Your search keyword '"Price, Karen"' showing total 20 results

1. Cardiotrophin‐1 therapy reduces disease severity in a murine model of glomerular disease.

Author

Perretta‐Tejedor, Nuria, Price, Karen L., Jafree, Daniyal J., Pomeranz, Gideon, Kolatsi‐Joannou, Maria, Martínez‐Salgado, Carlos, Long, David A., and Vasilopoulou, Elisavet

Subjects

*RENAL fibrosis, *KIDNEY cortex, *KIDNEY glomerulus diseases, *PARIETAL cells, *KIDNEY diseases, *DIABETIC nephropathies, *KIDNEY physiology

Abstract

Cardiotrophin‐1 (CT‐1), a member of the interleukin (IL)‐6 cytokine family, has renoprotective effects in mouse models of acute kidney disease and tubulointerstitial fibrosis, but its role in glomerular disease is unknown. To address this, we used the mouse model of nephrotoxic nephritis to test the hypothesis that CT‐1 also has a protective role in immune‐mediated glomerular disease. Using immunohistochemistry and analysis of single‐cell RNA‐sequencing data of isolated glomeruli, we demonstrate that CT‐1 is expressed in the glomerulus in male mice, predominantly in parietal epithelial cells and is downregulated in mice with nephrotoxic nephritis. Furthermore, analysis of data from patients revealed that human glomerular disease is also associated with reduced glomerular CT‐1 transcript levels. In male mice with nephrotoxic nephritis and established proteinuria, administration of CT‐1 resulted in reduced albuminuria, prevented podocyte loss, and sustained plasma creatinine, compared with mice administered saline. CT‐1 treatment also reduced fibrosis in the kidney cortex, peri‐glomerular macrophage accumulation and the kidney levels of the pro‐inflammatory mediator complement component 5a. In conclusion, CT‐1 intervention therapy delays the progression of glomerular disease in mice by preserving kidney function and inhibiting renal inflammation and fibrosis. [ABSTRACT FROM AUTHOR]

Published

2024

2. First‐in‐Human Study of Bamlanivimab in a Randomized Trial of Hospitalized Patients With COVID‐19.

Author

Chen, Peter, Datta, Gourab, Grace Li, Ying, Chien, Jenny, Price, Karen, Chigutsa, Emmanuel, Brown‐Augsburger, Patricia, Poorbaugh, Josh, Fill, Jeffrey, Benschop, Robert J., Rouphael, Nadine, Kay, Ariel, Mulligan, Mark J., Saxena, Amit, Fischer, William A., Dougan, Michael, Klekotka, Paul, Nirula, Ajay, and Benson, Charles

Subjects

COVID-19, HOSPITAL patients, SARS-CoV-2, MONOCLONAL antibodies, PANDEMICS

Abstract

Therapeutics for patients hospitalized with coronavirus disease 2019 (COVID‐19) are urgently needed during the pandemic. Bamlanivimab is a potent neutralizing monoclonal antibody that blocks severe acute respiratory syndrome‐coronavirus 2 (SARS‐CoV‐2) attachment and entry into human cells, which could potentially lead to therapeutic benefit. J2W‐MC‐PYAA was a randomized, double‐blind, sponsor unblinded, placebo‐controlled, single ascending dose first‐in‐human trial (NCT04411628) in hospitalized patients with COVID‐19. A total of 24 patients received either placebo or a single dose of bamlanivimab (700 mg, 2,800 mg, or 7,000 mg). The primary objective was assessment of safety and tolerability, including adverse events and serious adverse events, with secondary objectives of pharmacokinetic (PK) and pharmacodynamic analyses. Treatment‐emergent adverse event (TEAE) rates were identical in the placebo and pooled bamlanivimab groups (66.7%). There were no apparent dose‐related increases in the number or severity of TEAEs. There were no serious adverse events or deaths during the study, and no discontinuations due to adverse events. PKs of bamlanivimab is linear and exposure increased proportionally with dose following single i.v. administration. The half‐life was ~ 17 days. These results demonstrate the favorable safety profile of bamlanivimab, and provided the initial critical evaluation of safety, tolerability, and PKs in support of the development of bamlanivimab in several ongoing clinical trials. [ABSTRACT FROM AUTHOR]

