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1. First Case of HIV Seroconversion With Integrase Resistance Mutations on Long-Acting Cabotegravir for Prevention in Routine Care

Author

Koss, Catherine A, Gandhi, Monica, Halvas, Elias K, Okochi, Hideaki, Chu, Carolyn, Glidden, David V, Gomez, Lisa Georgetti, Heaps, Amy L, Conroy, Amy A, Tran, Michael, Shetler, Cory, Hoeth, Dianna, Kuncze, Karen, Louie, Alexander, Garza, Hana Rivera, Mugoma, Erick Wafula, Penrose, Kerri J, Chohan, Bhavna H, Ayieko, James O, Mills, Anthony, Patel, Rupa R, Mellors, John W, and Parikh, Urvi M

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Infectious Diseases, Women's Health, Sexually Transmitted Infections, Genetics, HIV/AIDS, Prevention, Infection, Good Health and Well Being, breakthrough infection, HIV prevention, pharmacokinetics, pre-exposure prophylaxis, resistance, Clinical sciences, Medical microbiology
Abstract

BackgroundLong-acting cabotegravir (CAB-LA) is highly effective for HIV prevention, but delayed HIV diagnoses and integrase strand transfer inhibitor (INSTI) resistance were observed in trials. We report the first case in routine clinical care of HIV infection on CAB-LA with INSTI resistance.MethodsThe SeroPrEP study enrolls individuals in the United States who acquire HIV on pre-exposure prophylaxis modalities to assess diagnostics, antiretroviral (ARV) drug levels, resistance, and treatment outcomes. Resistance mutations in full-length HIV-1 integrase were identified by single-genome sequencing (SGS). Cabotegravir concentrations in plasma and hair segments were measured by liquid chromatography-tandem mass spectrometry.ResultsA 23-year-old gender-nonbinary person, male at birth, restarted CAB-LA 6 months after discontinuation due to losing insurance. Prior to restart, HIV-1 RNA was not detected, but 20 days elapsed before CAB-LA injection. After the second CAB-LA injection, HIV antigen/antibody returned reactive (HIV-1 RNA 451 copies/mL). SGS of plasma HIV-1 RNA identified INSTI mutation Q148R in 2/24 sequences 2 days postdiagnosis; commercial genotype failed amplification. Cabotegravir hair concentration was 0.190 ng/mg 2 weeks prediagnosis; plasma cabotegravir was high (3.37 μg/mL; ∼20× PA-IC90) 14 days postdiagnosis. Viral suppression was maintained for 6 months on darunavir/cobicistat/emtricitabine/tenofovir alafenamide, then switched to doravirine + emtricitabine/tenofovir alafenamide due to nausea.ConclusionsIn this first case of HIV infection on CAB-LA with INSTI resistance in routine care, cabotegravir resistance was detected only with a sensitive research assay. Accelerated pathways to minimize time between HIV testing and CAB-LA initiation are needed to optimize acute HIV detection and mitigate resistance risk. Sustained product access regardless of insurance is imperative to reduce HIV infections on CAB-LA.

Published
2024

2. Cytokine-mediated CAR T therapy resistance in AML

Author

Bhagwat, Anand S., Torres, Leonel, Shestova, Olga, Shestov, Maksim, Mellors, Patrick W., Fisher, Han R., Farooki, Saamia N., Frost, Benjamin F., Loken, Michael R., Gaymon, Avery L., Frazee, Diane, Rogal, Walter, Frey, Noelle, Hexner, Elizabeth O., Luger, Selina M., Loren, Alison W., Martin, Mary Ellen, McCurdy, Shannon R., Perl, Alexander E., Stadtmauer, Edward A., Brogdon, Jennifer L., Fraietta, Joseph A., Hwang, Wei-Ting, Siegel, Don L., Plesa, Gabriela, Aplenc, Richard, Porter, David L., June, Carl H., and Gill, Saar I.

Published
2024
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3. Predictors of HIV rebound differ by timing of antiretroviral therapy initiation

Author

Li, Jonathan Z, Melberg, Meghan, Kittilson, Autumn, Abdel-Mohsen, Mohamed, Li, Yijia, Aga, Evgenia, Bosch, Ronald J, Wonderlich, Elizabeth R, Kinslow, Jennifer, Giron, Leila B, Di Germanio, Clara, Pilkinton, Mark, MacLaren, Lynsay, Keefer, Michael, Fox, Lawrence, Barr, Liz, Acosta, Edward, Ananworanich, Jintanat, Coombs, Robert, Mellors, John, Deeks, Steven, Gandhi, Rajesh T, Busch, Michael, Landay, Alan, Macatangay, Bernard, Smith, Davey M, and Team, for the AIDS Clinical Trials Group A5345 Study

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Pediatric, Infectious Diseases, Clinical Research, Clinical Trials and Supportive Activities, Pediatric AIDS, HIV/AIDS, Infection, Good Health and Well Being, Humans, HIV Infections, Proviruses, CD8-Positive T-Lymphocytes, Viral Load, DNA, AIDS Clinical Trials Group A5345 Study Team, AIDS vaccine, AIDS/HIV, Adaptive immunity, Biomedical and clinical sciences, Health sciences
Abstract

BACKGROUNDIdentifying factors that predict the timing of HIV rebound after treatment interruption will be crucial for designing and evaluating interventions for HIV remission.METHODSWe performed a broad evaluation of viral and immune factors that predict viral rebound (AIDS Clinical Trials Group A5345). Participants initiated antiretroviral therapy (ART) during chronic (N = 33) or early (N = 12) HIV infection with ≥ 2 years of suppressive ART and restarted ART if they had 2 viral loads ≥ 1,000 copies/mL after treatment interruption.RESULTSCompared with chronic-treated participants, early-treated individuals had smaller and fewer transcriptionally active HIV reservoirs. A higher percentage of HIV Gag-specific CD8+ T cell cytotoxic response was associated with lower intact proviral DNA. Predictors of HIV rebound timing differed between early- versus chronic-treated participants, as the strongest reservoir predictor of time to HIV rebound was level of residual viremia in early-treated participants and intact DNA level in chronic-treated individuals. We also identified distinct sets of pre-treatment interruption viral, immune, and inflammatory markers that differentiated participants who had rapid versus slow rebound.CONCLUSIONThe results provide an in-depth overview of the complex interplay of viral, immunologic, and inflammatory predictors of viral rebound and demonstrate that the timing of ART initiation modifies the features of rapid and slow viral rebound.TRIAL REGISTRATIONClinicalTrials.gov NCT03001128FUNDINGNIH National Institute of Allergy and Infectious Diseases, Merck.

Published
2024

4. Comparison Study of the Bio-Plex and Meso Scale Multiplexed SARS-CoV-2 Serology Assays Reveals Evidence of Diminished Host Antibody Responses to SARS-CoV-2 after Monoclonal Antibody Treatment

Author

Parikh, Urvi M, Heaps, Amy L, Moisi, Daniela, Gordon, Kelley C, Mellors, John W, Choudhary, Manish C, Deo, Rinki, Moser, Carlee, Klekotka, Paul, Landay, Alan L, Currier, Judith S, Eron, Joseph J, Chew, Kara W, Smith, Davey M, Li, Jonathan Z, Sieg, Scott F, and Study, Team ACTIV-2 A5401

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Biodefense, Immunization, Prevention, Clinical Research, Vaccine Related, Emerging Infectious Diseases, Coronaviruses, Infectious Diseases, Biotechnology, Infection, Good Health and Well Being, Team ACTIV-2/A5401 Study, Bio-Plex, COVID, COVID-19, Meso Scale Discovery, SARS-CoV-2, bamlanivimab, monoclonal antibodies, Clinical sciences, Immunology, Medical microbiology
Abstract

BackgroundAssessing the breadth and duration of antigen-specific binding antibodies provides valuable information for evaluating interventions to treat or prevent SARS-CoV-2 infection. Multiplex immunoassays are a convenient method for rapid measurement of antibody responses but can sometimes provide discordant results, and antibody positive percent agreement for COVID-19 diagnosis can vary depending on assay type, disease severity, and population sampled. Therefore, we compared two assays marked for research applications, MSD and Bio-Plex Pro, to evaluate qualitative interpretation of serostatus and quantitative detection of antibodies of varying isotypes (IgG, IgM, and IgA) against receptor binding domain (RBD) and nucleocapsid (N) antigens.MethodsSpecimens from ACTIV-2/A5401, a placebo-controlled clinical trial of the SARSCoV-2 monoclonal antibody (mAb) bamlanivimab to prevent COVID-19 disease progression, were used to evaluate the concordance of the Bio-Rad Bio-Plex Pro Human SARS-CoV-2 Serology Assay and the Meso Scale Discovery (MSD) V-PLEX COVID-19 Panel 1 serology assay in detecting and quantifying IgG, IgA, and IgM binding anti-SARS-CoV-2 antibody responses against the RBD and N antigens. Data were disaggregated by study arm, bamlanivimab dose, days post-enrollment, and presence of emerging resistance.ResultsWe observed 90.5% (412 of 455 tests) concordance for anti-RBD IgG and 87% (396 of 455) concordance for anti-N IgG in classifying samples as negative or positive based on assay-defined cutoffs. Antibody levels converted to the WHO standard BAU/mL were significantly correlated for all isotypes (IgG, IgM, and IgA) and SARS-CoV-2 antigen targets (RBD and N) tested that were common between the two assays (Spearman r 0.65 to 0.92, P < 0.0001). Both assays uncovered evidence of diminished host-derived IgG immune responses in participants treated with bamlanivimab compared to placebo. Assessment of immune responses in the four individuals treated with the 700 mg of bamlanivimab with emerging mAb resistance demonstrated a stronger anti-N IgG response (MSD) at day 28 (median 2.18 log BAU/mL) compared to participants treated with bamlanivimab who did not develop resistance (median 1.55 log BAU/mL).ConclusionsThese data demonstrate the utility in using multiplex immunoassays for characterizing the immune responses with and without treatment in a study population and provide evidence that monoclonal antibody treatment in acute COVID-19 may have a modest negative impact on development of host IgG responses.

