil, WENWEI TU, Sophie Valkenburg, and Malik Peiris
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High effectiveness of the third dose of BNT162b2 in healthy adolescents against Omicron BA.1 has been reported, but immune responses conferring this protection are not yet elucidated. In this analysis, our study (NCT04800133) aims to evaluate the humoral and cellular responses against wild-type and Omicron (BA.1, BA.2 and/or BA.5) SARS-CoV-2 before and after a third dose of BNT162b2 in healthy adolescents. At 6 months after 2 doses, S IgG, S IgG Fc receptor-binding, S-RBD IgG and neutralizing antibody responses waned significantly, yet neutralizing antibodies remained detectable in all tested adolescents and S IgG avidity increased from 1 month after 2 doses. The antibody responses and S-specific IFN-γ+ and IL-2+ CD8+ T cell responses were significantly boosted in healthy adolescents after a homologous third dose of BNT162b2. Compared to adults, humoral responses for the third dose were non-inferior or superior in adolescents. The S-specific IFN-γ+ and IL-2+ CD4+ and CD8+ T cell responses in adolescents and adults were comparable. Interestingly, after 3 doses, adolescents had preserved S IgG, S IgG avidity, S IgG FcγRIIIa-binding, and PRNT50 against Omicron BA.2, as well as preserved cellular responses against BA.1 S. Sera from 100% and 96% of adolescents tested at 1 and 6 months after 2 doses could also neutralize BA.1. Based on PRNT50, we predict 92%, 89% and 68% effectiveness against COVID-19 with WT, BA.2 and BA.5 1 month after 3 doses. Our study found high antibody and T cell responses, including potent cross-variant reactivity, after 3 doses of BNT162b2 vaccine in adolescents in its current formulation, suggesting that current vaccines can be protective against symptomatic Omicron disease.
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- 2022
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9. Humoral and Cellular Immunogenicity and Safety of 3 Doses of CoronaVac and BNT162b2 in Young Children and Adolescents with Kidney Diseases
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Leung, Daniel, primary, Chan, Eugene Yu-hin, additional, Mu, Xiaofeng, additional, Rosa Duque, Jaime S, additional, Cheng, Samuel MS, additional, Ho, Fanny Tsz-wai, additional, Tong, Pak-chiu, additional, Lai, Wai-ming, additional, Lee, Matthew HL, additional, Chim, Stella, additional, Tam, Issan YS, additional, Tsang, Leo CH, additional, Kwan, Kelvin KH, additional, Chung, Yuet, additional, Wong, Howard HW, additional, Lee, Amos MT, additional, Li, Wing Yan, additional, Sze, Summer TK, additional, Lam, Jennifer HY, additional, Lee, Derek HL, additional, Chan, Sau Man, additional, Tu, Wenwei, additional, Peiris, Malik, additional, Ma, Alison Lap-tak, additional, and Lau, Yu Lung, additional
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- 2022
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10. Antibody and T cell responses against wild-type and Omicron SARS-CoV-2 after the third dose of BNT162b2 in healthy adolescents
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Lau, Yu Lung, primary, Mu, Xiaofeng, additional, Cohen, Carolyn A, additional, Leung, Daniel, additional, Duque, Jaime S Rosa, additional, Cheng, Samuel MS, additional, Chung, Yuet, additional, Wong, Howard HW, additional, Lee, Amos MT, additional, Li, Wing Yan, additional, Tam, Issan, additional, Lam, Jennifer HY, additional, Lee, Derek HL, additional, Chan, Sau Man, additional, Tsang, Leo CH, additional, Chan, Karl CK, additional, Li, John KC, additional, Luk, Leo LH, additional, Chaothai, Sara, additional, Kwan, Kelvin KH, additional, Chu, Nym Coco, additional, Mori, Masashi, additional, Jeevan, Trushar, additional, Kandeil, Ahmed, additional, TU, WENWEI, additional, Valkenburg, Sophie, additional, and Peiris, Malik, additional
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- 2022
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11. Reduced Pathogenicity and Transmission Potential of Omicron BA.1 and BA.2 Sublineages Compared with the Early Severe Acute Respiratory Syndrome Coronavirus 2 D614G Variant in Syrian Hamsters
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Su, Wen, primary, Choy, Ka Tim, additional, Gu, Haogao, additional, Sia, Sin Fun, additional, Cheng, Ka Man, additional, Nizami, Sarea Islam Nuha, additional, Krishnan, Pavithra, additional, Ng, Yuet Mai, additional, Chang, Lydia Dai Jia, additional, Liu, Yingzhi, additional, Cheng, Samuel MS, additional, Peiris, Malik, additional, Poon, Leo LM, additional, Nicholls, John M, additional, and Yen, Hui Ling, additional
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- 2022
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12. SARS-CoV-2 Omicron variant BA.2 neutralisation in sera of people with Comirnaty or CoronaVac vaccination, infection or breakthrough infection, Hong Kong, 2020 to 2022
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Samuel MS Cheng, Chris Ka Pun Mok, Karl CK Chan, Susanna S Ng, Bosco HS Lam, Leo LH Luk, Fanny W Ko, Chunke Chen, Karen Yiu, John KC Li, Ken KP Chan, Leo CH Tsang, Leo LM Poon, David SC Hui, and Malik Peiris
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COVID-19 Vaccines ,SARS-CoV-2 ,Epidemiology ,Virology ,Vaccination ,Public Health, Environmental and Occupational Health ,COVID-19 ,Hong Kong ,Humans ,Antibodies, Viral ,Antibodies, Neutralizing ,BNT162 Vaccine - Abstract
Background Omicron subvariant BA.2 circulation is rapidly increasing globally. Aim We evaluated the neutralising antibody response from vaccination or prior SARS-CoV-2 infection against symptomatic infection by BA.2 or other variants. Methods Using 50% plaque reduction neutralisation tests (PRNT50), we assessed neutralising antibody titres to BA.2, wild type (WT) SARS-CoV-2 and other variants in Comirnaty or CoronaVac vaccinees, with or without prior WT-SARS-CoV-2 infection. Titres were also measured for non-vaccinees convalescing from a WT-SARS-CoV-2 infection. Neutralising antibodies in BA.2 and BA.1 breakthrough infections and in BA.2 infections affecting non-vaccinees were additionally studied. Results In vaccinees or prior WT-SARS-CoV-2-infected people, BA.2 and BA.1 PRNT50 titres were comparable but significantly (p − 5) lower than WT. In each group of 20 vaccinees with (i) three-doses of Comirnaty, (ii) two CoronaVac followed by one Comirnaty dose, or (iii) one dose of either vaccine after a WT-SARS-CoV-2 infection, ≥ 19 individuals developed detectable (PRNT50 titre ≥ 10) antibodies to BA.2, while only 15 of 20 vaccinated with three doses of CoronaVac did. Comirnaty vaccination elicited higher titres to BA.2 than CoronaVac. In people convalescing from a WT-SARS-CoV-2 infection, a single vaccine dose induced higher BA.2 titres than three Comirnaty (p = 0.02) or CoronaVac (p = 0.00001) doses in infection-naïve individuals. BA.2 infections in previously uninfected and unvaccinated individuals elicited low (PRNT50 titre ≤ 80) responses with little cross-neutralisation of other variants. However, vaccinees with BA.1 or BA.2 breakthrough infections had broad cross-neutralising antibodies to WT viruses, and BA.1, BA.2, Beta and Delta variants. Conclusions Existing vaccines can be of help against the BA.2 subvariant.
