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4. Phase I/II study of the clinical activity and safety of GSK3326595 in patients with myeloid neoplasms

Author

Justin Watts, Mark D. Minden, Kimo Bachiashvili, Andrew M. Brunner, Sameem Abedin, Timothy Crossman, Magdalena Zajac, Veronica Moroz, Jacqueline L. Egger, Aarti Tarkar, Brandon E. Kremer, Olena Barbash, and Gautam Borthakur

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

Background: GSK3326595 is a potent, selective, reversible protein arginine methyltransferase 5 (PRMT5) inhibitor under investigation for treatment of myelodysplastic syndrome (MDS), chronic myelomonocytic leukemia (CMML), and acute myeloid leukemia (AML). In preclinical models of AML, PRMT5 inhibition decreased proliferation and increased cell death, supporting additional clinical research in myeloid neoplasms. Objectives: To determine the clinical activity, safety, tolerability, dosing, additional measures of clinical activity, pharmacokinetics, and pharmacodynamics of GSK3326595. Design: In part 1 of this open-label, multicenter, multipart, phase I/II study, adults with relapsed/refractory myeloid neoplasms (e.g., MDS, CMML, and AML) received monotherapy with 400 or 300 mg oral GSK3326595 once daily. Study termination occurred prior to part 2 enrollment. Methods: Clinical activity was determined by the clinical benefit rate (CBR; proportion of patients achieving complete remission (CR), complete marrow remission (mCR), partial remission, stable disease (SD) >8 weeks, or hematologic improvement). Adverse events (AEs) were assessed by incidence and severity. Exploratory examination of spliceosome mutations was performed to determine the relationship between genomic profiles and clinical response to GSK3326595. Results: Thirty patients with a median age of 73.5 years (range, 47–90) were enrolled; 13 (43%) and 17 (57%) received 400 and 300 mg of GSK3326595, respectively. Five (17%) patients met CBR criteria: 4 (13%) with SD >8 weeks and 1 (3%) achieving mCR. Of five patients with clinical benefit: three had SRSF2 mutation, one U2AF1, and one was splicing factor wild-type. Frequent GSK3326595-related AEs were decreased platelet count (27%), dysgeusia (23%), fatigue (20%), and nausea (20%). GSK3326595 had rapid absorption, with a T max of approximately 2 h and a terminal half-life of 4–6 h. Conclusion: GSK3326595 monotherapy had limited clinical activity in heavily pretreated patients despite robust target engagement. The safety profile was broadly consistent with other published PRMT5 inhibitor studies. Trial registration: ClinicalTrials.gov: NCT03614728.

Published
2024
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5. Analytical evaluation and critical appraisal of early commercial SARS-CoV-2 immunoassays for routine use in a diagnostic laboratory

Author

Magdalena Dziadzio, Nigel Goodman, Timothy Cross, Vanya Gant, and Amanda Cramer

Subjects
Male, Clinical Biochemistry, Antibodies, Viral, Serology, 0302 clinical medicine, Medicine, Immunology and Allergy, Diagnostic laboratory, skin and connective tissue diseases, Aged, 80 and over, 0303 health sciences, evaluation, biology, medicine.diagnostic_test, Middle Aged, Infectious Diseases, 030220 oncology & carcinogenesis, Female, Original Article, ELISA, medicine.symptom, Antibody, Research Article, Adult, Microbiology (medical), medicine.medical_specialty, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Enzyme-Linked Immunosorbent Assay, Asymptomatic, Sensitivity and Specificity, Microbiology, 03 medical and health sciences, Young Adult, Humans, immunoassay, Symptom onset, Intensive care medicine, Igg elisa, Selection (genetic algorithm), Aged, Biochemistry, medical, 030306 microbiology, SARS-CoV-2, business.industry, fungi, Biochemistry (medical), COVID-19, Virology, First generation, body regions, Critical appraisal, Immunoassay, biology.protein, analytical, business
Abstract