Published
2024

5. Impact of SARS-CoV-2 Resistance to Antiviral Monoclonal Antibody Therapy on Neutralizing Antibody Response

Author

Paul, Marc-Kendy, Choudhary, Manish C, Heaps, Amy L, Deo, Rinki, Moisi, Daniela, Gordon, Kelley C, Mellors, John W, Moser, Carlee, Klekotka, Paul, Landay, Alan, Currier, Judith S, Eron, Joseph J, Chew, Kara W, Smith, Davey M, Sieg, Scott F, Parikh, Urvi M, Li, Jonathan Z, and Team, on behalf of the ACTIV-2 A5401 Study

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Biotechnology, Clinical Research, Biodefense, Immunization, Coronaviruses Therapeutics and Interventions, Clinical Trials and Supportive Activities, Coronaviruses, Emerging Infectious Diseases, Antimicrobial Resistance, Infectious Diseases, Vaccine Related, Genetics, 5.2 Cellular and gene therapies, Infection, Good Health and Well Being, ACTIV-2/A5401 Study Team, COVID-19, SARS-CoV-2, bamlanivimab, monoclonal antibody, pseudovirus neutralization, Clinical sciences, Medical microbiology
Abstract

BackgroundAnti-SARS-CoV-2 monoclonal antibodies (mAbs) have played a key role as an anti-viral against SARS-CoV-2, but there is a potential for resistance to develop. The interplay between host antibody responses and the development of monoclonal antibody (mAb) resistance is a critical area of investigation. In this study, we assessed host neutralizing antibody (nAb) responses against both ancestral virus and those with treatment-emergent E484K bamlanivimab resistance mutations.MethodsStudy participants were enrolled in the ACTIV-2/Advancing Clinical Therapeutics Globally (ACTG) A5401 phase 2 randomized, placebo-controlled trial of bamlanivimab 700 mg mAb therapy (NCT04518410). Anterior nasal and nasopharyngeal swabs were collected for SARS-CoV-2 RNA testing and S gene next-generation sequencing to identify the E484K bamlanivimab resistance mutation. Serum nAb titers were assessed by pseudovirus neutralization assays.ResultsHigher baseline (pre-treatment) nAb titers against either ancestral or E484K virus was associated with lower baseline viral load. Participants with emerging resistance had low levels of nAb titers against either ancestral or E484K nAb at the time of study entry. Participants with emergent E484K resistance developed significantly higher levels of E484K-specific nAb titers compared to mAb-treated individuals who did not develop resistance. All participants who developed the E484K mAb resistance mutation were eventually able to clear the virus.ConclusionEmerging drug resistance after SARS-CoV-2-specific mAb therapy led to a heightened host neutralizing antibody response to the mAb-resistant variant that was associated with eventual viral clearance. This demonstrates the interplay between the antiviral treatment-directed viral evolution and subsequent host immune response in viral clearance.

Published
2024

6. Serological analysis in humans in Malaysian Borneo suggests prior exposure to H5 avian influenza near migratory shorebird habitats

Author

Klim, Hannah, William, Timothy, Mellors, Jack, Brady, Caolann, Rajahram, Giri S., Chua, Tock H., Brazal Monzó, Helena, John, Jecelyn Leslie, da Costa, Kelly, Jeffree, Mohammad Saffree, Temperton, Nigel J., Tipton, Tom, Thompson, Craig P., Ahmed, Kamruddin, Drakeley, Chris J., Carroll, Miles W., and Fornace, Kimberly M.

Published
2024
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9. Serological analysis in humans in Malaysian Borneo suggests prior exposure to H5 avian influenza near migratory shorebird habitats

Author

Hannah Klim, Timothy William, Jack Mellors, Caolann Brady, Giri S. Rajahram, Tock H. Chua, Helena Brazal Monzó, Jecelyn Leslie John, Kelly da Costa, Mohammad Saffree Jeffree, Nigel J. Temperton, Tom Tipton, Craig P. Thompson, Kamruddin Ahmed, Chris J. Drakeley, Miles W. Carroll, and Kimberly M. Fornace

Subjects
Science
Abstract

Abstract Cases of H5 highly pathogenic avian influenzas (HPAI) are on the rise. Although mammalian spillover events are rare, H5N1 viruses have an estimated mortality rate in humans of 60%. No human cases of H5 infection have been reported in Malaysian Borneo, but HPAI has circulated in poultry and migratory avian species transiting through the region. Recent deforestation in coastal habitats in Malaysian Borneo may increase the proximity between humans and migratory birds. We hypothesise that higher rates of human-animal contact, caused by this habitat destruction, will increase the likelihood of potential zoonotic spillover events. In 2015, an environmentally stratified cross-sectional survey was conducted collecting geolocated questionnaire data in 10,100 individuals. A serological survey of these individuals reveals evidence of H5 neutralisation that persisted following depletion of seasonal H1/H3 HA binding antibodies from the plasma. The presence of these antibodies suggests that some individuals living near migratory sites may have been exposed to H5 HA. There is a spatial and environmental overlap between individuals displaying high H5 HA binding and the distribution of migratory birds. We have developed a novel surveillance approach including both spatial and serological data to detect potential spillover events, highlighting the urgent need to study cross-species pathogen transmission in migratory zones.

Published
2024
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10. Obesity Modifies the Relationship Between Raltegravir and Dolutegravir Hair Concentrations and Body Weight Gain in Women Living with HIV

Author

Lahiri, Cecile D, Mehta, C Christina, Sykes, Craig, Weiser, Sheri D, Palella, Frank, Lake, Jordan E, Mellors, John W, Gustafson, Deborah, French, Audrey L, Adimora, Adaora A, Konkle-Parker, Deborah, Sharma, Anjali, Bolivar, Hector, Kassaye, Seble G, Rubin, Leah H, Alvarez, Jessica A, Golub, Elizabeth T, Ofotokun, Igho, and Sheth, Anandi N

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Obesity, Infectious Diseases, Women's Health, Sexually Transmitted Infections, Nutrition, HIV/AIDS, Humans, Female, Middle Aged, Raltegravir Potassium, HIV Infections, HIV Integrase Inhibitors, HIV-1, Heterocyclic Compounds, 3-Ring, Oxazines, Weight Gain, HIV Integrase, HIV, women, weight gain, integrase inhibitors, pharmacology, Virology, Clinical sciences
Abstract

Integrase strand-transfer inhibitors (INSTIs) are associated with weight gain in women living with HIV (WLH). Relationships between drug exposure, baseline obesity, and INSTI-associated weight gain remain unclear. Data from 2006 to 2016 were analyzed from virally suppressed WLH enrolled in the Women's Interagency HIV Study, who switched/added an INSTI to antiretroviral therapy: [raltegravir (RAL), dolutegravir (DTG), or elvitegravir (EVG)]. Percent body weight change was calculated from weights obtained a median 6 months pre-INSTI and 14 months post-INSTI initiation. Hair concentrations were measured with validated liquid chromatography-mass spectrometry (MS)/MS assays. Baseline (preswitch) weight status evaluated obese (body mass index, BMI, ≥30 kg/m2) versus nonobese (BMI 500 cells/mm3, >75% with undetectable HIV-1 RNA. Over ∼1 year, women experienced median increases in body weight: 1.71% (-1.78, 5.00) with RAL; 2.40% (-2.82, 6.50) with EVG; and 2.48% (-3.60, 7.88) with DTG. Baseline obesity status modified the relationship between hair concentrations and percent weight change for DTG and RAL (p's

Published
2023

11. Using in-situ strain measurements to evaluate the accuracy of stress estimation procedures from fracture injection/shut-in tests