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- 2022
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13. ALTEN: A High-Fidelity Primary Tissue-Engineering Platform to Assess Cellular Responses Ex Vivo
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Law, AMK, Chen, J, Colino-Sanguino, Y, Fuente, LRDL, Fang, G, Grimes, SM, Lu, H, Huang, RJ, Boyle, ST, Venhuizen, J, Castillo, L, Tavakoli, J, Skhinas, JN, Millar, EKA, Beretov, J, Rossello, FJ, Tipper, JL, Ormandy, CJ, Samuel, MS, Cox, TR, Martelotto, L, Jin, D, Valdes-Mora, F, Ji, HP, Gallego-Ortega, D, Law, AMK, Chen, J, Colino-Sanguino, Y, Fuente, LRDL, Fang, G, Grimes, SM, Lu, H, Huang, RJ, Boyle, ST, Venhuizen, J, Castillo, L, Tavakoli, J, Skhinas, JN, Millar, EKA, Beretov, J, Rossello, FJ, Tipper, JL, Ormandy, CJ, Samuel, MS, Cox, TR, Martelotto, L, Jin, D, Valdes-Mora, F, Ji, HP, and Gallego-Ortega, D
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To fully investigate cellular responses to stimuli and perturbations within tissues, it is essential to replicate the complex molecular interactions within the local microenvironment of cellular niches. Here, the authors introduce Alginate-based tissue engineering (ALTEN), a biomimetic tissue platform that allows ex vivo analysis of explanted tissue biopsies. This method preserves the original characteristics of the source tissue's cellular milieu, allowing multiple and diverse cell types to be maintained over an extended period of time. As a result, ALTEN enables rapid and faithful characterization of perturbations across specific cell types within a tissue. Importantly, using single-cell genomics, this approach provides integrated cellular responses at the resolution of individual cells. ALTEN is a powerful tool for the analysis of cellular responses upon exposure to cytotoxic agents and immunomodulators. Additionally, ALTEN's scalability using automated microfluidic devices for tissue encapsulation and subsequent transport, to enable centralized high-throughput analysis of samples gathered by large-scale multicenter studies, is shown.
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- 2022
14. SARS-CoV-2 Omicron variant BA.2 neutralisation in sera of people with Comirnaty or CoronaVac vaccination, infection or breakthrough infection, Hong Kong, 2020 to 2022
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Cheng, Samuel MS, primary, Mok, Chris Ka Pun, additional, Chan, Karl CK, additional, Ng, Susanna S, additional, Lam, Bosco HS, additional, Luk, Leo LH, additional, Ko, Fanny W, additional, Chen, Chunke, additional, Yiu, Karen, additional, Li, John KC, additional, Chan, Ken KP, additional, Tsang, Leo CH, additional, Poon, Leo LM, additional, Hui, David SC, additional, and Peiris, Malik, additional
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- 2022
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15. Omicron BA.1 and BA.2 sub-lineages show reduced pathogenicity and transmission potential than the early SARS-CoV-2 D614G variant in Syrian hamsters
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Wen, Su, Ka Tim, Choy, Haogao, Gu, Sin Fun, Sia, Ka Man, Cheng, Sarea Islam Nuha, Nizami, Pavithra, Krishnan, Yuet Mai, Ng, Lydia Dai Jia, Chang, Yingzhi, Liu, Samuel Ms, Cheng, Malik, Peiris, Leo Lm, Poon, John M, Nicholls, and Hui Ling, Yen
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The epidemiological advantage of Omicron variant is evidenced by its rapid spread and the ability to outcompete prior variants. Among Omicron sub-lineages, early outbreaks were dominated by BA.1 while BA.2 has gained dominance since February 2022. The relative pathogenicity and transmissibility of BA.1 and BA.2 have not been fully defined.We compared viral loads and clinical signs in Syrian hamsters after infection with BA.1, BA.2, or D614G variant. A competitive transmission model and next generation sequencing were used to compare the relative transmission potential of BA.1 and BA.2.BA.1 and BA.2 caused no apparent clinical signs while D614G caused more than 10% weight loss. Higher viral loads were detected from the nasal washes, nasal turbinate and lungs of BA.1 than BA.2 inoculated hamsters. No aerosol transmission was observed for BA.1 or BA.2 under the experimental condition that D614G transmitted efficiently. BA.1 and BA.2 were able to transmit among hamsters via direct contact; however, BA.1 transmitted more efficiently than BA.2 under the competitive transmission model. No recombination was detected from direct contacts exposed simultaneously to BA.1 and BA.2.Omicron BA.1 and BA.2 demonstrated attenuated pathogenicity and reduced transmission potential in hamsters when compared to early SARS-CoV-2 strains.
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- 2022
16. Waning antibody levels after COVID-19 vaccination with mRNA Comirnaty and inactivated CoronaVac vaccines in blood donors, Hong Kong, April 2020 to October 2021
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Shirley LL Kwok, Samuel MS Cheng, Jennifer NS Leung, Kathy Leung, Cheuk-Kwong Lee, JS Malik Peiris, and Joseph T Wu
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Vaccines, Synthetic ,COVID-19 Vaccines ,SARS-CoV-2 ,Epidemiology ,Vaccination ,Public Health, Environmental and Occupational Health ,COVID-19 ,Blood Donors ,Antibodies, Viral ,Vaccines, Inactivated ,Virology ,Hong Kong ,Humans ,RNA, Messenger ,mRNA Vaccines - Abstract
The mRNA vaccine Comirnaty and the inactivated vaccine CoronaVac are both available in Hong Kong’s COVID-19 vaccination programme. We observed waning antibody levels in 850 fully vaccinated (at least 14 days passed after second dose) blood donors using ELISA and surrogate virus neutralisation test. The Comirnaty-vaccinated group’s (n = 593) antibody levels remained over the ELISA and sVNT positive cut-offs within the first 6 months. The CoronaVac-vaccinated group’s (n = 257) median antibody levels began to fall below the cut-offs 4 months after vaccination.
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- 2022
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17. Waning antibody levels after COVID-19 vaccination with mRNA Comirnaty and inactivated CoronaVac vaccines in blood donors, Hong Kong, April 2020 to October 2021
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Kwok, Shirley LL, primary, Cheng, Samuel MS, additional, Leung, Jennifer NS, additional, Leung, Kathy, additional, Lee, Cheuk-Kwong, additional, Peiris, JS Malik, additional, and Wu, Joseph T, additional
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- 2022
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18. Immunogenicity Against Wild-Type and Omicron SARS-CoV-2 After a Third Dose of Inactivated COVID-19 Vaccine in Healthy Adolescents
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Leung, Daniel, primary, Cohen, Carolyn A., additional, Mu, Xiaofeng, additional, Rosa Duque, Jaime Sou, additional, Cheng, Samuel MS, additional, Wang, Xiwei, additional, Wang, Manni, additional, Zhang, Wenyue, additional, Zhang, Yanmei, additional, Tam, Issan YS, additional, Lam, Jennifer HY, additional, Man Chan, Sau, additional, Chaothai, Sara, additional, Kwan, Kelvin KH, additional, Chan, Karl CK, additional, Li, John KC, additional, Luk, Leo LH, additional, Tsang, Chi H., additional, Chu, Nym Coco, additional, Wong, Wilfred Hing Sang, additional, Mori, Masashi, additional, Leung, Wing Hang, additional, Valkenburg, Sophie, additional, Peiris, J.S. Malik, additional, Tu, Wenwei, additional, and Lau, Yu Lung, additional
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- 2022
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19. Waning antibody levels after vaccination with mRNA BNT162b2 and inactivated CoronaVac COVID-19 vaccines in Hong Kong blood donors
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Shirley LL Kwok, Samuel MS Cheng, Jennifer NS Leung, Kathy Leung, Cheuk-Kwong Lee, JS Malik Peiris, and Joseph T Wu
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Both inactivated vaccine (CoronaVac; Sinovac) and mRNA vaccine (Comirnaty/BNT162b2; Fosun-Pharma/BioNTech) are available in Hong Kong’s COVID-19 Vaccination Programme. We reported waning antibody levels by enzyme-linked immunosorbent assays (ELISA) and surrogate virus neutralization test (sVNT) among 850 fully vaccinated blood donors (i.e., received two doses). The BNT162b2 group’s antibody levels remain over the 50% protection threshold within six months, and the CoronaVac’s group’s median antibody levels begin to fall below the 50% protection threshold two months after vaccination.
