67 results on '"Thomas C. King"'
Search Results
2. How to Design AI for Social Good: Seven Essential Factors.
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Luciano Floridi, Josh Cowls, Thomas C. King, and Mariarosaria Taddeo
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- 2020
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3. Tosca: Operationalizing Commitments Over Information Protocols.
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Thomas C. King, Akin Günay, Amit K. Chopra, and Munindar P. Singh
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- 2017
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4. Screening Echocardiography in Adults with Down Syndrome
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Thomas C. King, Abhinav Karan, Linda Edwards, and Rafik Jacob
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General Medicine - Published
- 2023
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5. Biomarkers for the Early Detection of Pancreatic Ductal Adenocarcinoma
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Carl A.K. Borrebaeck, Linda D. Mellby, and Thomas C. King
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- 2022
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6. Governing Governance: A Formal Framework for Analysing Institutional Design and Enactment Governance.
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Thomas C. King
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- 2017
7. Smudge Cells in Chronic Lymphocytic Leukemia: Pathophysiology, Laboratory Considerations, and Clinical Significance
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Shashi Mehta, Steven M Marionneaux, Thomas C King, Nicole Lamanna, and Elaine M. Keohane
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Oncology ,medicine.medical_specialty ,Chronic lymphocytic leukemia ,Clinical Biochemistry ,Spinal cord stimulation ,hemic and lymphatic diseases ,Internal medicine ,White blood cell ,medicine ,Humans ,Clinical significance ,Lymphocytes ,Smudge cells ,business.industry ,Biochemistry (medical) ,Reproducibility of Results ,Prognosis ,medicine.disease ,Leukemia, Lymphocytic, Chronic, B-Cell ,Pathophysiology ,Blood film ,Leukemia ,medicine.anatomical_structure ,Laboratories ,business ,Laboratories, Clinical - Abstract
Chronic lymphocytic leukemia (CLL) is the most commonly encountered leukemia in the clinical laboratory. Cytoskeletal defects in CLL lymphocytes can result in the formation of up to 75% smudge cells (SCs) during blood film preparation. Failure to account for these damaged lymphocytes in the white blood cell (WBC) differential diminishes the accuracy and reproducibility of the results. Lacking clear practice standards on handling SCs in CLL, different laboratories may employ different methods to mitigate SC-induced errors. This review explores the pathophysiology of SCs, their effect on WBC differentials in CLL, and how these results can impact clinical decisions. The pros and cons of various SC corrective methods are described to assist laboratories in developing an optimized protocol to reduce errors and inconsistencies in WBC differentials. Finally, the potential utility of SC enumeration as an indicator of CLL prognosis is discussed in terms of laboratories with differing access to technology.
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- 2021
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8. Governing Government: A Framework for Multi-tier Institution Specification and Reasoning.
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Thomas C. King
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- 2015
9. Detection of Early-Stage Pancreatic Ductal Adenocarcinoma From Blood Samples: Results of a Multiplex Biomarker Signature Validation Study
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Randall E. Brand, Jan Persson, Svein Olav Bratlie, Daniel C. Chung, Bryson W. Katona, Alfredo Carrato, Marién Castillo, Julie Earl, Arto Kokkola, Aimee L. Lucas, A. James Moser, Corinne DeCicco, Linda Dexlin Mellby, Thomas C. King, HUS Abdominal Center, and II kirurgian klinikka
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LEWIS ,endocrine system diseases ,IDENTIFICATION ,CA-19-9 Antigen ,Gastroenterology ,EARLY-DIAGNOSIS ,Adenocarcinoma ,CA19-9 ,CANCER ,digestive system diseases ,Pancreatic Neoplasms ,INDIVIDUALS ,CA-19-9 ,3121 General medicine, internal medicine and other clinical medicine ,Biomarkers, Tumor ,Humans ,Carcinoma, Pancreatic Ductal - Abstract
INTRODUCTION: The IMMray PanCan-d test combines an 8-plex biomarker signature with CA19-9 in a proprietary algorithm to detect pancreatic ductal adenocarcinoma (PDAC) in serum samples. This study aimed to validate the clinical performance of the IMMray PanCan-d test and to better understand test performance in Lewis-null (le/le) individuals who cannot express CA19-9. METHODS: Serum samples from 586 individuals were analyzed with the IMMray PanCan-d biomarker signature and CA19-9 assay, including 167 PDAC samples, 203 individuals at high risk of familial/hereditary PDAC, and 216 healthy controls. Samples were collected at 11 sites in the United States and Europe. The study was performed by Immunovia, Inc (Marlborough, MA), and sample identity was blinded throughout the study. Test results were automatically generated using validated custom software with a locked algorithm and predefined decision value cutoffs for sample classification. RESULTS: The IMMray PanCan-d test distinguished PDAC stages I and II (n = 56) vs high-risk individuals with 98% specificity and 85% sensitivity and distinguished PDAC stages I-IV vs high-risk individuals with 98% specificity and 87% sensitivity. We identified samples with a CA19-9 value of 2.5 U/mL or less as probable Lewis-null (le/le) individuals. Excluding these 55 samples from the analysis increased the IMMray PanCan-d test sensitivity to 92% for PDAC stages I-IV (n = 157) vs controls (n = 379) while maintaining specificity at 99%; test sensitivity for PDAC stages I and II increased from 85% to 89%. DISCUSSION: These results demonstrate the IMMray PanCan-d blood test can detect PDAC with high specificity (99%) and sensitivity (92%).
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- 2021
10. Initial clinical results of the first commercial clinical blood test dedicated to the early detection of pancreatic ductal adenocarcinoma (PDAC)
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Thomas C. King
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Cancer Research ,Oncology - Abstract
e16258 Background: The IMMray® PanCan-d blood test for early detection of PDAC has been commercially available in 45 U.S. states since the laboratory’s licensure in August 2021. This is the first clinically-available blood test dedicated to the early detection of PDAC, combining an 8-plex biomarker signature with CA19-9 in a proprietary algorithm. Here we report the initial results of this assay. Methods: All orders received and results reported were reviewed for the IMMray PanCan-d test between August 4, 2021 and February 11, 2022. Serum specimens were processed at the Immunovia, Inc. laboratory in Marlborough, Massachusetts. Demographic information of individuals undergoing testing is based on the completed test requisition submitted by their health care providers. All information was de-identified prior to this analysis. Results: The median age of those tested was 59 years and 46% were male. 76% of patients were referred because of a history of familial pancreatic cancer. Germline mutation prevalence is reported in the table below. 12% of patients had IPMNs or mucinous cystic neoplasms, 2% had chronic pancreatitis and 3% had new onset Diabetes Mellitus. Table. Demographics of Individuals Tested with the IMMray PanCan-d test 80.5% of IMMray PanCan-d results were negative, 1.1% were high-risk signature present, and 11.5% were borderline. These results are fully consistent with validation studies for this assay in high-risk surveillance populations (Brand RE et al Clin Transl Gastroenterol, doi: 10.14309/ctg.0000000000000468). 6.9% of individuals tested had a CA19-9 value of less than 2.5 U/ml, which we identify as presumptively Lewis null (le/le) and CA19-9 non-secretors. Given that CA19-9 contributes significantly to calculated decision values for the IMMray PanCan-d test, individuals with a CA19-9 less than 2.5 U/ml receive a result of test not performed. Conclusions: The commercial availability of a biomarker assay for the early detection of PDAC resulted in a testing population with demographics and referral criteria similar to that of PDAC high-risk surveillance programs in the U.S. IMMray PanCan-d test results were as expected based on prior validation studies.[Table: see text]
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- 2022
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11. Artificial Intelligence Crime: An Interdisciplinary Analysis of Foreseeable Threats and Solutions
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Thomas C. King, Nikita Aggarwal, Mariarosaria Taddeo, and Luciano Floridi
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History ,Polymers and Plastics ,Computer science ,business.industry ,media_common.quotation_subject ,05 social sciences ,Law enforcement ,06 humanities and the arts ,02 engineering and technology ,Space (commercial competition) ,Certainty ,0603 philosophy, ethics and religion ,Industrial and Manufacturing Engineering ,020204 information systems ,0202 electrical engineering, electronic engineering, information engineering ,0501 psychology and cognitive sciences ,Social media ,Artificial intelligence ,060301 applied ethics ,Business and International Management ,business ,050107 human factors ,media_common - Abstract
Artificial Intelligence (AI) research and regulation seek to balance the benefits of innovation against any potential harms and disruption. However, one unintended consequence of the recent surge in AI research is the potential re-orientation of AI technologies to facilitate criminal acts, which we term AI-Crime (AIC). We already know that AIC is theoretically feasible thanks to published experiments in automating fraud targeted at social media users, as well as demonstrations of AI-driven manipulation of simulated markets. However, because AIC is still a relatively young and inherently interdisciplinary area—spanning socio-legal studies to formal science—there is little certainty of what an AIC future might look like. This article offers the first systematic, interdisciplinary literature analysis of the foreseeable threats of AIC, providing law enforcement and policy-makers with a synthesis of the current problems, and a possible solution space.