Author

Guglielmi, Yves, McClure, Mark, Burghardt, Jeffrey, Morris, Joseph P, Doe, Thomas, Fu, Pengcheng, Knox, Hunter, Vermeul, Vince, Kneafsey, Tim, Team, The EGS Collab, Ajo-Franklin, J, Baumgartner, T, Beckers, K, Blankenship, D, Bonneville, A, Boyd, L, Brown, S, Burghardt, JA, Chai, C, Chakravarty, A, Chen, T, Chen, Y, Chi, B, Condon, K, Cook, PJ, Crandall, D, Dobson, PF, Doe, T, Doughty, CA, Elsworth, D, Feldman, J, Feng, Z, Foris, A, Frash, LP, Frone, Z, Fu, P, Gao, K, Ghassemi, A, Guglielmi, Y, Haimson, B, Hawkins, A, Heise, J, Hopp, C, Horn, M, Horne, RN, Horner, J, Hu, M, Huang, H, Huang, L, Im, KJ, Ingraham, M, Jafarov, E, Jayne, RS, Johnson, TC, Johnson, SE, Johnston, B, Karra, S, Kim, K, King, DK, Kneafsey, T, Knox, H, Knox, J, Kumar, D, Kutun, K, Lee, M, Li, D, Li, J, Li, K, Li, Z, Maceira, M, Mackey, P, Makedonska, N, Marone, CJ, Mattson, E, McClure, MW, McLennan, J, McLing, T, Medler, C, Mellors, RJ, Metcalfe, E, Miskimins, J, Moore, J, Morency, CE, Morris, JP, Myers, T, Nakagawa, S, Neupane, G, Newman, G, Nieto, A, Paronish, T, Pawar, R, Petrov, P, Pietzyk, B, Podgorney, R, Polsky, Y, Pope, J, Porse, S, Primo, JC, Pyatina, T, and Reimers, C

Subjects
Engineering, Resources Engineering and Extractive Metallurgy, Bioengineering, DFIT, Minifrac, SIMFIP, Collab, Civil Engineering, Mining & Metallurgy, Civil engineering, Resources engineering and extractive metallurgy
Abstract

Fracture injection/shut-in tests are commonly used to measure the state of stress in the subsurface. Injection creates a hydraulic fracture (or in some cases, opens a preexisting fracture), and then the pressure after shut-in is monitored to identify fracture closure. Different interpretation procedures have been proposed for estimating closure, and the procedures sometimes yield significantly different results. In this study, direct, in-situ strain measurements are used to observe fracture reopening and closure. The tests were performed as part of the EGS Collab project, a mesoscale project performed at 1.25 and 1.5 km depth at the Sanford Underground Research Facility. The tests were instrumented with the SIMFIP tool, a double-packer probe with a high-resolution three-dimensional borehole displacement sensor. The measurements provide a direct observation of the fracture closure signature, enabling a high-fidelity estimate of the fracture closure stress (ie, the normal stress on the fracture). In two of the four tests, injection created an opening mode fracture, and so the closure stress can be interpreted as the minimum principal stress. In the other two tests, injection probably opened preexisting natural fractures, and so the closure stress can be interpreted as the normal stress on the fractures. The strain measurements are compared against different proposed methods for estimating closure stress from pressure transients. The shut-in transients are analyzed with two techniques that are widely used in the field of petroleum engineering – the ‘tangent’ method and the ‘compliance’ method. In three of the four tests, the tangent method significantly underestimates the closure stress. The compliance method is reasonably accurate in all four tests. Closure stress is also interpreted using two other commonly-used methods – ‘first deviation from linearity’ and the method of (Hayashi and Haimson, 1991). In comparison with the SIMFIP data, these methods tend to overestimate the closure stress, evidently because they identify closure from early-time transient effects, such as near-wellbore tortuosity. In two of the tests, microseismic imaging provides an independent estimate of the size of the fracture created by injection. When combined with a simple mass balance calculation, the SIMFIP stress measurements yield predictions of fracture size that are reasonably consistent with the estimates from microseismic. The calculations imply an apparent fracture toughness 2-3x higher than typical laboratory-derived values.

Published
2023

24. Discovery of a novel highly specific, fully human PSCA antibody and its application as an antibody-drug conjugate in prostate cancer

Author

Xiaojie Chu, Seungmin Shin, Du-San Baek, Liyong Zhang, Alex Conard, Megan Shi, Ye-Jin Kim, Cynthia Adams, Maggie Hines, Xianglei Liu, Chuan Chen, Zehua Sun, Dontcho V. Jelev, John W. Mellors, Dimiter S. Dimitrov, and Wei Li

Subjects
Antibody drug conjugate, fully human antibody, monomethyl auristatin E, prostate cancer, PSCA, tumor xenograft mouse model, Therapeutics. Pharmacology, RM1-950, Immunologic diseases. Allergy, RC581-607
Abstract

Prostate stem cell antigen (PSCA) is expressed in all stages of prostate cancer, including in advanced androgen-independent tumors and bone metastasis. PSCA may associate with prostate carcinogenesis and lineage plasticity in prostate cancer. PSCA is also a promising theranostic marker for a variety of other solid tumors, including pancreatic adenocarcinoma and renal cell carcinoma. Here, we identified a novel fully human PSCA antibody using phage display methodology. The structure-based affinity maturation yielded a high-affinity binder, F12, which is highly specific and does not bind to 6,000 human membrane proteins based on a membrane proteome array assay. F12 targets PSCA amino acids 63–69 as tested by the peptide scanning microarray, and it cross-reacts with the murine PSCA. IgG1 F12 efficiently internalizes into PSCA-expressing tumor cells. The antimitotic reagent monomethyl auristatin E (MMAE)-conjugated IgG1 F12 (ADC, F12-MMAE) exhibits dose-dependent efficacy and specificity in a human prostate cancer PC-3-PSCA xenograft NSG mouse model. This is a first reported ADC based on a fully human PSCA antibody and MMAE that is characterized in a xenograft murine model, which warrants further optimizations and investigations in additional preclinical tumor models, including prostate and other solid tumors.

Published
2024
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25. Extended Analysis of HIV Infection in Cisgender Men and Transgender Women Who Have Sex with Men Receiving Injectable Cabotegravir for HIV Prevention: HPTN 083

Author

Marzinke, Mark A, Fogel, Jessica M, Wang, Zhe, Piwowar-Manning, Estelle, Kofron, Ryan, Moser, Amber, Bhandari, Pradip, Gollings, Ryann, Bushman, Lane R, Weng, Lei, Halvas, Elias K, Mellors, John, Anderson, Peter L, Persaud, Deborah, Hendrix, Craig W, McCauley, Marybeth, Rinehart, Alex R, St Clair, Marty, Ford, Susan L, Rooney, James F, Adeyeye, Adeola, Chariyalertsak, Suwat, Mayer, Kenneth, Arduino, Roberto C, Cohen, Myron S, Grinsztejn, Beatriz, Hanscom, Brett, Landovitz, Raphael J, and Eshleman, Susan H

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Infectious Diseases, Prevention, Sexual and Gender Minorities (SGM/LGBT*), HIV/AIDS, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Male, Humans, Female, HIV Infections, Anti-HIV Agents, Transgender Persons, Retrospective Studies, Tenofovir, Emtricitabine, Pre-Exposure Prophylaxis, HIV, preexposure prophylaxis, prevention, cabotegravir, injectable, TDF-FTC, long-acting, men who have sex with men, HPTN 083, Microbiology, Medical Microbiology, Pharmacology and Pharmaceutical Sciences, Medical microbiology, Pharmacology and pharmaceutical sciences
Abstract

HPTN 083 demonstrated that injectable cabotegravir (CAB) was superior to oral tenofovir disoproxil fumarate-emtricitabine (TDF-FTC) for HIV prevention in cisgender men and transgender women who have sex with men. We previously analyzed 58 infections in the blinded phase of HPTN 083 (16 in the CAB arm and 42 in the TDF-FTC arm). This report describes 52 additional infections that occurred up to 1 year after study unblinding (18 in the CAB arm and 34 in the TDF-FTC arm). Retrospective testing included HIV testing, viral load testing, quantification of study drug concentrations, and drug resistance testing. The new CAB arm infections included 7 with CAB administration within 6 months of the first HIV-positive visit (2 with on-time injections, 3 with ≥1 delayed injection, and 2 who restarted CAB) and 11 with no recent CAB administration. Three cases had integrase strand transfer inhibitor (INSTI) resistance (2 with on-time injections and 1 who restarted CAB). Among 34 CAB infections analyzed to date, diagnosis delays and INSTI resistance were significantly more common in infections with CAB administration within 6 months of the first HIV-positive visit. This report further characterizes HIV infections in persons receiving CAB preexposure prophylaxis and helps define the impact of CAB on the detection of infection and the emergence of INSTI resistance.