BACKGROUNDThe objective of this study was to evaluate the performance characteristics of early commercial SARS-CoV-2 antibody assays in mild and asymptomatic subjects to enable the selection of suitable serological assays for routine diagnostic use within HCA Healthcare UK.METHODSWe used serum samples from a pre-Covid era patient cohort (n=50, pre-December 2019), designated SARS-CoV-2 negative, and serum samples from a SARS-CoV-2 RT-PCR-positive cohort (n=90) taken > 14 days post symptom onset (April-May 2020). We evaluated 6 ELISA assays including one confirmation assay to investigate antibody specificity. We also evaluated one point-of-care lateral flow device and one high throughput electrochemiluminescence immunoassay.RESULTSThe ELISA specificities ranged from 84-100%, with sensitivities ranging from 75.3-90.0%. The LFIA showed 100% specificity and 80% sensitivity using smaller sample numbers. The Roche CLIA immunoassay showed 100% specificity and 90.7% sensitivity. When used in conjunction, the Euroimmun nucleocapsid (NC) and spike-1 (S1) IgG ELISA assays had a sensitivity of 95.6%. The confirmation IgG assay showed 92.6% of samples tested contained both NC and S1 antibodies, 32.7% had NC, S1 and S2 and 0% had either S1 or S2 only.CONCLUSIONSThese first generation assays were not calibrated against reference material and the results are reported qualitatively. The Roche assay and the Euroimmun NC and S1 assays had the best sensitivity overall in our hands. Combining the assays detecting NC and S1/S2 antibody increased diagnostic yield. A portfolio of next generation SARS-CoV-2 immunoassays will be necessary in any future studies of herd and vaccine induced immunity.

Published
2021
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8. External Validation of the Surgical Outcome Risk Tool (Sort) In 3305 Abdominal Surgery Patients In The Independent Sector In The United Kingdom

Author

Kathryn Oakland, Daria Cosentino, Timothy Cross, Cliff Bucknall, Sina Dorudi, and David Walker

Abstract

Background Assessing risk of post-surgical mortality is a key component of pre-surgical planning. The Surgical Outcome Risk Tool (SORT) uses pre-operative variables to predict 30-day mortality. The aim of this study was to externally validate SORT in patients undergoing major abdominal surgery. Methods Data were collected from patients treated in five Independent hospitals in the United Kingdom. Individualised SORT scores were calculated and area under the receiver operating characteristic (AUROC) and precision-recall curves (PRC) plus 95% confidence intervals (CI) were drawn to test the ability of SORT to identify in-hospital death. Outcomes of patients with a SORT predicted risk of mortality of ≥5% (high risk) were compared to those with a predicted risk of Results The study population comprised 3305 patients, mean age 51 years, 2783 (84.2%) underwent elective surgery most frequently involving the colon (24.6%), or liver, pancreas or gallbladder (18.2%). Overall 1551 (46.9%) patients were admitted to ICU and 29 (0.88%) died. The AUROC of SORT for discriminating patients at risk of death in hospital was 0.899 (95% CI 0.849 to 0.949) and the PRC 0.247. In total 72 (2.18%) patients were stratified as high risk. There were more unplanned ICU admissions and deaths in this group compared to the standard risk group (25.0% and 3.3%, versus 3.1% and 0.5%, respectively). Conclusion We externally validated SORT in a large population of abdominal surgery patients. SORT performed well in patients with lower risk profiles, but underpredicted adverse outcomes in the higher risk group.

Published
2020
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9. External validation of the Surgical Outcome Risk Tool (SORT) in 3305 abdominal surgery patients in the independent sector in the UK

Author

Timothy Cross, David Walker, Kathryn Oakland, Cliff Bucknall, Daria Cosentino, and Sina Dorudi

Subjects
medicine.medical_specialty, Receiver operating characteristic, Pre-assessment, business.industry, Research, lcsh:Surgery, lcsh:RD1-811, Outcomes, Lower risk, Confidence interval, 03 medical and health sciences, 0302 clinical medicine, 030202 anesthesiology, Internal medicine, Risk of mortality, Population study, Medicine, Surgery, 030212 general & internal medicine, Elective surgery, business, Risk assessment, Abdominal surgery
Abstract