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- 2021
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12. How to Design AI for Social Good: Seven Essential Factors
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Luciano Floridi, Josh Cowls, Thomas C. King, and Mariarosaria Taddeo
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- 2021
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13. Examining the mental health outcomes of school-based peer-led interventions on young people: A scoping review of range and a systematic review of effectiveness
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Mina Fazel and Thomas C. King
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Gerontology ,Databases, Factual ,Emotions ,Psychological intervention ,Social Sciences ,Database and Informatics Methods ,0302 clinical medicine ,Sociology ,Medicine and Health Sciences ,Psychology ,030212 general & internal medicine ,Database Searching ,media_common ,Multidisciplinary ,Schools ,05 social sciences ,050301 education ,Research Assessment ,Suicide ,Systematic review ,Health Education and Awareness ,Evidence-Based Practice ,Medicine ,Research Article ,Mental Health Services ,Adolescent ,Systematic Reviews ,Science ,media_common.quotation_subject ,education ,Research and Analysis Methods ,Peer Group ,Education ,03 medical and health sciences ,Young Adult ,Quality of life (healthcare) ,Intervention (counseling) ,Mental Health and Psychiatry ,Humans ,Narrative ,Quality (business) ,Students ,Social stress ,Biology and Life Sciences ,Mental health ,Self Concept ,Health Care ,Quality of Life ,0503 education - Abstract
Schools worldwide have implemented many different peer-led interventions with mixed results, but the evidence base on their effectiveness as mental health interventions remains limited. This study combines a scoping review and systematic review to map the variations of peer-led interventions in schools and to evaluate the quality of the existing evidence base. This scoping review and systematic review evaluated the existing literature across 11 academic databases. Studies were included if they reported a peer-led intervention that aimed to address a mental health or wellbeing issue using a peer from the same school setting. Data were extracted from published and unpublished reports and presented as a narrative synthesis. 54 studies met eligibility criteria for the scoping review, showing that peer-led interventions have been used to address a range of mental health and wellbeing issues globally. 11 studies met eligibility criteria for the systematic review with a total of 2,239 participants eligible for analysis (929 peer leaders; 1,310 peer recipients). Two studies out of seven that looked at peer leaders showed significant improvements in self-esteem and social stress, with one study showing an increase in guilt. Two studies out of five that looked at peer recipient outcomes showed significant improvements in self-confidence and in a quality of life measure, with one study showing an increase in learning stress and a decrease in overall mental health scores. The findings from these reviews show that despite widespread use of peer-led interventions, the evidence base for mental health outcomes is sparse. There appear to be better documented benefits of participation for those who are chosen and trained to be a peer leader, than for recipients. However, the small number of included studies means any conclusions about effectiveness are tentative.
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- 2020
14. Continuous Isoprene Measurements in a UK Temperate Forest for a Whole Growing Season: Effects of Drought Stress During the 2018 Heatwave
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Yadvinder Malhi, Neil R. P. Harris, Zosia Staniaszek, Frederick Otu-Larbi, R.A. Freshwater, Kirsti Ashworth, Roderic L. Jones, Conor G. Bolas, John Beale, Kerneels Jaars, Thomas C. King, Toby W. Waine, and Valerio Ferracci
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Tree canopy ,Drought stress ,long-term measurements ,Isoprene ,010504 meteorology & atmospheric sciences ,drought stress ,fungi ,food and beverages ,Temperate forest ,Growing season ,Vegetation ,010502 geochemistry & geophysics ,Atmospheric sciences ,01 natural sciences ,chemistry.chemical_compound ,Geophysics ,chemistry ,Photosynthetically active radiation ,General Earth and Planetary Sciences ,Environmental science ,Ecosystem ,BVOCs ,biosphere-atmosphere interactions ,0105 earth and related environmental sciences - Abstract
Isoprene concentrations were measured at four heights below, within and above the forest canopy in Wytham Woods (UK) throughout the summer of 2018 using custom-built gas chromatographs (the iDirac). These observations were complemented with selected ancillary variables, including air temperature, photosynthetically active radiation (PAR), occasional leaf gas exchange measurements and satellite retrievals of normalized difference vegetation and water indices (NDVI and NDWI). The campaign overlapped with a long and uninterrupted heatwave accompanied by moderate drought. Peak isoprene concentrations during the heatwave-drought were up to a factor of 4 higher than those before or after. Higher temperatures during the heatwave could not account for all the observed isoprene; the enhanced abundances correlated with drought stress. Leaf-level emissions confirmed this and also included compounds associated with ecosystem stress. This work highlights that a more in-depth understanding of the effects of drought stress is required to better characterize isoprene emissions.
