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364 results on '"Knapp, L."'

1. The relationship between the reporting of euphoria events and early treatment responses to pregabalin: an exploratory post-hoc analysis

Author

Parsons B, Freynhagen R, Schug S, Whalen E, Ortiz M, Bhadra Brown P, and Knapp L

Subjects
Euphoria, pain, pregabalin, sleep, Medicine (General), R5-920
Abstract

Bruce Parsons,1 Rainer Freynhagen,2,3 Stephan Schug,4,5 Ed Whalen,1 Marie Ortiz,1 Pritha Bhadra Brown,1 Lloyd Knapp61Pfizer Inc, New York, NY, USA; 2Department of Anesthesiology, Critical Care Medicine, Pain Therapy & Palliative Care, Pain Center Lake Starnberg, Benedictus Hospital, Tutzing, Germany; 3Department of Anesthesiology, Klinikum rechts der Isar, Technische Universität München, Munich, Germany; 4Discipline of Anaesthesiology and Pain Medicine, Medical School, University of Western Australia, Perth, WA, Australia; 5Department of Anaesthesia and Pain Medicine, Royal Perth Hospital, Perth, WA, Australia; 6Pfizer Inc, Groton, CT, USACorrespondence: Bruce ParsonsPfizer Inc, 235 East 42nd Street, New York, NY, USATel +1 212 573 1649Email bruce.parsons@pfizer.comBackground: Euphoria is a complex, multifactorial problem that is reported as an adverse event in clinical trials of analgesics including pregabalin. The relationship between the reporting of euphoria events and pregabalin early treatment responses was examined in this exploratory post-hoc analysis.Methods: Data were from patients with neuropathic or non-neuropathic chronic pain enrolled in 40 randomized clinical trials, who received pregabalin (75–600 mg/day) or placebo. Reports of treatment-emergent euphoria events were based on the Medical Dictionary of Regulatory Activities preferred term “euphoric mood”. Prevalence rates of euphoria events overall and by indication were assessed. Post-treatment endpoints included ≥30% improvements in pain and sleep scores up to 3 weeks as well as a ≥1-point improvement in daily pain score up to 11 days after treatment.Results: 13,252 patients were analyzed; 8,501 (64.1%) and 4,751 (35.9%) received pregabalin and placebo, respectively. Overall, 1.7% (n=222) of patients reported euphoria events. Among pregabalin-treated patients, a larger proportion who reported euphoria events achieved an early pain response compared with those who did not report euphoria (30% pain responders in week 1 with euphoria events [43.0%], without euphoria events [24.2%]). Results were similar for weeks 2 and 3. For Days 2–11, a larger proportion of pregabalin-treated patients with (relative to without) euphoria events were 1-point pain responders. Findings were similar in pregabalin-treated patients for sleep endpoints (30% sleep responders in week 1 with euphoria events [50.7%], without euphoria events [36.1%]). Similar results were found for weeks 2 and 3. Patients who received placebo showed similar patterns, although the overall number of them who reported euphoria events was small (n=13).Conclusion: In patients who received pregabalin for neuropathic or non-neuropathic chronic pain, those who experienced euphoria events may have better early treatment responses than those who did not report euphoria events.Keywords: euphoria, pain, pregabalin, sleep

Published
2019

3. Nitroglycerin enhances the propagation of cortical spreading depression: comparative studies with sumatriptan and novel kynurenic acid analogues

Author

Knapp L, Szita B, Kocsis K, Vécsei L, and Toldi J

Subjects
migraine, cortical spreading depression, nitroglycerin, sumatriptan, kynurenic acid analogues, Therapeutics. Pharmacology, RM1-950
Abstract