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- 2021
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20. Long-term persistence of SARS-CoV-2 neutralizing antibody responses after infection and estimates of the duration of protection
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Ronald L.W. Ko, Leo L.M. Poon, Eric H. Y. Lau, David S Hui, WY Chan, Samuel Ms Cheng, J. S. Malik Peiris, Owen Tak-Yin Tsang, John Kc Li, Chi H. Tsang, Susan S. Chiu, Mike Ye Kwan, and Sara Chaothai
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medicine.medical_specialty ,Medicine (General) ,Research paper ,Disease ,Disease cluster ,medicine.disease_cause ,Neutralization ,Virus ,R5-920 ,Informed consent ,Internal medicine ,Medicine ,Neutralizing antibody ,Coronavirus ,Protection ,Immunity, duration ,biology ,business.industry ,SARS-CoV-2 ,Antibody titer ,COVID-19 ,General Medicine ,Titer ,Kinetics ,Cohort ,Immunology ,biology.protein ,Antibody ,business - Abstract
The duration of immunity in SARS-CoV-2 infected people remains unclear. Neutralizing antibody responses are the best available correlate of protection against re-infection. Recent studies have estimated that the correlate of 50% protection from re-infection was 20% of the mean convalescent neutralizing antibody titre. We used sera collected from a cohort of 125 individuals with RT-PCR confirmed SARS-CoV-2 infections up to 386 days after symptom onset. In the subset of 65 sera collected from day 151 to 386 after symptom onset, all remained positive in 50% plaque reduction neutralization tests (PRNT50). Because antibody waning follows a bimodal pattern with slower waning beyond day 90 after illness, we fitted lines of decay to 115 sera from 62 patients collected beyond 90 after symptom onset and estimate that PRNT50 antibody will remain detectable for around 1,717 days after symptom onset and that 50% protective antibody titers will be maintained for around 990 days post-symptom onset, in symptomatic patients. Peak PRNT titres in mildly symptomatic children did not differ from those in mildly symptomatic adults but these antibody titres appear to wane faster in children. There was a high level of correlation between PRNT50 antibody titers and the % of inhibition in surrogate virus neutralization tests. We conclude that there will be relatively long-lived protection from re-infection following symptomatic COVID-19 disease. Funding Information: The study was supported by the Health and Medical Research Fund, Commissioned research on Novel Coronavirus Disease (COVID-19) (Reference no COVID190126) from the Food and Health Bureau, Hong Kong SAR Government and the Theme-based Research Scheme project no. T11-712/19-N, the University Grants Committee of the Hong Kong Government. Declaration of Interests: None of the authors have any conflicts of interest to declare. Ethics Approval Statement: Written informed consent was obtained from the participants or their parents (when the participant was a child) and the studies were approved by the institutional review boards of the respective hospitals, viz. Kowloon West Cluster (KW/EX-20-039 (144-27)), Kowloon Central / Kowloon East cluster (KC/KE-20-0154/ER2) and HKU/HA Hong Kong West Cluster (UW 20-273).
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- 2021
21. Waning antibody levels after vaccination with mRNA BNT162b2 and inactivated CoronaVac COVID-19 vaccines in Hong Kong blood donors
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Kwok, Shirley LL, primary, Cheng, Samuel MS, additional, Leung, Jennifer NS, additional, Leung, Kathy, additional, Lee, Cheuk-Kwong, additional, Wu, Joseph T, additional, and Peiris, Joseph Sriyal Malik, additional
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- 2021
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22. The SARS-CoV-2 antibody landscape is lower in magnitude for structural proteins, diversified for accessory proteins and stable long-term in children
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Susan S. Chiu, Fionn N L Ma, Mike Yw Kwan, Leo L.M. Poon, Sophie A. Valkenburg, Haogao Gu, J. S. M. Peiris, Samuel Ms Cheng, WY Chan, Eric H. Y. Lau, David S.C. Hui, Yat Sun Yau, Owen Ty Tsang, Otared Kavian, Niloufar Kavian, and Asmaa Hachim
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NSP1 ,biology ,Coronavirus disease 2019 (COVID-19) ,business.industry ,Immunoprecipitation ,Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) ,Asymptomatic ,Article ,Serology ,Immunology ,biology.protein ,Medicine ,Antibody ,ORFS ,medicine.symptom ,business - Abstract
BackgroundChildren are less clinically affected by SARS-CoV-2 infection than adults with the majority of cases being mild or asymptomatic and the differences in infection outcomes are poorly understood. The kinetics, magnitude and landscape of the antibody response may impact the clinical severity and serological diagnosis of COVID-19. Thus, a comprehensive investigation of the antibody landscape in children and adults is needed.MethodsWe tested 254 plasma from 122 children with symptomatic and asymptomatic SARS-CoV-2 infections in Hong Kong up to 206 days post symptom onset, including 146 longitudinal samples from 58 children. Adult COVID-19 patients and pre-pandemic controls were included for comparison. We assessed antibodies to a 14-wide panel of SARS-CoV-2 structural and accessory proteins by Luciferase Immunoprecipitation System (LIPS).FindingsChildren have lower levels of Spike and Nucleocapsid antibodies than adults, and their cumulative humoral response is more expanded to accessory proteins (NSP1 and Open Reading Frames (ORFs)). Sensitive serology using the three N, ORF3b, ORF8 antibodies can discriminate COVID-19 in children. Principal component analysis revealed distinct serological signatures in children and the highest contribution to variance were responses to non-structural proteins ORF3b, NSP1, ORF7a and ORF8. Longitudinal sampling revealed maintenance or increase of antibodies for at least 6 months, except for ORF7b antibodies which showed decline. It was interesting to note that children have higher antibody responses towards known IFN antagonists: ORF3b, ORF6 and ORF7a. The diversified SARS-CoV-2 antibody response in children may be an important factor in driving control of SARS-CoV-2 infection.
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- 2021
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23. Intravital imaging technology guides FAK-mediated priming in pancreatic cancer precision medicine according to Merlin status
- Author
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Murphy, KJ, Reed, DA, Vennin, C, Conway, JRW, Nobis, M, Yin, JX, Chambers, CR, Pereira, BA, Lee, V, Filipe, EC, Trpceski, M, Ritchie, S, Lucas, MC, Warren, SC, Skhinas, JN, Magenau, A, Metcalf, XL, Stoehr, J, Major, G, Parkin, A, Bidanel, R, Lyons, RJ, Zaratzian, A, Tayao, M, Da Silva, A, Abdulkhalek, L, Gill, AJ, Johns, AL, Biankin, A, Samra, J, Grimmond, SM, Chou, A, Goetz, JG, Samuel, MS, Lyons, JG, Burgess, A, Caldon, CE, Horvath, LG, Daly, RJ, Gadegaard, N, Wang, Y, Sansom, OJ, Morton, JP, Cox, TR, Pajic, M, Herrmann, D, Timpson, P, Murphy, KJ, Reed, DA, Vennin, C, Conway, JRW, Nobis, M, Yin, JX, Chambers, CR, Pereira, BA, Lee, V, Filipe, EC, Trpceski, M, Ritchie, S, Lucas, MC, Warren, SC, Skhinas, JN, Magenau, A, Metcalf, XL, Stoehr, J, Major, G, Parkin, A, Bidanel, R, Lyons, RJ, Zaratzian, A, Tayao, M, Da Silva, A, Abdulkhalek, L, Gill, AJ, Johns, AL, Biankin, A, Samra, J, Grimmond, SM, Chou, A, Goetz, JG, Samuel, MS, Lyons, JG, Burgess, A, Caldon, CE, Horvath, LG, Daly, RJ, Gadegaard, N, Wang, Y, Sansom, OJ, Morton, JP, Cox, TR, Pajic, M, Herrmann, D, and Timpson, P
- Abstract
Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic, chemoresistant malignancy and is characterized by a dense, desmoplastic stroma that modulates PDAC progression. Here, we visualized transient manipulation of focal adhesion kinase (FAK), which integrates bidirectional cell-environment signaling, using intravital fluorescence lifetime imaging microscopy of the FAK-based Förster resonance energy transfer biosensor in mouse and patient-derived PDAC models. Parallel real-time quantification of the FUCCI cell cycle reporter guided us to improve PDAC response to standard-of-care chemotherapy at primary and secondary sites. Critically, micropatterned pillar plates and stiffness-tunable matrices were used to pinpoint the contribution of environmental cues to chemosensitization, while fluid flow–induced shear stress assessment, patient-derived matrices, and personalized in vivo models allowed us to deconstruct how FAK inhibition can reduce PDAC spread. Last, stratification of PDAC patient samples via Merlin status revealed a patient subset with poor prognosis that are likely to respond to FAK priming before chemotherapy.