Background Assessing the risk of post-surgical mortality is a key component of pre-surgical planning. The Surgical Outcome Risk Tool (SORT) uses pre-operative variables to predict 30-day mortality. The aim of this study was to externally validate SORT in patients undergoing major abdominal surgery. Methods Data were collected from patients treated in five independent hospitals in the UK. Individualised SORT scores were calculated, and area under the receiver operating characteristic (AUROC) and precision-recall curves (PRC) plus 95% confidence intervals (CI) were drawn to test the ability of SORT to identify in-hospital death. Outcomes of patients with a SORT predicted risk of mortality of ≥ 5% (high risk) were compared to those with a predicted risk of < 5% (standard risk). Results The study population comprised 3305 patients, mean age 51 years, 2783 (84.2%) underwent elective surgery most frequently involving the colon (24.6%), or liver, pancreas or gallbladder (18.2%). Overall, 1551 (46.9%) patients were admitted to ICU and 29 (0.88%) died. The AUROC of SORT for discriminating patients at risk of death in hospital was 0.899 (95% CI 0.849 to 0.949) and the PRC 0.247. In total, 72 (2.18%) patients were stratified as high risk. There were more unplanned ICU admissions and deaths in this group compared to the standard risk group (25.0% and 3.3%, versus 3.1% and 0.5%, respectively). Conclusion We externally validated SORT in a large population of abdominal surgery patients. SORT performed well in patients with lower risk profiles, but underpredicted adverse outcomes in the higher risk group.

Published
2020

10. CyberKnife Radiosurgery of Skull-base Tumors: A UK Center Experience

Author

Amen Sibtain, Hannah C P Wilson, Patricia M Price, Christy Goldsmith, Andrew Edwards, Rhiannon Davies, Keyoumars Ashkan, Ronald Beaney, Timothy Cross, Nick P Plowman, and Melanie M Green

Subjects
tumors, STEREOTACTIC RADIOSURGERY, medicine.medical_specialty, intracranial, fractionated radiotherapy, medicine.medical_treatment, treatment outcomes, Schwannoma, Radiosurgery, Meningioma, 03 medical and health sciences, Medicine, General & Internal, 0302 clinical medicine, LONG-TERM OUTCOMES, Cyberknife, General & Internal Medicine, cyberknife, Medicine, Pathological, Science & Technology, business.industry, General Engineering, skull base, radiosurgery, medicine.disease, Acute toxicity, stereotactic, Oncology, 030220 oncology & carcinogenesis, Toxicity, MENINGIOMAS, Radiation Oncology, Radiology, CyberKnife Radiosurgery, GAMMA-KNIFE RADIOSURGERY, business, Life Sciences & Biomedicine, 030217 neurology & neurosurgery
Abstract

The study aim was to evaluate patient individualized Cyberknife® treatment for heterogeneous skull-base tumors. Patients treated between 2009 and 2013 at The Harley Street Clinic were studied. In total, 66 patients received 15–30 Gy in 1–5 fractions to a median planning target volume (PTV) of 6.4 cc, including patients with secondary, multiple, residual and recurrent tumors, and those with tumors of uncertain pathological type. Outcome analysis was pragmatically restricted to 35 patients who had single, primary tumors treated with curative intent, and sufficient diagnostic and outcome information. Sixteen vestibular schwannoma patients with median PTV 3.8 cc (range 0.81–19.6) received 18–25 Gy in 3–5 fractions: 81% showed no acute toxicity, 50% reported no late toxicity, 71% of symptoms were stable/improved and local control was 100% at 11.4 months median follow-up. Twelve meningioma patients with median PTV of 5.5 cc (range 0.68–22.3) received 17–30 Gy in 1–5 fractions: 83% experienced no acute toxicity, 33% reported no late toxicity, 88% of symptoms were stable/improved and local control was 100% at 22.1 months median follow-up. Seven patients with other tumor types with median PTV of 24.3 cc (range 7.6–100.5) received 15–28.5 Gy in 1–5 fractions: 57% experienced no acute toxicity, 57% reported no late toxicities, 66% of symptoms were stable and local control was 43% at 14.9 months median follow-up. When tumor types were considered together, smaller tumors (PTV < 6.4 cc) showed reduced acute toxicity (p = 0.01). Overall, smaller benign tumors showed low acute toxicity, excellent local control, and good symptom management: a focus on enhanced neurological preservation may refine outcomes. For other tumor types outcome was encouraging: a focus on optimal dose and fractionation scheduling may reduce toxicity and improve local control. Individual patient experiences are detailed where valuable lessons were gained for optimizing local control and minimizing toxicity.