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- 2020
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15. S8 The IMMray PanCan-d Test Performance and CA19-9: Results From the Blind Validation Study
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Thomas C. King
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Validation study ,Hepatology ,business.industry ,Gastroenterology ,Medicine ,Artificial intelligence ,business ,Machine learning ,computer.software_genre ,computer - Published
- 2021
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16. Examining the mental health outcomes of peer-led school-based interventions on young people aged between 4 and 18 years old: a systematic review protocol
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Mina Fazel and Thomas C. King
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Gerontology ,School ,Adolescent ,education ,Well-being ,MEDLINE ,Psychological intervention ,Medicine (miscellaneous) ,lcsh:Medicine ,Intervention ,CINAHL ,PsycINFO ,Peer support ,Global Health ,Peer Group ,03 medical and health sciences ,0302 clinical medicine ,Health care ,Medicine ,Humans ,030212 general & internal medicine ,Child ,School Health Services ,business.industry ,Delivery of Health Care, Integrated ,030503 health policy & services ,lcsh:R ,Mental health ,Mental Health ,Adolescent Behavior ,Child, Preschool ,Observational study ,0305 other medical science ,business ,Peer - Abstract
Background: Recent estimates suggest that one in ten young people worldwide experiences a diagnosable mental health disorder, with many more suffering subsyndromal levels of psychological distress. As young people spend much of their time in schools, the role of educational settings in the delivery of mental health provision is increasingly recognised. Advances in neurodevelopmental research have highlighted the important and complex role of peer influence on adolescent behaviours, suggesting peer-led support schemes have high potential utility. Schools worldwide have implemented peer-led interventions with mixed results, but the global evidence base on their effectiveness remains limited. This systematic review aims to examine the evidence base of the outcomes of school-based peer-led interventions on the mental health of young people aged 4–18.Methods: Eligible studies will be randomised controlled trials and observational studies that report on the mental health outcomes of a peer-led school-based intervention. Eligible participants will be aged 4–18 and will be current students of the intervention school. Individual- and group-based interventions will be included. The following 11 databases will be screened based upon their reach in healthcare and education: PsycINFO, MEDLINE, EMBASE, CINAHL, CENTRAL, BEI, Scopus, Web of Science, ERIC, SSCI and Social Care Online. There will be no restriction placed on publication period, original language or country of publication. Papers will be systematically screened for eligibility by two review authors. Data will be presented as a descriptive report. A meta-analysis will be carried out if a subset of studies allows, given the anticipated high levels of heterogeneity.Discussion: This systematic review will be the first to synthesise the global evidence on the mental health outcomes of peer-led interventions for children and adolescents in a school setting. It will analyse the available data in order to understand the role of these interventions in schools, inform future developers of peer support programmes and identify gaps in current research. This review will be of value to policy makers, health and education services, researchers and those involved in delivering peer support initiatives.
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- 2019
17. Projecting AI-Crime: A Review of Plausible Threats
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Thomas C. King
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Balance (metaphysics) ,Risk analysis (engineering) ,media_common.quotation_subject ,Law enforcement ,Social media ,Business ,Certainty ,Term (time) ,media_common - Abstract
Artificial Intelligence (AI) research and regulation seek to balance the benefits of innovation against any potential harms and disruption. However, one unintended consequence of the recent surge in AI research is the potential re-orientation of AI technologies to facilitate criminal acts, which I term AI-Crime (AIC). We already know that AIC is theoretically feasible thanks to published experiments in automating fraud targeted at social media users, as well as demonstrations of AI-driven manipulation of simulated markets. However, because AIC is still a relatively young and inherently interdisciplinary area of research—spanning socio-legal studies to formal science—there is little certainty of what an AIC future might look like. This article offers the first systematic, interdisciplinary literature analysis of the foreseeable threats of AIC, providing law enforcement and policy-makers with a synthesis of the current problems.
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- 2019
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18. Artificial Intelligence Crime: An Interdisciplinary Analysis of Foreseeable Threats and Solutions
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Mariarosaria Taddeo, Nikita Aggarwal, Thomas C. King, and Luciano Floridi
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Artificial intelligence ,Health (social science) ,AI-Crime ,Computer science ,media_common.quotation_subject ,Interdisciplinary Research ,02 engineering and technology ,Space (commercial competition) ,020204 information systems ,Management of Technology and Innovation ,Machine learning ,0202 electrical engineering, electronic engineering, information engineering ,Dual-use ,Humans ,Social media ,Drug Trafficking ,media_common ,Ethics ,Philosophy of science ,Original Paper ,business.industry ,Health Policy ,Fraud ,Sex Offenses ,Law enforcement ,Commerce ,AI and law ,Liability, Legal ,Certainty ,16. Peace & justice ,Issues, ethics and legal aspects ,020201 artificial intelligence & image processing ,Crime ,business ,Social Media ,Forecasting - Abstract
Artificial intelligence (AI) research and regulation seek to balance the benefits of innovation against any potential harms and disruption. However, one unintended consequence of the recent surge in AI research is the potential re-orientation of AI technologies to facilitate criminal acts, term in this article AI-Crime (AIC). AIC is theoretically feasible thanks to published experiments in automating fraud targeted at social media users, as well as demonstrations of AI-driven manipulation of simulated markets. However, because AIC is still a relatively young and inherently interdisciplinary area—spanning socio-legal studies to formal science—there is little certainty of what an AIC future might look like. This article offers the first systematic, interdisciplinary literature analysis of the foreseeable threats of AIC, providing ethicists, policy-makers, and law enforcement organisations with a synthesis of the current problems, and a possible solution space.
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- 2018
19. Revising institutions governed by institutions for compliant regulations
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Catholijn M. Jonker, Julian Padget, Marina De Vos, Thomas C. King, Tingting Li, and M. Birna van Riemsdijk
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Dilemma ,media_common.quotation_subject ,Corporate governance ,Institution ,Legislation ,Business ,Social science ,Public administration ,media_common ,Compliance (psychology) - Abstract
Institutions governing multi-agent systems (MASs) are a pervasive means to guide agents towards the aims of the MAS (e.g. collecting data) with regulations on the outcomes of agents’ behaviour. Yet, wider organisations/governments often intend to guide the design of institutions governing MAS in meeting different aims (e.g. preserving the rights of agents). A pervasive means to guide the design of MAS-governing institutions (or any institution, for that matter) is to use institutions at higher tiers of governance (e.g. directives, constitutions) to regulate the regulations of institutions at lower tiers of governance (e.g. national legislation, software policies). A recent innovation has been an automated means to determine the compliance of a lower-tier institution’s regulations with a higher-tier’s. However, for a designer of a non-compliant institution there remains a dilemma: be punished for non-compliant regulations or arduously determine and rectify the underlying causes of non-compliance. In this paper we propose a way to automatically determine how to revise an institution to be compliant that also minimises the change in the regulations’ outcomes thus keeping as closely as possible to the institution designers’ original intentions.
- Published
- 2018
20. T-SPOT.TB Interferon-γ Release Assay Performance in Healthcare Worker Screening at Nineteen U.S. Hospitals
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Chris P. Kadlecek, Kathy Murray, Philip Adamo, Pamela Drewry, Albert F. Rielly, John Balser, Peter Wrighton-Smith, Janet Matsubara, Thomas C. King, Mark Upfal, Marcie DeWitt, Andrew Gottlieb, Frances Humphrey-Carothers, Edward J Bernacki, Jeffrey G. Jones, and Louis St. L. O'Dea
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Pulmonary and Respiratory Medicine ,High rate ,medicine.medical_specialty ,business.industry ,Healthcare worker ,Tuberculin ,Tuberculosis screening ,Critical Care and Intensive Care Medicine ,Interferon γ ,Internal medicine ,Mean reversion ,Screening programs ,Medicine ,business ,T-SPOT.TB - Abstract
Rationale: Interferon-γ release assays have significant advantages over tuberculin skin testing in many clinical situations. However, recent studies have called into question their reliability in serial testing of healthcare workers because of reportedly high rates of positivity and high conversion/reversion rates on retesting.Objectives: To define the performance characteristics of the T-SPOT.TB test, an interferon-γ release assay, during serial screening programs of healthcare workers at 19 U.S. hospitals.Methods: A total of 42,155 T-SPOT.TB test results from healthcare workers at 19 geographically diverse hospitals obtained for routine tuberculosis screening programs were analyzed to determine the rates of positivity, reversion, and conversion in serial testing data.Measurements and Main Results: In 19,630 evaluable serial pairs from 16,076 healthcare workers, the mean test positivity rate was 2.3% (range, 0.0–27.4%). The mean conversion rate was 0.8% (range, 0.0–2.5%), and the mean reversion rate was ...