Published

2021

3. The importance of cultural humility and cultural safety in health care.

Author

So, Neda, Price, Karen, O'Mara, Peter, and Rodrigues, Michelle A

Abstract

The article discusses the importance of cultural humility and cultural safety in healthcare. While cultural competency is a well-established concept, the authors argue that there is a need to focus on more advanced frameworks of cultural humility and cultural safety. Cultural humility involves recognizing one's own biases and adopting a mindset of lifelong learning when working with diverse communities. Cultural safety involves addressing power imbalances, minimizing racism and discrimination, and prioritizing safety and inclusivity in healthcare. The article emphasizes the need for cultural humility and cultural safety in addressing health disparities and improving health outcomes for minority groups, including immigrants, refugees, racial and ethnic minorities, and Aboriginal and Torres Strait Islander people. [Extracted from the article]

Published

2024

4. Subtype‐specific differences in transmission cluster dynamics of HIV‐1 B and CRF01_AE in New South Wales, Australia.

Author

Di Giallonardo, Francesca, Pinto, Angie N, Keen, Phillip, Shaik, Ansari, Carrera, Alex, Salem, Hanan, Selvey, Christine, Nigro, Steven J, Fraser, Neil, Price, Karen, Holden, Joanne, Lee, Frederick J, Dwyer, Dominic E, Bavinton, Benjamin R, Geoghegan, Jemma L, Grulich, Andrew E, and Kelleher, Anthony D

Subjects

HIV, MEN who have sex with men

Abstract

Introduction: The human immunodeficiency virus 1 (HIV‐1) pandemic is characterized by numerous distinct sub‐epidemics (clusters) that continually fuel local transmission. The aims of this study were to identify active growing clusters, to understand which factors most influence the transmission dynamics, how these vary between different subtypes and how this information might contribute to effective public health responses. Methods: We used HIV‐1 genomic sequence data linked to demographic factors that accounted for approximately 70% of all new HIV‐1 notifications in New South Wales (NSW). We assessed differences in transmission cluster dynamics between subtype B and circulating recombinant form 01_AE (CRF01_AE). Separate phylogenetic trees were estimated using 2919 subtype B and 473 CRF01_AE sequences sampled between 2004 and 2018 in combination with global sequence data and NSW‐specific clades were classified as clusters, pairs or singletons. Significant differences in demographics between subtypes were assessed with Chi‐Square statistics. Results: We identified 104 subtype B and 11 CRF01_AE growing clusters containing a maximum of 29 and 11 sequences for subtype B and CRF01_AE respectively. We observed a > 2‐fold increase in the number of NSW‐specific CRF01_AE clades over time. Subtype B clusters were associated with individuals reporting men who have sex with men (MSM) as their transmission risk factor, being born in Australia, and being diagnosed during the early stage of infection (p < 0.01). CRF01_AE infections clusters were associated with infections among individuals diagnosed during the early stage of infection (p < 0.05) and CRF01_AE singletons were more likely to be from infections among individuals reporting heterosexual transmission (p < 0.05). We found six subtype B clusters with an above‐average growth rate (>1.5 sequences / 6‐months) and which consisted of a majority of infections among MSM. We also found four active growing CRF01_AE clusters containing only infections among MSM. Finally, we found 47 subtype B and seven CRF01_AE clusters that contained a large gap in time (>1 year) between infections and may be indicative of intermediate transmissions via undiagnosed individuals. Conclusions: The large number of active and growing clusters among MSM are the driving force of the ongoing epidemic in NSW for subtype B and CRF01_AE. [ABSTRACT FROM AUTHOR]