Published
2018

11. Dose-Volume Histogram Analysis of Stereotactic Body Radiotherapy Treatment of Pancreatic Cancer: A Focus on Duodenal Dose Constraints

Author

Timothy Cross, Sheila Loughlin, Ian Cowley, Christy Goldsmith, Nicholas P Plowman, and Patricia M Price

Subjects
Cancer Research, Dose-volume histogram, Duodenum, medicine.medical_treatment, Radiosurgery, Radiation Tolerance, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, Pancreatic cancer, Medicine, Humans, Radiology, Nuclear Medicine and imaging, business.industry, Stomach, Dose fractionation, Common Terminology Criteria for Adverse Events, Dose-Response Relationship, Radiation, Radiotherapy Dosage, medicine.disease, Primary tumor, Pancreatic Neoplasms, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Dose Fractionation, Radiation, business, Nuclear medicine
Abstract

Pancreatic carcinoma is an aggressive disease and radiotherapy treatment delivery to the primary tumor is constrained by the anatomical close location of the duodenum, stomach, and small bowel. Duodenal dose tolerance for radiosurgery in 2-5 fractions has been largely unknown. The literature was surveyed for quantitative models of risk in 1-5 fractions and we analyzed our own patient population of 44 patients with unresectable pancreatic tumors who received 3 or 5 fractions of stereotactic body radiotherapy (SBRT) between March 2009 and March 2013. A logistic model was constructed in the dose-volume histogram (DVH) Evaluator software for the duodenal D50%, D30cc, D5cc, D1cc, and maximum point dose D0.035cc. Dose tolerance limits from the literature were overlaid onto the clinical duodenal data in the form of a DVH Risk Map, with risk levels of the published limits estimated from the model of clinical data. In 3 fractions, Kopek 2010 found a statistically significant difference in D1cc of patients with no common terminology criteria for adverse events (CTCAE) v3 grade 2 or higher duodenal complications (mean D1cc = 25.3Gy) as compared with patients with grade 2 or higher toxicity (mean D1cc = 37.4Gy). From the logistic model of our duodenal data in 3 fractions, D1cc = 25.3Gy had 4.7% risk of grade 3-4 hemorrhage or stricture and D1cc = 37.4Gy had 20% risk. The 10% risk level was D1cc = 31.4Gy and we were able to keep duodenum dose for all our patients later this level.

Published
2016

12. The Case in Australia for Further Reform to the Cross-Examination and Court Management of Child Witnesses

Author

David Caruso and Timothy Cross

Subjects
Cross-examination, Sociology and Political Science, Political science, Law, Legislature, Remand (court procedure), Management, Monitoring, Policy and Law, Witness
Abstract

Recent legislative reforms in Australia designed to address the difficulties attending the reception and treatment of child evidence will have little, if any, success because they do not address the reasons for the difficulties, nor introduce improvements to existing practice for the child witness, counsel or court.