Levente Knapp,1 Bence Szita,1 Kitti Kocsis,1,2 László Vécsei,2,3 József Toldi1,2 1Department of Physiology, Anatomy, and Neuroscience, University of Szeged, 2MTA-SZTE Neuroscience Research Group, 3Department of Neurology, Faculty of Medicine, Albert Szent-Györgyi Clinical Centre, University of Szeged, Szeged, Hungary Background: The complex pathophysiology of migraine is not yet clearly understood; therefore, experimental models are essential for the investigation of the processes related to migraine headache, which include cortical spreading depression (CSD) and NO donor-induced neurovascular changes. Data on the assessment of drug efficacy in these models are often limited, which prompted us to investigate a novel combined migraine model in which an effective pharmacon could be more easily identified. Materials and methods: In vivo electrophysiological experiments were performed to investigate the effect of nitroglycerin (NTG) on CSD induced by KCl application. In addition, sumatriptan and newly synthesized neuroactive substances (analogues of the neuromodulator kynurenic acid [KYNA]) were also tested. Results: The basic parameters of CSDs were unchanged following NTG administration; however, propagation failure was decreased compared to the controls. Sumatriptan decreased the number of CSDs, whereas propagation failure was as minimal as in the NTG group. On the other hand, both of the KYNA analogues restored the ratio of propagation to the control level. Discussion: The ratio of propagation appeared to be the indicator of the effect of NTG. This is the first study providing direct evidence that NTG influences CSD; furthermore, we observed different effects of sumatriptan and KYNA analogues. Sumatriptan changed the generation of CSDs, whereas the analogues acted on the propagation of the waves. Our experimental design overlaps with a large spectrum of processes present in migraine pathophysiology, and it can be a useful experimental model for drug screening. Keywords: migraine, cortical spreading depression, nitroglycerin, sumatriptan, kynurenic acid analogues

Published
2016

6. Pregabalin for the treatment of postoperative pain: results from three controlled trials using different surgical models

Author

Singla NK, Chelly JE, Lionberger DR, Gimbel J, Sanin L, Sporn J, Yang R, Cheung R, Knapp L, and Parsons B

Subjects
Medicine (General), R5-920
Abstract

Neil K Singla,1 Jacques E Chelly,2 David R Lionberger,3 Joseph Gimbel,4 Luis Sanin,5 Jonathan Sporn,5 Ruoyong Yang,5 Raymond Cheung,5 Lloyd Knapp,6 Bruce Parsons5 1Lotus Clinical Research, Pasadena, CA, USA; 2Division of Acute Interventional Perioperative Pain, Department of Anesthesiology, University of Pittsburgh Medical Center, Pittsburgh, PA, USA; 3Department of Orthopedic Surgery, Baylor College of Medicine, Houston, TX, USA; 4Arizona Research Center, Phoenix, AZ, USA; 5Pfizer Inc., New York, NY, USA; 6Pfizer Inc., New London, CT, USA Purpose: To evaluate the efficacy and safety of pregabalin (150 or 300 mg/d) as an adjunctive therapy for the treatment of postoperative pain. Patients and methods: This study reports findings from three separate, multicenter, randomized, double-blind, placebo-controlled trials of adjunctive pregabalin for the treatment of postoperative pain. Patients underwent one of three categories of surgical procedures (one procedure per study): elective inguinal hernia repair (post-IHR); elective total knee arthroplasty (post-TKA); or total abdominal hysterectomy (posthysterectomy). The primary endpoint in each trial, mean worst pain over the past 24 hours, was assessed 24 hours post-IHR and posthysterectomy, and 48 hours post-TKA. Patients rated their pain on a scale from 0 to 10, with higher scores indicating greater pain severity. Results: In total, 425 (post-IHR), 307 (post-TKA), and 501 (posthysterectomy) patients were randomized to treatment. There were no statistically significant differences between the pregabalin and placebo groups with respect to the primary endpoint in any of the three trials. The least squares mean difference in worst pain, between 300 mg/d pregabalin and placebo, was -0.7 (95% confidence interval [CI] =-1.4, -0.1; Hochberg adjusted P=0.067) post-IHR; -0.34 (95% CI =-1.07, 0.39; P=0.362) post-TKA; and -0.2 (95% CI =-0.66, 0.31; P=0.471) posthysterectomy. Conclusion: There were no significant differences between pregabalin and placebo with respect to the primary pain intensity measure in each of the three clinical trials. These studies encompass a large dataset (1,233 patients in total), and their results should be considered when assessing pregabalin's effectiveness in postoperative pain. Further studies are required to determine the potential pain-reducing benefit of pregabalin in the postoperative setting. Keywords: arthroplasty, herniorrhaphy, hysterectomy, postoperative pain, pregabalin

