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2. Prognostic significance of haemodynamic parameters in patients with cardiogenic shock.

Author

Berg, David, Kaur, Gurleen, Bohula, Erin, Baird-Zars, Vivian, Alviar, Carlos, Barnett, Christopher, Barsness, Gregory, Burke, James, Chaudhry, Sunit-Preet, Chonde, Meshe, Cooper, Howard, Daniels, Lori, Dodson, Mark, Gerber, Daniel, Ghafghazi, Shahab, Gidwani, Umesh, Goldfarb, Michael, Guo, Jianping, Hillerson, Dustin, Kenigsberg, Benjamin, Kochar, Ajar, Kontos, Michael, Kwon, Younghoon, Lopes, Mathew, Loriaux, Daniel, Miller, P, Papolos, Alexander, Patel, Siddharth, Pisani, Barbara, Potter, Brian, Prasad, Rajnish, Rowsell, Robert, Shah, Kevin, Sinha, Shashank, Smith, Timothy, Solomon, Michael, Teuteberg, Jeffrey, Thompson, Andrea, Zakaria, Sammy, Katz, Jason, van Diepen, Sean, Morrow, David, and OBrien, Connor

Subjects
Cardiogenic shock, Haemodynamics, Outcomes, Pulmonary artery catheter, Humans, Shock, Cardiogenic, Prognosis, Hemodynamics, Vascular Resistance, Lactates
Abstract

AIMS: Invasive haemodynamic assessment with a pulmonary artery catheter is often used to guide the management of patients with cardiogenic shock (CS) and may provide important prognostic information. We aimed to assess prognostic associations and relationships to end-organ dysfunction of presenting haemodynamic parameters in CS. METHODS AND RESULTS: The Critical Care Cardiology Trials Network is an investigator-initiated multicenter registry of cardiac intensive care units (CICUs) in North America coordinated by the TIMI Study Group. Patients with CS (2018-2022) who underwent invasive haemodynamic assessment within 24 h of CICU admission were included. Associations of haemodynamic parameters with in-hospital mortality were assessed using logistic regression, and associations with presenting serum lactate were assessed using least squares means regression. Sensitivity analyses were performed excluding patients on temporary mechanical circulatory support and adjusted for vasoactive-inotropic score. Among the 3603 admissions with CS, 1473 had haemodynamic data collected within 24 h of CICU admission. The median cardiac index was 1.9 (25th-75th percentile, 1.6-2.4) L/min/m2 and mean arterial pressure (MAP) was 74 (66-86) mmHg. Parameters associated with mortality included low MAP, low systolic blood pressure, low systemic vascular resistance, elevated right atrial pressure (RAP), elevated RAP/pulmonary capillary wedge pressure ratio, and low pulmonary artery pulsatility index. These associations were generally consistent when controlling for the intensity of background pharmacologic and mechanical haemodynamic support. These parameters were also associated with higher presenting serum lactate. CONCLUSION: In a contemporary CS population, presenting haemodynamic parameters reflecting decreased systemic arterial tone and right ventricular dysfunction are associated with adverse outcomes and systemic hypoperfusion.

Published
2023

3. The management of heart failure cardiogenic shock: an international RAND appropriateness panel

Author

Williams, Stefan, Kalakoutas, Antonis, Olusanya, Segun, Schrage, Benedict, Tavazzi, Guido, Carnicelli, Anthony P., Montero, Santiago, Vandenbriele, Christophe, Luk, Adriana, Lim, Hoong Sern, Bhagra, Sai, Ott, Sascha C., Farrero, Marta, Samsky, Marc D., Kennedy, Jamie L. W., Sen, Sounok, Agrawal, Richa, Rampersad, Penelope, Coniglio, Amanda, Pappalardo, Federico, Barnett, Christopher, and Proudfoot, Alastair G.

Published
2024
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4. Pulmonary Artery Catheter Use and Mortality in the Cardiac Intensive Care Unit.

Author

Kadosh, Bernard, Berg, David, Bohula, Erin, Park, Jeong-Gun, Baird-Zars, Vivian, Alviar, Carlos, Alzate, James, Barnett, Christopher, Barsness, Gregory, Burke, James, Chaudhry, Sunit-Preet, Daniels, Lori, DeFilippis, Andrew, Delicce, Anthony, Fordyce, Christopher, Ghafghazi, Shahab, Gidwani, Umesh, Goldfarb, Michael, Katz, Jason, Keeley, Ellen, Kenigsberg, Benjamin, Kontos, Michael, Lawler, Patrick, Leibner, Evan, Menon, Venu, Metkus, Thomas, Miller, P, OBrien, Connor, Papolos, Alexander, Prasad, Rajnish, Shah, Kevin, Sinha, Shashank, Snell, R, So, Derek, Solomon, Michael, Ternus, Bradley, Teuteberg, Jeffrey, Toole, Joseph, van Diepen, Sean, Morrow, David, and Roswell, Robert

Subjects
cardiac intensive care, pulmonary artery catheter, shock, Humans, Pulmonary Artery, Heart Failure, Intensive Care Units, Hospitalization, Hospital Mortality, Catheters
Abstract

BACKGROUND: The appropriate use of pulmonary artery catheters (PACs) in critically ill cardiac patients remains debated. OBJECTIVES: The authors aimed to characterize the current use of PACs in cardiac intensive care units (CICUs) with attention to patient-level and institutional factors influencing their application and explore the association with in-hospital mortality. METHODS: The Critical Care Cardiology Trials Network is a multicenter network of CICUs in North America. Between 2017 and 2021, participating centers contributed annual 2-month snapshots of consecutive CICU admissions. Admission diagnoses, clinical and demographic data, use of PACs, and in-hospital mortality were captured. RESULTS: Among 13,618 admissions at 34 sites, 3,827 were diagnosed with shock, with 2,583 of cardiogenic etiology. The use of mechanical circulatory support and heart failure were the patient-level factors most strongly associated with a greater likelihood of the use of a PAC (OR: 5.99 [95% CI: 5.15-6.98]; P < 0.001 and OR: 3.33 [95% CI: 2.91-3.81]; P

Published
2023

5. Clinical and biological heterogeneity of multisystem inflammatory syndrome in adults following SARS-CoV-2 infection: a case series

Author

Barth, Kaia E, Spottiswoode, Natasha, Hurabielle, Charlotte, Subbaraj, Lakshmi, Consortium, COMET, Calfee, Carolyn S, Matthay, Michael A, French, Sarah, Connolly, Andrew, Hewitt, Stephen M, Vannella, Kevin M, Barnett, Christopher, Langelier, Charles R, and Patterson, Sarah

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Emerging Infectious Diseases, Coronaviruses Disparities and At-Risk Populations, Infectious Diseases, Coronaviruses, Prevention, Autoimmune Disease, 4.1 Discovery and preclinical testing of markers and technologies, 2.1 Biological and endogenous factors, Inflammatory and immune system, Infection, Good Health and Well Being, COVID-19, MIS-A, myocarditis, SARS-CoV-2, multisystem inflammatory syndrome, DKA, COMET Consortium, Biomedical and clinical sciences, Health sciences
Abstract

ImportanceMultisystem inflammatory syndrome in adults (MIS-A) is a poorly understood complication of SARS-CoV-2 infection with significant morbidity and mortality.ObjectiveIdentify clinical, immunological, and histopathologic features of MIS-A to improve understanding of the pathophysiology and approach to treatment.DesignThree cases of MIS-A following SARS-CoV-2 infection were clinically identified between October 2021 - March 2022 using the U.S. Centers for Disease Control and Prevention diagnostic criteria. Clinical, laboratory, imaging, and tissue data were assessed.FindingsAll three patients developed acute onset cardiogenic shock and demonstrated elevated inflammatory biomarkers at the time of hospital admission that resolved over time. One case co-occurred with new onset Type 1 diabetes and sepsis. Retrospective analysis of myocardial tissue from one case identified SARS-CoV-2 RNA. All three patients fully recovered with standard of care interventions plus immunomodulatory therapy that included intravenous immunoglobulin, corticosteroids, and in two cases, anakinra.ConclusionMIS-A is a severe post-acute sequela of COVID-19 characterized by systemic elevation of inflammatory biomarkers. In this series of three cases, we find that although clinical courses and co-existent diseases vary, even severe presentations have potential for full recovery with prompt recognition and treatment. In addition to cardiogenic shock, glucose intolerance, unmasking of autoimmune disease, and sepsis can be features of MIS-A, and SARS-CoV-2 myocarditis can lead to a similar clinical syndrome.