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- 2015
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21. Automated multi-level governance compliance checking
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Thomas C. King, Catholijn M. Jonker, Tingting Li, Marina De Vos, Julian Padget, Virginia Dignum, and M. Birna van Riemsdijk
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Multi-level governance ,Computer science ,media_common.quotation_subject ,0801 Artificial Intelligence And Image Processing ,Legislation ,ComputingMilieux_LEGALASPECTSOFCOMPUTING ,0102 computer and information sciences ,02 engineering and technology ,Institutions ,01 natural sciences ,Compliance (psychology) ,Artificial Intelligence ,Order (exchange) ,0202 electrical engineering, electronic engineering, information engineering ,Institution ,Artificial Intelligence & Image Processing ,media_common ,Law and economics ,Government ,Human rights ,business.industry ,Corporate governance ,1702 Cognitive Science ,Normative reasoning ,010201 computation theory & mathematics ,020201 artificial intelligence & image processing ,Artificial intelligence ,business - Abstract
An institution typically comprises constitutive rules, which give shape and meaning to social interactions and regulative rules, which prescribe agent behaviour in the society. Regulative rules guide social interaction, in particular when they are coupled with reward and punishment regulations that are enforced for (non-)compliance. Institution examples include legislation and contracts. Formal institutional reasoning frameworks automate ascribing social meaning to agent interaction and determining whether those actions have social meanings that comprise (non-)compliant behaviour. Yet, institutions do not just govern societies. Rather, in what is called multi-level governance, institutional designs at lower governance levels (e.g., national legislation at the national level) are governed by higher level institutions (e.g., directives, human rights charters and supranational agreements). When an institution design is found to be non-compliant, punishments can be issued by annulling the legislation or imposing fines on the responsible designers (i.e., government). In order to enforce multi-level governance, higher governance levels (e.g., courts applying human rights) must check lower level institution designs (e.g., national legislation) for compliance; in order to avoid punishment, lower governance levels (e.g., national governments) must check their institution designs are compliant with higher-level institutions before enactment. However, checking non-compliance of institution designs in multi-level governance is non-trivial. In particular, because institutions in multi-level governance operate at different levels of abstraction. Lower level institutions govern with concrete regulations whilst higher level institutions typically comprise increasingly vague and abstract regulations. To address this issue, in this paper we propose a formal framework with a novel semantics that defines compliance between concrete lower level institutions and abstract higher level institutions. The formal framework is complemented by a sound and complete computational framework that automates compliance checking, which we apply to a real-world case study.
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- 2017
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22. Artificial intelligence-enabled screening strategy for drug repurposing in monoclonal gammopathy of undetermined significance
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Alexander J. Ryu, Shaji Kumar, Angela Dispenzieri, Robert A. Kyle, S. Vincent Rajkumar, and Thomas C. Kingsley
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Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
Abstract Monoclonal gammopathy of undetermined significance (MGUS) is a benign hematological condition with the potential to progress to malignant conditions including multiple myeloma and Waldenstrom macroglobulinemia. Medications that modify progression risk have yet to be identified. To investigate, we leveraged machine-learning and electronic health record (EHR) data to screen for drug repurposing candidates. We extracted clinical and laboratory data from a manually curated MGUS database, containing 16,752 MGUS patients diagnosed from January 1, 2000 through December 31, 2021, prospectively maintained at Mayo Clinic. We merged this with comorbidity and medication data from the EHR. Medications were mapped to 21 drug classes of interest. The XGBoost module was then used to train a primary Cox survival model; sensitivity analyses were also performed limiting the study group to those with non-IgM MGUS and those with M-spikes >0.3 g/dl. The impact of explanatory features was quantified as hazard ratios after generating distributions using bootstrapping. Medication data were available for 12,253 patients; those without medications data were excluded. Our model achieved a good fit of the data with inverse probability of censoring weights concordance index of 0.883. The presence of multivitamins, immunosuppression, non-coronary NSAIDS, proton pump inhibitors, vitamin D supplementation, opioids, statins and beta-blockers were associated with significantly lower hazard ratio for MGUS progression in our primary model; multivitamins and non-coronary NSAIDs remained significant across both sensitivity analyses. This work could inform subsequent prospective studies, or similar studies in other disease states.
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- 2023
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23. Reply: Revisiting Healthcare Workers as a Risk Group for Progression toward Tuberculosis
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Mark Upfal, Louis St. L. O'Dea, and Thomas C. King
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Pulmonary and Respiratory Medicine ,Male ,medicine.medical_specialty ,Tuberculosis ,business.industry ,Critical Care and Intensive Care Medicine ,medicine.disease ,Surgery ,Personnel, Hospital ,Risk groups ,Health care ,Emergency medicine ,Medicine ,Humans ,Mass Screening ,Female ,business ,Mass screening ,Interferon-gamma Release Tests ,Personnel hospital - Published
- 2015
24. Chronic Cough and Bilateral Pneumothoraces in a Nonsmoker
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Sarah L. O’Beirne, Thomas C. King, Navneet Narula, Jordan E. Arkin, Joanna G. Escalon, Robert J. Kaner, Alan C. Legasto, and Brendon M. Stiles
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Pulmonary and Respiratory Medicine ,Male ,medicine.medical_specialty ,Biopsy ,Pulmonary Fibrosis ,Lung biopsy ,Critical Care and Intensive Care Medicine ,Diagnosis, Differential ,03 medical and health sciences ,Idiopathic pulmonary fibrosis ,0302 clinical medicine ,Usual interstitial pneumonia ,medicine ,Humans ,Pneumomediastinum ,Lung ,Aged, 80 and over ,medicine.diagnostic_test ,business.industry ,Pneumothorax ,Pleural Diseases ,medicine.disease ,Fibrosis ,respiratory tract diseases ,Surgery ,Chronic cough ,medicine.anatomical_structure ,030228 respiratory system ,Cough ,030220 oncology & carcinogenesis ,Chronic Disease ,Radiology ,medicine.symptom ,Cardiology and Cardiovascular Medicine ,business ,Tomography, X-Ray Computed - Abstract
An 82-year-old Japanese nonsmoking man presented with persistent dry cough and small left apical pneumothorax. High resolution CT scan of the chest demonstrated bilateral upper lobe pleuroparenchymal thickening and architectural distortion. Serial imaging revealed mild progression and development of small bilateral pneumothoraces, and pneumomediastinum. A surgical lung biopsy was required to confirm the diagnosis.
- Published
- 2015
25. Assessing the Generalizability of a Clinical Machine Learning Model Across Multiple Emergency Departments
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Alexander J. Ryu, MD, Santiago Romero-Brufau, MD, PhD, Ray Qian, MD, Heather A. Heaton, MD, David M. Nestler, MD, Shant Ayanian, MD, and Thomas C. Kingsley, MD
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Medicine (General) ,R5-920 - Abstract
Objective: To assess the generalizability of a clinical machine learning algorithm across multiple emergency departments (EDs). Patients and Methods: We obtained data on all ED visits at our health care system’s largest ED from May 5, 2018, to December 31, 2019. We also obtained data from 3 satellite EDs and 1 distant-hub ED from May 1, 2018, to December 31, 2018. A gradient-boosted machine model was trained on pooled data from the included EDs. To prevent the effect of differing training set sizes, the data were randomly downsampled to match those of our smallest ED. A second model was trained on this downsampled, pooled data. The model’s performance was compared using area under the receiver operating characteristic (AUC). Finally, site-specific models were trained and tested across all the sites, and the importance of features was examined to understand the reasons for differing generalizability. Results: The training data sets contained 1918-64,161 ED visits. The AUC for the pooled model ranged from 0.84 to 0.94 across the sites; the performance decreased slightly when Ns were downsampled to match those of our smallest ED site. When site-specific models were trained and tested across all the sites, the AUCs ranged more widely from 0.71 to 0.93. Within a single ED site, the performance of the 5 site-specific models was most variable for our largest and smallest EDs. Finally, when the importance of features was examined, several features were common to all site-specific models; however, the weight of these features differed. Conclusion: A machine learning model for predicting hospital admission from the ED will generalize fairly well within the health care system but will still have significant differences in AUC performance across sites because of site-specific factors.
