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5. SUcceSS, SUrgery for Spinal Stenosis: Protocol of a randomised, placebo-controlled trial

Author

Anderson, DB, Ferreira, ML, Harris, IA, Davis, GA, Stanford, R, Beard, D, Li, Q, Jan, S, Mobbs, RJ, Maher, CG, Yong, R, Zammit, T, Latimer, J, Buchbinder, R, Anderson, DB, Ferreira, ML, Harris, IA, Davis, GA, Stanford, R, Beard, D, Li, Q, Jan, S, Mobbs, RJ, Maher, CG, Yong, R, Zammit, T, Latimer, J, and Buchbinder, R

Abstract

© Author(s) (or their employer(s)) 2019. Introduction: Central lumbar spinal stenosis (LSS) is a common cause of pain, reduced function and quality of life in older adults. Current management of LSS includes surgery to decompress the spinal canal and alleviate symptoms. However, evidence supporting surgical decompression derives from unblinded randomised trials with high cross-over rates or cohort studies showing modest benefits. This protocol describes the design of the SUrgery for Spinal Stenosis (SUcceSS) trial-the first randomised placebo-controlled trial of decompressive surgery for symptomatic LSS. Methods and analysis: SUcceSS will be a prospectively registered, randomised placebo-controlled trial of decompressive spinal surgery. 160 eligible participants (80 participants/group) with symptomatic LSS will be randomised to either surgical spinal decompression or placebo surgical intervention. The placebo surgical intervention is identical to surgical decompression in all other ways with the exception of the removal of any bone or ligament. All participants and assessors will be blinded to treatment allocation. Outcomes will be assessed at baseline and at 3, 6, 12 and 24 months. The coprimary outcomes will be function measured with the Oswestry Disability Index and the proportion of participants who have meaningfully improved their walking capacity at 3 months postrandomisation. Secondary outcomes include back pain intensity, lower limb pain intensity, disability, quality of life, anxiety and depression, neurogenic claudication score, perceived recovery, treatment satisfaction, adverse events, reoperation rate and rehospitalisation rate. Those who decline to be randomised will be invited to participate in a parallel observational cohort. Data analysis will be blinded and by intention to treat. A trial-based cost-effectiveness analysis will determine the potential incremental cost per quality-adjusted life year gained. Ethics and dissemination: Ethics approval ha