Published
2023

6. Critical Care Cardiology Trials Network (CCCTN): a cohort profile.

Author

Metkus, Thomas, Baird-Zars, Vivian, Alfonso, Carlos, Alviar, Carlos, Barnett, Christopher, Barsness, Gregory, Berg, David, Bertic, Mia, Bohula, Erin, Burke, James, Burstein, Barry, Chaudhry, Sunit-Preet, Cooper, Howard, Daniels, Lori, Fordyce, Christopher, Ghafghazi, Shahab, Goldfarb, Michael, Katz, Jason, Keeley, Ellen, Keller, Norma, Kenigsberg, Benjamin, Kontos, Michael, Kwon, Younghoon, Lawler, Patrick, Leibner, Evan, Liu, Shuangbo, Menon, Venu, Miller, P, Newby, L, Papolos, Alexander, Pierce, Matthew, Prasad, Rajnish, Pisani, Barbara, Potter, Brian, Roswell, Robert, Sinha, Shashank, Shah, Kevin, Smith, Timothy, Snell, R, So, Derek, Solomon, Michael, Ternus, Bradley, Teuteberg, Jeffrey, van Diepen, Sean, Zakaria, Sammy, Morrow, David, and OBrien, Connor

Subjects
Cardiac ICU, Cohort, Critical care, Epidemiology, Humans, United States, Critical Illness, Coronary Care Units, Critical Care, Registries, Cardiology
Abstract

AIMS: The aims of the Critical Care Cardiology Trials Network (CCCTN) are to develop a registry to investigate the epidemiology of cardiac critical illness and to establish a multicentre research network to conduct randomised clinical trials (RCTs) in patients with cardiac critical illness. METHODS AND RESULTS: The CCCTN was founded in 2017 with 16 centres and has grown to a research network of over 40 academic and clinical centres in the United States and Canada. Each centre enters data for consecutive cardiac intensive care unit (CICU) admissions for at least 2 months of each calendar year. More than 20 000 unique CICU admissions are now included in the CCCTN Registry. To date, scientific observations from the CCCTN Registry include description of variations in care, the epidemiology and outcomes of all CICU patients, as well as subsets of patients with specific disease states, such as shock, heart failure, renal dysfunction, and respiratory failure. The CCCTN has also characterised utilization patterns, including use of mechanical circulatory support in response to changes in the heart transplantation allocation system, and the use and impact of multidisciplinary shock teams. Over years of multicentre collaboration, the CCCTN has established a robust research network to facilitate multicentre registry-based randomised trials in patients with cardiac critical illness. CONCLUSION: The CCCTN is a large, prospective registry dedicated to describing processes-of-care and expanding clinical knowledge in cardiac critical illness. The CCCTN will serve as an investigational platform from which to conduct randomised controlled trials in this important patient population.

Published
2022

7. Loss of non-motor kinesin KIF26A causes congenital brain malformations via dysregulated neuronal migration and axonal growth as well as apoptosis.

Author

Qian, Xuyu, DeGennaro, Ellen, Talukdar, Maya, Akula, Shyam, Lai, Abbe, Shao, Diane, Gonzalez, Dilenny, Marciano, Jack, Smith, Richard, Hylton, Norma, Yang, Edward, Bazan, J, Barrett, Lee, Yeh, Rebecca, Hill, R, Beck, Samantha, Otani, Aoi, Angad, Jolly, Mitani, Tadahiro, Posey, Jennifer, Pehlivan, Davut, Calame, Daniel, Aydin, Hatip, Yesilbas, Osman, Parks, Kendall, England, Eleina, Im, Kiho, Taranath, Ajay, Scott, Hamish, Barnett, Christopher, Arts, Peer, Sherr, Elliott, Lupski, James, Walsh, Christopher, and Argilli, Emanuela

Subjects
apoptosis, cerebral cortex, congenital brain malformation, corpus callosum, development, genetics, kinesin, migration, organoid, Humans, Animals, Mice, Kinesins, Neurons, Focal Adhesion Protein-Tyrosine Kinases, Apoptosis, Brain
Abstract

Kinesins are canonical molecular motors but can also function as modulators of intracellular signaling. KIF26A, an unconventional kinesin that lacks motor activity, inhibits growth-factor-receptor-bound protein 2 (GRB2)- and focal adhesion kinase (FAK)-dependent signal transduction, but its functions in the brain have not been characterized. We report a patient cohort with biallelic loss-of-function variants in KIF26A, exhibiting a spectrum of congenital brain malformations. In the developing brain, KIF26A is preferentially expressed during early- and mid-gestation in excitatory neurons. Combining mice and human iPSC-derived organoid models, we discovered that loss of KIF26A causes excitatory neuron-specific defects in radial migration, localization, dendritic and axonal growth, and apoptosis, offering a convincing explanation of the disease etiology in patients. Single-cell RNA sequencing in KIF26A knockout organoids revealed transcriptional changes in MAPK, MYC, and E2F pathways. Our findings illustrate the pathogenesis of KIF26A loss-of-function variants and identify the surprising versatility of this non-motor kinesin.

Published
2022

8. RNA variant assessment using transactivation and transdifferentiation

Author

Azmanov, Dimitar N., Barnett, Christopher P., Barry, Simon C., Baynam, Gareth, Berkovic, Samuel F., Christodoulou, John, Coman, David J., Cooper, Sandra, Corbett, Mark A., Delatycki, Martin, Dudding, Tracy E., Fletcher, Sue, Gardner, Alison E., Gecz, Jozef, Higgins, Megan J., Hildebrand, Michael S., Jolly, Lachlan A., Lister, Ryan, McGaughran, Julie, Pflueger, Christian, Poulton, Cathryn, Roscioli, Tony, Hamish S. Scott, Ingrid Scheffer, Sinclair, Andrew H., Spurdle, Amanda B., Tan, Tiong Y., van Eyk, Clare L., Voineagu, Irina, Nicolas-Martinez, Emmylou C., Robinson, Olivia, Gardner, Alison, Ritchie, Tarin, Kroes, Thessa, Scheffer, Ingrid E., Barnier, Jean-Vianney, Rousseau, Véronique, Genevieve, David, Haushalter, Virginie, Piton, Amélie, Denommé-Pichon, Anne-Sophie, Bruel, Ange-Line, Nambot, Sophie, Isidor, Bertrand, Grigg, John, Gonzalez, Tina, Ghedia, Sondhya, Marchant, Rhett G., Bournazos, Adam, Wong, Wui-Kwan, Webster, Richard I., Evesson, Frances J., Jones, Kristi J., and Cooper, Sandra T.