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- 2022
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26. Supporting Request Acceptance with Use Policies
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M. Birna van Riemsdijk, Virginia Dignum, Thomas C. King, and Catholijn M. Jonker
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Resource (project management) ,Knowledge management ,Work (electrical) ,Computer science ,business.industry ,media_common.quotation_subject ,Semantic reasoner ,Set (psychology) ,business ,Event calculus ,Autonomy ,media_common - Abstract
This paper deals with the problem of automating the contribution of resources owned by people to do work for others. This is by providing a means for owners of resources to maintain autonomy over how, when and to whom their resources are used with the specification of use policies governing resources. We give representations of requests for resource usage as a set of conditional norms and a use policy as specifying what norms should and should not be imposed on a resource i.e. a set of meta-norms. Our main contribution is a reasoner built on the Event Calculus, that detects conflicts between requests and use policies, determining whether the request can be accepted.
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- 2015
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27. Medications and Patient Factors Associated With Increased Readmission for Alcohol-Related Diagnoses
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Joseph C. Osborne, II, PharmD, Susan E. Horsman, PharmD, BCPS, Kristin C. Mara, MS, Thomas C. Kingsley, MD, MPH, Robert W. Kirchoff, MD, and Jonathan G. Leung, PharmD, BCPS, BCPP
- Subjects
Medicine (General) ,R5-920 - Abstract
Objective: To investigate medication factors and patient characteristics associated with readmissions following alcohol-related hospitalizations. Patients and Methods: Adult patients admitted from September 1, 2016, through August 31, 2019, who had an alcohol-related hospitalization were identified through electronic health records. Patient characteristics and medications of interest administered during hospitalization or prescribed at discharge were identified. Medications of interest included US Food and Drug Administration–approved medications for alcohol use disorder, benzodiazepines, barbiturates, gabapentin, opioids, and muscle relaxants. The primary outcome was to identify medications and patient factors associated with 30-day alcohol-related readmission. Secondary outcomes included medications and patient characteristics associated with multiple alcohol-related readmissions within a year from the index admission (ie, two or more readmissions) and factors associated with 30-day all-cause readmission. Results: Characteristics of the 932 patients included in this study associated with a 30-day alcohol-related readmission included younger age, severity of alcohol withdrawal, history of psychiatric disorder, marital status, and the number of prior alcohol-related admission in the previous year. Benzodiazepine or barbiturate use during hospitalization or upon discharge was associated with 30-day alcohol-related readmission (P=.006). Gabapentin administration during hospitalization or upon discharge was not associated with 30-day alcohol-related readmission (P=.079). Conclusion: The findings reinforce current literature identifying patient-specific factors associated with 30-day readmissions. Gabapentin use was not associated with readmissions; however, there was an association with benzodiazepine/barbiturate use.
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- 2022
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28. Characterization and localization to chromosome 7 of ψhGABPα, a human processed pseudogene related to the ets transcription factor, hGABPα
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Carl P. Simkevich, Thomas C King, Menglin Luo, Cynthia L. Jackson, Zhong-Fa Yang, Alan G. Rosmarin, and Jing Shang
- Subjects
Chromosome 7 (human) ,Genetics ,Base Sequence ,Proto-Oncogene Proteins c-ets ,Transcription, Genetic ,Pseudogene ,Intron ,Chromosome Mapping ,Transcription factor complex ,TAF9 ,General Medicine ,Biology ,genomic DNA ,Protein Biosynthesis ,Proto-Oncogene Proteins ,Humans ,Human genome ,Cloning, Molecular ,Chromosome 21 ,Pseudogenes ,Chromosomes, Human, Pair 8 ,DNA Primers ,Transcription Factors - Abstract
GABP is a heteromeric transcription factor complex which consists of the ets related protein, GABPalpha, and the Notch-related protein, GABPbeta. We isolated a human genomic DNA fragment which is highly homologous and colinear with human GABPalpha cDNA, but which lacks introns. This processed pseudogene, psihGABPalpha, is expressed as RNA in U937 human myeloid cells, but a mutation at the site that corresponds to the ATG start methionine codon prevents its translation into protein. The pseudogene was localized to chromosome 7 using a somatic cell hybrid mapping panel and it is not syntenic with authentic GABPalpha, which was localized to chromosome 21. We have identified psihGABPalpha, a novel, GABPalpha-related processed pseudogene which is expressed as a RNA transcript in human myeloid cells.
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- 1999
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29. Why Mayo Clinic Is Embracing the Cloud and What This Means for Clinicians and Researchers
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Alexander J. Ryu, MD, Dale R. Magnuson, MS, and Thomas C. Kingsley, MD, MPH, MS
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Medicine (General) ,R5-920 - Published
- 2021
- Full Text
- View/download PDF
30. Influence of breast cancer margin assessment method on the rates of positive margins and residual carcinoma
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Thomas C. King, Sandra Cerda, Michael D. Stone, Maureen T. Kavanah, Erwin F. Hirsch, Jane E. Méndez, Antonio de las Morenas, Robert Pistey, and Wayne W. LaMorte
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medicine.medical_specialty ,Neoplasm, Residual ,medicine.medical_treatment ,Mammary gland ,Urology ,Breast Neoplasms ,Mastectomy, Segmental ,Group A ,Group B ,Breast cancer ,Margin (machine learning) ,mental disorders ,Carcinoma ,Humans ,Medicine ,Retrospective Studies ,Histocytological Preparation Techniques ,business.industry ,Retrospective cohort study ,General Medicine ,medicine.disease ,Surgery ,medicine.anatomical_structure ,Female ,business ,Mastectomy - Abstract
Background We hypothesized that the method of breast cancer margin assessment may be associated with different rates of positive margins and residual carcinoma. Methods A total of 178 breast cancer specimens were divided into 2 groups (A and B) based on the margin assessment method used. Rates of positive margins, re-excision, and residual carcinoma at re-excision were compared and analyzed statistically. Results At least 1 margin was positive in 64.7% in group A and in 65.2% in group B. At directed re-excision 54% in group A and 51% in group B had residual carcinoma. The lateral margin was positive in 44% in group A compared with 26% in group B ( P = .06). The posterior margin was positive in 19% in group A and in 51% in group B ( P = .001). Conclusions Two different breast cancer specimen margin assessment methods had comparable rates of positive margins and residual carcinoma at re-excision. Different patterns of specific margin positivity suggest that the method of margin assessment may alter results.