Published
2019

10. Biodiversity inventories in high gear:DNA barcoding facilitates a rapid biotic survey of a temperate nature reserve

Author

Telfer, A. C. (Angela C.), Young, M. R. (Monica R.), Quinn, J. (Jenna), Perez, K. (Kate), Sobel, C. N. (Crystal N.), Sones, J. E. (Jayme E.), Levesque-Beaudin, V. (Valerie), Derbyshire, R. (Rachael), Fernandez-Triana, J. (Jose), Rougerie, R. (Rodolphe), Thevanayagam, A. (Abinah), Boskovic, A. (Adrian), Borisenko, A. V. (Alex, V), Cadel, A. (Alex), Brown, A. (Allison), Pages, A. (Anais), Castillo, A. H. (Anibal H.), Nicolai, A. (Annegret), Mockford, B. M. (Barb Mockford Glenn), Bukowski, B. (Belen), Wilson, B. (Bill), Trojahn, B. (Brock), Lacroix, C. A. (Carole Ann), Brimblecombe, C. (Chris), Hay, C. (Christoper), Ho, C. (Christmas), Steinke, C. (Claudia), Warne, C. P. (Connor P.), Cortes, C. G. (Cristina Garrido), Engelking, D. (Daniel), Wright, D. (Danielle), Lijtmaer, D. A. (Dario A.), Gascoigne, D. (David), Martich, D. H. (David Hernandez), Morningstar, D. (Derek), Neumann, D. (Dirk), Steinke, D. (Dirk), DeBruin, D. D. (Donna Debruin Marco), Dobias, D. (Dylan), Sears, E. (Elizabeth), Richard, E. (Ellen), Damstra, E. (Emily), Zakharov, E. V. (Evgeny, V), Laberge, F. (Frederic), Collins, G. E. (Gemma E.), Blagoev, G. A. (Gergin A.), Grainge, G. (Gerrie), Ansell, G. (Graham), Meredith, G. (Greg), Hogg, I. (Ian), McKeown, J. (Jaclyn), Topan, J. (Janet), Bracey, J. (Jason), Guenther, J. (Jerry), Sills-Gilligan, J. (Jesse), Addesi, J. (Joseph), Persi, J. (Joshua), Layton, K. K. (Kara K. S.), D'Souza, K. (Kareina), Dorji, K. (Kencho), Grundy, K. (Kevin), Nghidinwa, K. (Kirsti), Ronnenberg, K. (Kylee), Lee, K. M. (Kyung Min), Xie, L. (Linxi), Lu, L. (Liuqiong), Penev, L. (Lyubomir), Gonzalez, M. (Mailyn), Rosati, M. E. (Margaret E.), Kekkonen, M. (Mari), Kuzmina, M. (Maria), Iskandar, M. (Marianne), Mutanen, M. (Marko), Fatahi, M. (Maryam), Pentinsaari, M. (Mikko), Bauman, M. (Miriam), Nikolova, N. (Nadya), Ivanova, N. V. (Natalia, V), Jones, N. (Nathaniel), Weerasuriya, N. (Nimalka), Monkhouse, N. (Norman), Lavinia, P. D. (Pablo D.), Jannetta, P. (Paul), Hanisch, P. E. (Priscila E.), McMullin, R. T. (R. Troy), Flores, R. O. (Rafael Ojeda), Mouttet, R. (Raphaelle), Vender, R. (Reid), Labbee, R. N. (Renee N.), Forsyth, R. (Robert), Lauder, R. (Rob), Dickson, R. (Ross), Kroft, R. (Ruth), Miller, S. E. (Scott E.), MacDonald, S. (Shannon), Panthi, S. (Sishir), Pedersen, S. (Stephanie), Sobek-Swant, S. (Stephanie), Naik, S. (Suresh), Lipinskaya, T. (Tatsiana), Eagalle, T. (Thanushi), Decaens, T. (Thibaud), Kosuth, T. (Thibault), Braukmann, T. (Thomas), Woodcock, T. (Tom), Roslin, T. (Tomas), Zammit, T. (Tony), Campbell, V. (Victoria), Dinca, V. (Vlad), Peneva, V. (Vlada), Hebert, P. D. (Paul D. N.), deWaard, J. R. (Jeremy R.), Telfer, A. C. (Angela C.), Young, M. R. (Monica R.), Quinn, J. (Jenna), Perez, K. (Kate), Sobel, C. N. (Crystal N.), Sones, J. E. (Jayme E.), Levesque-Beaudin, V. (Valerie), Derbyshire, R. (Rachael), Fernandez-Triana, J. (Jose), Rougerie, R. (Rodolphe), Thevanayagam, A. (Abinah), Boskovic, A. (Adrian), Borisenko, A. V. (Alex, V), Cadel, A. (Alex), Brown, A. (Allison), Pages, A. (Anais), Castillo, A. H. (Anibal H.), Nicolai, A. (Annegret), Mockford, B. M. (Barb Mockford Glenn), Bukowski, B. (Belen), Wilson, B. (Bill), Trojahn, B. (Brock), Lacroix, C. A. (Carole Ann), Brimblecombe, C. (Chris), Hay, C. (Christoper), Ho, C. (Christmas), Steinke, C. (Claudia), Warne, C. P. (Connor P.), Cortes, C. G. (Cristina Garrido), Engelking, D. (Daniel), Wright, D. (Danielle), Lijtmaer, D. A. (Dario A.), Gascoigne, D. (David), Martich, D. H. (David Hernandez), Morningstar, D. (Derek), Neumann, D. (Dirk), Steinke, D. (Dirk), DeBruin, D. D. (Donna Debruin Marco), Dobias, D. (Dylan), Sears, E. (Elizabeth), Richard, E. (Ellen), Damstra, E. (Emily), Zakharov, E. V. (Evgeny, V), Laberge, F. (Frederic), Collins, G. E. (Gemma E.), Blagoev, G. A. (Gergin A.), Grainge, G. (Gerrie), Ansell, G. (Graham), Meredith, G. (Greg), Hogg, I. (Ian), McKeown, J. (Jaclyn), Topan, J. (Janet), Bracey, J. (Jason), Guenther, J. (Jerry), Sills-Gilligan, J. (Jesse), Addesi, J. (Joseph), Persi, J. (Joshua), Layton, K. K. (Kara K. S.), D'Souza, K. (Kareina), Dorji, K. (Kencho), Grundy, K. (Kevin), Nghidinwa, K. (Kirsti), Ronnenberg, K. (Kylee), Lee, K. M. (Kyung Min), Xie, L. (Linxi), Lu, L. (Liuqiong), Penev, L. (Lyubomir), Gonzalez, M. (Mailyn), Rosati, M. E. (Margaret E.), Kekkonen, M. (Mari), Kuzmina, M. (Maria), Iskandar, M. (Marianne), Mutanen, M. (Marko), Fatahi, M. (Maryam), Pentinsaari, M. (Mikko), Bauman, M. (Miriam), Nikolova, N. (Nadya), Ivanova, N. V. (Natalia, V), Jones, N. (Nathaniel), Weerasuriya, N. (Nimalka), Monkhouse, N. (Norman), Lavinia, P. D. (Pablo D.), Jannetta, P. (Paul), Hanisch, P. E. (Priscila E.), McMullin, R. T. (R. Troy), Flores, R. O. (Rafael Ojeda), Mouttet, R. (Raphaelle), Vender, R. (Reid), Labbee, R. N. (Renee N.), Forsyth, R. (Robert), Lauder, R. (Rob), Dickson, R. (Ross), Kroft, R. (Ruth), Miller, S. E. (Scott E.), MacDonald, S. (Shannon), Panthi, S. (Sishir), Pedersen, S. (Stephanie), Sobek-Swant, S. (Stephanie), Naik, S. (Suresh), Lipinskaya, T. (Tatsiana), Eagalle, T. (Thanushi), Decaens, T. (Thibaud), Kosuth, T. (Thibault), Braukmann, T. (Thomas), Woodcock, T. (Tom), Roslin, T. (Tomas), Zammit, T. (Tony), Campbell, V. (Victoria), Dinca, V. (Vlad), Peneva, V. (Vlada), Hebert, P. D. (Paul D. N.), and deWaard, J. R. (Jeremy R.)