Published
2024
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9. Meaningful coproduction with clinicians: establishing a practice-based research network with physiotherapists in regional Australia

Author

Gleadhill, Connor, Williams, Christopher M., Kamper, Steven J., Bolsewicz, Katarzyna, Delbridge, Andrew, Mahon, Benjamin, Donald, Bruce, Delore, Caitlin, Boettcher, Craig, Renfrew, David, Manvell, Joshua, Dooley, Katherine, Byrne, Michael, Watson, Toby, Makaroff, Andrew, Gibbs, Benedicta, Barnett, Christopher, Corrigan, Michael, Leyland, Murray, Mullen, Nicholas, Gallagher, Ryan, Zelinski, Samuel, Lamond, Steven, Maude, Travis, Davidson, Simon R. E., Robson, Emma, Da Silva, Priscilla Viana, and Manvell, Nicole

Published
2023
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10. Integrated multi-omics for rapid rare disease diagnosis on a national scale

Author

Lunke, Sebastian, Bouffler, Sophie E., Patel, Chirag V., Sandaradura, Sarah A., Wilson, Meredith, Pinner, Jason, Hunter, Matthew F., Barnett, Christopher P., Wallis, Mathew, Kamien, Benjamin, Tan, Tiong Y., Freckmann, Mary-Louise, Chong, Belinda, Phelan, Dean, Francis, David, Kassahn, Karin S., Ha, Thuong, Gao, Song, Arts, Peer, Jackson, Matilda R., Scott, Hamish S., Eggers, Stefanie, Rowley, Simone, Boggs, Kirsten, Rakonjac, Ana, Brett, Gemma R., de Silva, Michelle G., Springer, Amanda, Ward, Michelle, Stallard, Kirsty, Simons, Cas, Conway, Thomas, Halman, Andreas, Van Bergen, Nicole J., Sikora, Tim, Semcesen, Liana N., Stroud, David A., Compton, Alison G., Thorburn, David R., Bell, Katrina M., Sadedin, Simon, North, Kathryn N., Christodoulou, John, and Stark, Zornitza

Published
2023
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11. Author Correction: Genomic autopsy to identify underlying causes of pregnancy loss and perinatal death

Author

Byrne, Alicia B., Arts, Peer, Ha, Thuong T., Kassahn, Karin S., Pais, Lynn S., O’Donnell-Luria, Anne, Babic, Milena, Frank, Mahalia S. B., Feng, Jinghua, Wang, Paul, Lawrence, David M., Eshraghi, Leila, Arriola, Luis, Toubia, John, Nguyen, Hung, McGillivray, George, Pinner, Jason, McKenzie, Fiona, Morrow, Rebecca, Lipsett, Jill, Manton, Nick, Khong, T. Yee, Moore, Lynette, Liebelt, Jan E., Schreiber, Andreas W., King-Smith, Sarah L., Hardy, Tristan S. E., Jackson, Matilda R., Barnett, Christopher P., and Scott, Hamish S.

Published
2024
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12. Genomic autopsy to identify underlying causes of pregnancy loss and perinatal death

Author

Byrne, Alicia B., Arts, Peer, Ha, Thuong T., Kassahn, Karin S., Pais, Lynn S., O’Donnell-Luria, Anne, Babic, Milena, Frank, Mahalia S. B., Feng, Jinghua, Wang, Paul, Lawrence, David M., Eshraghi, Leila, Arriola, Luis, Toubia, John, Nguyen, Hung, McGillivray, George, Pinner, Jason, McKenzie, Fiona, Morrow, Rebecca, Lipsett, Jill, Manton, Nick, Khong, T. Yee, Moore, Lynette, Liebelt, Jan E., Schreiber, Andreas W., King-Smith, Sarah L., Hardy, Tristan S. E., Jackson, Matilda R., Barnett, Christopher P., and Scott, Hamish S.

Published
2023
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16. Role of Critical Care Medicine Training in the Cardiovascular Intensive Care Unit: Survey Responses From Dual Certified Critical Care Cardiologists.

Author

Brusca, Samuel, Barnett, Christopher, Barnhart, Brendan, Weng, Weifeng, Morrow, David, Soble, Jeffrey, Katz, Jason, Wiley, Brandon, van Diepen, Sean, Gomez, Antonio, and Solomon, Michael

Subjects
American Board of Internal Medicine survey, cardiology training, cardiovascular intensive care units, critical care cardiology, Aged, Cardiologists, Cardiovascular Diseases, Certification, Clinical Competence, Critical Care, Education, Medical, Graduate, Female, Humans, Intensive Care Units, Male, Middle Aged, United States
Abstract

Background Cardiovascular intensive care units ( CICUs ) have evolved from coronary care wards into distinct units for critically ill patients with primary cardiac diseases, often suffering from illnesses that cross multiple disciplines. Mounting evidence has demonstrated improved survival with the incorporation of dedicated CICU providers with expertise in critical care medicine ( CCM ). This is the first study to systematically survey dual certified physicians in order to assess the relevance of CCM training to contemporary CICU care. Methods and Results Utilizing American Board of Internal Medicine data through 2014, 397 eligible physicians had obtained initial certification in both cardiovascular disease and CCM . A survey to delineate the role of critical care training in the CICU was provided to these physicians. Among those surveyed, 120 physicians (30%) responded. Dual certified physicians reported frequent use of their CCM skills in the CICU , highlighting ventilator management, multiorgan dysfunction management, end-of-life care, and airway management. The majority (85%) cited these skills as the reason CCM training should be prioritized by future CICU providers. Few (17%) agreed that general cardiology fellowship alone is currently sufficient to care for patients in the modern CICU . Furthermore, there was a consensus that there is an unmet need for cardiologists trained in CCM (70%) and that CICU s should adopt a level system similar to trauma centers (61%). Conclusions Citing specific skills acquired during CCM training, dual certified critical care cardiologists reported that their additional critical care experience was necessary in their practice to effectively deliver care in the modern CICU .

Published
2019

17. Genetic determinants of risk in pulmonary arterial hypertension: international genome-wide association studies and meta-analysis

Author

Rhodes, Christopher J, Batai, Ken, Bleda, Marta, Haimel, Matthias, Southgate, Laura, Germain, Marine, Pauciulo, Michael W, Hadinnapola, Charaka, Aman, Jurjan, Girerd, Barbara, Arora, Amit, Knight, Jo, Hanscombe, Ken B, Karnes, Jason H, Kaakinen, Marika, Gall, Henning, Ulrich, Anna, Harbaum, Lars, Cebola, Inês, Ferrer, Jorge, Lutz, Katie, Swietlik, Emilia M, Ahmad, Ferhaan, Amouyel, Philippe, Archer, Stephen L, Argula, Rahul, Austin, Eric D, Badesch, David, Bakshi, Sahil, Barnett, Christopher, Benza, Raymond, Bhatt, Nitin, Bogaard, Harm J, Burger, Charles D, Chakinala, Murali, Church, Colin, Coghlan, John G, Condliffe, Robin, Corris, Paul A, Danesino, Cesare, Debette, Stéphanie, Elliott, C Gregory, Elwing, Jean, Eyries, Melanie, Fortin, Terry, Franke, Andre, Frantz, Robert P, Frost, Adaani, Garcia, Joe GN, Ghio, Stefano, Ghofrani, Hossein-Ardeschir, Gibbs, J Simon R, Harley, John, He, Hua, Hill, Nicholas S, Hirsch, Russel, Houweling, Arjan C, Howard, Luke S, Ivy, Dunbar, Kiely, David G, Klinger, James, Kovacs, Gabor, Lahm, Tim, Laudes, Matthias, Machado, Rajiv D, Ross, Robert V MacKenzie, Marsolo, Keith, Martin, Lisa J, Moledina, Shahin, Montani, David, Nathan, Steven D, Newnham, Michael, Olschewski, Andrea, Olschewski, Horst, Oudiz, Ronald J, Ouwehand, Willem H, Peacock, Andrew J, Pepke-Zaba, Joanna, Rehman, Zia, Robbins, Ivan, Roden, Dan M, Rosenzweig, Erika B, Saydain, Ghulam, Scelsi, Laura, Schilz, Robert, Seeger, Werner, Shaffer, Christian M, Simms, Robert W, Simon, Marc, Sitbon, Olivier, Suntharalingam, Jay, Tang, Haiyang, Tchourbanov, Alexander Y, Thenappan, Thenappan, Torres, Fernando, Toshner, Mark R, Treacy, Carmen M, Noordegraaf, Anton Vonk, Waisfisz, Quinten, and Walsworth, Anna K

