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51. Challenges with sirolimus experimental data to inform QSP model of post‐transplantation cyclophosphamide regimens

Author

Ezhilpavai Mohanan, Guofang Shen, Suping Ren, Hsuan‐Hao Fan, Kao Tang Ying Moua, Aleksandra Karolak, Russell C. Rockne, Ryotaro Nakamura, David A. Horne, Christopher G. Kanakry, Donald E. Mager, and Jeannine S. McCune

Subjects
Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270
Abstract

Abstract Dose optimization of sirolimus may further improve outcomes in allogeneic hematopoietic cell transplant (HCT) patients receiving post‐transplantation cyclophosphamide (PTCy) to prevent graft‐versus‐host disease (GVHD). Sirolimus exposure–response association studies in HCT patients (i.e., the association of trough concentration with clinical outcomes) have been conflicting. Sirolimus has important effects on T‐cells, including conventional (Tcons) and regulatory T‐cells (Tregs), both of which have been implicated in the mechanisms by which PTCy prevents GVHD, but there is an absence of validated biomarkers of sirolimus effects on these cell subsets. Considering the paucity of existing biomarkers and the complexities of the immune system, we conducted a literature review to inform a quantitative systems pharmacology (QSP) model of GVHD. The published literature presented multiple challenges. The sirolimus pharmacokinetic models insufficiently describe sirolimus distribution to relevant physiological compartments. Despite multiple publications describing sirolimus effects on Tcons and Tregs in preclinical and human ex vivo models, consistent parameters relating sirolimus concentrations to circulating Tcons and Tregs could not be found. Each aspect presents a challenge in building a QSP model of sirolimus and its temporal effects on T‐cell subsets and GVHD prevention. To optimize GVHD prevention regimens, phase I studies and systematic studies of immunosuppressant concentration–effect association are needed for QSP modeling.

Published
2024
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52. Mental Imagery to Reduce Alcohol-related harm in patients with alcohol use disorder and alcohol-related liver damaGE: the MIRAGE randomised pilot trial results

Author

Victoria Allgar, Christopher Hayward, Ashwin Dhanda, Angela King, Annie Hawton, Ben Hudson, Crispin Musicha, Richard Parker, Wendy Ingram, Lynne Callaghan, Alison Jeffery, Laura Cocking, C Anne McCune, Elizabeth Goodwin, Hannah Allende, Jackie Andrade, Victoria Lavers, Joe Lomax, Christopher Rollinson, Jonny Wilks, E Siobhan Creanor, and Matthew Bailey

Subjects
Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Objective The healthcare burden of alcohol-related liver disease (ARLD) is increasing. ARLD and alcohol use disorder (AUD) is best managed by reduction or cessation of alcohol use, but effective treatments are lacking. We tested whether people with ARLD and AUD admitted to hospital could be recruited to and retained in a trial of Functional Imagery Training (FIT), a psychological therapy that uses mental imagery to reduce alcohol craving. We conducted a multicentre randomised pilot trial of treatment as usual (TAU) versus FIT+TAU in people admitted to hospital with ARLD and AUD.Design Participants were randomised to TAU (a single session of brief intervention) or FIT+TAU (TAU with one hospital-based FIT session then eight telephone sessions over 6 months). Pilot outcomes included recruitment rate and retention at day 180. Secondary outcomes included fidelity of FIT delivery, alcohol use, and severity of alcohol dependence.Results Fifty-four participants (mean age 49; 63% male) were recruited and randomised, 28 to TAU and 26 to FIT+TAU. The retention rate at day 180 was 43%. FIT was delivered adequately by most alcohol nurses. 50% of intervention participants completed FIT sessions 1 and 2. There were no differences in alcohol use or severity of alcohol dependence between treatment groups at day 180.Conclusion Participants with ARLD and AUD could be recruited to a trial of FIT versus FIT+TAU. However, retention at day 180 was suboptimal. Before conducting a definitive trial of FIT in this patient group, modifications in the intervention and recruitment/retention strategy must be tested.Trial registration number ISRCTN41353774.

Published
2024
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53. From Fast Food to a Well-Balanced Diet: Toward a Programme Focused Approach to Feedback in Higher Education

Author

Wilder-Davis, Kimberly, Carless, David, Huxham, Mark, McCune, Velda, McLatchie, Joan, Jessop, Tansy, and Marzetti, Hazel

Abstract

Feedback may be considered 'good' according to many of the criteria in the literature whilst still having little or no impact on students' learning in the longer term. Feedback in the context of this paper is defined as the process of learners obtaining information about their work in order to produced improved learning. This comes from tutors, peers, or even self-evaluation. Here we argue for greater prominence for feedback in curriculum design. Clear principles for giving guidance on assessments and feedback at the programme level, which complement those already established and widely used for single assessments, would help curriculum designers consider communication to students about assessments in a broader context. These processes should create a dialogue that aids the students' progression in their learning from one module to the next and encourages the development of autonomous learners. Based on a review of the literature on programme-focused approaches to teaching, assessment and feedback, the current paper delineates the benefits of a programme level approach to communication around assessments and proffers a list of broad principles that will help academics achieve a coherent and developmental approach to feedback.