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- 2006
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31. Re-checking Normative System Coherence
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Virginia Dignum, Thomas C. King, and M. Birna van Riemsdijk
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Action (philosophy) ,Normative systems ,Computer science ,Selection rule ,Law ,Normative ,Coherence (statistics) ,Obligation ,Principle of legality ,Set (psychology) ,Law and economics - Abstract
Sets of related norms (normative systems) are likely to evolve due to changing goals of an organization or changing values of a society, this may introduce incoherence, such as the simultaneous prohibition and obligation of an action or a set of deadlocked duties. This paper presents a compositional framework that may be used for detecting whether normative systems are coherent by analysing traces of actions and their legality. Unlike other mechanisms for checking normative system coherence, the framework makes it possible to re-check just those parts of the system that have changed, without re-checking the entirety.
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- 2014
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32. 11βOH-Progesterone Affects Vascular Glucocorticoid Metabolism and Contractile Response
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David J. Morris, Robert B. Bina, Andrew S. Brem, and Thomas C. King
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medicine.medical_specialty ,Vascular smooth muscle ,Dehydrogenase ,In Vitro Techniques ,Biology ,Muscle, Smooth, Vascular ,Rats, Sprague-Dawley ,chemistry.chemical_compound ,Corticosterone ,In vivo ,Internal medicine ,Renin–angiotensin system ,Hydroxyprogesterones ,Internal Medicine ,medicine ,Animals ,Glucocorticoids ,Phenylephrine ,Progesterone ,Angiotensin II ,Enzymes ,Rats ,Kinetics ,Endocrinology ,chemistry ,Vasoconstriction ,Glucocorticoid ,medicine.drug - Abstract
Abstract Vascular smooth muscle (VSM) contains a bidirectional isoform of 11β-hydroxysteroid dehydrogenase (11β-HSD), the enzyme that can metabolize endogenous glucocorticoids to their respective 11-dehydro derivatives. 11βOH-progesterone (11βOH-P), a compound that can be produced in vivo, is as potent or more potent than licorice derivatives in inhibiting renal and hepatic 11β-HSD. When studied in homogenates prepared from primary cultures of rat VSM, 11βOH-P and its derivative, 11-keto-progesterone (11-keto-P), proved to be potent, directionally specific inhibitors of vascular 11β-HSD. 11βOH-P selectively inhibited the forward dehydrogenase reaction (corticosterone→11-dehydrocorticosterone), whereas 11-keto-P selectively blocked the reverse oxidoreductase reaction. To test the physiological effects, vascular rings were prepared from rat aorta. Rings were incubated in culture media containing either a submaximal concentration of corticosterone (10 nmol/L), 11-dehydrocorticosterone (100 nmol/L), 11βOH-P (1 μmol/L), 11-keto-P (1 μmol/L), or a combination of glucocorticoid and inhibitor for 24 hours. After the 24-hour incubation, rings were briefly stimulated sequentially with phenylephrine (10 nmol/L to 1 μmol/L) and angiotensin II (1 μmol/L). The immediate contractile response in rings incubated with both corticosterone and 11βOH-P was greater than in rings previously incubated with either the corticosterone or 11βOH-P alone (eg, response to 100 nmol/L phenylephrine in milligrams of force, mean±SE: corticosterone, 728±56, n=9; 11βOH-P, 325±105, n=4; both, 1132±122, n=8; corticosterone versus both, P
- Published
- 1997
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33. Paclitaxel and concurrent radiation for lung, pancreatic, and gastric carcinomas: Significance of p53 gene mutations for treatment response
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Thomas C. King, Wallace Akerley, Howard Safran, and Hak Choy
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Oncology ,Cisplatin ,Cancer Research ,medicine.medical_specialty ,Radiosensitizer ,Tumor suppressor gene ,business.industry ,medicine.medical_treatment ,Gene mutation ,Cell cycle ,Spindle apparatus ,Radiation therapy ,chemistry.chemical_compound ,Paclitaxel ,chemistry ,Internal medicine ,medicine ,Radiology, Nuclear Medicine and imaging ,business ,medicine.drug - Abstract
Paclitaxel (Taxol; Bristol-Myers Squibb Company, Princeton, NJ) and concurrent radiation (paclitaxel/RT) are being actively evaluated as treatment for locally advanced lung, pancreatic, and gastric cancers. Paclitaxel is a potent chemotherapeutic agent that interferes with mitotic spindle function to synchronize cells at G 2 M, the most radiosensitive phase of the cell cycle. Because G 2 M arrest is necessary but not sufficient for paclitaxel radiosensitization, other cellular factors must interact with paclitaxel to produce radiosensitization. We have investigated whether molecular genetic alterations that disturb cell cycle regulation in tumor cells affect the action of paclitaxel as a radiosensitizer. The p53 tumor suppressor gene serves a critical role at the G 1 S transi tion of the cell cycle by blocking entry into S phase under conditions that would result in genetic instability. Mutations in the tumor suppressor gene, p53, confer resistance to radiation therapy and most chemotherapeutic agents, including cisplatin and 5-fluorouracil. In striking contrast, we have now shown that p53 mutations in non-small cell lung cancer do not confer resistance to paclitaxel/RT. The effect of p53 mutations on response to paclitaxel/RT in pancreatic and gastric cancers is currently being investigated. Knowledge of specific genetic alterations in individual tumors may permit the selection of optimal therapeutic strategy for individual patients.
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- 1997
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34. Transcription factor YY1 expression in human gastrointestinal cancer cells
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H. Christian Weber, Dongmei Xiao, Dharmaraj Chinnappan, Chris Andry, Thomas C King, and Anita Ratnasari
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Cancer Research ,Colorectal cancer ,Biology ,medicine ,Humans ,Gastrointestinal cancer ,RNA, Messenger ,Cells, Cultured ,YY1 Transcription Factor ,Gastrointestinal Neoplasms ,Regulation of gene expression ,Oncogene ,Protein Stability ,Carcinoma ,Cancer ,Cell cycle ,medicine.disease ,Gene Expression Regulation, Neoplastic ,Oncology ,Apoptosis ,embryonic structures ,Cancer cell ,Cancer research ,Caco-2 Cells ,HT29 Cells ,HeLa Cells ,Transcription Factors - Abstract
Over-expression of the multifunctional zinc-finger transcription factor Yin Yang 1 (YY1) has been associated with cellular proliferation and resistance to apoptotic stimuli. In this study, we report that YY1 was uniformly highly over-expressed in a wide range of human cancer cell lines and in human colon cancer tissue samples. The examination of YY1-specific mRNA expression demonstrated at least six mRNA isoforms ubiquitously expressed in normal human adult and fetal tissues. Substantial over-expression of two specific mRNA isoforms of 7.5 and 2.9 kb size, respectively, was detected in gastrointestinal and other cancer cells in vitro, whereby mRNA stability differed significantly between various cell lines. YY1 protein expression levels were similar in different colon cancer cell lines. Using FISH analysis of several colorectal cancer cell lines, the human YY1 locus was expectedly identified on chromosome 14q32 and no evidence of gene amplification and chromosomal translocation was observed. However, varying degree of aneuploidy was noted in vitro. YY1 immunoreactivity in human colon tumor samples was found more intense in poorly differentiated tumors than in moderately and well differentiated colon cancers and lower expression levels tended to be associated with shorter survival. In conclusion, YY1 was over-expressed in colon cancer in the absence of gene amplification and chromosomal translocation. YY1 mRNA and protein stability are important regulatory mechanisms of YY1 expression in colon cancer.