Abstract

Background: Comprehensive biotic surveys, or ‘all taxon biodiversity inventories’ (ATBI), have traditionally been limited in scale or scope due to the complications surrounding specimen sorting and species identification. To circumvent these issues, several ATBI projects have successfully integrated DNA barcoding into their identification procedures and witnessed acceleration in their surveys and subsequent increase in project scope and scale. The Biodiversity Institute of Ontario partnered with the rare Charitable Research Reserve and delegates of the 6th International Barcode of Life Conference to complete its own rapid, barcode-assisted ATBI of an established land trust in Cambridge, Ontario, Canada. New information: The existing species inventory for the rare Charitable Research Reserve was rapidly expanded by integrating a DNA barcoding workflow with two surveying strategies — a comprehensive sampling scheme over four months, followed by a one-day bioblitz involving international taxonomic experts. The two surveys resulted in 25,287 and 3,502 specimens barcoded, respectively, as well as 127 human observations. This barcoded material, all vouchered at the Biodiversity Institute of Ontario collection, covers 14 phyla, 29 classes, 117 orders, and 531 families of animals, plants, fungi, and lichens. Overall, the ATBI documented 1,102 new species records for the nature reserve, expanding the existing long-term inventory by 49%. In addition, 2,793 distinct Barcode Index Numbers (BINs) were assigned to genus or higher level taxonomy, and represent additional species that will be added once their taxonomy is resolved. For the 3,502 specimens, the collection, sequence analysis, taxonomic assignment, data release and manuscript submission by 100+ co-authors all occurred in less than one week. This demonstrates the speed at which barcode-assisted inventories can be completed and the utility that barcoding provides in minimizing and guiding valuable taxonomic spec

Published
2015

14. 107

Author

Zammit, T.