Published
2021

54. A wearable electrochemical biosensor for the monitoring of metabolites and nutrients

Author

Wang, Minqiang, Yang, Yiran, Min, Jihong, Song, Yu, Tu, Jiaobing, Mukasa, Daniel, Ye, Cui, Xu, Changhao, Heflin, Nicole, McCune, Jeannine S, Hsiai, Tzung K, Li, Zhaoping, and Gao, Wei

Subjects
Bioengineering, Nutrition, Networking and Information Technology R&D (NITRD), Good Health and Well Being, Humans, Wearable Electronic Devices, Monitoring, Physiologic, Sweat, Biosensing Techniques, Nutrients
Abstract

Wearable non-invasive biosensors for the continuous monitoring of metabolites in sweat can detect a few analytes at sufficiently high concentrations, typically during vigorous exercise so as to generate sufficient quantity of the biofluid. Here we report the design and performance of a wearable electrochemical biosensor for the continuous analysis, in sweat during physical exercise and at rest, of trace levels of multiple metabolites and nutrients, including all essential amino acids and vitamins. The biosensor consists of graphene electrodes that can be repeatedly regenerated in situ, functionalized with metabolite-specific antibody-like molecularly imprinted polymers and redox-active reporter nanoparticles, and integrated with modules for iontophoresis-based sweat induction, microfluidic sweat sampling, signal processing and calibration, and wireless communication. In volunteers, the biosensor enabled the real-time monitoring of the intake of amino acids and their levels during physical exercise, as well as the assessment of the risk of metabolic syndrome (by correlating amino acid levels in serum and sweat). The monitoring of metabolites for the early identification of abnormal health conditions could facilitate applications in precision nutrition.

Published
2022

55. REPAIRS Delphi: A UK and Ireland Consensus Statement on the Management of Infected Arterial Pseudoaneurysms Secondary to Groin Injecting Drug Use

Author

Munro, Euan N., Flett, Murray M., Hussey, Keith, Wolf, Bernhard, Jamieson, Russell W., Wallace, David, Vesey, Alex T., McCaslin, James, Wong, Peng, Tenna, Adriano, Badger, Stephen, Harrison, Gareth, Ghosh, Jon, Al-Khaffaf, Haytham, Torella, Francesco, McBride, Richard, Drinkwater, Susan, Antoniou, George A., Bhasin, Neeraj, Pradhan, Aniket, Smith, George, Coughlin, Patrick, Brar, Ranjeet, Elsherif, Mohamed, Lau, Simon, Peach, George, Kulkarni, Sachin, Brooks, Marcus, Wijesinghe, Lasantha, McCune, Ken, Hopper, Neil, Cowan, Andrew, Hunter, Ian, Mittapalli, Devender, Garnham, Andrew, Jones, Steven, Rajagopalan, Sriram, Tiwari, Alok, Imray, Chris, Atwal, Amarjit, Bahia, Sandeep, Jones, Keith G., Handa, Ashok, Bowbrick, Ginny, Nordon, Ian, Button, Matthew, Rudarakanchana, Nung, D’Souza, Rovan, Tai, Nigel, Moxey, Paul, Bicknell, Colin, Gibbs, Richard, Zayed, Hany, Saratzis, Athanasios, Kannan, Ramesh, Batchelder, Andrew, Chong, Peter Lee, Rowlands, Timothy, Hildebrand, Diane, Thapar, Ankur, Chaudhuri, Arindam, Howard, Adam, Metcalfe, Matthew, Al-Jundi, Wissam, Sayer, Gabriel, Lewis, David, Sohrabi, Soroush, Woolgar, Justin, Fligelstone, Louis, Davies, Huw, Hill, Susan, Fulton, Greg, Moneley, Daragh, McDonnell, Ciaran, Martin, Zenia, Dowdall, Joseph, Tierney, Sean, Walsh, Stewart, Medani, Mekki, Gosi, Gergely, MacLeod, Caitlin S., Nagy, John, Radley, Andrew, Khan, Faisel, Rae, Nikolas, Wilson, Michael S.J., and Suttie, Stuart A.

Published
2024
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58. Structural optimization of siRNA conjugates for albumin binding achieves effective MCL1-directed cancer therapy

Author

Ella N. Hoogenboezem, Shrusti S. Patel, Justin H. Lo, Ashley B. Cavnar, Lauren M. Babb, Nora Francini, Eva F. Gbur, Prarthana Patil, Juan M. Colazo, Danielle L. Michell, Violeta M. Sanchez, Joshua T. McCune, Jinqi Ma, Carlisle R. DeJulius, Linus H. Lee, Jonah C. Rosch, Ryan M. Allen, Larry D. Stokes, Jordan L. Hill, Kasey C. Vickers, Rebecca S. Cook, and Craig L. Duvall

Subjects
Science
Abstract

Abstract The high potential of siRNAs to silence oncogenic drivers remains largely untapped due to the challenges of tumor cell delivery. Here, divalent lipid-conjugated siRNAs are optimized for in situ binding to albumin to improve pharmacokinetics and tumor delivery. Systematic variation of the siRNA conjugate structure reveals that the location of the linker branching site dictates tendency toward albumin association versus self-assembly, while the lipid hydrophobicity and reversibility of albumin binding also contribute to siRNA intracellular delivery. The lead structure increases tumor siRNA accumulation 12-fold in orthotopic triple negative breast cancer (TNBC) tumors over the parent siRNA. This structure achieves approximately 80% silencing of the anti-apoptotic oncogene MCL1 and yields better survival outcomes in three TNBC models than an MCL-1 small molecule inhibitor. These studies provide new structure-function insights on siRNA-lipid conjugate structures that are intravenously injected, associate in situ with serum albumin, and improve pharmacokinetics and tumor treatment efficacy.