Published

2021

5. Vangl2, a planar cell polarity molecule, is implicated in irreversible and reversible kidney glomerular injury.

Author

Papakrivopoulou, Eugenia, Vasilopoulou, Elisavet, Lindenmeyer, Maja T, Pacheco, Sabrina, Brzóska, Hortensja Ł, Price, Karen L, Kolatsi‐Joannou, Maria, White, Kathryn E, Henderson, Deborah J, Dean, Charlotte H, Cohen, Clemens D, Salama, Alan D, Woolf, Adrian S, and Long, David A

Abstract

Planar cell polarity (PCP) pathways control the orientation and alignment of epithelial cells within tissues. Van Gogh‐like 2 (Vangl2) is a key PCP protein that is required for the normal differentiation of kidney glomeruli and tubules. Vangl2 has also been implicated in modifying the course of acquired glomerular disease, and here, we further explored how Vangl2 impacts on glomerular pathobiology in this context. Targeted genetic deletion of Vangl2 in mouse glomerular epithelial podocytes enhanced the severity of not only irreversible accelerated nephrotoxic nephritis but also lipopolysaccharide‐induced reversible glomerular damage. In each proteinuric model, genetic deletion of Vangl2 in podocytes was associated with an increased ratio of active‐MMP9 to inactive MMP9, an enzyme involved in tissue remodelling. In addition, by interrogating microarray data from two cohorts of renal patients, we report increased VANGL2 transcript levels in the glomeruli of individuals with focal segmental glomerulosclerosis, suggesting that the molecule may also be involved in certain human glomerular diseases. These observations support the conclusion that Vangl2 modulates glomerular injury, at least in part by acting as a brake on MMP9, a potentially harmful endogenous enzyme. © 2018 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland. [ABSTRACT FROM AUTHOR]

Published

2018

6. Statistical modeling for Bayesian extrapolation of adult clinical trial information in pediatric drug evaluation.

Author

Gamalo‐Siebers, Margaret, Savic, Jasmina, Basu, Cynthia, Zhao, Xin, Gopalakrishnan, Mathangi, Gao, Aijun, Song, Guochen, Baygani, Simin, Thompson, Laura, Xia, H. Amy, Price, Karen, Tiwari, Ram, and Carlin, Bradley P.

Subjects

STATISTICAL methods in clinical trials, PEDIATRIC drug therapy, BAYESIAN analysis, ULCERATIVE colitis in children, INFLIXIMAB, DRUG efficacy, DRUG development, EXTRAPOLATION, THERAPEUTICS

Abstract

Children represent a large underserved population of 'therapeutic orphans,' as an estimated 80% of children are treated off-label. However, pediatric drug development often faces substantial challenges, including economic, logistical, technical, and ethical barriers, among others. Among many efforts trying to remove these barriers, increased recent attention has been paid to extrapolation; that is, the leveraging of available data from adults or older age groups to draw conclusions for the pediatric population. The Bayesian statistical paradigm is natural in this setting, as it permits the combining (or 'borrowing') of information across disparate sources, such as the adult and pediatric data. In this paper, authored by the pediatric subteam of the Drug Information Association Bayesian Scientific Working Group and Adaptive Design Working Group, we develop, illustrate, and provide suggestions on Bayesian statistical methods that could be used to design improved pediatric development programs that use all available information in the most efficient manner. A variety of relevant Bayesian approaches are described, several of which are illustrated through 2 case studies: extrapolating adult efficacy data to expand the labeling for Remicade to include pediatric ulcerative colitis and extrapolating adult exposure-response information for antiepileptic drugs to pediatrics. [ABSTRACT FROM AUTHOR]

Published

2017

7. Incorporation of individual-patient data in network meta-analysis for multiple continuous endpoints, with application to diabetes treatment.

Author

Hong, Hwanhee, Fu, Haoda, Price, Karen L., and Carlin, Bradley P.