Published
2014

7. Unexpected effects of peripherally administered kynurenic acid on cortical spreading depression and related blood–brain barrier permeability

Author

Oláh G, Herédi J, Menyhárt Á, Czinege Z, Nagy D, Fuzik J, Kocsis K, Knapp L, Krucsó E, Gellért L, Kis Z, Farkas T, Fülöp F, Párdutz Á, Tajti J, Vécsei L, and Toldi J

Subjects
Therapeutics. Pharmacology, RM1-950
Abstract

Gáspár Oláh,1 Judit Herédi,1 Ákos Menyhárt,1 Zsolt Czinege,2 Dávid Nagy,1 János Fuzik,1 Kitti Kocsis,1 Levente Knapp,1 Erika Krucsó,1 Levente Gellért,1 Zsolt Kis,1 Tamás Farkas,1 Ferenc Fülöp,3 Árpád Párdutz,4 János Tajti,4 László Vécsei,4 József Toldi1 1Department of Physiology, Anatomy and Neuroscience, 2Department of Software Engineering, 3Institute of Pharmaceutical Chemistry and MTA-SZTE Research Group for Stereochemistry, 4Department of Neurology and MTA-SZTE Neuroscience Research Group, University of Szeged, Szeged, Hungary Abstract: Cortical spreading depression (CSD) involves a slowly-propagating depolarization wave in the cortex, which can appear in numerous pathophysiological conditions, such as migraine with aura, stroke, and traumatic brain injury. Neurons and glial cells are also depolarized transiently during the phenomena. CSD is followed by a massive increase in glutamate release and by changes in the brain microcirculation. The aim of this study was to investigate the effects of two N-methyl-D-aspartate receptor antagonists, endogenous kynurenic acid (KYNA) and dizocilpine, on CSD and the related blood–brain barrier (BBB) permeability in rats. In intact animals, KYNA hardly crosses the BBB but has some positive features as compared with its precursor L-Kynurenine, which is frequently used in animal studies (KYNA cannot be metabolized to excitotoxic agents such as 3-hydroxy-L-kynurenine and quinolinic acid). We therefore investigated the possible effects of peripherally administered KYNA. Repetitive CSD waves were elicited by the application of 1 M KCl solution to the cortex. Direct current-electrocorticograms were measured for 1 hour. Four parameters of the waves were compared. Evans blue dye and fluorescent microscopy were used to study the possible changes in the permeability of the BBB. The results demonstrated that N-methyl-D-aspartate receptor antagonists can reduce the number of CSD waves and decrease the permeability of the BBB during CSD. These results suggest that KYNA itself or its derivatives may offer a new approach in the therapy of migraines. Keywords: blood–brain barrier, cortical spreading depression, glutamate receptors, kynurenic acid, kynurenines, NMDAR

Published
2013

22. 1856–1858

Author

Feuerbach, L., primary, Kampe, Ferdinand, additional, Schachtel, J., additional, Roth, J., additional, Goldberg, August, additional, Benecke, Heinrich, additional, Wigand, Otto, additional, Kolb, G. F., additional, Rüge, Arnold, additional, Knapp, L., additional, Ludwig, F., additional, Bolin, Wilhelm, additional, Tilliard, L., additional, Benecke, Heinr., additional, Wuzer, Heinrich, additional, Moleschott, Jac., additional, and Meißner, Otto, additional

Published
1996
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32. Projekt Optimilch: Wirtschaftlichkeit der Vollweidestrategie – Ergebnisse 2000 bis 2010

Author

Blättler, Thomas, Durgiai, Bruno, Knapp, L., and Haller, T.