Published
2024
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60. Unraveling the genomic underpinnings of unbalanced MYC break-apart FISH results using whole genome sequencing analysis

Author

Marie-France Gagnon, Alan R. Penheiter, Faye Harris, Dorsay Sadeghian, Sarah H. Johnson, Giannoula Karagouga, Alexa McCune, Cinthya Zepeda-Mendoza, Patricia T. Greipp, Xinjie Xu, Rhett P. Ketterling, Ellen D. McPhail, Rebecca L. King, Jess F. Peterson, George Vasmatzis, and Linda B. Baughn

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Published
2023
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61. A new species of Diploschistes ( Lecanoromycetes ) occurring on Stereocaulon from the Pacific Northwest of North America

Author

Helge Thorsten Lumbsch, Bruce McCune, and Claire Morris

Subjects
diploschistes, lichenized fungi, new species, parasitic lichens, stereocaulon, Botany, QK1-989
Abstract

We describe Diploschistes stereocauloru m as a new species of lichenized fungi growing on phyllocladia and stalks of Stereocaulon in the Pacific Northwest of North America. The larger ascospores of this species, the absence of a noticeable thallus, and the ITS barcode locus distinguish it from D. muscorum , which has been reported as growing on Stereocaulon , but has smaller ascospores and a distinct thallus. In phylogenetic reconstruction, the new species is sister to D. diacapsis , albeit without support.

Published
2023
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62. Stereocaulon tomentosoides , a new combination for a western North American endemic species with cyanobiont and chemotype polymorphisms

Author

Bruce McCune, Lucie Vančurová, and Leena Myllys

Subjects
lichens, lichenized fungi, north america, nuits rdna, nulsu rdna, stereocaulaceae, stereocaulon cyaneum, stereocaulon sasakii, stereocaulon tomentosum, Botany, QK1-989
Abstract

Based on resampling the type locality and surrounding regions, along with phylogenetic analysis of molecular data, we elevate Stereocaulon sasakii var. tomentosoides to the species level, while we treat S. sasakii var. simplex as an environmental modification of S. tomentosoide s. We found no phylogenetic evidence that any variety of S. sasakii occurs in North America, so we suggest that the species be removed from the North American list and its North American varieties transferred to S. tomentosoides . Stereocaulon tomentosoides is so far confirmed only from the Pacific Northwest of North America. Furthermore, it is largely allopatric with S. tomentosum , apart from a small region of overlap in northern Idaho and western Montana. While S. tomentosum always contains stictic acid and never lobaric acid as secondary metabolites, S. tomentosoides differs in having a predominant chemotype of lobaric acid as the major substance, with an infrequent chemotype containing both lobaric and stictic acids. While S. tomentosoides usually contains Nostoc in the cephalodia, occasional individuals, especially from old mossy lava flows, contain Stigonema ; one specimen was found with both kinds of cephalodia on a single thallus. Phylogenetic analysis of these species and other close relatives revealed an additional species described here, S. cyaneum , so far known only from the Great Lakes region of the United States and Canada and separated from S. tomentosum by its bluish coloration, wet or dry

Published
2023
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63. The presence of busulfan metabolites and pharmacometabolomics in plasma drawn immediately before allograft infusion in hematopoietic cell transplant recipients

Author

Jeannine S. McCune, Sandi L. Navarro, Linda J. Risler, Brian R. Phillips, Suping Ren, H. Gary Schoch, and K. Scott Baker

Subjects
Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270
Abstract

Abstract Busulfan is hepatically metabolized through glutathione (GSH) conjugation; in vitro, this process depletes hepatocyte GSH stores and generates the cytotoxic metabolite γ‐glutamyldehydroalanylglycine, which is too unstable to be quantitated in vivo. We sought to evaluate if pre‐graft (i.e., immediately before allograft infusion) concentrations of busulfan metabolites' and of endogenous metabolomic compounds (EMCs) representing the glutathione pathway were associated with clinical outcomes in hematopoietic cell transplant (HCT) recipients receiving busulfan. The clinical outcomes evaluated were relapse, acute graft versus host disease (GVHD), chronic GVHD, non‐relapse mortality, and neutrophil nadir. In pre‐graft samples obtained from patients immediately before allograft infusion, our objectives were to evaluate for: (1) the presence of busulfan and its metabolites tetrahydrothiophenium ion (THT+), tetrahydrothiophene 1‐oxide, sulfolane, and 3‐hydroxysulfolane (N = 124); (2) EMCs using a global metabolomics assay (N = 77); and (3) the association of the busulfan metabolites and the EMCs with clinical outcomes. In the pre‐graft samples, busulfan and THT+ could not be detected. THT 1‐oxide, sulfolane, and 3‐hydroxysulfolane were quantitated in 9.6%, 26%, and 58% of pre‐graft samples; their concentrations were not associated with clinical outcomes. Four pre‐graft EMCs were statistically significantly associated with the neutrophil nadir. The pre‐graft EMCs were not associated with the other clinical outcomes. In conclusion, busulfan's metabolites are present in patients' plasma immediately before allograft infusion; the neutrophil nadir is associated with pre‐graft EMCs. Future research should investigate the association of clinical outcomes with the concentrations of busulfan's metabolites and EMCs in the pre‐graft plasma from allogeneic HCT recipients.

Published
2023
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64. Long-term memory of experienced jays facilitates problem-solving by naïve group members in the wild

Author

Hyein Jo, Kelsey B. McCune, Piotr G. Jablonski, and Sang‑im Lee

Subjects
Medicine, Science
Abstract

Abstract Long-term memory affects animal fitness, especially in social species. In these species, the memory of group members facilitates the acquisition of novel foraging skills through social learning when naïve individuals observe and imitate the successful foraging behavior. Long-term memory and social learning also provide the framework for cultural behavior, a trait found in humans but very few other animal species. In birds, little is known about the duration of long-term memories for complex foraging skills, or the impact of long-term memory on group members. We tested whether wild jays remembered a complex foraging task more than 3 years after their initial experience and quantified the effect of this memory on naïve jay behavior. Experienced jays remembered how to solve the task and their behavior had significant positive effects on interactions by naïve group members at the task. This suggests that natural selection may favor long-term memory of solutions to foraging problems to facilitate the persistence of foraging skills that are specifically useful in the local environment in social birds with long lifespans and overlapping generations.