Published
2012
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14. Serine/Threonine Protein Kinases and Apoptosis

Author

Nick V. Henriquez, Timothy Cross, Dagmar Scheel-Toellner, Janet M. Lord, Mike Salmon, and Elizabeth M. Deacon

Subjects
Serine/threonine-specific protein kinase, biology, p38 mitogen-activated protein kinases, JNK Mitogen-Activated Protein Kinases, Apoptosis, Cell Biology, Serine threonine protein kinase, Protein Serine-Threonine Kinases, Cyclic AMP-Dependent Protein Kinases, Models, Biological, AKT3, MAP2K7, Cell biology, Biochemistry, Proto-Oncogene Proteins, Mitogen-activated protein kinase, biology.protein, Animals, Humans, ASK1, c-Raf, Mitogen-Activated Protein Kinases, Proto-Oncogene Proteins c-akt, Protein Kinase C, Signal Transduction
Abstract

Over the past decade, our understanding of apoptosis, or programmed cell death, has increased greatly, with the identification of some of the major components of the apoptotic programme and the processes regulating their activation. Although apoptosis is an intrinsic process present in all cells, it can be regulated by extrinsic factors, including hormones, growth factors, cell surface receptors, and cellular stress. The actions of both pro- and antiapoptotic factors are often affected by modulation of the phosphorylation status of key elements of the apoptotic process. This minireview will focus on the role of protein kinases in apoptosis. Apoptosis is a multistep process and protein kinases have been implicated both in the upstream induction phase of apoptosis and in the downstream execution stage, as the direct targets for caspases. Due to the space constraints of this review it is not possible to discuss all of the kinases involved in the apoptotic process and we have focused here on the role of the serine/threonine protein kinases. The kinases of this family that have been suggested to play a role in apoptosis are the mitogen-activated protein kinase (MAPK) family, specifically p42/44 ERK, p38 MAPK and c-Jun N-terminal kinase (JNK), cyclic AMP-dependent protein kinase (PKA), protein kinase B (PKB), or Akt and protein kinase C (PKC). We have also considered briefly the potential for the regulation of these kinases by tyrosine protein kinases, such as c-abl.

Published
2000
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15. Contributors

Author

Sheila Adam, Neill Adhikari, William C. Aird, Amalia Alcón, Peter Andrews, Massimo Antonelli, Soja Anubkumar, Andrea Arcangeli, Vicente Arroyo, Andrew J. Baker, Robert P. Baughman, Judith Bellapart, Rinaldo Bellomo, Mette M. Berger, Maria Grazia Bocci, Malte Book, Josep M. Bordas, Luca Brazzi, Timothy G. Buchman, Christian Byhahn, B. Cabello, Pietro Caironi, Anselmo Caricato, Andre F. Charest, René L. Chioléro, Davide Chiumello, Chung-Wai Chow, Vanessa Cobb, Stephen M. Cohn, Timothy Cross, Marc de Moya, Yves Debaveye, Paul Dorian, Gregory P. Downey, Philippe Eggimann, Björn Ellger, E. Wesley Ely, Àngels Escorsell, Neus Fábregas, Vito Fanelli, Faust Feu, Bernard G. Fikkers, Joseph A. Fisher, Marco Fontanella, Ognjen Gajic, Luciano Gattinoni, Gordon Giesbrecht, Pere Ginès, Salvatore Grasso, Thorsteinn Gunnarsson, Richard Haddon, Mitchell L. Halperin, C. William Hargett, Michael Hiesmayr, Ken Hillman, Frank Hubbell, Rolf D. Hubmayr, Leonard D. Hudson, Richard L. Hughes, Robert M. Kacmarek, Kamel S. Kamel, Catherine L. Kelleher, Sungmin Kiem, Sven Klaschik, Anil Kumar, Donald W. Landry, Stephen E. Lapinsky, Lutz Eric Lehmann, Mitchell M. Levy, Patricia C.Y. Liaw, Shih-Hua Lin, Stuart L. Linas, José A. Lorente, John M. Luce, Thomas Luecke, Edward H. Maa, Sheldon Magder, Atul Malhotra, Jordi Mancebo, Iqwal Mangat, John C. Marshall, Antoni Mas, Luciana Mascia, Eric M. Massicotte, Greg McAnulty, Maureen Meade, Thomas John Morgan, Matthew T. Naughton, Santiago Nogué-Xarau, James O'Beirne, Juan A. Oliver, Ilkka Parviainen, Paolo Pelosi, Michael R. Pinsky, Margaret A. Pisani, Didier Pittet, Christian Putensen, Graham Ramsay, Andrew Rhodes, Claudio Ronco, Charis Roussos, Gordon D. Rubenfeld, Lewis Rubinson, Joshua Rucker, Miguel Sánchez, Eduardo Sanjurjo-Golpe, Hugo Sax, Jerome J. Schentag, Jens-Christian Schewe, Daniel Schmidlin, Paul T. Schumacker, Dror Soffer, Ludivine Soguel, Ulrike Stamer, R. Scott Stephens, Frank Stüber, Peter M. Suter, Jukka Takala, Victor F. Tapson, Charles H. Tator, Carlos Terra, Aldo Torre, Antoni Torres, David V. Tuxen, Ilker Uçkay, Franco Valenza, Greet Van den Berghe, Theodoros Vassilakopoulos, Jesús Villar, Christopher Wallace, Stefan Weber, Jeffrey I. Weitz, Julia Wendon, Charles M. Wiener, Stephan Windecker, Hermann Wrigge, and Richard G. Wunderink