- Published
- 2009
35. Extracorporeal membrane oxygenation for perioperative support in pediatric heart transplantation
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Mark Galantowicz, Charles J.H. Stolar, and Thomas C. King
- Subjects
Pulmonary and Respiratory Medicine ,Heart transplantation ,Resuscitation ,medicine.medical_specialty ,Membrane oxygenator ,business.industry ,medicine.medical_treatment ,Perioperative ,medicine.disease ,Preoperative care ,Surgery ,Transplantation ,surgical procedures, operative ,Heart failure ,Anesthesia ,medicine ,Extracorporeal membrane oxygenation ,Cardiology and Cardiovascular Medicine ,business - Abstract
Extracorporeal membrane oxygenation has demonstrated effectiveness for cardiopulmonary support in a variety of clinical situations. This article reviews the cases in which extracorporeal membrane oxygenation was used as an adjunct to pediatric cardiac transplantation. Twenty children, aged 7 days to 17 years, with cardiac failure refractory to conventional therapy received extracorporeal membrane oxygenation for 6 to 192 hours. In 4 cases it was used as a bridge to transplantation; in 10 cases it facilitated resuscitation of the cardiac allograft in the immediate postoperative period; and in 6 cases it complemented therapy for severe rejection in the late postoperative period. Twelve patients survived extracorporeal membrane oxygenation, 7 of whom lived more than 8 months. One long-term survivor was in the bridge-to-transplant group, 4 in the immediate postoperative group, and 2 in the rejection group. All survivors have normal cardiac allograft function. These data suggest that extracorporeal membrane oxygenation can be used to support profound cardiac failure in the pediatric heart transplant patient as a bridge to transplantation, in the resuscitation of the cardiac allograft, or to supplement a rejecting allograft.
- Published
- 1991
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36. Hydroxyethyl Starch Effects on Rat Warm Renal Ischemia
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Vivette D. D'Agati, Thomas C. King, Scott T. Shih, Paul F. McCleod, Mehmet C. Oz, Bashir A. Zikria, and Roman Nowygrod
- Subjects
medicine.medical_specialty ,Kidney ,Creatinine ,Renal ischemia ,business.industry ,medicine.medical_treatment ,Ischemia ,Urology ,Hydroxyethyl starch ,medicine.disease ,Human serum albumin ,Surgery ,chemistry.chemical_compound ,medicine.anatomical_structure ,chemistry ,medicine.artery ,Medicine ,Renal artery ,Cardiology and Cardiovascular Medicine ,business ,Saline ,medicine.drug - Abstract
Fractions of hydroxyethyl starch (HES), 100,000-1,000,000 daltons, have been shown to reduce increased permeability changes in postcapillary venules associated with ischemia-reperfusion injury in canine myocardium and rat skel etal muscle. The authors studied the effect of intravenous administration of two fractions of the biodegradable HES, Fm (100,000-300,000 daltons) and FLm (300,000-1,000,000 daltons), in the prevention of acute renal failure in a rat warm renal ischemia model. A series of renal artery cross-clamp times was used to determine the threshold for irreversible damage (thirty minutes). After thirty minutes of warm renal ischemia, 2.5 cc of 6 % Fm or FLm solution, 5% human serum albumin, or 9% normal saline was administered. The effect of the solutions was evaluated by four criteria: (1) forty-eight hours' serum BUN/creatinine, (2) forty-eight hours' urine output, (3) percent of water content in the kidney, and (4) a histopathologic grading. There were no differences among the animals in any of the four groups in renal function at forty-eight hours, percent of water content of the kidneys, urine output, and extent of medullary and cortical injury. The authors attribute the lack of protective effect by the HES macromolecules to intrinsic properties of the kidney such as the extensive endothelial cell surface area of the well-vascularized kidney and the hypersensitivity of the kidney to hypoxic injury.
- Published
- 1991
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37. Identification of novel epigenetic markers for clear cell renal cell carcinoma
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Michele Drever, Charles DeLisi, Gul S. Dalgin, Tara Williams, Thomas C. King, and Louis S. Liou
- Subjects
Pathology ,medicine.medical_specialty ,Urology ,Cell ,Blotting, Western ,Down-Regulation ,Biology ,Epigenesis, Genetic ,Synaptotagmins ,medicine ,Biomarkers, Tumor ,Humans ,Epigenetics ,Epithelial Sodium Channels ,Eye Proteins ,Gene ,Carcinoma, Renal Cell ,Reverse Transcriptase Polymerase Chain Reaction ,Membrane Proteins ,DNA Methylation ,medicine.disease ,Kidney Neoplasms ,Clear cell renal cell carcinoma ,medicine.anatomical_structure ,CpG site ,Transcription Factor AP-2 ,Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization ,Clear cell carcinoma ,DNA methylation ,Cancer research ,Intercellular Signaling Peptides and Proteins ,CpG Islands ,Metallothionein ,Clear cell ,Transcription Factors - Abstract
We identified significantly hypermethylated genes in clear cell renal cell carcinoma.We previously identified a set of under expressed genes in renal cell carcinoma tissue through transcriptional profiling and a robust computational screen. We selected 19 of these genes for hypermethylation analysis using a rigorous search for the best candidate regions, considering CpG islands and transcription factor binding sites. The genes were analyzed for hypermethylation in the DNA of 38 matched clear cell renal cell carcinoma and normal samples using matrix assisted laser desorption ionization time-of-flight mass spectrometry. The significance of hypermethylation was assessed using 3 statistical tests. We validated the down-regulation of significantly hypermethylated genes at the RNA and protein levels in a separate set of patients using reverse transcriptase-polymerase chain reaction, immunohistochemistry and Western blots.We found 7 significantly hypermethylated regions from 6 down-regulated genes, including SFRP1, which was previously shown to be hypermethylated in renal cell carcinoma and other cancer types.To our knowledge we report for the first time that another 5 genes (SCNN1B, SYT6, DACH1, and the tumor suppressors TFAP2A and MT1G) are hypermethylated in renal cell carcinoma. Robust computational screens and the high throughput methylation assay resulted in an enriched set of novel genes that are epigenetically altered in clear cell renal cell carcinoma. Overall the detection of hypermethylation in these highly down-regulated genes suggests that assaying for their methylation using cells from urine or blood could provide the basis for a viable diagnostic test.
- Published
- 2007
38. Gastrointestinal Pathology
- Author
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Thomas C. King
- Subjects
Pathology ,medicine.medical_specialty ,business.industry ,medicine ,Gastrointestinal pathology ,business - Published
- 2007
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39. Endocrine Pathology
- Author
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Thomas C. King
- Subjects
Pathology ,medicine.medical_specialty ,business.industry ,Endocrine pathology ,medicine ,business - Published
- 2007
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40. Tissue Homeostasis, Damage, and Repair
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Thomas C. King
- Subjects
business.industry ,Medicine ,business ,Tissue homeostasis ,Cell biology - Published
- 2007
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41. Hematopoietic Pathology
- Author
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Thomas C. King
- Subjects
Pathology ,medicine.medical_specialty ,Haematopoiesis ,business.industry ,Medicine ,business - Published
- 2007
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42. Male and Female Genital Tracts and Breast Pathology
- Author
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Thomas C. King
- Subjects
Female circumcision ,business.industry ,Medicine ,Physiology ,Breast pathology ,business - Published
- 2007
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43. Nervous System
- Author
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Thomas C. King
- Subjects
Nervous system ,medicine.anatomical_structure ,business.industry ,Medicine ,business ,Neuroscience - Published
- 2007
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44. Preface
- Author
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Thomas C. King
- Published
- 2007
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45. Renal and Urinary Tract
- Author
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Thomas C. King
- Subjects
medicine.medical_specialty ,business.industry ,Urinary system ,Urology ,medicine ,business - Published
- 2007
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- View/download PDF
46. Respiratory Tract and Pleura
- Author
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Thomas C. King
- Subjects
Pathology ,medicine.medical_specialty ,medicine.anatomical_structure ,business.industry ,medicine ,business ,Respiratory tract - Published
- 2007
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47. Cardiovascular Pathology
- Author
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Thomas C. King
- Subjects
medicine.medical_specialty ,Cardiovascular pathology ,business.industry ,Internal medicine ,medicine ,Cardiology ,business - Published
- 2007
- Full Text
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48. Blockchain for Electronic Vaccine Certificates: More Cons Than Pros?