Published
2023
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69. Computational Concepts, Practices, and Perspectives in K-8 Computer Science Teaching Readiness

Author

McCune, Jacqueline Christiane

Abstract

The purpose of this qualitative descriptive study was to understand how K-8 teachers in Nevada describe computational concepts, practices, and perspectives preparation in making them ready to teach computer science. Brennan and Resnick's computational thinking served as the theoretical framework for this study. Four research questions guided this study: (1) How do K-8 teachers in Nevada describe computational concepts in making them ready to teach computer science?; (2) How do K-8 teachers in Nevada describe computational practices in making them ready to teach computer science?; (3) How do K-8 teachers in Nevada describe computational perspectives in making them ready to teach computer science?; and (4) How do K-8 teachers in Nevada describe the "collective" role of computational concepts, practices, and perspectives in making them ready to teach computer science? Data was collected via questionnaire (n = 41) and semi-structured interviews (n = 16). The sample included licensed K-8 teachers in Nevada who completed computational thinking or computer science professional development. Nine themes were identified through thematic analysis: (1) building conceptual understanding; (2) understanding computational thinking; (3) skills in computer science; (4) confusion between EdTech and computer science; (5) beliefs/feelings about computer science; (6) computational perspectives in computer science; (7) connections and influences of computer science education; (8) preparation to teach computer science; and (9) describing computer science education. Study findings suggest that K-8 teachers have some conceptual knowledge, but fall behind in pedagogical knowledge, which contributes to refinement of teacher programs to increase computer science teaching readiness. [The dissertation citations contained here are published with the permission of ProQuest LLC. Further reproduction is prohibited without permission. Copies of dissertations may be obtained by Telephone (800) 1-800-521-0600. Web page: http://www.proquest.com/en-US/products/dissertations/individuals.shtml.]

Published
2023

70. Teaching Wicked Problems in Higher Education: Ways of Thinking and Practising

Author

McCune, Velda, Tauritz, Rebekah, Boyd, Sharon, Cross, Andrew, Higgins, Peter, and Scoles, Jenny

Abstract

This paper reports on teachers' perspectives on preparing students for working with 'wicked' problems (Rittel and Webber [1973]. 'Dilemmas in a General Theory of Planning.' "Policy Sciences" 4 (2): 155-169.). These problems are complex, lack clear boundaries, and attempts to solve them -- generally by bringing together multiple stakeholders with contrasting viewpoints -- have unforeseen consequences. Examples include many of the most significant current global challenges. We conducted semi-structured interviews with twenty teachers who focused on wicked problems, and a comparison group of 15 . We used the theoretical lenses 'ways of thinking and practising in the subject area' (Anderson and Hounsell [2007]. 'Knowledge Practices: 'Doing the Subject' in Undergraduate Courses.' "The Curriculum Journal" 18 (4): 463-478. ) and 'figured worlds' (Holland et al. [1998]. "Identity and Agency in Cultural Worlds." Cambridge, MA: Harvard University Press.) to frame our analysis. Our findings elaborate four key aspects of learning for wicked problems.

Published
2023
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71. Exploring Alternative Ways to Allocate Delegates

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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72. Paradoxes

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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73. Apportionment in the US Presidential Primaries

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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74. The Democratic Party Primary

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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75. The Republican Party Primary

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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76. Properties of the Apportionment Methods Used in the Primaries

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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77. The Iowa and Nevada Democratic Caucuses

Author

Jones, Michael A., McCune, David, Wilson, Jennifer M., Fleurbaey, Marc, Editor-in-Chief, Salles, Maurice, Editor-in-Chief, Dutta, Bhaskar, Series Editor, Gaertner, Wulf, Series Editor, Herrero Blanco, Carmen, Series Editor, Klaus, Bettina, Series Editor, Pattanaik, Prasanta K., Series Editor, Thomson, William, Series Editor, Jones, Michael A., McCune, David, and Wilson, Jennifer M.

Published
2023
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81. Stereotactic Body Radiation Therapy for Stage IIA to IIIA Inoperable Non-Small Cell Lung Cancer: A Phase 1 Dose-Escalation Trial

Author

Rimner, Andreas, Gelblum, Daphna Y., Wu, Abraham J., Shepherd, Annemarie F., Mueller, Boris, Zhang, Siyuan, Cuaron, John, Shaverdian, Narek, Flynn, Jessica, Fiasconaro, Megan, Zhang, Zhigang, von Reibnitz, Donata, Li, Henry, McKnight, Dominique, McCune, Megan, Gelb, Emily, Gomez, Daniel R., Simone, Charles B., II, Deasy, Joseph O., Yorke, Ellen D., Ng, Kenneth K., and Chaft, Jamie E.