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Genetics, Human Genome, Lung, Aetiology, 2.1 Biological and endogenous factors, Cardiovascular, Female, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Genotyping Techniques, HLA-DP alpha-Chains, HLA-DP beta-Chains, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Pulmonary Arterial Hypertension, Risk Assessment, SOXF Transcription Factors, Signal Transduction, Survival Analysis, UK NIHR BioResource Rare Diseases Consortium, UK PAH Cohort Study Consortium, US PAH Biobank Consortium, Public Health and Health Services, Other Medical and Health Sciences, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundRare genetic variants cause pulmonary arterial hypertension, but the contribution of common genetic variation to disease risk and natural history is poorly characterised. We tested for genome-wide association for pulmonary arterial hypertension in large international cohorts and assessed the contribution of associated regions to outcomes.MethodsWe did two separate genome-wide association studies (GWAS) and a meta-analysis of pulmonary arterial hypertension. These GWAS used data from four international case-control studies across 11 744 individuals with European ancestry (including 2085 patients). One GWAS used genotypes from 5895 whole-genome sequences and the other GWAS used genotyping array data from an additional 5849 individuals. Cross-validation of loci reaching genome-wide significance was sought by meta-analysis. Conditional analysis corrected for the most significant variants at each locus was used to resolve signals for multiple associations. We functionally annotated associated variants and tested associations with duration of survival. All-cause mortality was the primary endpoint in survival analyses.FindingsA locus near SOX17 (rs10103692, odds ratio 1·80 [95% CI 1·55-2·08], p=5·13 × 10-15) and a second locus in HLA-DPA1 and HLA-DPB1 (collectively referred to as HLA-DPA1/DPB1 here; rs2856830, 1·56 [1·42-1·71], p=7·65 × 10-20) within the class II MHC region were associated with pulmonary arterial hypertension. The SOX17 locus had two independent signals associated with pulmonary arterial hypertension (rs13266183, 1·36 [1·25-1·48], p=1·69 × 10-12; and rs10103692). Functional and epigenomic data indicate that the risk variants near SOX17 alter gene regulation via an enhancer active in endothelial cells. Pulmonary arterial hypertension risk variants determined haplotype-specific enhancer activity, and CRISPR-mediated inhibition of the enhancer reduced SOX17 expression. The HLA-DPA1/DPB1 rs2856830 genotype was strongly associated with survival. Median survival from diagnosis in patients with pulmonary arterial hypertension with the C/C homozygous genotype was double (13·50 years [95% CI 12·07 to >13·50]) that of those with the T/T genotype (6·97 years [6·02-8·05]), despite similar baseline disease severity.InterpretationThis is the first study to report that common genetic variation at loci in an enhancer near SOX17 and in HLA-DPA1/DPB1 is associated with pulmonary arterial hypertension. Impairment of SOX17 function might be more common in pulmonary arterial hypertension than suggested by rare mutations in SOX17. Further studies are needed to confirm the association between HLA typing or rs2856830 genotyping and survival, and to determine whether HLA typing or rs2856830 genotyping improves risk stratification in clinical practice or trials.FundingUK NIHR, BHF, UK MRC, Dinosaur Trust, NIH/NHLBI, ERS, EMBO, Wellcome Trust, EU, AHA, ACClinPharm, Netherlands CVRI, Dutch Heart Foundation, Dutch Federation of UMC, Netherlands OHRD and RNAS, German DFG, German BMBF, APH Paris, INSERM, Université Paris-Sud, and French ANR.

Published
2019

18. Current practices in the management of temporary mechanical circulatory support: A survey of CICU directors in North America.

Author

Balgobind, Amrita, Pierce, Matthew, Alviar, Carlos, Barnett, Christopher, Barsness, Gregory, Chaudhry, Sunit-preet, Chonde, Meshe, Cooper, Howard, Daniels, Lori, Gidwani, Umesh, Fordyce, Christopher, Goldfarb, Michael, Katz, Jason N., Kontos, Michael, Kwon, Younghoon, Liebner, Evan, Liu, Shuangbo, Miller, P. Elliott, Newby, L.K., and O'Brien, Connor

Abstract

Despite the growing use of temporary mechanical circulatory support (tMCS), little data exists to inform management and weaning of these devices. We performed an online survey among cardiac intensive care unit directors in North America to examine current practices in the management of patients treated with intraaortic balloon pump and Impella. We received responses from 84% of surveyed centers (n=37). Our survey focused on three key aspects of daily management: 1. Hemodynamic monitoring; 2. Hemocompatibility; and 3. Weaning and removal. We found substantial variability surrounding all three areas of care. Our findings highlight the need for consensus around practices associated with improved outcomes in patients treated with tMCS. [ABSTRACT FROM AUTHOR]

Published
2024
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19. Nanoparticles for Undergraduates: Creation, Characterization, and Catalysis

Author

Strachan, Jyah, Barnett, Christopher, Maschmeyer, Thomas, Masters, Anthony F., Motion, Alice, and Yuen, Alexander K. L.

Abstract

We report a research-enhanced undergraduate laboratory practical in which students synthesize and characterize color-controllable, stable silver nanoparticles for use in a simple catalytic reaction analyzed by UV-vis spectroscopy. The practical has been prepared for students using electronic laboratory notebooks, enables collaborative data sharing, and can be altered to suit time, experience, and instrumentation constraints. This experiment is conducted as part of our Talented Student Program and introduces students to the themes of nanoscience, catalysis, and green chemistry as well as to a range of relevant instrumentation and techniques.

Published
2020
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21. Targeted sequencing identifies 91 neurodevelopmental-disorder risk genes with autism and developmental-disability biases

Author

Stessman, Holly AF, Xiong, Bo, Coe, Bradley P, Wang, Tianyun, Hoekzema, Kendra, Fenckova, Michaela, Kvarnung, Malin, Gerdts, Jennifer, Trinh, Sandy, Cosemans, Nele, Vives, Laura, Lin, Janice, Turner, Tychele N, Santen, Gijs, Ruivenkamp, Claudia, Kriek, Marjolein, van Haeringen, Arie, Aten, Emmelien, Friend, Kathryn, Liebelt, Jan, Barnett, Christopher, Haan, Eric, Shaw, Marie, Gecz, Jozef, Anderlid, Britt-Marie, Nordgren, Ann, Lindstrand, Anna, Schwartz, Charles, Kooy, R Frank, Vandeweyer, Geert, Helsmoortel, Celine, Romano, Corrado, Alberti, Antonino, Vinci, Mirella, Avola, Emanuela, Giusto, Stefania, Courchesne, Eric, Pramparo, Tiziano, Pierce, Karen, Nalabolu, Srinivasa, Amaral, David G, Scheffer, Ingrid E, Delatycki, Martin B, Lockhart, Paul J, Hormozdiari, Fereydoun, Harich, Benjamin, Castells-Nobau, Anna, Xia, Kun, Peeters, Hilde, Nordenskjöld, Magnus, Schenck, Annette, Bernier, Raphael A, and Eichler, Evan E

Subjects
Biological Sciences, Bioinformatics and Computational Biology, Genetics, Brain Disorders, Behavioral and Social Science, Genetic Testing, Intellectual and Developmental Disabilities (IDD), Mental Health, Neurosciences, Pediatric, Autism, Aetiology, 2.1 Biological and endogenous factors, Mental health, Autistic Disorder, Developmental Disabilities, Female, Humans, Intellectual Disability, Male, Mutation, Phenotype, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology
Abstract

Gene-disruptive mutations contribute to the biology of neurodevelopmental disorders (NDDs), but most of the related pathogenic genes are not known. We sequenced 208 candidate genes from >11,730 cases and >2,867 controls. We identified 91 genes, including 38 new NDD genes, with an excess of de novo mutations or private disruptive mutations in 5.7% of cases. Drosophila functional assays revealed a subset with increased involvement in NDDs. We identified 25 genes showing a bias for autism versus intellectual disability and highlighted a network associated with high-functioning autism (full-scale IQ >100). Clinical follow-up for NAA15, KMT5B, and ASH1L highlighted new syndromic and nonsyndromic forms of disease.