Published
2006
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16. Generation of diacylglycerol molecular species through the cell cycle: a role for 1-stearoyl, 2-arachidonyl glycerol in the activation of nuclear protein kinase C-betaII at G2/M

Author

Hema Chahal, Timothy Cross, Paul Webb, Trevor R. Pettitt, Janet M. Lord, Elizabeth M. Deacon, and Michael J.O. Wakelam

Subjects
G2 Phase, Active Transport, Cell Nucleus, Phosphatidic Acids, Biology, Diglycerides, chemistry.chemical_compound, Protein Kinase C beta, Humans, Nuclear protein, Mitosis, Protein kinase C, Protein Kinase C, Diacylglycerol kinase, Cell Nucleus, Cell growth, Cell Biology, Phosphatidic acid, U937 Cells, Cell cycle, Cell biology, Isoenzymes, Eukaryotic Cells, Biochemistry, chemistry, Lamin, Signal Transduction
Abstract

Protein kinase C (PKC) is a family of 11 isoenzymes that are differentially involved in the regulation of cell proliferation. PKC-betaII, a mitotic lamin kinase, has been shown previously to translocate to the nucleus at G(2)/M and this was coupled to the generation of nuclear diacylglycerol. However, it is not clear how isoenzyme selective translocation and nuclear targeting is achieved during cell cycle. To investigate further the role of nuclear diacylglycerol we measured PKC isoenzyme translocation and analysed diacylglycerol species at different stages of the cell cycle in U937 cells synchronized by centrifugal elutriation. Translocation of PKC-betaII to the membrane fraction, an indicator of activation, occurred at S and G(2)/M, although PKC-betaII was targeted to the nucleus only at G(2)/M. Levels of nuclear diacylglycerol, specifically tetraunsaturated species, increased during G(2)/M. By contrast, there were no obvious changes in nuclear phosphatidic acid species or mass. 1-stearoyl, 2-arachidonyl glycerol (SAG), the major polyunsaturated nuclear diacylglycerol, was able to activate classical PKC isoenzymes (PKC-alpha and beta), but was less effective for activation of novel isoenzymes (PKC-delta), in an in vitro PKC assay. We propose that PKC-betaII nuclear translocation during G(2)/M phase transition is mediated in part by generation of SAG at the nucleus.

Published
2002

17. Generation of diacylglycerol molecular species through the cell cycle: a role for 1-stearoyl, 2-arachidonyl glycerol in the activation of nuclear protein kinase C-betaII at G2/M.