Published
2024
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84. Bacillus Calmette-Guérin vaccination as defense against SARS-CoV-2 (BADAS): a randomized controlled trial to protect healthcare workers in the USA by enhanced trained immune responses

Author

DiNardo, Andrew R., Arditi, Moshe, Kamat, Ashish M., Koster, Kent J., Carrero, Santiago, Nishiguchi, Tomoki, Lebedev, Maxim, Benjamin, Aaron B., Avalos, Pablo, Lozano, Marisa, Moule, Madeleine G., McCune, Brittany, Herron, Baysia, Ladki, Malik, Sheikh, Daanish, Spears, Matthew, Herrejon, Ivan A., Dodge, Courtney, Kumar, Sathish, Hutchison, Robert W., Ofili, Theresa U., Opperman, Lynne A., Bernard, Jessica A., Lerner, Seth P., Udeani, George, Neal, Gabriel, Netea, Mihai G., and Cirillo, Jeffrey D.

Published
2023
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86. Interferons and tuft cell numbers are bottlenecks for persistent murine norovirus infection.

Author

Somya Aggarwal, Forrest C Walker, James S Weagley, Broc T McCune, Xiaofen Wu, Lawrence A Schriefer, Heyde Makimaa, Dylan Lawrence, Pratyush Sridhar, and Megan T Baldridge

Subjects
Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5
Abstract

Noroviruses (NoVs) are a leading cause of viral gastroenteritis. Despite global clinical relevance, our understanding of how host factors, such as antiviral cytokines interferons (IFNs), modulate NoV population dynamics is limited. Murine NoV (MNoV) is a tractable in vivo model for the study of host regulation of NoV. A persistent strain of MNoV, CR6, establishes a reservoir in intestinal tuft cells for chronic viral shedding in stool. However, the influence of host innate immunity and permissive cell numbers on viral population dynamics is an open question. We generated a pool of 20 different barcoded viruses (CR6BC) by inserting 6-nucleotide barcodes at the 3' position of the NS4 gene and used this pool as our viral inoculum for in vivo infections of different mouse lines. We found that over the course of persistent CR6 infection, shed virus was predominantly colon-derived, and viral barcode richness decreased over time irrespective of host immune status, suggesting that persistent infection involves a series of reinfection events. In mice lacking the IFN-λ receptor, intestinal barcode richness was enhanced, correlating with increased viral intestinal replication. IL-4 treatment, which increases tuft cell numbers, also increased barcode richness, indicating the abundance of permissive tuft cells to be a bottleneck during CR6 infection. In mice lacking type I IFN signaling (Ifnar1-/-) or all IFN signaling (Stat1-/-), barcode diversity at extraintestinal sites was dramatically increased, implicating different IFNs as critical bottlenecks at specific tissue sites. Of interest, extraintestinal barcodes were overlapping but distinct from intestinal barcodes, indicating that disseminated virus represents a distinct viral population than that replicating in the intestine. Barcoded viruses are a valuable tool to explore the influence of host factors on viral diversity in the context of establishment and maintenance of infection as well as dissemination and have provided important insights into how NoV infection proceeds in immunocompetent and immunocompromised hosts.

Published
2024
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87. Erratum to: Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner?

Author

Justiin Harper, Michael Betts, Mathias Lichterfeld, Michaela Müller-Trutwin, David Margolis, Katharine Bar, Jonathan Li, Joseph McCune, Sharon Lewin, Deanna Kulpa, Santiago Ávila-Ríos, Dázon Diallo, Michael Lederman, and Mirko Paiardini

Subjects
HIV, SIV, reservoir, persistence, ART, HIV cure, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607
Abstract

Erratum to: Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner? doi: 10.20411/pai.v8i2.665 In the original publication, the comments provided by Santiago Ávila-Ríos were mistakenly omitted. In this version, his comments are included in the “Comments by Leaders” section, and his name has been included in the list of authors. --- Once a death sentence, HIV is now considered a manageable chronic disease due to the development of antiretroviral therapy (ART) regimens with minimal toxicity and a high barrier for genetic resistance. While highly effective in arresting AIDS progression and rendering the virus untransmissible in people living with HIV (PLWH) with undetectable viremia (U=U) [1, 2]), ART alone is incapable of eradicating the “reservoir” of resting, latently infected CD4+ T cells from which virus recrudesces upon treatment cessation. As of 2022 estimates, there are 39 million PLWH, of whom 86% are aware of their status and 76% are receiving ART [3]. As of 2017, ART-treated PLWH exhibit near normalized life expectancies without adjustment for socioeconomic differences [4]. Furthermore, there is a global deceleration in the rate of new infections [3] driven by expanded access to pre-exposure prophylaxis (PrEP), HIV testing in vulnerable populations, and by ART treatment [5]. Therefore, despite outstanding issues pertaining to cost and access in developing countries, there is strong enthusiasm that aggressive testing, treatment, and effective viral suppression may be able to halt the ongoing HIV epidemic (ie, UNAIDS’ 95-95-95 targets) [6–8]; especially as evidenced by recent encouraging observations in Sydney [9]. Despite these promising efforts to limit further viral transmission, for PLWH, a “cure” remains elusive; whether it be to completely eradicate the viral reservoir (ie, cure) or to induce long-term viral remission in the absence of ART (ie, control; Figure 1). In a previous salon hosted by Pathogens and Immunity in 2016 [10], some researchers were optimistic that a cure was a feasible, scalable goal, albeit with no clear consensus on the best route. So, how are these cure strategies panning out? In this commentary, 8 years later, we will provide a brief overview on recent advances and failures towards identifying determinants of viral persistence and developing a scalable cure for HIV. Based on these observations, and as in the earlier salon, we have asked several prominent HIV cure researchers for their perspectives.

Published
2024
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88. Progress Note 2024: Curing HIV; Not in My Lifetime or Just Around the Corner?