Published
2017

22. Epidemiology of cardiogenic shock using the Shock Academic Research Consortium (SHARC) consensus definitions

Author

Berg, David D, Bohula, Erin A, Patel, Siddharth M, Alfonso, Carlos E, Alviar, Carlos L, Baird-Zars, Vivian M, Barnett, Christopher F, Barsness, Gregory W, Bennett, Courtney E, Chaudhry, Sunit-Preet, Fordyce, Christopher B, Ghafghazi, Shahab, Gidwani, Umesh K, Goldfarb, Michael J, Katz, Jason N, Menon, Venu, Miller, P Elliott, Newby, L Kristin, Papolos, Alexander I, Park, Jeong-Gun, Pierce, Matthew J, Proudfoot, Alastair G, Sinha, Shashank S, Sridharan, Lakshmi, Thompson, Andrea D, van Diepen, Sean, and Morrow, David A

Published
2024
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23. Continuum of Preshock to Classic Cardiogenic Shock in the Critical Care Cardiology Trials Network Registry

Author

Patel, Siddharth M., Berg, David D., Bohula, Erin A., Baird-Zars, Vivian M., Park, Jeong-Gun, Barnett, Christopher F., Daniels, Lori B., Fordyce, Christopher B., Ghafghazi, Shahab, Goldfarb, Michael J., Gorder, Kari, Kwon, Younghoon, Leibner, Evan, Menon, Venu, Potter, Brian J., Prasad, Rajnish, Solomon, Michael A., Teuteberg, Jeffrey J., Thompson, Andrea D., Zakaria, Sammy, Katz, Jason N., van Diepen, Sean, and Morrow, David A.

Abstract

The prognostic implications of phenotypes along the preshock to cardiogenic shock (CS) continuum remain uncertain.

Published
2024
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24. Parental experiences of ultrarapid genomic testing for their critically unwell infants and children

Author

Brett, Gemma R., Martyn, Melissa, Lynch, Fiona, de Silva, Michelle G., Ayres, Samantha, Gallacher, Lyndon, Boggs, Kirsten, Baxendale, Anne, Schenscher, Sarah, King-Smith, Sarah, Fowles, Lindsay, Springer, Amanda, Lunke, Sebastian, Vasudevan, Anand, Krzesinski, Emma, Pinner, Jason, Sandaradura, Sarah A., Barnett, Christopher, Patel, Chirag, Wilson, Meredith, and Stark, Zornitza

Published
2020
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27. Procalcitonin predicts mortality in HIV-infected Ugandan adults with lower respiratory tract infections.

Author

Tokman, Sofya, Barnett, Christopher, Jarlsberg, Leah, den Boon, Saskia, Davis, J, Worodria, William, Maisel, Alan, Huang, Laurence, Cattamanchi, Adithya, and Taub, Pam

Subjects
human immunodeficiency virus, pneumonia, procalcitonin, prognosis, tuberculosis, Adult, Aged, Biomarkers, Calcitonin, Calcitonin Gene-Related Peptide, Case-Control Studies, False Negative Reactions, Female, HIV Infections, Hospital Mortality, Humans, Male, Middle Aged, Predictive Value of Tests, Prevalence, Prospective Studies, Protein Precursors, Respiratory Tract Infections, Risk Assessment, Sensitivity and Specificity, Uganda
Abstract

BACKGROUND AND OBJECTIVE: In low and middle-income countries where HIV infection is prevalent, identifying patients at high risk of dying from lower respiratory tract infections is challenging and validated prognostic models are lacking. Serum procalcitonin may be a useful prognostic tool in these settings. We sought to determine if elevated serum procalcitonin is associated with increased in-hospital mortality and to combine serum procalcitonin with available clinical characteristics to create a clinically useful prognostic model. METHODS: We conducted a prospective, nested case-control study of 241 HIV-infected adults admitted to Mulago Hospital in Kampala, Uganda with cough ≥2 weeks in duration. We collected demographic and clinical information, baseline serum for procalcitonin analysis, and followed patients to determine in-hospital mortality. RESULTS: Serum procalcitonin was a strong and independent predictor of inpatient mortality (aOR = 7.69, p = 0.01, sensitivity = 93%, negative predictive value = 97%). Best subset multivariate analysis identified 3 variables that were combined into a prognostic model to risk stratify patients; these variables included respiratory rate ≥30 breaths/minute (aOR = 2.07, p = 0.11), oxygen saturation 0.5 ng/ml (aOR = 7.69, p = 0.01). The predicted probability of inpatient mortality ranged from 1% when no variables were present, to 42% when all variables were present. CONCLUSIONS: Elevated serum procalcitonin >0.5 ng/ml is an independent predictor of in-hospital mortality. Elevated serum procalcitonin, tachypnea, and hypoxemia may be combined into a prognostic model to identify patients at high risk of dying in the hospital. This model may be used to estimate the probability of death and to guide triage and treatment decisions.

Published
2014

28. PCT predicts death in adults with LRTI

Author

Tokman, Sofya, Barnett, Christopher F, Jarlsberg, Leah G, Taub, Pam R, Boon, Saskia, Davis, J Lucian, Cattamanchi, Adithya, Worodria, William, Maisel, Alan, Huang, Laurence, and Study, the International HIV‐Associated Opportunistic Pneumonias

Subjects
Clinical Research, Lung, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Infection, Good Health and Well Being, Adult, Aged, Biomarkers, Calcitonin, Calcitonin Gene-Related Peptide, Case-Control Studies, False Negative Reactions, Female, HIV Infections, Hospital Mortality, Humans, Male, Middle Aged, Predictive Value of Tests, Prevalence, Prospective Studies, Protein Precursors, Respiratory Tract Infections, Risk Assessment, Sensitivity and Specificity, Uganda, human immunodeficiency virus, pneumonia, procalcitonin, prognosis, tuberculosis, International HIV-Associated Opportunistic Pneumonias (IHOP) Study Group, Medical and Health Sciences, Respiratory System
Abstract

Background and objectiveIn low and middle-income countries where HIV infection is prevalent, identifying patients at high risk of dying from lower respiratory tract infections is challenging and validated prognostic models are lacking. Serum procalcitonin may be a useful prognostic tool in these settings. We sought to determine if elevated serum procalcitonin is associated with increased in-hospital mortality and to combine serum procalcitonin with available clinical characteristics to create a clinically useful prognostic model.MethodsWe conducted a prospective, nested case-control study of 241 HIV-infected adults admitted to Mulago Hospital in Kampala, Uganda with cough ≥2 weeks in duration. We collected demographic and clinical information, baseline serum for procalcitonin analysis, and followed patients to determine in-hospital mortality.ResultsSerum procalcitonin was a strong and independent predictor of inpatient mortality (aOR = 7.69, p = 0.01, sensitivity = 93%, negative predictive value = 97%). Best subset multivariate analysis identified 3 variables that were combined into a prognostic model to risk stratify patients; these variables included respiratory rate ≥30 breaths/minute (aOR = 2.07, p = 0.11), oxygen saturation 0.5 ng/ml (aOR = 7.69, p = 0.01). The predicted probability of inpatient mortality ranged from 1% when no variables were present, to 42% when all variables were present.ConclusionsElevated serum procalcitonin >0.5 ng/ml is an independent predictor of in-hospital mortality. Elevated serum procalcitonin, tachypnea, and hypoxemia may be combined into a prognostic model to identify patients at high risk of dying in the hospital. This model may be used to estimate the probability of death and to guide triage and treatment decisions.

Published
2014

30. Medicare‐funded reproductive genetic carrier screening in Australia has arrived: are we ready?

Author

Rogers, Alice P, Fitzgerald, Lara, Liebelt, Jan, and Barnett, Christopher

Abstract

The article discusses the introduction of Medicare-funded reproductive genetic carrier screening (RGCS) in Australia and examines the country's readiness for this screening. RGCS is a preventive health strategy that identifies healthy individuals and couples who have an increased chance of having a child affected by a serious genetic condition. The article emphasizes the benefits of RGCS in allowing informed reproductive choices and reducing the chance of having an affected child. It also addresses the factors that have limited the uptake of RGCS, such as lack of awareness and understanding, and the cost of testing. The article provides information on the three genetic conditions included in the Medicare-funded screening and the complexities involved in pre- and post-test counseling. It highlights the importance of choice-based counseling and the need to provide individuals and couples with information about the limitations and potential implications of screening. The article concludes by discussing the reproductive options available to reduce the risk of an affected pregnancy and the demand for clinical genetics services in Australia. It also mentions the implementation and outcomes of Mackenzie's Mission, a study funded by the Australian Government Medical Research Future Fund, which aimed to assess the feasibility and acceptability of expanded carrier screening for Australian couples. Preliminary results showed that about 1 in 50 Australian reproductive couples would be identified as having an increased chance of carrying a genetic condition. The study underscores the need for ongoing education and resources to support the implementation of expanded carrier screening. [Extracted from the article]

Published
2024
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31. Prognostic performance of the IABP-SHOCK II Risk Score among cardiogenic shock subtypes in the critical care cardiology trials network registry.