Published
1924

28. Prolonged Grief Disorder, but Not Death From COVID-19, Elicits Public Stigma: A Vignette-Based Experiment.

Author

Zammit T, Mancini VO, Reid C, Singer J, Staniland L, and Breen LJ

Abstract

We investigated the effects of cause of death (COVID-19 with an underlying medical condition vs. without) and prolonged grief disorder status (PGD present or absent) on participants' reported public stigma towards the bereaved. Participants ( N = 304, 66% women; M age = 39.39 years) were randomly assigned to read one of four vignettes describing a bereaved man. Participants completed stigma measures assessing negative attributions, desired social distance, and emotional reactions. Participants reported significantly stronger stigmatizing responses towards an individual with PGD (vs. without PGD) across all stigma measures. There was no significant difference in stigma based on cause of death; however, stigma was reported regardless of cause of death. There was no significant interaction between cause of death and PGD on stigma. This study supports the robust finding of public stigma being reported toward an individual with PGD, suggesting these individuals are at risk of public stigma and not receiving adequate bereavement support., Competing Interests: Declaration of Conflicting InterestsThe author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published
2024
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29. Public stigma toward prolonged grief and COVID-19 bereavement: A vignette-based experiment.

Author

Zammit T, Mancini VO, Reid C, Singer J, Staniland L, and Breen LJ

Subjects
Male, Humans, Female, Adult, Grief, Social Stigma, Social Perception, COVID-19, Bereavement
Abstract

We investigated the effects of cause of death and the presence of prolonged grief disorder (PGD) on eliciting public stigma toward the bereaved. Participants ( N  = 328, 76% female; M age = 27.55 years) were randomly assigned to read one of four vignettes describing a bereaved man. Each vignette differed by his PGD status (PGD diagnosis or no PGD diagnosis) and his wife's cause of death (COVID-19 or brain hemorrhage). Participants completed public stigma measures assessing negative attributions, desired social distance, and emotional reactions. Bereavement with PGD (versus without PGD) elicited large and significantly stronger responses across all stigma measures. Both causes of death elicited public stigma. There was no interaction between cause of death and PGD on stigma. With increased PGD rates expected during the pandemic, the potential for public stigma and reduced social support for people bereaved via traumatic deaths and people with PGD requires mitigation.

Published
2024
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30. SUcceSS, SUrgery for Spinal Stenosis: protocol of a randomised, placebo-controlled trial.

Author

Anderson DB, Ferreira ML, Harris IA, Davis GA, Stanford R, Beard D, Li Q, Jan S, Mobbs RJ, Maher CG, Yong R, Zammit T, Latimer J, and Buchbinder R

Subjects
Back Pain surgery, Cost-Benefit Analysis, Double-Blind Method, Humans, Pain Management, Pain Measurement, Prospective Studies, Quality of Life, Randomized Controlled Trials as Topic, Reoperation statistics & numerical data, Spinal Stenosis economics, Decompression, Surgical methods, Lumbar Vertebrae, Spinal Stenosis surgery, Walking
Abstract