Subjects
H Social Sciences (General), S Agriculture (General)
Abstract

Im Projekt Optimilch (2000–2004) wurde die produktionstechnische Umsetzbarkeit der Vollweidestrategie mit saisonaler Abkalbung für Milchwirtschaftsbetriebe im schweizerischen Mittelland aufgezeigt. Die betriebswirtschaftlichen Perspektiven der Strategie können erst in der vorliegenden Arbeit mit einer Analyse der Vollkosten-Ergebnisse dieser Milchproduktionsbetriebe über den Zeitraum von 1999–2010 Jahren beschrieben werden. Die Strategie erlaubte eine deutliche Senkung der Produktionskosten pro kg Milch, die massgeblich durch die konsequente arbeitstechnische Vereinfachung mittels saisonaler Abkalbung der Herden im Frühjahr und der damit entscheidend verbesserten Arbeitsproduktivität erreicht wurde. Bei kleiner Vergrösserung der Milchmenge lag der Arbeitsverdienst am Ende des Beobachtungszeitraums bei acht von neun Vollweidebetrieben deutlich über dem Schweizer Durchschnitt. Die Strategie stellt im Schweizer Talgebiet eine wirtschaftlich sehr interessante, sozial und ökologisch nachhaltige Alternative zu den etablierten Milchproduktionsstrategien dar.

Published
2015
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33. Projekt Optimilch: Wirtschaftlichkeit der Hochleistungsstrategie – Ergebnisse 2000 bis 2010

Author

Blättler, Thomas, Durgiai, Bruno, Knapp, L., and Haller, T.

Subjects
H Social Sciences (General), S Agriculture (General)
Abstract

Im Projekt Optimilch (2000–2004) wurde die produktionstechnische Umsetzbarkeit der Hochleistungs- oder High-Output-Strategie für Milchwirtschaftsbetriebe im schweizerischen Mittelland aufgezeigt. Die damals als erfolgsversprechend beurteilten betriebswirtschaftlichen Perspektiven der Strategie konnten erst mit einer Analyse der Vollkosten- Ergebnisse dieser Milchproduktionsbetriebe über den Zeitraum von 1999–2011 überprüft werden. Die Strategie erlaubte in der Tat eine deutliche Senkung der Produktionskosten pro kg Milch, die massgeblich durch die stark ausgedehnte Milchmenge und der damit entscheidend verbesserten Arbeitsproduktivität erreicht wurde; die Skaleneffekte bewirkten auch eine Reduktion der fremden Strukturkosten je kg Milch. Am Ende des Beobachtungszeitraums lag der Arbeitsverdienst bei drei von sieben Hochleistungsbetrieben deutlich über dem Schweizer Durchschnitt. Diese Strategie kann im Schweizer Talgebiet wirtschaftlich interessant sein, konfrontiert die Betriebsleiterfamilien aber mit ausserordentlichen Herausforderungen.

Published
2015
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36. The MHC class I genes of the rhesus monkey. Different evolutionary histories of MHC class I and II genes in primates

Author

Boyson, J. E., Shufflebotham, C., Luis F. Cadavid, Urvater, J. A., Knapp, L. A., Hughes, A. L., and Watkins, D. I.

Subjects
Immunology, Immunology and Allergy
Abstract

Homologues of the human HLA-A and -B MHC class I loci have been found in great apes and Old World primates suggesting that these two loci have existed for at least 30 million years. The C locus, however, shows some sequence similarity to the B locus and has been found only in gorillas, chimpanzees, and humans. To determine the age of the MHC class I C locus and to examine the evolution of the A and B loci we have cloned, sequenced, and in vitro translated 16 MHC class I cDNAs from two unrelated rhesus monkeys (Macaca mulatta) using both cDNA library screening and PCR amplification. Analyses of these sequences suggest that the C locus is not present in the rhesus monkey, indicating that this locus may be of recent origin in gorillas, chimpanzees, and humans. The rhesus monkey's complement of MHC class I genes includes the products of at least one expressed A locus and at least two expressed B loci, indicating that a duplication of the B locus has taken place in the lineage leading to these Old World primates. Comparison of rhesus monkey MHC class I cDNAs to their primate counterparts reveals fundamental differences between MHC class I and class II evolution in primates. Although MHC class II allelic lineages are shared between humans and Old World primates, no such trans-species sharing of allelic lineages is seen at the MHC class I loci.