Author

Alviar, Carlos L., Li, Boyangzi K., Keller, Norma M., Bohula-May, Erin, Barnett, Christopher, Berg, David D., Burke, James A., Chaudhry, Sunit-Preet, Daniels, Lori B., DeFilippis, Andrew P., Gerber, Daniel, Horowitz, James, Jentzer, Jacob C., Katrapati, Praneeth, Keeley, Ellen, Lawler, Patrick R., Park, Jeong-Gun, Sinha, Shashank S., Snell, Jeffrey, and Solomon, Michael A.

Abstract

Risk stratification has potential to guide triage and decision-making in cardiogenic shock (CS). We assessed the prognostic performance of the IABP-SHOCK II score, derived in Europe for acute myocardial infarct-related CS (AMI-CS), in a contemporary North American cohort, including different CS phenotypes. The critical care cardiology trials network (CCCTN) coordinated by the TIMI study group is a multicenter network of cardiac intensive care units (CICU). Participating centers annually contribute ≥2 months of consecutive medical CICU admissions. The IABP-SHOCK II risk score includes age > 73 years, prior stroke, admission glucose > 191 mg/dl, creatinine > 1.5 mg/dl, lactate > 5 mmol/l, and post-PCI TIMI flow grade < 3. We assessed the risk score across various CS etiologies. Of 17,852 medical CICU admissions 5,340 patients across 35 sites were admitted with CS. In patients with AMI-CS (n = 912), the IABP-SHOCK II score predicted a >3-fold gradient in in-hospital mortality (low risk = 26.5%, intermediate risk = 52.2%, high risk = 77.5%, P <.0001; c-statistic = 0.67; Hosmer-Lemeshow P =.79). The score showed a similar gradient of in-hospital mortality in patients with non-AMI-related CS (n = 2,517, P <.0001) and mixed shock (n = 923, P <.001), as well as in left ventricular (<0.0001), right ventricular (P =.0163) or biventricular (<0.0001) CS. The correlation between the IABP-SHOCK II score and SOFA was moderate (r2 = 0.17) and the IABP-SHOCK II score revealed a significant risk gradient within each SCAI stage. In an unselected international multicenter registry of patients admitted with CS, the IABP- SHOCK II score only moderately predicted in-hospital mortality in a broad population of CS regardless of etiology or irrespective of right, left, or bi-ventricular involvement. [ABSTRACT FROM AUTHOR]

Published
2024
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33. Human Immunodeficiency Virus–Associated Pulmonary Arterial Hypertension

Author

Barnett, Christopher F and Hsue, Priscilla Y

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Cardiovascular, Infectious Diseases, Clinical Research, HIV/AIDS, Rare Diseases, Lung, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Anti-Retroviral Agents, Familial Primary Pulmonary Hypertension, HIV Infections, Heart Failure, Hemodynamics, Humans, Hypertension, Pulmonary, Survival Analysis, Pulmonary arterial hypertension, HIV, AIDS, Antiretroviral therapy, Clinical Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

Antiretroviral therapy has greatly increased longevity for individuals with human immunodeficiency virus (HIV) infection. About 0.5% of patients with HIV infection develop moderate to severe pulmonary arterial hypertension, which is several thousand times higher than the incidence of idiopathic pulmonary arterial hypertension. As more than 30 million individuals are chronically infected, HIV infection could soon become one of the most common causes of pulmonary arterial hypertension worldwide. Pulmonary arterial hypertension is a relentlessly progressive disease leading to right heart failure and death. In this article the available data on epidemiology, hemodynamics, mechanisms, and therapeutic strategies for HIV-associated pulmonary arterial hypertension are reviewed.

Published
2013

35. Effects of Commercial Air Travel on Patients With Pulmonary Hypertension

Author

Roubinian, Nareg, Elliott, C Gregory, Barnett, Christopher F, Blanc, Paul D, Chen, Joan, De Marco, Teresa, and Chen, Hubert

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Lung, Clinical Research, Cardiovascular, Aerospace Medicine, Aircraft, Altitude, Compressed Air, Female, Humans, Hypertension, Pulmonary, Hypoxia, Incidence, Male, Middle Aged, Occupational Exposure, Oxygen Consumption, Prospective Studies, Time Factors, Travel, United States, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundLimited data are available on the effects of air travel in patients with pulmonary hypertension (PH), despite their risk of physiologic compromise. We sought to quantify the incidence and severity of hypoxemia experienced by people with PH during commercial air travel.MethodsWe recruited 34 participants for a prospective observational study during which cabin pressure, oxygen saturation (Sp O 2 ), heart rate, and symptoms were documented serially at multiple predefined time points throughout commercial flights. Oxygen desaturation was defined as SpO2,

Published
2012

36. Doppler echocardiography does not accurately estimate pulmonary artery systolic pressure in HIV-infected patients

Author

Selby, Van N, Scherzer, Rebecca, Barnett, Christopher F, MacGregor, John S, Morelli, Juliana, Donovan, Catherine, Deeks, Steven G, Martin, Jeffrey N, and Hsue, Priscilla Y

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Heart Disease, Sexually Transmitted Infections, Infectious Diseases, Clinical Research, HIV/AIDS, Cardiovascular, Lung, Biomedical Imaging, 4.2 Evaluation of markers and technologies, Acquired Immunodeficiency Syndrome, Blood Pressure, Echocardiography, Doppler, Familial Primary Pulmonary Hypertension, Female, Humans, Hypertension, Pulmonary, Male, Middle Aged, Pulmonary Artery, Treatment Outcome, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Virology, Biomedical and clinical sciences, Health sciences
Abstract

Doppler echocardiography is used to screen for HIV-related pulmonary arterial hypertension (HRPAH). We studied patients with HIV infection to determine the accuracy of Doppler echocardiography-estimated pulmonary artery systolic pressure (PASP) compared with PASP measured during right heart catheterization. Doppler echocardiography-estimated PASP was inaccurate in 19.7% of cases. Using Doppler echocardiography-estimated PASP, one in three patients with HRPAH was missed. Doppler echocardiography estimates of PASP are not accurate in patients with HIV.

Published
2012

37. Complex Heart–Lung Ventilator Emergencies in the CICU

Author

Lopez, Mireia Padilla, Applefeld, Willard, Miller, Elliott, Elliott, Andrea, Bennett, Courtney, Lee, Burton, Barnett, Christopher, Solomon, Michael A., Corradi, Francesco, Sionis, Alessandro, Mireles-Cabodevila, Eduardo, Tavazzi, Guido, and Alviar, Carlos L.

Abstract

This review aims to enhance the comprehension and management of cardiopulmonary interactions in critically ill patients with cardiovascular disease undergoing mechanical ventilation. Highlighting the significance of maintaining a delicate balance, this article emphasizes the crucial role of adjusting ventilation parameters based on both invasive and noninvasive monitoring. It provides recommendations for the induction and liberation from mechanical ventilation. Special attention is given to the identification of auto-PEEP (positive end-expiratory pressure) and other situations that may impact hemodynamics and patients’ outcomes.

Published
2024
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38. Synthesis, Structure, and Properties of 2O-BaPtO3, a Phase Derived from Hexagonal Perovskite

Author

Brown, Alex J., Miller, Laura A., Berry, Andrew J., Lewis, William, Barnett, Christopher, Yuen, Alexander, Brennan, Mia J., Auckett, Josie E., Maynard-Casely, Helen E., and Ling, Chris D.