- Published
- 2021
24. SARS-CoV-2 virus culture from the upper respiratory tract: Correlation with viral load, subgenomic viral RNA and duration of illness
- Author
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Eugene Tso, Owen Ty Tsang, Dominic N.C. Tsang, Kitty S. C. Fung, Malik Peiris, Vivien Wm Chuang, Samuel Ms Cheung, Alex W.H. Chin, Daniel Kw Chu, Ranawaka A.P.M. Perera, Yonna W.Y. Leung, and Leo L.M. Poon
- Subjects
Viral culture ,business.industry ,viruses ,RNA ,Virology ,Virus ,medicine.anatomical_structure ,Cohort ,medicine ,Respiratory system ,business ,Viral load ,Subgenomic mRNA ,Respiratory tract - Abstract
In 68 respiratory specimens from a cohort of 35 COVID-19 patients, 32 of them with mild disease, we found SARS coronavirus-2 virus culture and sub-genomic RNA was rarely detectable beyond 8 days after onset of illness although virus RNA by RT-PCR remained detectable for many weeks.
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- 2020
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25. SARS-CoV-2 specific T cell responses are lower in children and increase with age and time after infection
- Author
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Cohen, Carolyn A, primary, Li, Athena PY, additional, Hachim, Asmaa, additional, Hui, David SC, additional, Kwan, Mike YW, additional, Tsang, Owen TY, additional, Chiu, Susan S, additional, Chan, Wai Hung, additional, Yau, Yat Sun, additional, Kavian, Niloufar, additional, Ma, Fionn NL, additional, Lau, Eric HY, additional, Cheng, Samuel MS, additional, Poon, Leo LM, additional, Peiris, JS Malik, additional, and Valkenburg, Sophie A, additional
- Published
- 2021
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26. The SARS-CoV-2 antibody landscape is lower in magnitude for structural proteins, diversified for accessory proteins and stable long-term in children
- Author
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Hachim, Asmaa, primary, Gu, Haogao, additional, Kavian, Otared, additional, Kwan, Mike YW, additional, Chan, Wai-hung, additional, Yau, Yat Sun, additional, Chiu, Susan S, additional, Tsang, Owen TY, additional, Hui, David SC, additional, Ma, Fionn, additional, Lau, Eric HY, additional, Cheng, Samuel MS, additional, Poon, Leo LM, additional, Peiris, JS Malik, additional, Valkenburg, Sophie A, additional, and Kavian, Niloufar, additional
- Published
- 2021
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27. Long-Term Persistence of SARS-CoV-2 Neutralizing Antibody Responses After Infection and Estimates of the Duration of Protection
- Author
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Lau, Eric H.Y., primary, Hui, David S. C., additional, Tsang, Owen Tak-Yin, additional, Chan, Wai-Hung, additional, Kwan, Mike YE, additional, Chiu, Susan S., additional, Cheng, Samuel MS, additional, Ko, Ronald LW, additional, Li, John KC, additional, Chaothai, Sara, additional, Tsang, Chi H., additional, Poon, Leo LM, additional, and Peiris, J.S. Malik, additional
- Published
- 2021
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28. Evaluation of a SARS-CoV-2 surrogate virus neutralization test for detection of antibody in human, canine, cat and hamster sera
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Perera, Ranawaka APM, primary, Ko, Ronald, additional, Tsang, Owen TY, additional, Brackman, Christopher J, additional, To, Esther M. W., additional, Yen, Hui-ling, additional, Leung, Kathy, additional, Cheng, Samuel MS, additional, Chan, Kin Ho, additional, Chan, Karl CK, additional, Li, Ka-Chi, additional, Saif, Linda, additional, Barrs, Vanessa R., additional, Wu, Joseph T, additional, Sit, Thomas H. C., additional, Poon, Leo LM, additional, and Peiris, Malik, additional
- Published
- 2020
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29. SARS-CoV-2 virus culture from the upper respiratory tract: Correlation with viral load, subgenomic viral RNA and duration of illness.
- Author
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Perera, Ranawaka APM, primary, Tso, Eugene, additional, Tsang, Owen TY, additional, Tsang, Dominic NC, additional, Fung, Kitty, additional, Leung, Yonna WY, additional, Chin, Alex WH, additional, Chu, Daniel KW, additional, Cheung, Samuel MS, additional, Poon, Leo LM, additional, Chuang, Vivien WM, additional, and Peiris, Malik, additional
- Published
- 2020
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30. Longitudinal study of Middle East Respiratory Syndrome coronavirus infection in dromedary camel herds in Saudi Arabia, 2014–2015
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Leo L.M. Poon, Ranawaka A.P.M. Perera, Richard J. Webby, Maged Gomaa Hemida, Samuel Ms Chan, Emily M Yau, Faisal Almathen, Daniel Kw Chu, Brian Cy Ng, Abdulmohsen Al-Naeem, and Malik Peiris
- Subjects
0301 basic medicine ,endocrine system ,Longitudinal study ,camel ,Camelus ,Dromedary camel ,Epidemiology ,Middle East respiratory syndrome coronavirus ,education ,Immunology ,coronavirus ,Saudi Arabia ,Nose ,Biology ,Antibodies, Viral ,medicine.disease_cause ,Polymerase Chain Reaction ,Microbiology ,reinfection ,03 medical and health sciences ,dromedary ,Zoonoses ,Virology ,parasitic diseases ,Drug Discovery ,Disease Transmission, Infectious ,medicine ,Animals ,Longitudinal Studies ,Phylogeny ,Coronavirus ,Rectum ,cohort ,General Medicine ,Viral Load ,immunity ,eye diseases ,030104 developmental biology ,Infectious Diseases ,Middle East Respiratory Syndrome Coronavirus ,Herd ,RNA, Viral ,Original Article ,Parasitology ,Coronavirus Infections ,geographic locations ,MERS coronavirus - Abstract
Two herds of dromedary camels were longitudinally sampled with nasal and rectal swabs and serum, between September 2014 and May 2015, and the samples were tested for Middle East Respiratory Syndrome (MERS) coronavirus RNA and antibodies. Evidence of MERS-CoV infection was confirmed in one herd on the basis of detection of virus RNA in nasal swabs from three camels and significant increases in the antibody titers from three others. The three viruses were genetically identical, thus indicating introduction of a single virus into this herd. There was evidence of reinfection of camels that were previously seropositive, thus suggesting that prior infection does not provide complete immunity from reinfection, a finding that is relevant to camel vaccination strategies as a means to prevent zoonotic transmission.