Published
1996
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37. Geographic variation of the major histocompatibility complex in Eastern Atlantic grey seals (Halichoerus grypus)

Author

Cammen, K., Hoffman, Joseph, Knapp, L. A., Harwood, J., and Amos, W.

Subjects
Canada, Base Sequence, Geography, Seals, Earless, Denmark, Genes, MHC Class II, Molecular Sequence Data, Genetic Variation, Sequence Analysis, DNA, United Kingdom, Major Histocompatibility Complex, Genetics, Population, Gene Frequency, Animals, Sequence Alignment, Ecosystem, Microsatellite Repeats
Abstract

Pathogen-driven balancing selection maintains high genetic diversity in many vertebrates, particularly in the major histocompatibility complex (MHC) immune system gene family, which is often associated with disease susceptibility. In large natural populations where subpopulations face different pathogen pressures, the MHC should show greater genetic differentiation within a species than neutral markers. We examined genetic diversity at the MHC-DQB locus and nine putatively neutral microsatellite markers in grey seals (Halichoerus grypus) from eight United Kingdom (UK) colonies, the Faeroe Islands and Sable Island, Canada. Five DQB alleles were identified in grey seals, which varied in prevalence across the grey seal range. Among the seal colonies, significant differences in DQB allele and haplotype frequencies and in average DQB heterozygosity were observed. Additionally, the DQB gene exhibited greater differentiation among colonies compared with neutral markers, yet a weaker pattern of isolation by distance (IBD). After correcting for the underlying IBD pattern, subpopulations breeding in similar habitats were more similar to one another in DQB allele frequencies than populations breeding in different habitats, but the same did not hold true for microsatellites, suggesting that habitat-specific pathogen pressure influences MHC evolution. Overall, the data are consistent with selection at MHC-DQB loci in grey seals with both varying selective pressures and geographic population structure appearing to influence the DQB genetic composition of breeding colonies.

Published
2011

38. Ibrutinib in combination with low-dose dexamethasone in patients with relapsed or relapsed and refractory multiple myeloma: results from a multicenter phase 2 trial

Author

Richardson, P.G., primary, Bensinger, W.I., additional, Huff, C.A., additional, Costello, C.L., additional, Lendvai, N., additional, Berdeja, J.G., additional, Anderson, L.D., additional, Siegel, D.S., additional, Jagannath, S., additional, Laubach, J.P., additional, Stockerl-Goldstein, K.E., additional, Knapp, L., additional, Kwei, L., additional, Clow, F., additional, Graef, T., additional, Bilotti, E., additional, and Vij, R., additional

Published
2015
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40. Pregabalin for the treatment of postoperative pain: Results from three controlled trials using different surgical models

Author

Singla, NK, Echelly, J, Lionberger, DR, Gimbel, J, Sanin, L, Sporn, J, Yang, R, Cheung, R, Knapp, L, Parsons, B, Singla, NK, Echelly, J, Lionberger, DR, Gimbel, J, Sanin, L, Sporn, J, Yang, R, Cheung, R, Knapp, L, and Parsons, B

Abstract

Conclusion: There were no significant differences between pregabalin and placebo with respect to the primary pain intensity measure in each of the three clinical trials. These studies encompass a large dataset (1,233 patients in total), and their results should be considered when assessing pregabalin’s effectiveness in postoperative pain. Further studies are required to determine the potential pain-reducing benefit of pregabalin in the postoperative setting.

Published
2014

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