Author

Justin Harper, Michael Betts, Mathias Lichterfeld, Michaela Müller-Trutwin, David Margolis, Katharine Bar, Jonathan Li, Joseph McCune, Sharon Lewin, Deanna Kulpa, Dázon Diallo, Michael M. Lederman, and Mirko Paiardini

Subjects
HIV, SIV, reservoir, persistence, ART, HIV cure, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607
Abstract

Once a death sentence, HIV is now considered a manageable chronic disease due to the development of antiretroviral therapy (ART) regimens with minimal toxicity and a high barrier for genetic resistance. While highly effective in arresting AIDS progression and rendering the virus untransmissible in people living with HIV (PLWH) with undetectable viremia (U=U) [1, 2]), ART alone is incapable of eradicating the “reservoir” of resting, latently infected CD4+ T cells from which virus recrudesces upon treatment cessation. As of 2022 estimates, there are 39 million PLWH, of whom 86% are aware of their status and 76% are receiving ART [3]. As of 2017, ART-treated PLWH exhibit near normalized life expectancies without adjustment for socioeconomic differences [4]. Furthermore, there is a global deceleration in the rate of new infections [3] driven by expanded access to pre-exposure prophylaxis (PrEP), HIV testing in vulnerable populations, and by ART treatment [5]. Therefore, despite outstanding issues pertaining to cost and access in developing countries, there is strong enthusiasm that aggressive testing, treatment, and effective viral suppression may be able to halt the ongoing HIV epidemic (ie, UNAIDS’ 95-95-95 targets) [6–8]; especially as evidenced by recent encouraging observations in Sydney [9]. Despite these promising efforts to limit further viral transmission, for PLWH, a “cure” remains elusive; whether it be to completely eradicate the viral reservoir (ie, cure) or to induce long-term viral remission in the absence of ART (ie, control; Figure 1). In a previous salon hosted by Pathogens and Immunity in 2016 [10], some researchers were optimistic that a cure was a feasible, scalable goal, albeit with no clear consensus on the best route. So, how are these cure strategies panning out? In this commentary, 8 years later, we will provide a brief overview on recent advances and failures towards identifying determinants of viral persistence and developing a scalable cure for HIV. Based on these observations, and as in the earlier salon, we have asked several prominent HIV cure researchers for their perspectives.

Published
2024
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89. IFNα-blockade during ART-treated SIV infection lowers tissue vDNA, rescues immune function, and improves overall health

Author

Swainson, Louise A, Sharma, Ashish Arunkumar, Ghneim, Khader, Ribeiro, Susan Pereira, Wilkinson, Peter, Dunham, Richard M, Albright, Rebecca G, Wong, Samson, Estes, Jacob D, Piatak, Michael, Deeks, Steven G, Hunt, Peter W, Sekaly, Rafick-Pierre, and McCune, Joseph M

Subjects
Genetics, HIV/AIDS, Infectious Diseases, Hematology, Inflammatory and immune system, Infection, Animals, Anti-Retroviral Agents, DNA, Viral, HIV Infections, Immunity, Interferon-alpha, Macaca mulatta, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, Weight Loss, Simian immunodeficiency virus, AIDS/HIV, Immunology, Immunotherapy
Abstract

Type I IFNs (TI-IFNs) drive immune effector functions during acute viral infections and regulate cell cycling and systemic metabolism. That said, chronic TI-IFN signaling in the context of HIV infection treated with antiretroviral therapy (ART) also facilitates viral persistence, in part by promoting immunosuppressive responses and CD8+ T cell exhaustion. To determine whether inhibition of IFN-α might provide benefit in the setting of chronic, ART-treated SIV infection of rhesus macaques, we administered an anti-IFN-α antibody followed by an analytical treatment interruption (ATI). IFN-α blockade was well-tolerated and associated with lower expression of TI-IFN-inducible genes (including those that are antiviral) and reduced tissue viral DNA (vDNA). The reduction in vDNA was further accompanied by higher innate proinflammatory plasma cytokines, expression of monocyte activation genes, IL-12-induced effector CD8+ T cell genes, increased heme/metabolic activity, and lower plasma TGF-β levels. Upon ATI, SIV-infected, ART-suppressed nonhuman primates treated with anti-IFN-α displayed lower levels of weight loss and improved erythroid function relative to untreated controls. Overall, these data demonstrated that IFN-α blockade during ART-treated SIV infection was safe and associated with the induction of immune/erythroid pathways that reduced viral persistence during ART while mitigating the weight loss and anemia that typically ensue after ART interruption.

Published
2022

90. Co‐consuming green tea with raloxifene decreases raloxifene systemic exposure in healthy adult participants

Author

John D. Clarke, Sabrina M. Judson, Dan‐Dan Tian, Trevor O. Kirby, Rakshit S. Tanna, Adrienn Matula‐Péntek, Miklós Horváth, Matthew E. Layton, John R. White, Nadja B. Cech, Kenneth E. Thummel, Jeannine S. McCune, Danny D. Shen, and Mary F. Paine