Published
2023

26. HIV-1 remission and possible cure in a woman after haplo-cord blood transplant

Author

Hsu, Jingmei, Van Besien, Koen, Glesby, Marshall J, Pahwa, Savita, Coletti, Anne, Warshaw, Meredith G, Petz, Larry, Moore, Theodore B, Chen, Ya Hui, Pallikkuth, Suresh, Dhummakupt, Adit, Cortado, Ruth, Golner, Amanda, Bone, Frederic, Baldo, Maria, Riches, Marcie, Mellors, John W, Tobin, Nicole H, Browning, Renee, Persaud, Deborah, Bryson, Yvonne, Team, the International Maternal Pediatric Adolescent AIDS Clinical Trials Network P1107, Anthony, Patricia, Hazra, Rohan, Mitsuyasu, Ronald, Pahwe, Savita, Petz, Lawrence, and Yin, Dwight

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Immunology, Clinical Research, Pediatric, Infectious Diseases, Stem Cell Research - Nonembryonic - Human, Immunotherapy, Transplantation, Hematology, Stem Cell Research - Umbilical Cord Blood/ Placenta, Cancer, Stem Cell Research, Regenerative Medicine, Sexually Transmitted Infections, Stem Cell Research - Umbilical Cord Blood/ Placenta - Human, HIV/AIDS, 5.2 Cellular and gene therapies, Infection, Male, Adult, Female, Humans, Hematopoietic Stem Cell Transplantation, HIV-1, Cord Blood Stem Cell Transplantation, Fetal Blood, HIV Infections, Leukemia, Myeloid, Acute, International Maternal Pediatric Adolescent AIDS Clinical Trials Network (IMPAACT) P1107 Team, HIV CCR5 dela 32 transplant, HIV cure, HIV remission, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

Previously, two men were cured of HIV-1 through CCR5Δ32 homozygous (CCR5Δ32/Δ32) allogeneic adult stem cell transplant. We report the first remission and possible HIV-1 cure in a mixed-race woman who received a CCR5Δ32/Δ32 haplo-cord transplant (cord blood cells combined with haploidentical stem cells from an adult) to treat acute myeloid leukemia (AML). Peripheral blood chimerism was 100% CCR5Δ32/Δ32 cord blood by week 14 post-transplant and persisted through 4.8 years of follow-up. Immune reconstitution was associated with (1) loss of detectable replication-competent HIV-1 reservoirs, (2) loss of HIV-1-specific immune responses, (3) in vitro resistance to X4 and R5 laboratory variants, including pre-transplant autologous latent reservoir isolates, and (4) 18 months of HIV-1 control with aviremia, off antiretroviral therapy, starting at 37 months post-transplant. CCR5Δ32/Δ32 haplo-cord transplant achieved remission and a possible HIV-1 cure for a person of diverse ancestry, living with HIV-1, who required a stem cell transplant for acute leukemia.

Published
2023

27. Using Dark Fiber and Distributed Acoustic Sensing to Characterize a Geothermal System in the Imperial Valley, Southern California

Author

Cheng, Feng, Ajo‐Franklin, Jonathan B, Nayak, Avinash, Tribaldos, Veronica Rodriguez, Mellors, Robert, Dobson, Patrick, and Team, the Imperial Valley Dark Fiber

Subjects
Earth Sciences, Geology, Geophysics, Affordable and Clean Energy, distributed acoustic sensing, ambient noise interferometry, geothermal imaging, Vp, Vs imaging, surface wave imaging, Geochemistry
Abstract

The Imperial Valley, CA, is a tectonically active transtensional basin located south of the Salton Sea; the area hosts numerous geothermal fields, including significant hidden hydrothermal resources without surface manifestations. Development of inexpensive, rugged, and highly sensitive exploration techniques for undiscovered geothermal systems is critical for accelerating geothermal power deployment as well as unlocking a low-carbon energy future. We present a case study utilizing distributed acoustic sensing (DAS) and ambient noise interferometry for geothermal reservoir imaging, utilizing unlit fiber-optic telecommunication infrastructure (dark fiber). The study exploits two days of passive DAS data acquired in early November 2020 over a ∼28-km section of fiber from Calipatria, CA to Imperial, CA. We apply ambient noise interferometry to retrieve coherent signals from DAS records and develop a bin stacking technique to attenuate the effects from persistent localized noise sources and to enhance retrieval of coherent surface waves. As a result, we are able to obtain high-resolution two-dimensional (2D) S wave velocity (Vs) structure to 3 km depth, based on joint inversion of both the fundamental and higher overtones. We observe a previously unmapped high Vs and low Vp/Vs ratio feature beneath the Brawley geothermal system, which we interpret to be a zone of hydrothermal mineralization and lower porosity. This interpretation is consistent with a host of other measurements including surface heat flow, gravity anomalies, and available borehole wireline data. These results demonstrate the potential utility of DAS deployed on dark fiber for geothermal system exploration and characterization in the appropriate geological settings.

Published
2023

29. Impact of SARS-CoV-2 Resistance to Antiviral Monoclonal Antibody Therapy on Neutralizing Antibody Response

Author

Marc-Kendy Paul, Manish Choudhary, Amy Heaps, Rinki Deo, Daniela Moisi, Kelley Gordon, John Mellors, Carlee Moser, Paul Klekotka, Alan Landay, Judith Currier, Joseph Eron, Kara Chew, Davey Smith, Scott Sieg, Urvi Parikh, and Jonathan Li

Subjects
bamlanivimab, COVID-19, monoclonal antibody, SARS-CoV-2, pseudovirus neutralization, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607
Abstract

Background: Anti-SARS-CoV-2 monoclonal antibodies (mAbs) have played a key role as an antiviral against SARS-CoV-2, but there is a potential for resistance to develop. The interplay between host antibody responses and the development of monoclonal antibody (mAb) resistance is a critical area of investigation. In this study, we assessed host neutralizing antibody (nAb) responses against both ancestral virus and those with treatment-emergent E484K bamlanivimab resistance mutations. Methods: Study participants were enrolled in the ACTIV-2/Advancing Clinical Therapeutics Globally (ACTG) A5401 phase 2 randomized, placebo-controlled trial of bamlanivimab 700 mg mAb therapy (NCT04518410). Anterior nasal and nasopharyngeal swabs were collected for SARS-CoV-2 RNA testing and S gene next-generation sequencing to identify the E484K bamlanivimab resistance mutation. Serum nAb titers were assessed by pseudovirus neutralization assays. Results: Higher baseline (pre-treatment) nAb titers against either ancestral or E484K virus was associated with lower baseline viral load. Participants with emerging resistance had low levels of nAb titers against either ancestral or E484K nAb at the time of study entry. Participants with emergent E484K resistance developed significantly higher levels of E484K-specific nAb titers compared to mAb-treated individuals who did not develop resistance. All participants who developed the E484K mAb resistance mutation were eventually able to clear the virus. Conclusion: Emerging drug resistance after SARS-CoV-2-specific mAb therapy led to a heightened host neutralizing antibody response to the mAb-resistant variant that was associated with eventual viral clearance. This demonstrates the interplay between the antiviral treatment-directed viral evolution and subsequent host immune response in viral clearance.

Published
2024
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30. Comparison Study of the Bio-Plex and Meso Scale Multiplexed SARS-CoV-2 Serology Assays Reveals Evidence of Diminished Host Antibody Responses to SARS-CoV-2 after Monoclonal Antibody Treatment

Author

Urvi Parikh, Amy Heaps, Daniela Moisi, Kelley Gordon, John Mellors, Manish Choudhary, Rinki Deo, Carlee Moser, Paul Klekotka, Alan Landay, Judith Currier, Joseph Eron, Kara Chew, Davey Smith, Jonathan Li, Scott Sieg, and ACTIV-2/A5401 Study Team

Subjects
SARS-CoV-2, COVID, COVID-19, Bio-Plex, Meso Scale Discovery, monoclonal antibodies, Pathology, RB1-214, Immunologic diseases. Allergy, RC581-607
Abstract

Background: Assessing the breadth and duration of antigen-specific binding antibodies provides valuable information for evaluating interventions to treat or prevent SARS-CoV-2 infection. Multiplex immunoassays are a convenient method for rapid measurement of antibody responses but can sometimes provide discordant results, and antibody positive percent agreement for COVID-19 diagnosis can vary depending on assay type, disease severity, and population sampled. Therefore, we compared two assays marked for research applications, MSD and Bio-Plex Pro, to evaluate qualitative interpretation of serostatus and quantitative detection of antibodies of varying isotypes (IgG, IgM, and IgA) against receptor binding domain (RBD) and nucleocapsid (N) antigens. Methods: Specimens from ACTIV-2/A5401, a placebo-controlled clinical trial of the SARS-CoV-2 monoclonal antibody (mAb) bamlanivimab to prevent COVID-19 disease progression, were used to evaluate the concordance of the Bio-Rad Bio-Plex Pro Human SARS-CoV-2 Serology Assay and the Meso Scale Discovery (MSD) V-PLEX COVID-19 Panel 1 serology assay in detecting and quantifying IgG, IgA, and IgM binding anti-SARS-CoV-2 antibody responses against the RBD and N antigens. Data were disaggregated by study arm, bamlanivimab dose, days post-enrollment, and presence of emerging resistance. Results: We observed 90.5% (412 of 455 tests) concordance for anti-RBD IgG and 87% (396 of 455) concordance for anti-N IgG in classifying samples as negative or positive based on assay-defined cutoffs. Antibody levels converted to the WHO standard BAU/mL were significantly correlated for all isotypes (IgG, IgM, and IgA) and SARS-CoV-2 antigen targets (RBD and N) tested that were common between the two assays (Spearman r 0.65 to 0.92, P < 0.0001). Both assays uncovered evidence of diminished host-derived IgG immune responses in participants treated with bamlanivimab compared to placebo. Assessment of immune responses in the four individuals treated with the 700 mg of bamlanivimab with emerging mAb resistance demonstrated a stronger anti-N IgG response (MSD) at day 28 (median 2.18 log BAU/mL) compared to participants treated with bamlanivimab who did not develop resistance (median 1.55 log BAU/mL). Conclusions: These data demonstrate the utility in using multiplex immunoassays for characterizing the immune responses with and without treatment in a study population and provide evidence that monoclonal antibody treatment in acute COVID-19 may have a modest negative impact on development of host IgG responses.