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- 2017
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31. Lack of serological evidence of Middle East respiratory syndrome coronavirus infection in virus exposed camel abattoir workers in Nigeria, 2016
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Leo L.M. Poon, Daniel Kw Chu, Malik Peiris, Samuel Ms Cheng, S A Kuranga, Kin-ho Chan, Jamiu O Oladipo, Richard J. Webby, Ray T.Y. So, Eric H. Y. Lau, and Ranawaka A.P.M. Perera
- Subjects
0301 basic medicine ,endocrine system ,medicine.medical_specialty ,camel ,Camelus ,Epidemiology ,Middle East respiratory syndrome coronavirus ,viruses ,abattoir ,030231 tropical medicine ,coronavirus ,serology ,Nigeria ,Biology ,medicine.disease_cause ,Virus ,Serology ,03 medical and health sciences ,0302 clinical medicine ,MERS ,Zoonoses ,Virology ,Environmental health ,parasitic diseases ,medicine ,Animals ,Humans ,human ,Disease Reservoirs ,Coronavirus ,Middle East ,Transmission (medicine) ,Public health ,Public Health, Environmental and Occupational Health ,virus diseases ,occupational exposure ,030104 developmental biology ,Middle East Respiratory Syndrome Coronavirus ,Enzootic ,Coronavirus Infections ,Abattoirs ,Research Article - Abstract
Middle East respiratory syndrome coronavirus (MERS-CoV) is an ongoing threat to global public health [1]. Serological and virological studies have shown evidence of MERS-CoV infection in camels in the Middle East, as well as in East, North and West Africa [2-5] and in Central Asia [6]. In spite of MERS-CoV being enzootic in camels in Africa, zoonotic MERS has not been reported from the African continent. Our recent genetic and phenotypic analysis of MERS-CoV from camels in West (Burkina Faso, Nigeria) Africa has shown that West African viruses were phylogenetically and phenotypically distinct from those associated with human disease in the Arabian Peninsula [7], raising the possibility that virus strain differences may be associated with differences in zoonotic potential. Abattoir workers with exposure to infected camels are a high-risk group for MERS-CoV infection in the Arabian Peninsula [8]. However, there is a paucity of serological data on MERS-CoV infection in people occupationally exposed to camels in Africa, a knowledge gap identified as a priority research question at a Food and Agriculture Organization of the United Nations-World Organisation for Animal Health-World Health Organization (FAO-OIE-WHO) Global Technical Meeting on MERS in September 2017 [1]. A previous study in Egypt in 2013 showed no serologic evidence of MERS-CoV among 179 serum samples from humans working in two camel abattoirs [3]. None of 760 people with household exposure to seropositive camels in Kenya in 2013 had evidence of MERS-CoV antibody [9]. Another study in Kenya in 2013–14 of 1,122 people (not with necessarily high exposure to camels) found two sera with low and inconclusive levels of neutralising antibody to MERS-CoV [10]. It remains important to carry out more sero-epidemiological studies on humans with occupational exposure to infected camels to understand whether or not zoonotic transmission is taking place in Africa. We therefore investigated for serological evidence of MERS-CoV infection of humans occupationally exposed to infected dromedary camels in an abattoir in Kano, Nigeria.
- Published
- 2018
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32. Targeting stromal remodeling and cancer stem cell plasticity overcomes chemoresistance in triple negative breast cancer
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Cazet, AS, Hui, MN, Elsworth, BL, Wu, SZ, Roden, D, Chan, CL, Skhinas, JN, Collot, R, Yang, J, Harvey, K, Johan, MZ, Cooper, C, Nair, R, Herrmann, D, McFarland, A, Deng, N, Ruiz-Borrego, M, Rojo, F, Trigo, JM, Bezares, S, Caballero, R, Lim, E, Timpson, P, O’Toole, S, Watkins, DN, Cox, TR, Samuel, MS, Martín, M, Swarbrick, A, Cazet, AS, Hui, MN, Elsworth, BL, Wu, SZ, Roden, D, Chan, CL, Skhinas, JN, Collot, R, Yang, J, Harvey, K, Johan, MZ, Cooper, C, Nair, R, Herrmann, D, McFarland, A, Deng, N, Ruiz-Borrego, M, Rojo, F, Trigo, JM, Bezares, S, Caballero, R, Lim, E, Timpson, P, O’Toole, S, Watkins, DN, Cox, TR, Samuel, MS, Martín, M, and Swarbrick, A
- Abstract
The cellular and molecular basis of stromal cell recruitment, activation and crosstalk in carcinomas is poorly understood, limiting the development of targeted anti-stromal therapies. In mouse models of triple negative breast cancer (TNBC), Hedgehog ligand produced by neoplastic cells reprograms cancer-associated fibroblasts (CAFs) to provide a supportive niche for the acquisition of a chemo-resistant, cancer stem cell (CSC) phenotype via FGF5 expression and production of fibrillar collagen. Stromal treatment of patient-derived xenografts with smoothened inhibitors (SMOi) downregulates CSC markers expression and sensitizes tumors to docetaxel, leading to markedly improved survival and reduced metastatic burden. In the phase I clinical trial EDALINE, 3 of 12 patients with metastatic TNBC derived clinical benefit from combination therapy with the SMOi Sonidegib and docetaxel chemotherapy, with one patient experiencing a complete response. These studies identify Hedgehog signaling to CAFs as a novel mediator of CSC plasticity and an exciting new therapeutic target in TNBC.
- Published
- 2018
33. Transient tissue priming via ROCK inhibition uncouples pancreatic cancer progression, sensitivity to chemotherapy, and metastasis
- Author
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Vennin, C, Chin, VT, Warren, SC, Lucas, MC, Herrmann, D, Magenau, A, Melenec, P, Walters, SN, Del Monte-Nieto, G, Conway, JRW, Nobis, M, Allam, AH, McCloy, RA, Currey, N, Pinese, M, Boulghourjian, A, Zaratzian, A, Adam, AAS, Heu, C, Nagrial, AM, Chou, A, Steinmann, A, Drury, A, Froio, D, Giry-Laterriere, M, Harris, NLE, Phan, T, Jain, R, Weninger, W, McGhee, EJ, Whan, R, Johns, AL, Samra, JS, Chantrill, L, Gill, AJ, Kohonen-Corish, M, Harvey, RP, Biankin, AV, Australian Pancreatic Cancer Genome Initiative (APGI), Evans, TRJ, Anderson, KI, Grey, ST, Ormandy, CJ, Gallego-Ortega, D, Wang, Y, Samuel, MS, Sansom, OJ, Burgess, A, Cox, TR, Morton, JP, Pajic, M, and Timpson, P
- Subjects
rho-Associated Kinases ,Antineoplastic Agents ,Biosensing Techniques ,Deoxycytidine ,Extracellular Matrix ,Pancreatic Neoplasms ,Actin Cytoskeleton ,Mice ,Treatment Outcome ,src-Family Kinases ,Liver ,1-(5-Isoquinolinesulfonyl)-2-Methylpiperazine ,Cell Line, Tumor ,CDC2 Protein Kinase ,06 Biological Sciences, 11 Medical and Health Sciences ,Disease Progression ,Animals ,Humans ,Neoplasm Invasiveness ,Collagen ,Albumin-Bound Paclitaxel ,Neoplasm Metastasis ,Protein Kinase Inhibitors ,Cell Proliferation ,Signal Transduction - Abstract
The emerging standard of care for patients with inoperable pancreatic cancer is a combination of cytotoxic drugs gemcitabine and Abraxane, but patient response remains moderate. Pancreatic cancer development and metastasis occur in complex settings, with reciprocal feedback from microenvironmental cues influencing both disease progression and drug response. Little is known about how sequential dual targeting of tumor tissue tension and vasculature before chemotherapy can affect tumor response. We used intravital imaging to assess how transient manipulation of the tumor tissue, or "priming," using the pharmaceutical Rho kinase inhibitor Fasudil affects response to chemotherapy. Intravital Förster resonance energy transfer imaging of a cyclin-dependent kinase 1 biosensor to monitor the efficacy of cytotoxic drugs revealed that priming improves pancreatic cancer response to gemcitabine/Abraxane at both primary and secondary sites. Transient priming also sensitized cells to shear stress and impaired colonization efficiency and fibrotic niche remodeling within the liver, three important features of cancer spread. Last, we demonstrate a graded response to priming in stratified patient-derived tumors, indicating that fine-tuned tissue manipulation before chemotherapy may offer opportunities in both primary and metastatic targeting of pancreatic cancer.