Subjects
Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270
Abstract

Abstract Green tea is a popular beverage worldwide. The abundant green tea catechin (−)‐epigallocatechin gallate (EGCG) is a potent in vitro inhibitor of intestinal UDP‐glucuronosyltransferase (UGT) activity (Ki ~2 μM). Co‐consuming green tea with intestinal UGT drug substrates, including raloxifene, could increase systemic drug exposure. The effects of a well‐characterized green tea on the pharmacokinetics of raloxifene, raloxifene 4′‐glucuronide, and raloxifene 6‐glucuronide were evaluated in 16 healthy adults via a three‐arm crossover, fixed‐sequence study. Raloxifene (60 mg) was administered orally with water (baseline), with green tea for 1 day (acute), and on the fifth day after daily green tea administration for 4 days (chronic). Unexpectedly, green tea decreased the geometric mean green tea/baseline raloxifene AUC0–96h ratio to ~0.60 after both acute and chronic administration, which is below the predefined no‐effect range (0.75–1.33). Lack of change in terminal half‐life and glucuronide‐to‐raloxifene ratios indicated the predominant mechanism was not inhibition of intestinal UGT. One potential mechanism includes inhibition of intestinal transport. Using established transfected cell systems, a green tea extract normalized to EGCG inhibited 10 of 16 transporters tested (IC50, 0.37–12 μM). Another potential mechanism, interruption by green tea of gut microbe‐mediated raloxifene reabsorption, prompted a follow‐up exploratory clinical study to evaluate the potential for a green tea–gut microbiota–drug interaction. No clear mechanisms were identified. Overall, results highlight that improvements in current models and methods used to predict UGT‐mediated drug interactions are needed. Informing patients about the risk of co‐consuming green tea with raloxifene may be considered.

Published
2023
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91. Estimating the contribution of CD4 T cell subset proliferation and differentiation to HIV persistence

Author

Daniel B. Reeves, Charline Bacchus-Souffan, Mark Fitch, Mohamed Abdel-Mohsen, Rebecca Hoh, Haelee Ahn, Mars Stone, Frederick Hecht, Jeffrey Martin, Steven G. Deeks, Marc K. Hellerstein, Joseph M. McCune, Joshua T. Schiffer, and Peter W. Hunt

Subjects
Science
Abstract

Abstract Persistence of HIV in people living with HIV (PWH) on suppressive antiretroviral therapy (ART) has been linked to physiological mechanisms of CD4+ T cells. Here, in the same 37 male PWH on ART we measure longitudinal kinetics of HIV DNA and cell turnover rates in five CD4 cell subsets: naïve (TN), stem-cell- (TSCM), central- (TCM), transitional- (TTM), and effector-memory (TEM). HIV decreases in TTM and TEM but not in less-differentiated subsets. Cell turnover is ~10 times faster than HIV clearance in memory subsets, implying that cellular proliferation consistently creates HIV DNA. The optimal mathematical model for these integrated data sets posits HIV DNA also passages between CD4 cell subsets via cellular differentiation. Estimates are heterogeneous, but in an average participant’s year ~10 (in TN and TSCM) and ~104 (in TCM, TTM, TEM) proviruses are generated by proliferation while ~103 proviruses passage via cell differentiation (per million CD4). In simulations, therapies blocking proliferation and/or enhancing differentiation could reduce HIV DNA by 1-2 logs over 3 years. In summary, HIV exploits cellular proliferation and differentiation to persist during ART but clears faster in more proliferative/differentiated CD4 cell subsets and the same physiological mechanisms sustaining HIV might be temporarily modified to reduce it.

Published
2023
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92. Bacillus Calmette-Guérin vaccination as defense against SARS-CoV-2 (BADAS): a randomized controlled trial to protect healthcare workers in the USA by enhanced trained immune responses

Author

Andrew R. DiNardo, Moshe Arditi, Ashish M. Kamat, Kent J. Koster, Santiago Carrero, Tomoki Nishiguchi, Maxim Lebedev, Aaron B. Benjamin, Pablo Avalos, Marisa Lozano, Madeleine G. Moule, Brittany McCune, Baysia Herron, Malik Ladki, Daanish Sheikh, Matthew Spears, Ivan A. Herrejon, Courtney Dodge, Sathish Kumar, Robert W. Hutchison, Theresa U. Ofili, Lynne A. Opperman, Jessica A. Bernard, Seth P. Lerner, George Udeani, Gabriel Neal, Mihai G. Netea, and Jeffrey D. Cirillo

Subjects
COVID-19, Randomized controlled trial, BCG vaccination, Immune training, Pandemic, Healthcare workers, Medicine (General), R5-920
Abstract

Abstract Background A large epidemic, such as that observed with SARS-CoV-2, seriously challenges available hospital capacity, and this would be augmented by infection of healthcare workers (HCW). Bacillus Calmette-Guérin (BCG) is a vaccine against tuberculosis, with protective non-specific effects against other respiratory tract infections in vitro and in vivo. Preliminary analyses suggest that regions of the world with existing BCG vaccination programs have lower incidence and mortality from COVID-19. We hypothesize that BCG vaccination can reduce SARS-CoV-2 infection and disease severity. Methods This will be a placebo-controlled adaptive multi-center randomized controlled trial. A total of 1800 individuals considered to be at high risk, including those with comorbidities (hypertension, diabetes, obesity, reactive airway disease, smokers), racial and ethnic minorities, elderly, teachers, police, restaurant wait-staff, delivery personnel, health care workers who are defined as personnel working in a healthcare setting, at a hospital, medical center or clinic (veterinary, dental, ophthalmology), and first responders (paramedics, firefighters, or law enforcement), will be randomly assigned to two treatment groups. The treatment groups will receive intradermal administration of BCG vaccine or placebo (saline) with groups at a 1:1 ratio. Individuals will be tracked for evidence of SARS-CoV-2 infection and severity as well as obtaining whole blood to track immunological markers, and a sub-study will include cognitive function and brain imaging. The majority of individuals will be followed for 6 months, with an option to extend for another 6 months, and the cognitive sub-study duration is 2 years. We will plot Kaplan-Meier curves that will be plotted comparing groups and hazard ratios and p-values reported using Cox proportional hazard models. Discussion It is expected this trial will allow evaluation of the effects of BCG vaccination at a population level in high-risk healthcare individuals through a mitigated clinical course of SARS-CoV-2 infection and inform policy making during the ongoing epidemic. Trial registration ClinicalTrials.gov NCT04348370. Registered on April 16, 2020.