Published
2024
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31. Utilising Online Gamification to Promote Student Success and Retention in Tertiary Settings

Author

Harrington, Ingrid and Mellors, Marc J.

Abstract

The role of gamification in Australian higher educational learning has gained increasing currency in recent years, with many proponents promoting its usefulness for improving the university student experience by increasing progression and lowering attrition, particularly among first year students (Charles, Charles, McNeill, Bustard, & Black, 2011). However, some students express reservations that the inherently competitive nature of some gamified learning activities negatively impact their learning experience, especially when compared to classic instructional methods (Charles et al., 2011). This discussion and instructional paper undertakes a review of the gamification literature within the Australian higher education context, concurrently exploring what it means and how to use gamification to enhance student learning. The paper provides a short biographic summary of the positive impact selected popular gamified activities has had on improving student engagement, participation and retention in tertiary settings.

Published
2021

32. HIV RNA Screening Reduces Integrase Strand Transfer Inhibitor Resistance Risk in Persons Receiving Long-Acting Cabotegravir for HIV Prevention

Author

Eshleman, Susan H, Fogel, Jessica M, Halvas, Elias K, Piwowar-Manning, Estelle, Marzinke, Mark A, Kofron, Ryan, Wang, Zhe, Mellors, John, McCauley, Marybeth, Rinehart, Alex R, St Clair, Marty, Adeyeye, Adeola, Hinojosa, Juan C, Cabello, Robinson, Middelkoop, Keren, Hanscom, Brett, Cohen, Myron S, Grinsztejn, Beatriz, Landovitz, Raphael J, Seisa, Michael, Lie, Yolanda, Meyer, William, Marrazzo, Jeanne, Peel, Sheila, Wallis, Carole, Asmelash, Aida, Daar, Eric, Rooney, James, and Clark, Richard

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Prevention, Genetics, Infectious Diseases, HIV/AIDS, Infection, Good Health and Well Being, Humans, HIV Infections, Drug Resistance, Viral, HIV-1, RNA, Pyridones, HIV Integrase Inhibitors, HIV Integrase, Mutation, HIV, HPTN, INSTI, cabotegravir, injectable, integrase, PrEP, prevention, resistance, HPTN 083 Study Team, Biological Sciences, Medical and Health Sciences, Microbiology, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundThe HPTN 083 trial demonstrated that long-acting cabotegravir (CAB-LA) was superior to tenofovir-disoproxil fumarate/emtricitabine for human immunodeficiency virus (HIV) preexposure prophylaxis (PrEP). Integrase strand transfer inhibitor (INSTI) resistance-associated mutations (RAMs) were detected in some participants with HIV infection. We used a low viral load INSTI genotyping assay to evaluate the timing of emergence of INSTI RAMs and assessed whether HIV screening with a sensitive RNA assay would have detected HIV infection before INSTI resistance emerged.MethodsSingle-genome sequencing to detect INSTI RAMs was performed for samples with viral loads

Published
2022

34. High Levels of Pretreatment HIV-1 Drug Resistance Mutations Among South African Women Who Acquired HIV During a Prospective Study

Author

Beesham, Ivana, Parikh, Urvi M, Mellors, John W, Davey, Dvora L Joseph, Heffron, Renee, Palanee-Phillips, Thesla, Bosman, Shannon L, Beksinska, Mags, Smit, Jennifer, Ahmed, Khatija, Makkan, Heeran, Selepe, Pearl, Louw, Cheryl, Kotze, Philip, Hofmeyr, G Justus, Singata‐Madliki, Mandisa, Rees, Helen, Baeten, Jared M, and Wallis, Carole

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Antimicrobial Resistance, Clinical Research, HIV/AIDS, Infectious Diseases, Clinical Trials and Supportive Activities, Genetics, Development of treatments and therapeutic interventions, 6.1 Pharmaceuticals, 5.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Infection, Good Health and Well Being, Adult, Anti-HIV Agents, Drug Resistance, Viral, Female, Genotype, HIV Infections, HIV Seropositivity, HIV-1, Humans, Mutation, Prospective Studies, Reverse Transcriptase Inhibitors, South Africa, Young Adult, antiretroviral resistance, women, pretreatment resistance, Public Health and Health Services, Virology, Clinical sciences, Epidemiology, Public health
Abstract

BackgroundPretreatment HIV drug resistance (PDR) undermines individual treatment success and threatens the achievement of UNAIDS 95-95-95 targets. In many African countries, limited data are available on PDR as detection of recent HIV infection is uncommon and access to resistance testing is limited. We describe the prevalence of PDR among South African women with recent HIV infection from the Evidence for Contraceptive Options and HIV Outcomes (ECHO) Trial.MethodsHIV-uninfected, sexually active women, aged 18-35 years, and seeking contraception were enrolled in the ECHO Trial at sites in South Africa, from 2015 to 2018. HIV testing was done at trial entry and repeated quarterly. We tested stored plasma samples collected at HIV diagnosis from women who seroconverted during follow-up and had a viral load >1000 copies/mL for antiretroviral resistant mutations using a validated laboratory-developed population genotyping assay, which sequences the full protease and reverse transcriptase regions. Mutation profiles were determined using the Stanford Drug Resistance Database.ResultsWe sequenced 275 samples. The median age was 23 years, and majority (98.9%, n = 272) were infected with HIV-1 subtype C. The prevalence of surveillance drug resistance mutations (SDRMs) was 13.5% (n = 37). Nonnucleoside reverse transcriptase inhibitor (NNRTI) mutations were found in 12.4% of women (n = 34). Few women had NRTI (1.8%, n = 5) and protease inhibitor (1.1%, n = 3) mutations. Five women had multiple NRTI and NNRTI SDRMs.ConclusionsThe high levels of PDR, particularly to NNRTIs, strongly support the recent change to the South African national HIV treatment guidelines to transition to a first-line drug regimen that excludes NNRTIs.

Published
2022

35. Seagrass spatial data synthesis from north‐east Australia, Torres Strait and Gulf of Carpentaria, 1983 to 2022

Author

A Carter, S McKenna, MA Rasheed, H Taylor, C van deWetering, K Chartrand, C Reason, C Collier, L Shepherd, J Mellors, L McKenzie, NC Duke, A Roelofs, N Smit, R Groom, D Barrett, S Evans, R Pitcher, N Murphy, M Carlisle, M David, S Lui, Torres Strait Indigenous Rangers, and RG Coles

Subjects
Oceanography, GC1-1581
Abstract

Abstract The Gulf of Carpentaria and Torres Strait in north‐eastern Australia support globally significant seagrass ecosystems that underpin fishing and cultural heritage of the region. Reliable data on seagrass distribution are critical to understanding how these ecosystems are changing, while managing for resilience. Spatial data on seagrass have been collected since the early 1980s, but the early data were poorly curated. Some was not publicly available, and some already lost. We validated and synthesized historical seagrass spatial data to create a publicly available database. We include a site layer of 48,612 geolocated data points including information on seagrass presence/absence, sediment, collection date, and data custodian. We include a polygon layer with 641 individual seagrass meadows. Thirteen seagrass species are identified in depths ranging from intertidal to 38 m below mean sea level. Our synthesis includes scientific survey data from 1983 to 2022 and provides an important evidence base for marine resource management.

Published
2024
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36. Single-cell analysis reveals the stromal dynamics and tumor-specific characteristics in the microenvironment of ovarian cancer

Author

Linan Zhang, Sandra Cascio, John W. Mellors, Ronald J. Buckanovich, and Hatice Ulku Osmanbeyoglu

Subjects
Biology (General), QH301-705.5
Abstract

Abstract High-grade serous ovarian carcinoma (HGSOC) is a heterogeneous disease, and a highstromal/desmoplastic tumor microenvironment (TME) is associated with a poor outcome. Stromal cell subtypes, including fibroblasts, myofibroblasts, and cancer-associated mesenchymal stem cells, establish a complex network of paracrine signaling pathways with tumor-infiltrating immune cells that drive effector cell tumor immune exclusion and inhibit the antitumor immune response. In this work, we integrate single-cell transcriptomics of the HGSOC TME from public and in-house datasets (n = 20) and stratify tumors based upon high vs. low stromal cell content. Although our cohort size is small, our analyses suggest a distinct transcriptomic landscape for immune and non-immune cells in high-stromal vs. low-stromal tumors. High-stromal tumors have a lower fraction of certain T cells, natural killer (NK) cells, and macrophages, and increased expression of CXCL12 in epithelial cancer cells and cancer-associated mesenchymal stem cells (CA-MSCs). Analysis of cell-cell communication indicate that epithelial cancer cells and CA-MSCs secrete CXCL12 that interacte with the CXCR4 receptor, which is overexpressed on NK and CD8+ T cells. Dual IHC staining show that tumor infiltrating CD8 T cells localize in proximity of CXCL12+ tumor area. Moreover, CXCL12 and/or CXCR4 antibodies confirm the immunosuppressive role of CXCL12-CXCR4 in high-stromal tumors.