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Raphaëlle Toubiana, Millie Macdonald, Sivananda Rajananda, Tale Lokvenec, Thomas C. Kingsley, and Santiago Romero-Brufau
- Subjects
blockchain (BC) ,electronic vaccination record ,electronic vaccine certificate ,cryptography ,COVID-19 ,clinical informatics ,Information technology ,T58.5-58.64 - Abstract
Electronic vaccine certificates (EVC) for COVID-19 vaccination are likely to become widespread. Blockchain (BC) is an electronic immutable distributed ledger and is one of the more common proposed EVC platform options. However, the principles of blockchain are not widely understood by public health and medical professionals. We attempt to describe, in an accessible style, how BC works and the potential benefits and drawbacks in its use for EVCs. Our assessment is BC technology is not well suited to be used for EVCs. Overall, blockchain technology is based on two key principles: the use of cryptography, and a distributed immutable ledger in the format of blockchains. While the use of cryptography can provide ease of sharing vaccination records while maintaining privacy, EVCs require some amount of contribution from a centralized authority to confirm vaccine status; this is partly because these authorities are responsible for the distribution and often the administration of the vaccine. Having the data distributed makes the role of a centralized authority less effective. We concluded there are alternative ways to use cryptography outside of a BC that allow a centralized authority to better participate, which seems necessary for an EVC platform to be of practical use.
- Published
- 2022
- Full Text
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49. The human B cell response to IL-13 is dependent on cellular phenotype as well as mode of activation
- Author
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Dwayne Ford, Catherine Sheehan, Christopher Girasole, Rory Priester, Nicola Kouttab, John Tigges, Thomas C. King, Andrea Luciani, John W. Morgan, and Abby L. Maizel
- Subjects
Interleukin-13 ,Membrane Glycoproteins ,Immunology ,CD40 Ligand ,Palatine Tonsil ,Receptors, Interleukin-13 ,B-Lymphocyte Subsets ,Receptors, Interleukin-2 ,Receptors, Interleukin ,Ligands ,Lymphocyte Activation ,Interleukin-13 Receptor alpha1 Subunit ,Immunophenotyping ,Receptors, Interleukin-4 ,Immunology and Allergy ,Cytokines ,Humans ,RNA, Messenger ,CD40 Antigens ,Immunologic Memory ,Interphase ,Cell Division ,Cells, Cultured - Abstract
Normal mature quiescent human B lymphocytes, isolated as a function of buoyant density, require activation for up-regulation of IL-13R constituents. Cell activation through a combination of surface Ig and CD40 receptor ligation leads to the most substantial message production for IL-13Rα1. Functional consequences of this receptor variation, in initially quiescent cells, includes demonstrable effects on cellular proliferation in response to ligand exposure. Variations in the method of surface activation, with particular emphasis on the CD40 receptor, reveals that immobilized CD40 ligand may be sufficient, in and of itself, to up-regulate IL-13Rα1, which may bear significance for B-lymphocyte bystander proliferation. Regulation of the IL-13Rα1 protein and message also differs as a function of cellular phenotype. Although values are greater in memory than naive B cells, as they are initially isolated from extirpated tonsils, variations in the magnitude of message and protein, as a function of surface stimulation, are more substantial in the naive subset. The magnitude of variation in message production in naive cells is associated with a more vigorous proliferative response to IL-13 than seen in memory lymphocytes. The cellular response to IL-13, as a function of activation and phenotype, is the converse of that demonstrated for IL-2. Evaluation of proliferation, receptor message, ligand binding protein production, and the response to putatively synergistic cytokines reveals that IL-2 is the predominant lymphokine utilized by memory cells. This is in contradistinction to IL-13, which along with IL-4, are the predominant moieties for naive lymphocytes.
- Published
- 1999
50. Rapid Simultaneous Amplification and Detection of the MBR/JH Chromosomal Translocation by Fluorescence Melting Curve Analysis
- Author
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Carl T. Wittwer, Sandra D. Bohling, Kojo S.J. Elenitoba-Johnson, and Thomas C. King
- Subjects
Electrophoresis ,Technical Advances ,Biology ,Diamines ,Melting curve analysis ,Fluorescence spectroscopy ,Translocation, Genetic ,Pathology and Forensic Medicine ,chemistry.chemical_compound ,Fluorometer ,Multiplex polymerase chain reaction ,Humans ,Benzothiazoles ,Organic Chemicals ,Molecular Biology ,Fluorescent Dyes ,Gel electrophoresis ,Gene Rearrangement ,Thermal cycler ,Receptors, Antigen, T-Cell, gamma-delta ,Molecular biology ,Hematologic Diseases ,Genes, bcl-2 ,chemistry ,Agarose gel electrophoresis ,SYBR Green I ,Quinolines ,Immunoglobulin Heavy Chains - Abstract
Polymerase chain reaction (PCR) amplification and product analysis for the detection of chromosomal translocations, such as the t(14;18), has traditionally been a two-step process. PCR product detection has generally entailed gel electrophoresis and/or hybridization or sequencing for confirmation of assay specificity. Using a microvolume fluorimeter integrated with a thermal cycler and a PCR-compatible double-stranded DNA (dsDNA) binding fluorescent dye (SYBR Green I), we investigated the feasibility of simultaneous thermal amplification and detection of MBR/JH translocation products by fluorescence melting curve analysis. We analyzed DNA from 30 cases of lymphoproliferative disorders comprising 19 cases of previously documented MBR/JH-positive follicle center lymphoma and 11 reactive lymphadenopathies. The samples were coded and analyzed blindly for the presence of MBR/JH translocations by fluorescence melting curve analysis. We also performed dilutional assays using the MBR/JH-positive cell line SUDHL-6. Multiplex PCR for MBR/JH and β-globin was used to simultaneously assess sample adequacy. All (100%) of the 19 cases previously determined to be MBR/JH positive by conventional PCR analysis showed a characteristic sharp decrease in fluorescence at ∼90°C by melting curve analysis after amplification. Fluorescence melting peaks obtained by plotting the negative derivative of fluorescence over temperature (− d F/ d T) versus temperature ( T ) showed melting temperatures ( T m ) at 88.85 ± 1.15°C. In addition, multiplex assays using both MBR/JH and β-globin primers yielded easily distinguishable fluorescence melting peaks at ∼90°C and 81.2°C, respectively. Dilutional assays revealed that fluorescence melting curve analysis was more sensitive than conventional PCR and agarose gel electrophoresis with ultraviolet transillumination by as much as 100-fold. Simultaneous amplification and fluorescence melting curve analysis is a simple, reliable, and sensitive method for the detection of MBR/JH translocations. The feasibility of specific PCR product detection without electrophoresis or utilization of expensive fluorescently labeled probes makes this method attractive for routine molecular diagnostics.
- Published
- 1999
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