Published
2023
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96. Mycophenolate mofetil withdrawal in patients with systemic lupus erythematosus: a multicentre, open-label, randomised controlled trial

Author

Chakravarty, Eliza F, Utset, Tammy, Kamen, Diane L, Contreras, Gabriel, McCune, W Joseph, Aranow, Cynthia, Kalunian, Kenneth, Massarotti, Elena, Clowse, Megan E B, Rovin, Brad H, Lim, S Sam, Majithia, Vikas, Dall'Era, Maria, Looney, R John, Erkan, Doruk, Saxena, Amit, Olsen, Nancy J, Ko, Kichul, Guthridge, Joel M, Goldmuntz, Ellen, Springer, Jessica, D'Aveta, Carla, Keyes-Elstein, Lynette, Barry, Bill, Pinckney, Ashley, McNamara, James, and James, Judith A

Published
2024
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98. The Muon Smasher's Guide

Author

Ali, Hind Al, Arkani-Hamed, Nima, Banta, Ian, Benevedes, Sean, Buttazzo, Dario, Cai, Tianji, Cheng, Junyi, Cohen, Timothy, Craig, Nathaniel, Ekhterachian, Majid, Fan, JiJi, Forslund, Matthew, Garcia, Isabel Garcia, Homiller, Samuel, Koren, Seth, Koszegi, Giacomo, Liu, Zhen, Lu, Qianshu, Lyu, Kun-Feng, Mariotti, Alberto, McCune, Amara, Meade, Patrick, Ojalvo, Isobel, Oktem, Umut, Redigolo, Diego, Reece, Matthew, Sala, Filippo, Sundrum, Raman, Sutherland, Dave, Tesi, Andrea, Trott, Timothy, Tully, Chris, Wang, Lian-Tao, and Wang, Menghang

Subjects
High Energy Physics - Phenomenology, High Energy Physics - Experiment
Abstract

We lay out a comprehensive physics case for a future high-energy muon collider, exploring a range of collision energies (from 1 to 100 TeV) and luminosities. We highlight the advantages of such a collider over proposed alternatives. We show how one can leverage both the point-like nature of the muons themselves as well as the cloud of electroweak radiation that surrounds the beam to blur the dichotomy between energy and precision in the search for new physics. The physics case is buttressed by a range of studies with applications to electroweak symmetry breaking, dark matter, and the naturalness of the weak scale. Furthermore, we make sharp connections with complementary experiments that are probing new physics effects using electric dipole moments, flavor violation, and gravitational waves. An extensive appendix provides cross section predictions as a function of the center-of-mass energy for many canonical simplified models., Comment: 105 pages, 41 figures, 5 tables

Published
2021
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99. Gaps and Opportunities to Improve Prevention of Human Papillomavirus-Related Cancers.

Author

Aninye, Irene, Berry-Lawhorn, J, Blumenthal, Paul, Felder, Tamika, Jay, Naomi, Merrill, Janette, Messman, Jenna, Nielsen, Sarah, Perkins, Rebecca, Rowen, Tami, Saslow, Debbie, Trimble, Connie, and Smith-McCune, Karen

Subjects
HPV vaccine, anal cancer, cancer screening, cervical cancer, stigma, vaginal cancer, vulvar cancer, Alphapapillomavirus, Female, Humans, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, United States, Uterine Cervical Neoplasms, Vulvar Neoplasms
Abstract

Human papillomavirus (HPV) infections cause more than 35,900 cancers annually in the United States. Although cervical cancer is the most prevalent HPV-related malignancy in women, the virus is also responsible for a significant percentage of anal, vaginal, and vulvar cancers. A comprehensive approach to mitigating cervical cancer includes HPV vaccination (primary prevention), screening and treatment of precancerous lesions (secondary prevention), and diagnosis and treatment of invasive cancer (tertiary prevention). Although a successful strategy, there are opportunities to innovate and increase access that can also be adapted to address the unique clinical care gaps that exist with the other anogenital cancers. The Society for Womens Health Research held a series of interdisciplinary meetings and events, during which expert researchers, clinicians, patient advocates, and health care policy leaders evaluated the current landscape of HPV-related cancers and their effects on womens health. This report summarizes the discussions of this working group and areas it identified in which to address gaps in primary and secondary prevention approaches to improve access and health outcomes for women with HPV-related anogenital cancers.

Published
2021

100. P not PQ

Author

Craig, Nathaniel, Garcia, Isabel Garcia, Koszegi, Giacomo, and McCune, Amara

Subjects
High Energy Physics - Phenomenology, High Energy Physics - Experiment, High Energy Physics - Theory
Abstract

Parity solutions to the strong CP problem are a compelling alternative to approaches based on Peccei-Quinn symmetry, particularly given the expected violation of global symmetries in a theory of quantum gravity. The most natural of these solutions break parity at a low scale, giving rise to a host of experimentally accessible signals. We assess the status of the simplest parity-based solution in light of LHC data and flavor constraints, highlighting the prospects for near-future tests at colliders, tabletop experiments, and gravitational wave observatories. The origin of parity breaking and associated gravitational effects play crucial roles, providing new avenues for discovery through EDMs and gravity waves. These experimental opportunities underline the promise of generalized parity, rather than Peccei-Quinn symmetry, as a robust and testable solution to the strong CP problem.

Published
2020
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