Introduction: Central lumbar spinal stenosis (LSS) is a common cause of pain, reduced function and quality of life in older adults. Current management of LSS includes surgery to decompress the spinal canal and alleviate symptoms. However, evidence supporting surgical decompression derives from unblinded randomised trials with high cross-over rates or cohort studies showing modest benefits. This protocol describes the design of the SUrgery for Spinal Stenosis (SUcceSS) trial -the first randomised placebo-controlled trial of decompressive surgery for symptomatic LSS., Methods and Analysis: SUcceSS will be a prospectively registered, randomised placebo-controlled trial of decompressive spinal surgery. 160 eligible participants (80 participants/group) with symptomatic LSS will be randomised to either surgical spinal decompression or placebo surgical intervention. The placebo surgical intervention is identical to surgical decompression in all other ways with the exception of the removal of any bone or ligament. All participants and assessors will be blinded to treatment allocation. Outcomes will be assessed at baseline and at 3, 6, 12 and 24 months. The coprimary outcomes will be function measured with the Oswestry Disability Index and the proportion of participants who have meaningfully improved their walking capacity at 3 months postrandomisation. Secondary outcomes include back pain intensity, lower limb pain intensity, disability, quality of life, anxiety and depression, neurogenic claudication score, perceived recovery, treatment satisfaction, adverse events, reoperation rate and rehospitalisation rate. Those who decline to be randomised will be invited to participate in a parallel observational cohort. Data analysis will be blinded and by intention to treat. A trial-based cost-effectiveness analysis will determine the potential incremental cost per quality-adjusted life year gained., Ethics and Dissemination: Ethics approval has been granted by the NSW Health (reference:17/247/POWH/601) and the Monash University (reference: 12371) Human Research Ethics Committees. Dissemination of results will be via journal articles and presentations at national and international conferences., Trial Registration Number: ACTRN12617000884303; Pre-results., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2019. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2019
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31. Biodiversity inventories in high gear: DNA barcoding facilitates a rapid biotic survey of a temperate nature reserve.

Author

Telfer AC, Young MR, Quinn J, Perez K, Sobel CN, Sones JE, Levesque-Beaudin V, Derbyshire R, Fernandez-Triana J, Rougerie R, Thevanayagam A, Boskovic A, Borisenko AV, Cadel A, Brown A, Pages A, Castillo AH, Nicolai A, Glenn Mockford BM, Bukowski B, Wilson B, Trojahn B, Lacroix CA, Brimblecombe C, Hay C, Ho C, Steinke C, Warne CP, Garrido Cortes C, Engelking D, Wright D, Lijtmaer DA, Gascoigne D, Hernandez Martich D, Morningstar D, Neumann D, Steinke D, Marco DeBruin DD, Dobias D, Sears E, Richard E, Damstra E, Zakharov EV, Laberge F, Collins GE, Blagoev GA, Grainge G, Ansell G, Meredith G, Hogg I, McKeown J, Topan J, Bracey J, Guenther J, Sills-Gilligan J, Addesi J, Persi J, Layton KK, D'Souza K, Dorji K, Grundy K, Nghidinwa K, Ronnenberg K, Lee KM, Xie L, Lu L, Penev L, Gonzalez M, Rosati ME, Kekkonen M, Kuzmina M, Iskandar M, Mutanen M, Fatahi M, Pentinsaari M, Bauman M, Nikolova N, Ivanova NV, Jones N, Weerasuriya N, Monkhouse N, Lavinia PD, Jannetta P, Hanisch PE, McMullin RT, Ojeda Flores R, Mouttet R, Vender R, Labbee RN, Forsyth R, Lauder R, Dickson R, Kroft R, Miller SE, MacDonald S, Panthi S, Pedersen S, Sobek-Swant S, Naik S, Lipinskaya T, Eagalle T, Decaëns T, Kosuth T, Braukmann T, Woodcock T, Roslin T, Zammit T, Campbell V, Dinca V, Peneva V, Hebert PD, and deWaard JR