Abstract

Availability of individual patient-level data (IPD) broadens the scope of network meta-analysis (NMA) and enables us to incorporate patient-level information. Although IPD is a potential gold mine in biomedical areas, methodological development has been slow owing to limited access to such data. In this paper, we propose a Bayesian IPD NMA modeling framework for multiple continuous outcomes under both contrast-based and arm-based parameterizations. We incorporate individual covariate-by-treatment interactions to facilitate personalized decision making. Furthermore, we can find subpopulations performing well with a certain drug in terms of predictive outcomes. We also impute missing individual covariates via an MCMC algorithm. We illustrate this approach using diabetes data that include continuous bivariate efficacy outcomes and three baseline covariates and show its practical implications. Finally, we close with a discussion of our results, a review of computational challenges, and a brief description of areas for future research. Copyright © 2015 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2015

8. Bayesian methods for design and analysis of safety trials.

Author

Price, Karen L., Amy Xia, H., Lakshminarayanan, Mani, Madigan, David, Manner, David, Scott, John, Stamey, James D., and Thompson, Laura

Subjects

*BAYESIAN analysis, *CLINICAL trials, *MEDICATION safety, *DRUG development, *TYPE 2 diabetes treatment

Abstract

Safety assessment is essential throughout medical product development. There has been increased awareness of the importance of safety trials recently, in part due to recent US Food and Drug Administration guidance related to thorough assessment of cardiovascular risk in the treatment of type 2 diabetes. Bayesian methods provide great promise for improving the conduct of safety trials. In this paper, the safety subteam of the Drug Information Association Bayesian Scientific Working Group evaluates challenges associated with current methods for designing and analyzing safety trials and provides an overview of several suggested Bayesian opportunities that may increase efficiency of safety trials along with relevant case examples. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2014

9. Guidance on the implementation and reporting of a drug safety Bayesian network meta-analysis.

Author

Ohlssen, David, Price, Karen L., Amy Xia, H., Hong, Hwanhee, Kerman, Jouni, Fu, Haoda, Quartey, George, Heilmann, Cory R., Ma, Haijun, and Carlin, Bradley P.

Subjects

*MEDICATION safety, *DRUG development, *BAYESIAN analysis, *HEALTH outcome assessment, *ANTI-inflammatory agents, *META-analysis

Abstract

The Drug Information Association Bayesian Scientific Working Group (BSWG) was formed in 2011 with a vision to ensure that Bayesian methods are well understood and broadly utilized for design and analysis and throughout the medical product development process, and to improve industrial, regulatory, and economic decision making. The group, composed of individuals from academia, industry, and regulatory, has as its mission to facilitate the appropriate use and contribute to the progress of Bayesian methodology. In this paper, the safety sub-team of the BSWG explores the use of Bayesian methods when applied to drug safety meta-analysis and network meta-analysis. Guidance is presented on the conduct and reporting of such analyses. We also discuss different structural model assumptions and provide discussion on prior specification. The work is illustrated through a case study involving a network meta-analysis related to the cardiovascular safety of non-steroidal anti-inflammatory drugs. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2014

10. Bayesian modeling of cost-effectiveness studies with unmeasured confounding: a simulation study.

Author

Stamey, James D., Beavers, Daniel P., Faries, Douglas, Price, Karen L., and Seaman, John W.

Subjects

BAYESIAN analysis, COST effectiveness, SIMULATION methods & models, HEALTH policy, MEDICAL decision making

Abstract

Unmeasured confounding is a common problem in observational studies. Failing to account for unmeasured confounding can result in biased point estimators and poor performance of hypothesis tests and interval estimators. We provide examples of the impacts of unmeasured confounding on cost-effectiveness analyses using observational data along with a Bayesian approach to correct estimation. Assuming validation data are available, we propose a Bayesian approach to correct cost-effectiveness studies for unmeasured confounding. We consider the cases where both cost and effectiveness are assumed to have a normal distribution and when costs are gamma distributed and effectiveness is normally distributed. Simulation studies were conducted to determine the impact of ignoring the unmeasured confounder and to determine the size of the validation data required to obtain valid inferences. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2014

11. Referrals into services for offenders with intellectual disabilities: Variables predicting community or secure provision.