Published
2024
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37. Impact of antiretroviral therapy during acute or early HIV infection on virologic and immunologic outcomes: results from a multinational clinical trial

Author

Crowell, Trevor A., Ritz, Justin, Zheng, Lu, Naqvi, Asma, Cyktor, Joshua C., Puleo, Joseph, Clagett, Brian, Lama, Javier R., Kanyama, Cecilia, Little, Susan J., Cohn, Susan E., Riddler, Sharon A., Collier, Ann C., Heath, Sonya L., Tantivitayakul, Pornphen, Grinsztejn, Beatriz, Arduino, Roberto C., Rooney, James F., van Zyl, Gert U., Coombs, Robert W., Fox, Lawrence, Ananworanich, Jintanat, Eron, Joseph J., Sieg, Scott F., Mellors, John W., and Daar, Eric S.

Published
2024
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38. A multi-Physics Experiment for Low-Yield Nuclear Explosion Monitoring

Author

Myers, S, primary, Abbott, G, additional, Alexander, T, additional, Alger, E, additional, Alvarez, A, additional, Annabelle, N, additional, Antoun, T, additional, Auld, G, additional, Malach, A, additional, Banuelos, H, additional, Barela, M, additional, Barnhart, T, additional, Barrow, P, additional, Bartlett, T, additional, Bockman, A, additional, Bodmer, M, additional, Bogolub, K, additional, Bonner, J, additional, Borden, R, additional, Boukhalfa, H, additional, Bowman, D, additional, Britt, C, additional, Broman, B, additional, Broome, S, additional, Brown, B, additional, Burghardt, J, additional, Chester, D, additional, Choens, C, additional, Chojnicki, K, additional, Churby, A, additional, Cole, J, additional, Coleman, T, additional, Collard, J, additional, Couture, A, additional, Crosby, G, additional, Cruz-Cabrera, A, additional, D'Saint Angelo, D, additional, Dea, M, additional, Dekin, W, additional, DeVisser, B, additional, Dietel, M, additional, Downs, C, additional, Downs, N, additional, Dzenitis, E, additional, Eckert, E, additional, Eras, S, additional, Euler, G, additional, Ezzedine, S, additional, Fast, J, additional, Feldman, J, additional, Featherston, K, additional, Foxe, M, additional, Freimuth, C, additional, Fritz, B, additional, Galvin, G, additional, Gamboa, S, additional, Garner, L, additional, Gascoigne, T, additional, Gastelum, J, additional, Gaylord, J, additional, Gessey, D, additional, Glasgow, B, additional, Glavin, G, additional, Glomski, A, additional, Goodwin, M, additional, Green, D, additional, Griego, J, additional, Grover, S, additional, Gutierrez, J, additional, Haas, D, additional, Hall, R, additional, Hall, A, additional, Hardy, D, additional, Hauk, D, additional, Heath, J, additional, Holand, A, additional, Holdcroft, J, additional, Holland, A, additional, Honjas, W, additional, Howard, K, additional, Hudson, C, additional, Ingraham, M, additional, Jaramillo, J, additional, Jenkins, A, additional, Johnson, C, additional, Jones, K, additional, Falliner, F, additional, Junor, W, additional, Keillor, M, additional, Kent, G, additional, Keogh, M, additional, Kibikas, W, additional, Kleadbeater, K, additional, Knox, H, additional, Knox, J, additional, Kuhlman, K, additional, Kwiatkowski, C, additional, Laintz, K, additional, Lapka, J, additional, Larotonda, J, additional, Layne, J, additional, Ledoux, N, additional, Li, S, additional, Linneman, D, additional, Lipkowitz, P, additional, MacLeod, G, additional, McCann, E, additional, McCombe, R, additional, Meierbachtol, C, additional, Mellors, R, additional, Memmott, B, additional, Mendenhall, W, additional, Mendez, J, additional, Miller, X, additional, Miller, A, additional, Miranda, F, additional, Montano, M, additional, Moore, M, additional, Morris, J, additional, Munley, W, additional, Murillo, E, additional, Myers, T, additional, Navarro, A, additional, Nippress, S, additional, Otto, S, additional, Peacock, S, additional, Pemberton, S, additional, Perea, R, additional, Peterson, J, additional, Pierre-Yves, L, additional, Plank, G, additional, Podrasky, A, additional, Podrasky, D, additional, Pope, J, additional, Poskey, M, additional, Powell, M, additional, Price, A, additional, Puyleart, A, additional, Quintana, B, additional, Rahn, T, additional, Rendon, C, additional, Reppart, J, additional, Rico, H, additional, Roberts, B, additional, Robey, E, additional, Rodd, R, additional, Rodriguez, M, additional, Rogall, A, additional, Romanczuk, A, additional, Roth, M, additional, Salyer, G, additional, Savran, B, additional, Schalk, W, additional, Seifert, C, additional, Seitz, D, additional, Shao, X, additional, Sirota, D, additional, Slack, J, additional, Slater, D, additional, Smith, K, additional, Smith, D, additional, Spears, B, additional, Sprinkle, D, additional, Stead, R, additional, Stephens, M, additional, Strickland, C, additional, Tafoya, A, additional, Tafoya, J, additional, Tagoe, M, additional, Taguba, C, additional, Tarnecki, L, additional, Tatge, R, additional, Teich-McGoldrick, S, additional, Terry, B, additional, Thompson, R, additional, Townsend, M, additional, Tubbs, G, additional, Turley, R, additional, Valdez, N, additional, Van Morris, A, additional, Vergara, S, additional, Vigil, J, additional, Villanueva, J, additional, Vorobiev, O, additional, Wallace, D, additional, Walrath, T, additional, Wharton, S, additional, White, R, additional, White, H, additional, Whitehill, A, additional, Williams, M, additional, Wilson, J, additional, Wood, L, additional, Wright, C, additional, Wright, A, additional, Xu, G, additional, Yang, X, additional, Yost, R, additional, and Zeiler, C, additional

Published
2024
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40. Infrared hyperspectral imaging for point-of-care wound assessment

Author

Mellors, Ben O. L.

Subjects
Q Science (General), QC Physics
Abstract

Wound healing assessment and management are both important in ensuring a correct healing sequence. Most of these assessment techniques involve simple observation with the naked eye, which causes two main issues: the parameters assessed are highly subjective, and they rely upon the knowledge and experience of a trained medical professional. Any failure or incorrect management can result in further complications and even fatality, therefore quantitative wound assessment techniques are the next step towards a more accessible and reliable wound management strategy. Current research in this field is focused on utilising non-invasive imaging techniques, mainly within the visible and infrared (IR) range, to identify the biological and chemical changes during the wound healing process. Any abnormalities can then be identified earlier to aid in the correct diagnosis and treatment of the wound. Technologies that utilise concepts of non-contact imaging, such as optical imaging and spectroscopy can be used to obtain spatial and spectral maps of biomarkers, which provide valuable information on the wound (e.g., precursors to improper healing or delineate viable and necrotic tissue). This work extends this research further by investigating two different imaging modalities, Negative Contrast Imaging (NCI), along with Spatial Frequency Domain Imaging (SFDI) for the applications of point of care wound assessment. Intelligent data analysis algorithms, in the form of k-means clustering and principal component analysis were applied to spectral data, collected from wound biopsies as part of a previous study, highlighting the ability to diagnose wound healing status from the contrast of spectral information, which is not reliant upon a subjective clinical diagnosis. These methods provided the motivation for a larger cell culture trauma study, in which the NCI was utilised to obtain spectral reflectance maps across a 2.5- 3.5 μm wavelength region of both healthy and traumatised human epidermal fibroblasts, induced via chemical assays. Using the same intelligent analysis tools, along with pre-processing methods including spectral derivatives, the resulting clusters can be utilised as a diagnostic tool for the assessment of cellular health and were quantifiable metrics were defined to compare the different analysis methods Near infrared (NIR) methodologies were also investigated, with two areas of SFDI identified for further advancements. Current SFDI acquisition and optical property parameter recovery is performed via a pixel-wise process, generating large amounts of data and a high computational burden for parameter recovery. Data reduction, through the application of Compressive Sensing (CS) at both the image acquisition and data analysis stages provided up to a 90% reduction in data, whilst maintaining < 10% error in recovered absorption and reduced scattering optical maps. This pixel-wise methodology also affects the forward modelling and inverse problem (imaging), based upon the diffusion approximation or Monte-Carlo methods due to their pixel-independent nature. NIRFAST, an existing FEM based NIR modelling tool, was adapted to produce pixel-dependent forward modelling for heterogenic samples, providing a mechanism towards a pixel dependent SFDI image modelling and parameter recovery system.