Author

M, Deacon Elizabeth, R, Pettitt Trevor, Paul, Webb, Timothy, Cross, Hema, Chahal, O, Wakelam Michael J, and M, Lord Janet

Abstract

Protein kinase C (PKC) is a family of 11 isoenzymes that are differentially involved in the regulation of cell proliferation. PKC-betaII, a mitotic lamin kinase, has been shown previously to translocate to the nucleus at G(2)/M and this was coupled to the generation of nuclear diacylglycerol. However, it is not clear how isoenzyme selective translocation and nuclear targeting is achieved during cell cycle. To investigate further the role of nuclear diacylglycerol we measured PKC isoenzyme translocation and analysed diacylglycerol species at different stages of the cell cycle in U937 cells synchronized by centrifugal elutriation. Translocation of PKC-betaII to the membrane fraction, an indicator of activation, occurred at S and G(2)/M, although PKC-betaII was targeted to the nucleus only at G(2)/M. Levels of nuclear diacylglycerol, specifically tetraunsaturated species, increased during G(2)/M. By contrast, there were no obvious changes in nuclear phosphatidic acid species or mass. 1-stearoyl, 2-arachidonyl glycerol (SAG), the major polyunsaturated nuclear diacylglycerol, was able to activate classical PKC isoenzymes (PKC-alpha and beta), but was less effective for activation of novel isoenzymes (PKC-delta), in an in vitro PKC assay. We propose that PKC-betaII nuclear translocation during G(2)/M phase transition is mediated in part by generation of SAG at the nucleus.

Published
2002

18. PKC-δ is an apoptotic lamin kinase

Author

Dianne Watters, Elizabeth M. Deacon, Rosemary Sallis, Timothy Cross, Michael Gough, Janet M. Lord, and Gareth Griffiths

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, animal structures, integumentary system, Kinase, Hyperphosphorylation, Caspase 3, Caspase 6, Biology, Molecular biology, Cell biology, embryonic structures, Genetics, Nuclear lamina, Protein kinase A, Molecular Biology, Lamin, Protein kinase C
Abstract

Protein kinase C-δ is activated during apoptosis, following proteolytic cleavage by caspase 3. Furthermore, overexpression of the catalytic kinase fragment of PKC-δ induces the nuclear phenotype associated with apoptosis, though the molecular basis of this effect has not been determined. In these studies we have examined the role of PKC-δ in the disassembly of the nuclear lamina at apoptosis. The nuclear lamina is disassembled during mitosis and apoptosis and mitotic disassembly involves hyperphosphorylation of lamin proteins by mitotic lamin kinases. During apoptosis, lamin proteins are degraded by caspase 6 and the contribution made by phosphorylation has not been proven. We show here that protein kinase C-δ co-localized with lamin B during apoptosis and activation of PKC-δ by caspase 3 was concomitant with lamin B phosphorylation and proteolysis. Inhibition of PKC-δ delayed lamin proteolysis, even in the presence of active caspase 6, whilst inhibitors of mitotic lamin kinases were without effect. In addition recombinant human PKC-δ was able to phosphorylate lamin B in vitro suggesting that its actions are direct and not via an intermediary kinase. We propose that PKC-δ is an apoptotic lamin kinase and that efficient lamina disassembly at apoptosis requires both lamin hyperphosphorylation and caspase mediated proteolysis.

19. Physician Practice Patterns Within an Acute Care Facility (Cost Reduction, Quality Monitoring, Hospital/Medical Staff).

Author

McKee, Timothy Cross

Abstract

Under a prospective case-based payment system (PPS), the financial viability of an institution depends on the ability to produce its overall case load at total costs which are less than total payments. Cost reduction is possible in a case-based PPS environment by improving clinical productivity through altering the volume and or changing the mix of input intermediate products. Variation in the volume and or type of intermediate product use resulting from physician differences is probably inappropriate. It is believed, therefore, that intermediate product use can be reduced without affecting the quality of care. The current research tests the feasibility of a cost-reduction strategy based on improving clinical productivity. Utilizing Cluster Analysis, patients within a Diagnosis-Related Group (DRG) were classified into different practice patterns which reflected differences in the volume and or type of intermediate products consumed in the treatment process. Utilizing Multivariate Nominal Analysis, variation in clinical productivities among the practice patterns were differentiated with respect to patient, physician, and outcome differences. Finally, individual physicians were associated with the different practice patterns. The research concluded that a cost-reduction strategy based on improving clinical productivity through modification of inappropriate physican practice styles is feasible to implement.

Published
1986

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