Author

Carson, Derek, Lindsay, William R., O'Brien, Gregory, Holland, Anthony J., Taylor, John L., Wheeler, Jessica R., Middleton, Claire, Price, Karen, Steptoe, Lesley, and Johnston, Susan

Subjects

CRIMINALS with mental illness, DISABILITIES, ALTERNATIVE treatment for developmental disabilities, FORENSIC sciences, DEMOGRAPHIC surveys, MULTIVARIATE analysis, CASE studies

Abstract

Background There is a need for research to promote an understanding among service developers on why people with intellectual disabilities (ID) are referred to offender services in order for them to receive appropriate assessment and treatment. Previous studies investigating referrals into forensic ID services have concentrated on referral sources and administrative variables such as legal status. Aims To construct a predictive model for choice of service referral based on a comprehensive range of information about the clientele. Method We conducted a case record study of 336 people referred to community services and 141 to secure provision. We gathered information on referral source, demographics, diagnosis, index behaviour, prior problem behaviours and history of abuse. Results Comparisons revealed 19 candidate variables which were then entered into multivariate logistic regression. The resulting model retained six variables: community living at time of referral, physical aggression, being charged, referral from tertiary health care, diverse problem behaviour and IQ < 50, which correctly predicted the referral pathway for 85.7% of cases. Conclusions An index act of physical aggression and a history of diversity of problem behaviours as predictors against the likelihood of community service referral suggest that professionals have similar concerns about people with ID as they do about their more average offending peers; however, the more severe levels of ID mitigated in favour of community referral, regardless. Offenders with ID tend to be referred within levels of service rather than between them, for example, form tertiary services into generic community services. Copyright © 2010 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2010

12. Correlation of vibratory quantitative sensory testing and nerve conduction studies in patients with diabetes.

Author

Kincaid, John C., Price, Karen L., Jimenez, Maria C., and Skljarevski, Vladimir

Abstract

Monitoring the course of diabetic peripheral neuropathy (DPN) remains a challenge. Besides clinical examination, nerve conduction studies (NCS) and quantitative sensory testing (QST) are the most commonly used methods for evaluating peripheral nerve function in clinical trials and population studies. In this study the correlation between vibratory QST and NCS was determined. Patients ( N = 227) with diabetes mellitus participated in this multicenter, single-visit, cross-sectional study. QST of vibration measured with the CASE IV system was compared with a composite score of peroneal motor and tibial motor NCS and with individual attributes of peroneal, tibial, and sural nerves. The correlation between QST and composite score of NCS was 0.234 (Pearson correlation coefficient, P = 0.001). The correlations between QST and individual attributes of NCS ranged from 0.189 to 0.480 (Pearson correlation coefficients, P < 0.001). The low to moderate correlation between QST and NCS suggests that these tests cannot replace each other but are complementary. Muscle Nerve, 2007 [ABSTRACT FROM AUTHOR]

Published

2007

13. The phagocytic capacity of neurones.

Author

Bowen, Samantha, Ateh, Davidson D., Deinhardt, Katrin, Bird, Margaret M., Price, Karen M., Baker, Cathy S., Robson, Joanna C., Swash, Michael, Shamsuddin, Wassim, Kawar, Shalini, El‐Tawil, Tariq, Roos, Jesper, Hoyle, Andrew, Nickols, Carole D., Knowles, Charles H., Pullen, Anthony H., Luthert, Phillip J., Weller, Roy O., Hafezparast, Majid, and Franklin, Robin J. M.