- Published
- 2017
34. Lack of serological evidence of Middle East respiratory syndrome coronavirus infection in virus exposed camel abattoir workers in Nigeria, 2016
- Author
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So, Ray TY, primary, Perera, Ranawaka APM, additional, Oladipo, Jamiu O, additional, Chu, Daniel KW, additional, Kuranga, Sulyman A, additional, Chan, Kin-ho, additional, Lau, Eric HY, additional, Cheng, Samuel MS, additional, Poon, Leo LM, additional, Webby, Richard J, additional, and Peiris, Malik, additional
- Published
- 2018
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35. ROCK signaling promotes collagen remodeling to facilitate invasive pancreatic ductal adenocarcinoma tumor cell growth
- Author
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Rath, N, Morton, JP, Julian, L, Helbig, L, Kadir, S, McGhee, EJ, Anderson, KI, Kalna, G, Mullin, M, Pinho, AV, Rooman, I, Samuel, MS, Olson, MF, Rath, N, Morton, JP, Julian, L, Helbig, L, Kadir, S, McGhee, EJ, Anderson, KI, Kalna, G, Mullin, M, Pinho, AV, Rooman, I, Samuel, MS, and Olson, MF
- Abstract
© 2016 Cancer Research UK Beatson Institute. Published under the terms of the CC BY 4.0 license Pancreatic ductal adenocarcinoma (PDAC) is a major cause of cancer death; identifying PDAC enablers may reveal potential therapeutic targets. Expression of the actomyosin regulatory ROCK1 and ROCK2 kinases increased with tumor progression in human and mouse pancreatic tumors, while elevated ROCK1/ROCK2 expression in human patients, or conditional ROCK2 activation in a KrasG12D/p53R172Hmouse PDAC model, was associated with reduced survival. Conditional ROCK1 or ROCK2 activation promoted invasive growth of mouse PDAC cells into three-dimensional collagen matrices by increasing matrix remodeling activities. RNA sequencing revealed a coordinated program of ROCK-induced genes that facilitate extracellular matrix remodeling, with greatest fold-changes for matrix metalloproteinases (MMPs) Mmp10 and Mmp13. MMP inhibition not only decreased collagen degradation and invasion, but also reduced proliferation in three-dimensional contexts. Treatment of KrasG12D/p53R172HPDAC mice with a ROCK inhibitor prolonged survival, which was associated with increased tumor-associated collagen. These findings reveal an ancillary role for increased ROCK signaling in pancreatic cancer progression to promote extracellular matrix remodeling that facilitates proliferation and invasive tumor growth.
- Published
- 2017
36. A RhoA-FRET Biosensor Mouse for Intravital Imaging in Normal Tissue Homeostasis and Disease Contexts
- Author
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Nobis, M, Herrmann, D, Warren, SC, Kadir, S, Leung, W, Killen, M, Magenau, A, Stevenson, D, Lucas, MC, Reischmann, N, Vennin, C, Conway, JRW, Boulghourjian, A, Zaratzian, A, Law, AM, Gallego-Ortega, D, Ormandy, CJ, Walters, SN, Grey, ST, Bailey, J, Chtanova, T, Quinn, JMW, Baldock, PA, Croucher, PI, Schwarz, JP, Mrowinska, A, Zhang, L, Herzog, H, Masedunskas, A, Hardeman, EC, Gunning, PW, del Monte-Nieto, G, Harvey, RP, Samuel, MS, Pajic, M, McGhee, EJ, Johnsson, AKE, Sansom, OJ, Welch, HCE, Morton, JP, Strathdee, D, Anderson, KI, Timpson, P, Nobis, M, Herrmann, D, Warren, SC, Kadir, S, Leung, W, Killen, M, Magenau, A, Stevenson, D, Lucas, MC, Reischmann, N, Vennin, C, Conway, JRW, Boulghourjian, A, Zaratzian, A, Law, AM, Gallego-Ortega, D, Ormandy, CJ, Walters, SN, Grey, ST, Bailey, J, Chtanova, T, Quinn, JMW, Baldock, PA, Croucher, PI, Schwarz, JP, Mrowinska, A, Zhang, L, Herzog, H, Masedunskas, A, Hardeman, EC, Gunning, PW, del Monte-Nieto, G, Harvey, RP, Samuel, MS, Pajic, M, McGhee, EJ, Johnsson, AKE, Sansom, OJ, Welch, HCE, Morton, JP, Strathdee, D, Anderson, KI, and Timpson, P
- Abstract
The small GTPase RhoA is involved in a variety of fundamental processes in normal tissue. Spatiotemporal control of RhoA is thought to govern mechanosensing, growth, and motility of cells, while its deregulation is associated with disease development. Here, we describe the generation of a RhoA-fluorescence resonance energy transfer (FRET) biosensor mouse and its utility for monitoring real-time activity of RhoA in a variety of native tissues in vivo. We assess changes in RhoA activity during mechanosensing of osteocytes within the bone and during neutrophil migration. We also demonstrate spatiotemporal order of RhoA activity within crypt cells of the small intestine and during different stages of mammary gestation. Subsequently, we reveal co-option of RhoA activity in both invasive breast and pancreatic cancers, and we assess drug targeting in these disease settings, illustrating the potential for utilizing this mouse to study RhoA activity in vivo in real time. Nobis et al. generated a RhoA-FRET biosensor mouse to characterize and quantify the spatiotemporal distribution of RhoA activity in native mammalian tissues in vivo during development and disease progression. They show that RhoA activity is tightly regulated during various normal biological processes and is co-opted in disease settings, such as invasive breast and pancreatic cancers.
- Published
- 2017
37. Longitudinal study of Middle East Respiratory Syndrome coronavirus infection in dromedary camel herds in Saudi Arabia, 2014–2015
- Author
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Hemida, Maged Gomaa, primary, Alnaeem, Abdulmohsen, additional, Chu, Daniel KW, additional, Perera, Ranawaka APM, additional, Chan, Samuel MS, additional, Almathen, Faisal, additional, Yau, Emily, additional, Ng, Brian CY, additional, Webby, Richard J, additional, Poon, Leo LM, additional, and Peiris, Malik, additional
- Published
- 2017
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38. Epidermal YAP2-5SA-ΔC Drives β-Catenin Activation to Promote Keratinocyte Proliferation in the Mouse Skin in vivo
- Author
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Akladios, B, Mendoza-Reinoso, V, Samuel, MS, Hardeman, EC, Khosrotehrani, K, Key, B, Beverdam, A, Akladios, B, Mendoza-Reinoso, V, Samuel, MS, Hardeman, EC, Khosrotehrani, K, Key, B, and Beverdam, A
- Published
- 2016
39. Responsive Changes in Mental Health Practice in Wisconsin
- Author
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Otr Linda Samuel Ms
- Subjects
Occupational therapy ,medicine.medical_specialty ,Rehabilitation ,business.industry ,medicine.medical_treatment ,Public Health, Environmental and Occupational Health ,Staffing ,Certification ,Mental health ,Psychiatry and Mental health ,Nursing ,Intervention (counseling) ,Acute care ,Health care ,Medicine ,business ,Applied Psychology - Abstract
SUMMARY Delivery of mental health care is changing dramatically at the state and county levels in Wisconsin. These new trends are affecting psychiatric institutions and rehabilitation personnel in reference to staffing patterns, the roles of occupational therapists, certified occupational therapy assistants, patient population and level of acute care and the type and site of intervention. Therapists are moving to more community-based and innovative programming and are leading state and local advocacy initiatives. Many occupational therapists in Wisconsin have become pioneers pursuing nontraditional occupational therapy roles in response to changes in philosophy, funding, population demographics and evolving needs.