Published
2022

41. Understanding the role of the complement system in Ebola virus and SARS-CoV-2 pathogenesis

Author

Mellors, Jack

Abstract

The role of the complement system in viral infections is often complex, with significant implications for pathogenesis and disease. The complement system can form part of the early innate immune response through the binding of glycosylated viral proteins, or through spontaneous activation on viral surfaces. The complement system can also be activated by antibodies in complex with viral antigens. These mechanisms have the potential to inhibit virus interactions with host proteins, mediate opsonisation, promote inflammation and chemotaxis, cause the agglutination of virions, lyse virions, and lyse virus-infected cells. Despite the diverse and significant roles of the complement system in viral infection, it is a relatively under-researched aspect of antiviral immunity. The complement system has been associated with more severe symptoms and fatal outcomes of Ebola virus (EBOV) disease (EVD) and Coronavirus disease (COVID)-19. However, the underlying mechanisms of the complement system in response to EBOV and SARS-CoV-2 (the causative agent of COVID-19), and the wider implications for immunity, are poorly understood. We first investigated the antibody-independent mechanisms of the complement system in response to Ebolavirus and Coronavirus glycoproteins (GPs), to better understand the underlying mechanisms of complement activation in the early stages of infection. Using novel ELISAs and western blot assays, we identified MBL binding to a range of Ebolavirus and Coronavirus GPs, and demonstrated their potential to activate the complement system, eventuating in formation of the membrane attack complex (MAC). We also utilised PCR assays, next-generation sequencing, and LC-MS/MS, to identify potential differences in the structure and expression of complement proteins in EVD survivors. We found broad diversity in the SNPs of several complement proteins but were restricted by the sample size to determine significance. These findings showed potential mechanisms for antibody-independent complement activation that could influence the pathogenesis of EBOV and SARS-CoV-2 in the early stages of infection. Next, we evaluated the antibody-dependent mechanisms of the complement system. We developed novel flow cytometry assays to assess the ability of EVD convalescent, COVID-19 convalescent, and SARS-CoV-2 vaccinated plasma to mediate antibody-dependent complement deposition (ADCD) in response to the respective Ebolavirus and Coronavirus GPs. We found a differential response in ADCD between EVD plasma that was influenced by neutralisation titre, IgG titre, and/or the Ebolavirus GP present. For SARS-CoV-2, we found that ChAdOx1 nCoV-19 vaccine-induced antibodies could mediate ADCD, and that levels of ADCD correlated with disease severity in COVID-19 convalescent individuals. These findings are important for understanding the variability of responses in mediating the complement system, with particular relevance to recrudescence, re-infection, infection post-vaccination, and cross-reactivity. Lastly, we evaluated the significance of these antibody-independent and antibody-dependent complement mechanisms on wild-type EBOV and SARS-CoV-2 neutralisation. Independent of antibodies, the complement system did not influence virus neutralisation. However, in the presence of low-neutralising, virus-specific antibodies, we observed an enhancement in neutralisation of both EBOV and SARS-CoV-2 when the complement system was present. Neutralisation assays are a fundamental aspect of identifying therapeutic antibodies and determining correlates of protection, with further implications for vaccine licensure. Our observed effect of the complement system on neutralisation has implications for the initial assessments of therapeutic candidates, evaluating vaccine-induced immune responses, defining correlates of protection, and could be a consideration for the therapeutic use of complement inhibitors.

Published
2022
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42. Cost-effectiveness of easy-access, risk-informed oral pre-exposure prophylaxis in HIV epidemics in sub-Saharan Africa: a modelling study

Author

Phillips, Andrew N, Bershteyn, Anna, Revill, Paul, Bansi-Matharu, Loveleen, Kripke, Katharine, Boily, Marie-Claude, Martin-Hughes, Rowan, Johnson, Leigh F, Mukandavire, Zindoga, Jamieson, Lise, Meyer-Rath, Gesine, Hallett, Timothy B, Brink, Debra ten, Kelly, Sherrie L, Nichols, Brooke E, Bendavid, Eran, Mudimu, Edinah, Taramusi, Isaac, Smith, Jennifer, Dalal, Shona, Baggaley, Rachel, Crowley, Siobhan, Terris-Prestholt, Fern, Godfrey-Faussett, Peter, Mukui, Irene, Jahn, Andreas, Case, Kelsey K, Havlir, Diane, Petersen, Maya, Kamya, Moses, Koss, Catherine A, Balzer, Laura B, Apollo, Tsitsi, Chidarikire, Thato, Mellors, John W, Parikh, Urvi M, Godfrey, Catherine, Cambiano, Valentina, and Consortium, HIV Modelling

Subjects
Cost Effectiveness Research, Mental Health, Clinical Research, Prevention, HIV/AIDS, Infectious Diseases, Infection, Good Health and Well Being, Adult, Anti-HIV Agents, Cost-Benefit Analysis, Epidemics, Female, HIV Infections, Humans, Male, Pre-Exposure Prophylaxis, HIV Modelling Consortium, Medical and Health Sciences
Abstract

BackgroundApproaches that allow easy access to pre-exposure prophylaxis (PrEP), such as over-the-counter provision at pharmacies, could facilitate risk-informed PrEP use and lead to lower HIV incidence, but their cost-effectiveness is unknown. We aimed to evaluate conditions under which risk-informed PrEP use is cost-effective.MethodsWe applied a mathematical model of HIV transmission to simulate 3000 setting-scenarios reflecting a range of epidemiological characteristics of communities in sub-Saharan Africa. The prevalence of HIV viral load greater than 1000 copies per mL among all adults (HIV positive and negative) varied from 1·1% to 7·4% (90% range). We hypothesised that if PrEP was made easily available without restriction and with education regarding its use, women and men would use PrEP, with sufficient daily adherence, during so-called seasons of risk (ie, periods in which individuals are at risk of acquiring infection). We refer to this as risk-informed PrEP. For each setting-scenario, we considered the situation in mid-2021 and performed a pairwise comparison of the outcomes of two policies: immediate PrEP scale-up and then continuation for 50 years, and no PrEP. We estimated the relationship between epidemic and programme characteristics and cost-effectiveness of PrEP availability to all during seasons of risk. For our base-case analysis, we assumed a 3-monthly PrEP cost of US$29 (drug $11, HIV test $4, and $14 for additional costs necessary to facilitate education and access), a cost-effectiveness threshold of $500 per disability-adjusted life-year (DALY) averted, an annual discount rate of 3%, and a time horizon of 50 years. In sensitivity analyses, we considered a cost-effectiveness threshold of $100 per DALY averted, a discount rate of 7% per annum, the use of PrEP outside of seasons of risk, and reduced uptake of risk-informed PrEP.FindingsIn the context of PrEP scale-up such that 66% (90% range across setting-scenarios 46-81) of HIV-negative people with at least one non-primary condomless sex partner take PrEP in any given period, resulting in 2·6% (0·9-6·0) of all HIV negative adults taking PrEP at any given time, risk-informed PrEP was predicted to reduce HIV incidence by 49% (23-78) over 50 years compared with no PrEP. PrEP was cost-effective in 71% of all setting-scenarios, and cost-effective in 76% of setting-scenarios with prevalence of HIV viral load greater than 1000 copies per mL among all adults higher than 2%. In sensitivity analyses with a $100 per DALY averted cost-effectiveness threshold, a 7% per year discount rate, or with PrEP use that was less well risk-informed than in our base case, PrEP was less likely to be cost-effective, but generally remained cost-effective if the prevalence of HIV viral load greater than 1000 copies per mL among all adults was higher than 3%. In sensitivity analyses based on additional setting-scenarios in which risk-informed PrEP was less extensively used, the HIV incidence reduction was smaller, but the cost-effectiveness of risk-informed PrEP was undiminished.InterpretationUnder the assumption that making PrEP easily accessible for all adults in sub-Saharan Africa in the context of community education leads to risk-informed use, PrEP is likely to be cost-effective in settings with prevalence of HIV viral load greater than 1000 copies per mL among all adults higher than 2%, suggesting the need for implementation of such approaches, with ongoing evaluation.FundingUS Agency for International Development, US President's Emergency Plan for AIDS Relief, and Bill & Melinda Gates Foundation.