Subjects

NEURONS, PHAGOCYTOSIS, MACROPHAGES, CELL receptors, CELL death

Abstract

Phagocytosis is defined as the ingestion of particulates over 0.5 µm in diameter and is associated with cells of the immune system such as macrophages or monocytes. Neurones are not generally recognized to be phagocytic. Using light, confocal, time-lapse and electron microscopy, we carried out a wide range of in-vitro and in-vivo experiments to examine the phagocytic capacity of different neuronal cell types. We demonstrated phagocytosis of material by neurones, including cell debris and synthetic particles up to 2.8 µm in diameter. We showed phagocytosis in different neuronal types, and demonstrated that debris can be transported from neurite extremities to cell bodies and persist within neurones. Flow cytometry analysis demonstrated the lack of certain complement receptors on neurones but the presence of others, including integrin receptors known to mediate macrophage phagocytosis, indicating that a restricted set of phagocytosis receptors may mediate this process. Neuronal phagocytosis occurs in vitro and in vivo, and we propose that this is a more widespread and significant process than previously recognized. Neuronal phagocytosis may explain certain inclusions in neurones during disease, cell-to-cell spread of disease, neuronal death during disease progression and provide a potential mechanism for therapeutic intervention through the delivery of particulate drug carriers. [ABSTRACT FROM AUTHOR]

Published

2007

14. Ki-67 expression in breast carcinoma.

Author

Trihia, Helen, Murray, Susan, Price, Karen, Gelber, Richard D., Golouh, Rastko, Goldhirsch, Aron, Coates, Alan S., Collins, John, Castiglione-Gertsch, Monica, and Gusterson, Barry A.

Published

2003

15. EPIPHYTIC LICHEN ABUNDANCE: EFFECTS OF STAND AGE AND COMPOSITION IN COASTAL BRITISH COLUMBIA.

Author

Price, Karen and Hochachka, Gail

Subjects

EPIPHYTIC lichens, AGE of plants, COASTAL ecology, EPIPHYTES

Abstract

The article focuses on a study on epiphytic lichen abundance in in coastal British Columbia. It states the analysis of stand age and type on epiphytic lichen composition in the study, and mentions increase in the epiphytic lichen abundance and the percentage of alectorioid lichens with increasing stand age. It notes that composition varied with location.

Published

2001

16. Present and future projects of the international breast cancer study group.

Author

Goldhirsch, Aron, Gelber, Richard D., Castiglione, Monica, Price, Karen N., Rudenstam, Carl-Magnus, Lindtner, Jurij, Collins, John, Senn, Hans-Jörg, Brunner, Kurt W., Galligioni, Enzo, Cavalli, Franco, Gudgeon, Anne, Cortes-Funes, Hernan, Tattersall, Martin, Marini, Giovanni, Byrne, Michael, Snyder, Ray, Forbes, John F., Hürny, Christoph, and Coates, Alan

Published

1994

17. Bayesian Methods in Medical Product Development and Regulatory Reviews.

Author

Price, Karen and LaVange, Lisa

Subjects

*BAYESIAN analysis, *NONLINEAR statistical models

Abstract

An introduction is presented in which the author discusses various articles within the issue on topics including Bayesian group sequential designs, nonlinear mixed-effects models, and the Bayesian approach for evaluating the impact of unmeasured confounding.

Published

2014

18. Comparing aromatase inhibitors in the absence of clinical trial results can be misleading.

Author

Goldhirsch, Aron and Price, Karen N.

Published

2007

19. Cognition Impairment Precedes and Predicts Functional Impairment in Mild Alzhiemer's Disease.

Author

Liu-Seifert, Hong, Siemers, Eric, Price, Karen, Han, Baoguang, Selzler, Katherine, Henley, David, Sundell, Karen, Aisen, Paul, Cummings, Jeffrey, Raskin, Joel, and Mohs, Richard

Published

2014

20. A Convenient One-Pot Synthesis of 4-, 6-, and 7-Azaindoles from Aminopyridines.

Author

Debenham, Sheryl D., Chan, Audrey, Liu, Kun, Price, Karen, and Wood, Harold B.

Published

2005