- Published
- 1998
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40. Molecular Regulation and Function of the Protein Tyrosine Kinase Pyk2 in Cytotoxic T Lymphocytes
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Cheung, Samuel MS
- Published
- 2013
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41. Middle East respiratory syndrome coronavirus (MERS-CoV) in dromedary camels in Nigeria, 2015
- Author
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Chu, Daniel KW, primary, Oladipo, Jamiu O, additional, Perera, Ranawaka APM, additional, Kuranga, Sulaiman A, additional, Chan, Samuel MS, additional, Poon, Leo LM, additional, and Peiris, Malik, additional
- Published
- 2015
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42. Genetic Dissection of Differential Signaling Threshold Requirements for the Wnt/beta-Catenin Pathway In Vivo
- Author
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Nusse, R, Buchert, M, Athineos, D, Abud, HE, Burke, ZD, Faux, MC, Samuel, MS, Jarnicki, AG, Winbanks, CE, Newton, IP, Meniel, VS, Suzuki, H, Stacker, SA, Nathke, IS, Tosh, D, Huelsken, J, Clarke, AR, Heath, JK, Sansom, OJ, Ernst, M, Nusse, R, Buchert, M, Athineos, D, Abud, HE, Burke, ZD, Faux, MC, Samuel, MS, Jarnicki, AG, Winbanks, CE, Newton, IP, Meniel, VS, Suzuki, H, Stacker, SA, Nathke, IS, Tosh, D, Huelsken, J, Clarke, AR, Heath, JK, Sansom, OJ, and Ernst, M
- Abstract
Contributions of null and hypomorphic alleles of Apc in mice produce both developmental and pathophysiological phenotypes. To ascribe the resulting genotype-to-phenotype relationship unambiguously to the Wnt/beta-catenin pathway, we challenged the allele combinations by genetically restricting intracellular beta-catenin expression in the corresponding compound mutant mice. Subsequent evaluation of the extent of resulting Tcf4-reporter activity in mouse embryo fibroblasts enabled genetic measurement of Wnt/beta-catenin signaling in the form of an allelic series of mouse mutants. Different permissive Wnt signaling thresholds appear to be required for the embryonic development of head structures, adult intestinal polyposis, hepatocellular carcinomas, liver zonation, and the development of natural killer cells. Furthermore, we identify a homozygous Apc allele combination with Wnt/beta-catenin signaling capacity similar to that in the germline of the Apc(min) mice, where somatic Apc loss-of-heterozygosity triggers intestinal polyposis, to distinguish whether co-morbidities in Apc(min) mice arise independently of intestinal tumorigenesis. Together, the present genotype-phenotype analysis suggests tissue-specific response levels for the Wnt/beta-catenin pathway that regulate both physiological and pathophysiological conditions.
- Published
- 2010
43. The Major Proteins of Wheat Endosperm Starch Granules
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Rahman, S, primary, Kosar-Hashemi, B, additional, Samuel, MS, additional, Hill, A, additional, Abbott, DC, additional, Skerritt, JH, additional, Preiss, J, additional, Appels, R, additional, and Morell, MK, additional
- Published
- 1995
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44. The Major Proteins of Wheat Endosperm Starch Granules
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Rahman, S, Kosar-Hashemi, B, Samuel, MS, Hill, A, Abbott, DC, Skerritt, JH, Preiss, J, Appels, R, and Morell, MK
- Abstract
Wheat starch contains two classes of associated proteins: proteins which are embedded within the granule and loosely associated surface proteins. The characterisation of the major proteins that are embedded in the granule are described. Gel electrophoresis on the basis of size resolved these proteins into five bands of molecular weights 60, 75, 85, 100 and 105 kDa. These polypeptides were demonstrated to be within the granule by their resistance to proteinase K digestion when granules were ungelatinised. The N-terminal sequences of these polypeptides are reported. The most prominent polypeptide is the 60 kDa granule-bound starch synthase. The N-terminal sequence obtained from the 75 kDa polypeptide shows homology to rice soluble starch synthase. The 85 kDa band was resolved into at least two types of polypeptides, one of which reacted with polyclonal antiserum to the maize branching enzyme IIb. The 100 and 105 kDa polypeptides were located only in the granule and are related, on the basis of N-terminal sequence similarity and cross-reactivity to monoclonal antibodies. SDS-PAGE and monoclonal antibody cross-reactivity experiments suggest that the 100 and 105 kDa polypeptides are absent from starch granules from all other species examined, including other cereals. It is speculated that all the major granule proteins are involved in starch biosynthesis.
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- 1995
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45. Accelerated Closure of Diabetic Wounds by Efficient Recruitment of Fibroblasts upon Inhibiting a 14-3-3/ROCK Regulatory Axis.
- Author
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Johan MZ, Pyne NT, Kolesnikoff N, Poltavets V, Esmaeili Z, Woodcock JM, Lopez AF, Cowin AJ, Pitson SM, and Samuel MS
- Subjects
- Animals, Mice, Diabetes Mellitus, Type 2 metabolism, Humans, Mice, Knockout, Disease Models, Animal, Male, Mice, Inbred C57BL, 14-3-3 Proteins metabolism, rho-Associated Kinases antagonists & inhibitors, rho-Associated Kinases metabolism, Wound Healing drug effects, Fibroblasts metabolism, Diabetes Mellitus, Experimental metabolism, Signal Transduction drug effects
- Abstract
Chronic non-healing wounds negatively impact quality of life and are a significant financial drain on health systems. The risk of infection that exacerbates comorbidities in patients necessitates regular application of wound care. Understanding the mechanisms underlying impaired wound healing are therefore a key priority to inform effective new-generation treatments. In this study, we demonstrate that 14-3-3-mediated suppression of signaling through ROCK is a critical mechanism that inhibits the healing of diabetic wounds. Accordingly, pharmacological inhibition of 14-3-3 by topical application of the sphingo-mimetic drug RB-11 to diabetic wounds on a mouse model of type II diabetes accelerated wound closure more than 2-fold than vehicle control, phenocopying our previous observations in 14-3-3ζ-knockout mice. We also demonstrate that accelerated closure of the wounded epidermis by 14-3-3 inhibition causes enhanced signaling through the Rho-ROCK pathway and that the underlying cellular mechanism involves the efficient recruitment of dermal fibroblasts into the wound and the rapid production of extracellular matrix proteins to re-establish the injured dermis. Our observations that the 14-3-3/ROCK inhibitory axis characterizes impaired wound healing and that its suppression facilitates fibroblast recruitment and accelerated re-epithelialization suggest new possibilities for treating diabetic wounds by pharmacologically targeting this axis., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)
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- 2024
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46. Association Between Chrononutrition Patterns and Multidimensional Sleep Health.
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Kim N, Conlon RK, Farsijani S, and Hawkins MS
- Subjects
- Humans, Female, Middle Aged, Male, Cross-Sectional Studies, Adult, Circadian Rhythm physiology, Time Factors, United States, Diet statistics & numerical data, Sleep Quality, Aged, Sleep physiology, Nutrition Surveys, Feeding Behavior physiology
- Abstract
Background/objectives: Sleep health has been associated with diet quality, but the relationship between chrononutrition patterns and multidimensional sleep health is unclear. This study identifies chrononutrition patterns among U.S. adults and examines their associations with multidimensional sleep health., Methods: This cross-sectional analysis used data from the 2017-2020 National Health and Nutrition Examination Survey. Chrononutrition behaviors were assessed using two 24 h dietary recalls. Latent profile analysis was used to identify chrononutrition profiles. Multivariable survey regression models determined the associations between chrononutrition patterns and sleep health dimensions., Results: The sample included 5228 subjects with a median age of 49 years. Of the sample, 52% of the participants were female, and 65% were White. In adjusted models, each additional hour between wake time and first instance of eating was associated with a 19% increase in the odds of poor timing (sleep midpoint < 2:00 a.m. or >4:00 a.m.; 95% CI: 1.07-1.33) and a 21% increase in poor duration (<7 or >9 h/night; 95% CI: 1.09-1.33). Each additional hour between last eating and bedtime was associated with 9% higher odds of poor duration (95% CI: 1.03-1.16). A one-hour longer eating window was associated with 10% lower odds of poor timing (95% CI: 0.84-0.98). We identified five chrononutrition profiles: Typical Eating (reference), Early Finished Eating, Later Heavy Eating, Extended Window Eating, and Restricted Window Eating. The Later Heavy Eating profile exhibited 96% higher odds of poor timing (95% CI: 1.09-3.51) and the Restricted Window Eating profile had 94% higher odds of poor duration (95% CI: 1.10-3.43)., Conclusions: These findings highlight the importance of unique chrononutrition patterns in relation to multidimensional sleep health. We provide a framework for future studies to identify personalized chrononutrition interventions and their role in improving sleep health.
- Published
- 2024
- Full Text
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47. In-vitro biomineralization of magnesium and copper co-doped wollastonite.