Abstract

We have made the compound 2O-BaPtO3by high-pressure, high-temperature synthesis, determined its structure, and tested its catalytic activity. Compounds of the same stoichiometry have been reported and tentatively identified as hexagonal perovskites, and although no structural model was ever established, 2O-BaPtO3is clearly different and, to the best of our knowledge, unique. It features continuous chains of face-sharing PtO6octahedra, like the well-known 2H hexagonal perovskite type, but with a staggered offset between the chains that breaks hexagonal symmetry and disrupts the close-packed array of A= Ba and X= O that is a defining characteristic of ABX3perovskites. We investigated this structure and its stability vsthe conventional 2H form using X-ray and neutron diffraction, X-ray absorption spectroscopy, and ab initiocalculations. Catalytic testing of 2O-BaPtO3showed that it is active for hydrogen evolution.

Published
2024
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40. Interhospital Variation in Admissions Managed With Critical Care Therapies or Invasive Hemodynamic Monitoring in Tertiary Cardiac Intensive Care Units: An Analysis From the Critical Care Cardiology Trials Network Registry.

Author

Donnelly, Sarah, Barnett, Christopher F., Bohula, Erin A., Chaudhry, Sunit-Preet, Chonde, Meshe D., Cooper, Howard A., Daniels, Lori B., Dodson, Mark W., Gerber, Daniel, Goldfarb, Michael J., Jianping Guo, Kontos, Michael C., Shuangbo Liu, Luk, Adriana C., Menon, Venu, O'Brien, Connor G., Papolos, Alexander I., Pisani, Barbara A., Potter, Brian J., and Prasad, Rajnish

Abstract

BACKGROUND: Wide interhospital variations exist in cardiovascular intensive care unit (CICU) admission practices and the use of critical care restricted therapies (CCRx), but little is known about the differences in patient acuity, CCRx utilization, and the associated outcomes within tertiary centers. METHODS: The Critical Care Cardiology Trials Network is a multicenter registry of tertiary and academic CICUs in the United States and Canada that captured consecutive admissions in 2-month periods between 2017 and 2022. This analysis included 17 843 admissions across 34 sites and compared interhospital tertiles of CCRx (eg, mechanical ventilation, mechanical circulatory support, continuous renal replacement therapy) utilization and its adjusted association with in-hospital survival using logistic regression. The Pratt index was used to quantify patient-related and institutional factors associated with CCRx variability. RESULTS: The median age of the study population was 66 (56--77) years and 37% were female. CCRx was provided to 62.2% (interhospital range of 21.3%--87.1%) of CICU patients. Admissions to CICUs with the highest tertile of CCRx utilization had a greater burden of comorbidities, had more diagnoses of ST--elevation myocardial infarction, cardiac arrest, or cardiogenic shock, and had higher Sequential Organ Failure Assessment scores. The unadjusted in-hospital mortality (median, 12.7%) was 9.6%, 11.1%, and 18.7% in low, intermediate, and high CCRx tertiles, respectively. No clinically meaningful differences in adjusted mortality were observed across tertiles when admissions were stratified by the provision of CCRx. Baseline patient-level variables and institutional differences accounted for 80% and 5.3% of the observed CCRx variability, respectively. CONCLUSIONS: In a large registry of tertiary and academic CICUs, there was a >4-fold interhospital variation in the provision of CCRx that was primarily driven by differences in patient acuity compared with institutional differences. No differences were observed in adjusted mortality between low, intermediate, and high CCRx utilization sites. [ABSTRACT FROM AUTHOR]

Published
2024
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41. Feasibility of Ultra-Rapid Exome Sequencing in Critically Ill Infants and Children With Suspected Monogenic Conditions in the Australian Public Health Care System

Author

Lunke, Sebastian, Eggers, Stefanie, Wilson, Meredith, Patel, Chirag, Barnett, Christopher P., Pinner, Jason, Sandaradura, Sarah A., Buckley, Michael F., Krzesinski, Emma I., de Silva, Michelle G., Brett, Gemma R., Boggs, Kirsten, Mowat, David, Kirk, Edwin P., Adès, Lesley C., Akesson, Lauren S., Amor, David J., Ayres, Samantha, Baxendale, Anne, Borrie, Sarah, Bray, Alessandra, Brown, Natasha J., Chan, Cheng Yee, Chong, Belinda, Cliffe, Corrina, Delatycki, Martin B., Edwards, Matthew, Elakis, George, Fahey, Michael C., Fennell, Andrew, Fowles, Lindsay, Gallacher, Lyndon, Higgins, Megan, Howell, Katherine B., Hunt, Lauren, Hunter, Matthew F., Jones, Kristi J., King, Sarah, Kumble, Smitha, Lang, Sarah, Le Moing, Maelle, Ma, Alan, Phelan, Dean, Quinn, Michael C. J., Richards, Anna, Richmond, Christopher M., Riseley, Jessica, Rodgers, Jonathan, Sachdev, Rani, Sadedin, Simon, Schlapbach, Luregn J., Smith, Janine, Springer, Amanda, Tan, Natalie B., Tan, Tiong Y., Temple, Suzanna L., Theda, Christiane, Vasudevan, Anand, White, Susan M., Yeung, Alison, Zhu, Ying, Martyn, Melissa, Best, Stephanie, Roscioli, Tony, Christodoulou, John, and Stark, Zornitza

Published
2020
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43. Australian Genomics: Outcomes of a 5-year national program to accelerate the integration of genomics in healthcare

Author

Stark, Zornitza, primary, Boughtwood, Tiffany, additional, Haas, Matilda, additional, Braithwaite, Jeffrey, additional, Gaff, Clara L., additional, Goranitis, Ilias, additional, Spurdle, Amanda B., additional, Hansen, David P., additional, Hofmann, Oliver, additional, Laing, Nigel, additional, Metcalfe, Sylvia, additional, Newson, Ainsley J., additional, Scott, Hamish S., additional, Thorne, Natalie, additional, Ward, Robyn L., additional, Dinger, Marcel E., additional, Best, Stephanie, additional, Long, Janet C., additional, Grimmond, Sean M., additional, Pearson, John, additional, Waddell, Nicola, additional, Barnett, Christopher P., additional, Cook, Matthew, additional, Field, Michael, additional, Fielding, David, additional, Fox, Stephen B., additional, Gecz, Jozef, additional, Jaffe, Adam, additional, Leventer, Richard J., additional, Lockhart, Paul J., additional, Lunke, Sebastian, additional, Mallett, Andrew J., additional, McGaughran, Julie, additional, Mileshkin, Linda, additional, Nones, Katia, additional, Roscioli, Tony, additional, Scheffer, Ingrid E., additional, Semsarian, Christopher, additional, Simons, Cas, additional, Thomas, David M., additional, Thorburn, David R., additional, Tothill, Richard, additional, White, Deborah, additional, Dunwoodie, Sally, additional, Simpson, Peter T., additional, Phillips, Peta, additional, Brion, Marie-Jo, additional, Finlay, Keri, additional, Quinn, Michael CJ., additional, Mattiske, Tessa, additional, Tudini, Emma, additional, Boggs, Kirsten, additional, Murray, Sean, additional, Wells, Kathy, additional, Cannings, John, additional, Sinclair, Andrew H., additional, Christodoulou, John, additional, and North, Kathryn N., additional

Published
2023
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46. Discovering a new part of the phenotypic spectrum of Coffin-Siris syndrome in a fetal cohort