Published
2022

45. Extended optical treatment versus early patching with an intensive patching regimen in children with amblyopia in Europe (EuPatch): a multicentre, randomised controlled trial

Author

Mellors, Ashleigh, Mallory, Lucy, Teli, Seema, Sheth, Viral, Langmann, Andrea, Bruce, Alison, Smith, Angie, Powell, Christine, Cross, Meriel, North, Lorraine, Abbott, Joseph, Mohan, Meyyammai, Kafil-Hussain, Namir, Joseph, Annie, Webb, Hilary, Redmill, Brian, Lawler, Carly, Sturm, Veit, Purohit, Ravi, Gupta, Mohit, Elliott, Sue, Mataftsi, Asimina, Hamada, Samer, Evans, Megan, Hatebur, Simone, Hussain, Shazia, Orr, Julie, Farooq, Shegufta, Osborne, Daniel, Begum, Farzana, Crofts, Catherine, Pausch, Franziska, Gaugl, Heike, Haug, Jennifer, Jones, Ruth, Steinmair, Karin, Sharma, Tina, Hillier, Stephanie, Dent, Michelle, Patel, Selina, Lienhart, Anna, Pennington, Emma, Maymond, Sian, Ludden, Siobhán, Zafeiropoulos, Parakevas, Asproudis, Ioannis, Tsironi, Evangelia, Scheitlin, Caroline, Chauhan, Monica, Toor, Sonia, Bennett, Carolyn, McPherson, Charlie, Ramm, Laura, Bibi, Mashal, Hussain, Hafsah, Samaddar, Julie, Shinh, Raadhika, Sarna, Sachi, Amlani, Kavita, Sauer, Wiebke, Kurt, Andrea, Chung-Crossley, Jenny, Ashraf, Nabila, Tailor, Vijay, Stewart, Catherine, Proudlock, Frank A, Hisaund, Michael, Maconachie, Gail, Papageorgiou, Eleni, Manouchehrinia, Ali, Dahlmann-Noor, Annegret, Khandelwal, Payal, Self, Jay, Beisse, Christina, and Gottlob, Irene

Published
2024
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47. Time to Viral Rebound After Interruption of Modern Antiretroviral Therapies

Author

Li, Jonathan Z, Aga, Evgenia, Bosch, Ronald J, Pilkinton, Mark, Kroon, Eugène, MacLaren, Lynsay, Keefer, Michael, Fox, Lawrence, Barr, Liz, Acosta, Edward, Ananworanich, Jintanat, Coombs, Robert, Mellors, John W, Landay, Alan L, Macatangay, Bernard, Deeks, Steven, Gandhi, Rajesh T, and Smith, Davey M

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Infectious Diseases, Clinical Research, Clinical Trials and Supportive Activities, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Anti-Retroviral Agents, HIV Infections, Humans, Viral Load, HIV treatment interruption, viral rebound, posttreatment controller, Biological Sciences, Medical and Health Sciences, Microbiology, Clinical sciences
Abstract

BackgroundDevelopment of human immunodeficiency virus (HIV) remission strategies requires precise information on time to HIV rebound after treatment interruption, but there is uncertainty regarding whether modern antiretroviral therapy (ART) regimens and timing of ART initiation may affect this outcome.MethodsAIDS Clinical Trials Group (ACTG) A5345 enrolled individuals who initiated ART during chronic or early HIV infection and on suppressive ART for ≥2 years. Participants underwent carefully monitored antiretroviral interruption. ART was restarted upon 2 successive viral loads ≥1000 copies/mL. We compared participants of A5345 with participants of 6 historic ACTG treatment interruption studies.ResultsThirty-three chronic-treated and 12 early-treated participants interrupted ART with evaluable time to viral rebound. Median time to viral rebound ≥1000 HIV RNA copies/mL was 22 days. Acute retroviral rebound syndrome was diagnosed in 9% of the chronic-treated and none of the early-treated individuals. All participants of the historic studies were on older protease inhibitor-based regimens, whereas 97% of A5345 participants were on integrase inhibitor-based ART. There were no differences in the timing of viral rebound comparing A5345 versus historic studies. In a combined analysis, a higher percentage of early-treated participants remained off ART at posttreatment interruption week 12 (chronic vs early: 2% vs 9%, P = .0496). One chronic-treated and one early-treated A5345 participant remained off ART for >24 weeks. All participants resuppressed after ART reinitiation.ConclusionsEarly ART initiation, using either older or newer ART regimens, was associated with a significant delay in the time to HIV rebound after ART interruption, lowering the barrier for HIV remission.

Published
2022

49. Associations of HIV persistence, cigarette smoking, inflammation, and pulmonary dysfunction in people with HIV on antiretroviral therapy

Author

Cyktor, Joshua, Qin, Shulin, Staines, Brittany, Nouraie, Mehdi, Fitzpatrick, Meghan, Kessinger, Cathy, DeSensi, Rebecca, Huang, Laurence, Rinaldo, Charles R, Kingsley, Lawrence, Tien, Phyllis C, Mellors, John W, and Morris, Alison

Subjects
Tobacco, Infectious Diseases, Tobacco Smoke and Health, Genetics, HIV/AIDS, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Infection, Anti-HIV Agents, Cigarette Smoking, DNA, Viral, Female, HIV Infections, HIV-1, Humans, Inflammation, Leukocytes, Mononuclear, Male, Middle Aged, RNA, RNA, Viral, Retrospective Studies, Viral Load, cytokines, HIV-1 reservoirs, inflammation, pulmonary function, single copy assay, smoking, Clinical Sciences, Arthritis & Rheumatology
Abstract

We aimed to investigate the relationship between measures of HIV persistence with antiretroviral therapy (ART) and cigarette smoking, systemic markers of inflammation, and pulmonary function. Retrospective study of 82 people with HIV (PWH) on ART for a median of 6.9 years (5.6-7.8) and plasma HIV RNA levels

Published
2022

50. The EGS Collab Project-Stimulations at Two Depths

Author

Kneafsey, TJ, Dobson, PF, Ulrich, C, Hopp, C, Rodríguez-Tribaldos, V, Guglielmi, Y, Blankenship, D, Schwering, PC, Ingraham, M, Burghardt, JA, White, MD, Johnson, TC, Strickland, C, Vermuel, V, Knox, HA, Morris, JP, Fu, P, Smith, M, Wu, H, Ajo-Franklin, JB, Huang, L, Neupane, G, Horne, R, Roggenthen, W, Weers, J, Doe, TW, Pyatina, T, Ajo-Franklin, J, Baumgartner, T, Beckers, K, Bonneville, A, Boyd, L, Brown, S, Chai, C, Chakravarty, A, Chen, T, Chen, Y, Chi, B, Condon, K, Cook, PJ, Crandall, D, Doe, T, Doughty, CA, Elsworth, D, Feldman, J, Feng, Z, Foris, A, Frash, LP, Frone, Z, Gao, K, Ghassemi, A, Haimson, B, Hawkins, A, Heise, J, Horn, M, Horne, RN, Horner, J, Hu, M, Huang, H, Im, KJ, Jafarov, E, Jayne, RS, Johnson, SE, Johnston, B, Karra, S, Kim, K, King, DK, Kneafsey, T, Knox, H, Knox, J, Kumar, D, Kutun, K, Lee, M, Li, D, Li, J, Li, K, Li, Z, Maceira, M, Mackey, P, Makedonska, N, Marone, CJ, Mattson, E, McClure, MW, McLennan, J, McLing, T, Medler, C, Mellors, RJ, Metcalfe, E, Miskimins, J, Moore, J, and Morency, CE

Abstract

The EGS Collab project, supported by the US Department of Energy, is performing intensively monitored rock stimulation and flow tests at the 10-m scale in an underground research laboratory to address challenges in implementing enhanced geothermal systems (EGS). Data and observations from the field tests are compared to simulations to understand processes and build confidence in numerical modeling of the processes. We have completed Experiment 1 (of 3), which examined hydraulic fracturing in a well-characterized underground fractured phyllite test bed at a depth of approximately 1.5 km at the Sanford Underground Research Facility (SURF) in Lead, South Dakota. Testbed characterization included fracture mapping, borehole acoustic and optical televiewers, full waveform sonic, conductivity, resistivity, temperature, campaign p- and s-wave investigations and electrical resistance tomography. Borehole geophysical techniques including passive seismic, continuous active source seismic monitoring, electrical resistance tomography, fiber-based distributed strain, distributed temperature, and distributed acoustic monitoring, were used to carefully monitor stimulation events and flow tests. More than a dozen stimulations and nearly one year of flow tests were performed. Quality data and detailed observations were collected and analyzed during stimulation and water flow tests using ambient temperature and chilled water. We achieved adaptive control of the tests using real-time monitoring and rapid dissemination of data and near-real-time simulation. More detailed numerical simulation was performed to answer key experimental design questions, forecast fracture propagation trajectories and extents, and analyze and evaluate results. Data are freely available from the Geothermal Data Repository. Experiment 2 examines the potential for hydraulic shearing in amphibolite at a depth of about 1.25 km at SURF. This site has a different set of stress and fracture conditions than Experiment 1. The Experiment 2 testbed consists of nine subhorizontal boreholes configured in two fans of two boreholes which surround the testbed and contain grouted-in electrical resistance tomography, seismic sensors, active seismic sources and distributed fiber sensors. A “five-spot” set of test wells that extends from a custom mined alcove includes an injection well and four production/monitoring wells. The testbed was characterized geophysically and hydrologically, and three stimulations have been performed using the Step-Rate Injection Method for Fracture In-Situ Properties (SIMFIP) tool to measure strains, and a new strain quantifying tool (downhole robotic strain analysis tool -DORSA) was deployed in a monitoring hole during stimulation. Real-time data were broadcast during stimulations to allow real-time response to arising issues.

Published
2022

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