- Author
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Collin MS, Rakshana B, Abraham J, and S S
- Abstract
Calcium silicate-based ceramics, particularly wollastonite (CaSiO
3 ), are gaining prominence in hard tissue engineering due to their biocompatibility and bioactivity. However, pure wollastonite faces challenges such as insufficient mechanical strength and susceptibility to bacterial colonization. This study addresses these issues by systematically synthesizing magnesium and copper co-doped wollastonite (MgCuW) using the sol-gel combustion technique, aiming to enhance its mechanical stability and antibacterial properties. The average crystalline size of the synthesized materials ranged from 25 to 47 nm. In vitro biomineralization studies showed significant hydroxyapatite deposition, confirming enhanced bioactivity. Antibacterial tests against Gram-positive (S. aureus, S. epidermidis) and Gram-negative (E. coli, P. aeruginosa) bacteria demonstrated superior antibacterial activity with increased copper doping. The results indicate that MgCuW is a promising biomaterial for bone tissue engineering, combining bioactivity and antibacterial efficacy., Competing Interests: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests:Sasikumar S reports financial support was provided by Vellore Institute of Technology. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2024 The Authors.)- Published
- 2024
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48. Effects of sildenafil on gas exchange, ventilatory, and sensory responses to exercise in subjects with mild-to-moderate COPD: A randomized cross-over trial.
- Author
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Gass R, Plachi F, Silva FOB, Nolasco T, Tonetto MS, Goelzer LS, Muller PT, Knorst MM, Neder JA, and Berton DC
- Abstract
Excess exercise ventilation (high ventilation (V̇
E )/carbon dioxide output (V̇CO2 )) contributes significantly to dyspnea and exercise intolerance since the earlier stages of chronic obstructive pulmonary disease (COPD). A selective pulmonary vasodilator (inhaled nitric oxide) has shown to increase exercise tolerance secondary to lower V̇E /V̇CO2 and dyspnea in this patient population. We aimed to assess whether a clinically more practical option - oral sildenafil - would be associated with similar beneficial effects. In a randomized, placebo-controlled study, twenty-four patients with mild-to-moderate COPD completed, on different days, two incremental cardiopulmonary exercise tests (CPET) one hour after sildenafil or placebo. Eleven healthy participants performed a CPET in a non-interventional visit for comparative purposes with patients when receiving placebo. Patients (FEV1 = 69.4 ± 13.5 % predicted) showed higher ventilatory demands (V̇E /V̇CO2 ), worse pulmonary gas exchange, and higher dyspnea during exercise compared to controls (FEV1 = 98.3 ±11.6 % predicted). Contrary to our expectations, however, sildenafil (50 mg; N= 15) did not change exertional V̇E /V̇CO2 , dead space/tidal volume ratio, operating lung volumes, dyspnea, or exercise tolerance compared to placebo (P>0.05). Due to the lack of significant beneficial effects, nine additional patients were trialed with a higher dose (100 mg). Similarly, active intervention was not associated with positive physiological or sensory effects. In conclusion, acute oral sildenafil (50 or 100 mg) failed to improve gas exchange efficiency or excess exercise ventilation in patients with predominantly moderate COPD. The current study does not endorse a therapeutic role for sildenafil to mitigate exertional dyspnea in this specific patient subpopulation. Clinical trial registry: https://ensaiosclinicos.gov.br/rg/RBR-4qhkf4 Web of Science Researcher ID: O-7665-2019., Competing Interests: Declaration of Competing Interest No authors declare conflicts of interest related to this work., (Copyright © 2024 Elsevier B.V. All rights reserved.)- Published
- 2024
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49. Fetal bone engraftment reconstitutes the immune system in pigs with severe combined immunodeficiency.
- Author
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Monarch K, Yoon J, Uh K, Reese E, Restrepo DC, de Carvalho Madrid DM, Touchard L, Spate LD, Samuel MS, Driver JP, Lim JH, Schlink S, Whitworth KM, Wells KD, Prather RS, Chen PR, and Lee K
- Subjects
- Animals, Swine, Disease Models, Animal, Female, Severe Combined Immunodeficiency immunology, Severe Combined Immunodeficiency genetics, Bone Transplantation methods
- Abstract
Genetic modification of genes such as recombination activating gene 2 (RAG2) or interleukin-2 receptor-γ (IL2RG) results in pigs exhibiting severe combined immunodeficiency (SCID). Pigs presenting a SCID phenotype are important animal models that can be used to establish xenografts and to study immune system development and various immune-related pathologies. However, due to their immunocompromised nature, SCID pigs have shortened lifespans and are notoriously difficult to maintain. The failure-to-thrive phenotype makes the establishment of a breeding population of RAG2/IL2RG double-knockout pigs virtually impossible. Here, to overcome this limitation, we investigated whether reconstituting the immune system of SCID piglets with a fetal bone allograft would extend their lifespan. Following intramuscular transplantation, allografts gave rise to lymphocytes expressing T cell (CD3, CD4 and CD8), B cell (CD79α) and natural killer cell (CD335) lineage markers, which were detected in circulation as well in the spleen, liver, bone marrow and thymic tissues. The presence of lymphocytes indicates broad engraftment of donor cells in the recipient SCID pigs. Unlike unreconstituted SCID pigs, the engrafted animals thrived and reached puberty under standard housing conditions. This study demonstrates a novel method to extend the survival of SCID pigs, which may improve the availability and use of SCID pigs as a biomedical animal model., (© 2024. The Author(s).)
- Published
- 2024
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50. Enhanced perfluorooctanoic acid (PFOA) degradation by electrochemical activation of peroxydisulfate (PDS) during electrooxidation for water treatment.
- Author
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Samuel MS, Kadarkarai G, Ryan DR, McBeath ST, Mayer BK, and McNamara PJ
- Abstract
Improved treatment of per- and polyfluoroalkyl substances (PFAS) in water is critically important in light of the proposed United States Environmental Protection Agency (USEPA) drinking water regulations at ng L
-1 levels. The addition of peroxymonosulfate (PMS) during electrooxidation (EO) can remove and destroy PFAS, but ng L-1 levels have not been tested, and PMS itself can be toxic. The objective of this research was to test peroxydisulfate (PDS, an alternative to PMS) activation by boron-doped diamond (BDD) electrodes for perfluorooctanoic acid (PFOA) degradation. The influence of PDS concentration, temperature, and environmental water matrix effects, and PFOA concentration on PDS-EO performance were systematically examined. Batch reactor experiments revealed that 99 % of PFOA was degraded and 69 % defluorination was achieved, confirming PFOA mineralization. Scavenging experiments implied that sulfate radicals (SO4 - ) and hydroxyl radicals (HO) played a more important role for PFOA degradation than1 O2 ). Further identification of PFOA degradation and transformation products by liquid chromatography-mass spectrometry (LC-MS) analysis established plausible PFOA degradation pathways. The analysis corroborates that direct electron transfers at the electrode initiate PFOA oxidation and SO- ). Further identification of PFOA degradation and transformation products by liquid chromatography-mass spectrometry (LC-MS) analysis established plausible PFOA degradation pathways. The analysis corroborates that direct electron transfers at the electrode initiate PFOA oxidation and SO4 - improves overall treatment by cleaving the CC bond between the C7 F15 and COOH moieties in PFOA, leading to possible products such as C7 F15 and F- . The perfluoroalkyl radicals can be oxidized by SO4 - and HO, resulting in the formation of shorter chain perfluorocarboxylic acids (e.g., perfluorobutanoic acid [PFBA]), with eventual mineralization to CO2 and F- . At an environmentally relevant low initial concentration of 100 ng L-1 PFOA, 99 % degradation was achieved. The degradation of PFOA was slightly affected by the water matrix as less removal was observed in an environmental river water sample (91 %) compared to tests conducted in Milli-Q water (99 %). Overall, EO with PDS provided a destructive approach for the elimination of PFOA., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier B.V. All rights reserved.)- Published
- 2024
- Full Text
- View/download PDF
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