Author

van der Sluijs, Pleuntje J., primary, Joosten, Marieke, additional, Alby, Caroline, additional, Attié-Bitach, Tania, additional, Gilmore, Kelly, additional, Dubourg, Christele, additional, Fradin, Mélanie, additional, Wang, Tianyun, additional, Kurtz-Nelson, Evangeline C., additional, Ahlers, Kaitlyn P., additional, Arts, Peer, additional, Barnett, Christopher P., additional, Ashfaq, Myla, additional, Baban, Anwar, additional, van den Born, Myrthe, additional, Borrie, Sarah, additional, Busa, Tiffany, additional, Byrne, Alicia, additional, Carriero, Miriam, additional, Cesario, Claudia, additional, Chong, Karen, additional, Cueto-González, Anna Maria, additional, Dempsey, Jennifer C., additional, Diderich, Karin E.M., additional, Doherty, Dan, additional, Farholt, Stense, additional, Gerkes, Erica H., additional, Gorokhova, Svetlana, additional, Govaerts, Lutgarde C.P., additional, Gregersen, Pernille A., additional, Hickey, Scott E., additional, Lefebvre, Mathilde, additional, Mari, Francesca, additional, Martinovic, Jelena, additional, Northrup, Hope, additional, O’Leary, Melanie, additional, Parbhoo, Kareesma, additional, Patrier, Sophie, additional, Popp, Bernt, additional, Santos-Simarro, Fernando, additional, Stoltenburg, Corinna, additional, Thauvin-Robinet, Christel, additional, Thompson, Elisabeth, additional, Vulto-van Silfhout, Anneke T., additional, Zahir, Farah R., additional, Scott, Hamish S., additional, Earl, Rachel K., additional, Eichler, Evan E., additional, Vora, Neeta L., additional, Wilnai, Yael, additional, Giordano, Jessica L., additional, Wapner, Ronald J., additional, Rosenfeld, Jill A., additional, Haak, Monique C., additional, and Santen, Gijs W.E., additional

Published
2023
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47. Hotspots of missense mutation identify neurodevelopmental disorder genes and functional domains

Author

Geisheker, Madeleine R, Heymann, Gabriel, Wang, Tianyun, Coe, Bradley P, Turner, Tychele N, Stessman, Holly A F, Hoekzema, Kendra, Kvarnung, Malin, Shaw, Marie, Friend, Kathryn, Liebelt, Jan, Barnett, Christopher, Thompson, Elizabeth M, Haan, Eric, Guo, Hui, Anderlid, Britt-Marie, Nordgren, Ann, Lindstrand, Anna, Vandeweyer, Geert, Alberti, Antonino, Avola, Emanuela, Vinci, Mirella, Giusto, Stefania, Pramparo, Tiziano, Pierce, Karen, Nalabolu, Srinivasa, Michaelson, Jacob J, Sedlacek, Zdenek, Santen, Gijs W E, Peeters, Hilde, Hakonarson, Hakon, Courchesne, Eric, Romano, Corrado, Kooy, R Frank, Bernier, Raphael A, Nordenskjöld, Magnus, Gecz, Jozef, Xia, Kun, Zweifel, Larry S, and Eichler, Evan E

Published
2017
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48. Genomic and phenotypic characterization of 404 individuals with neurodevelopmental disorders caused by CTNNB1 variants

Author

Kayumi, Sayaka, primary, Pérez-Jurado, Luis A., additional, Palomares, María, additional, Rangu, Sneha, additional, Sheppard, Sarah E., additional, Chung, Wendy K., additional, Kruer, Michael C., additional, Kharbanda, Mira, additional, Amor, David J., additional, McGillivray, George, additional, Cohen, Julie S., additional, García-Miñaúr, Sixto, additional, van Eyk, Clare L., additional, Harper, Kelly, additional, Jolly, Lachlan A., additional, Webber, Dani L., additional, Barnett, Christopher P., additional, Santos-Simarro, Fernando, additional, Pacio-Míguez, Marta, additional, Pozo, Angela del, additional, Bakhtiari, Somayeh, additional, Deardorff, Matthew, additional, Dubbs, Holly A., additional, Izumi, Kosuke, additional, Grand, Katheryn, additional, Gray, Christopher, additional, Mark, Paul R., additional, Bhoj, Elizabeth J., additional, Li, Dong, additional, Ortiz-Gonzalez, Xilma R., additional, Keena, Beth, additional, Zackai, Elaine H., additional, Goldberg, Ethan M., additional, Perez de Nanclares, Guiomar, additional, Pereda, Arrate, additional, Llano-Rivas, Isabel, additional, Arroyo, Ignacio, additional, Fernández-Cuesta, María Ángeles, additional, Thauvin-Robinet, Christel, additional, Faivre, Laurence, additional, Garde, Aurore, additional, Mazel, Benoit, additional, Bruel, Ange-Line, additional, Tress, Michael L., additional, Brilstra, Eva, additional, Fine, Amena Smith, additional, Crompton, Kylie E., additional, Stegmann, Alexander P.A., additional, Sinnema, Margje, additional, Stevens, Servi C.J., additional, Nicolai, Joost, additional, Lesca, Gaetan, additional, Lion-François, Laurence, additional, Haye, Damien, additional, Chatron, Nicolas, additional, Piton, Amelie, additional, Nizon, Mathilde, additional, Cogne, Benjamin, additional, Srivastava, Siddharth, additional, Bassetti, Jennifer, additional, Muss, Candace, additional, Gripp, Karen W., additional, Procopio, Rebecca A., additional, Millan, Francisca, additional, Morrow, Michelle M., additional, Assaf, Melissa, additional, Moreno-De-Luca, Andres, additional, Joss, Shelagh, additional, Hamilton, Mark J., additional, Bertoli, Marta, additional, Foulds, Nicola, additional, McKee, Shane, additional, MacLennan, Alastair H., additional, Gecz, Jozef, additional, and Corbett, Mark A., additional

Published
2022
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49. Genetic variation affecting DNA methylation and the human imprinting disorder, Beckwith-Wiedemann syndrome

Author

Dagar, Vinod, Hutchison, Wendy, Muscat, Andrea, Krishnan, Anita, Hoke, David, Buckle, Ashley, Siswara, Priscillia, Amor, David J., Mann, Jeffrey, Pinner, Jason, Colley, Alison, Wilson, Meredith, Sachdev, Rani, McGillivray, George, Edwards, Matthew, Kirk, Edwin, Collins, Felicity, Jones, Kristi, Taylor, Juliet, Hayes, Ian, Thompson, Elizabeth, Barnett, Christopher, Haan, Eric, Freckmann, Mary-Louise, Turner, Anne, White, Susan, Kamien, Ben, Ma, Alan, Mackenzie, Fiona, Baynam, Gareth, Kiraly-Borri, Cathy, Field, Michael, Dudding-Byth, Tracey, and Algar, Elizabeth M.

Published
2018
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50. Discovering a new part of the phenotypic spectrum of Coffin-Siris syndrome in a fetal cohort

Author

van der Sluijs, Pleuntje J., primary, Joosten, Marieke, additional, Alby, Caroline, additional, Attié-Bitach, Tania, additional, Gilmore, Kelly, additional, Dubourg, Christele, additional, Fradin, Mélanie, additional, Wang, Tianyun, additional, Kurtz-Nelson, Evangeline C., additional, Ahlers, Kaitlyn P., additional, Arts, Peer, additional, Barnett, Christopher P., additional, Ashfaq, Myla, additional, Baban, Anwar, additional, van den Born, Myrthe, additional, Borrie, Sarah, additional, Busa, Tiffany, additional, Byrne, Alicia, additional, Carriero, Miriam, additional, Cesario, Claudia, additional, Chong, Karen, additional, Cueto-González, Anna Maria, additional, Dempsey, Jennifer C., additional, Diderich, Karin E.M., additional, Doherty, Dan, additional, Farholt, Stense, additional, Gerkes, Erica H., additional, Gorokhova, Svetlana, additional, Govaerts, Lutgarde C.P., additional, Gregersen, Pernille A., additional, Hickey, Scott E., additional, Lefebvre, Mathilde, additional, Mari, Francesca, additional, Martinovic, Jelena, additional, Northrup, Hope, additional, O’Leary, Melanie, additional, Parbhoo, Kareesma, additional, Patrier, Sophie, additional, Popp, Bernt, additional, Santos-Simarro, Fernando, additional, Stoltenburg, Corinna, additional, Thauvin-Robinet, Christel, additional, Thompson, Elisabeth, additional, Vulto-van Silfhout, Anneke T., additional, Zahir, Farah R., additional, Scott, Hamish S., additional, Earl, Rachel K., additional, Eichler, Evan E., additional, Vora, Neeta L., additional, Wilnai, Yael, additional, Giordano, Jessica L., additional, Wapner, Ronald J., additional, Rosenfeld, Jill A., additional, Haak, Monique C., additional, and Santen, Gijs W.E., additional

Published
2022
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