Abstract

Background: Comprehensive biotic surveys, or 'all taxon biodiversity inventories' (ATBI), have traditionally been limited in scale or scope due to the complications surrounding specimen sorting and species identification. To circumvent these issues, several ATBI projects have successfully integrated DNA barcoding into their identification procedures and witnessed acceleration in their surveys and subsequent increase in project scope and scale. The Biodiversity Institute of Ontario partnered with the rare Charitable Research Reserve and delegates of the 6th International Barcode of Life Conference to complete its own rapid, barcode-assisted ATBI of an established land trust in Cambridge, Ontario, Canada., New Information: The existing species inventory for the rare Charitable Research Reserve was rapidly expanded by integrating a DNA barcoding workflow with two surveying strategies - a comprehensive sampling scheme over four months, followed by a one-day bioblitz involving international taxonomic experts. The two surveys resulted in 25,287 and 3,502 specimens barcoded, respectively, as well as 127 human observations. This barcoded material, all vouchered at the Biodiversity Institute of Ontario collection, covers 14 phyla, 29 classes, 117 orders, and 531 families of animals, plants, fungi, and lichens. Overall, the ATBI documented 1,102 new species records for the nature reserve, expanding the existing long-term inventory by 49%. In addition, 2,793 distinct Barcode Index Numbers (BINs) were assigned to genus or higher level taxonomy, and represent additional species that will be added once their taxonomy is resolved. For the 3,502 specimens, the collection, sequence analysis, taxonomic assignment, data release and manuscript submission by 100+ co-authors all occurred in less than one week. This demonstrates the speed at which barcode-assisted inventories can be completed and the utility that barcoding provides in minimizing and guiding valuable taxonomic specialist time. The final product is more than a comprehensive biotic inventory - it is also a rich dataset of fine-scale occurrence and sequence data, all archived and cross-linked in the major biodiversity data repositories. This model of rapid generation and dissemination of essential biodiversity data could be followed to conduct regional assessments of biodiversity status and change, and potentially be employed for evaluating progress towards the Aichi Targets of the Strategic Plan for Biodiversity 2011-2020.

Published
2015
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32. Recovery of male rats from major abdominal surgery after treatment with various analgesics.

Author

Sharp J, Zammit T, Azar T, and Lawson D

Subjects
Animals, Blood Pressure drug effects, Body Weight drug effects, Buprenorphine pharmacology, Butorphanol pharmacology, Feeding Behavior drug effects, Heart Rate drug effects, Ketoprofen pharmacology, Male, Motor Activity drug effects, Rats, Sprague-Dawley, Time Factors, Abdomen surgery, Analgesics, Opioid pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Rats physiology
Abstract

The objective of this study was to compare the recovery of male rats after a major abdominal surgical procedure (the implantation of a radiotelemetry transmitter) when treated with buprenorphine, butorphanol, or ketoprofen and subcutaneous fluids (5% dextrose) or with subcutaneous fluids only. The parameters for assessing recovery were heart rate (HR), mean arterial blood pressure (MAP), home cage activity, food and water consumption, and body weight. HR, MAP, and activity were continuously monitored by radiotelemetry methods, food and water intakes were determined daily, and body weights were measured once or three times a week. In light of HR, nocturnal home cage activity, water consumption, and body weight gain, animals were recovered by about 7 days after surgery. MAP normalized by 1 to 2 days postsurgery, and food consumption returned to presurgical levels 5 to 12 days after surgery, depending on the analgesic treatment. On the basis of nocturnal activity, HR, and food and water intakes, buprenorphine-treated animals recovered more slowly than did the other two analgesic-treated groups. By the other parameters, all three analgesic-treated groups showed very similar responses across time. Surprisingly, when compared with the groups receiving only subcutaneous fluids, buprenorphine and butorphanol delayed or did not advance recovery, whereas ketoprofen neither retarded nor advanced recovery. Explanations for these results include: (a) the analgesics were effective in relieving pain but had pharmacological side effects that altered the measured parameters, making it difficult to determine recovery; (b) the level of pain experienced did not notably affect recovery; (c) the analgesics, at the doses and/or dosing schedules used, were not effective in the relief of pain, thereby causing both groups of animals to recover at the same rate; and (d) the analgesics interfered with recovery. Final resolution of these issues awaits further investigation.

Published
2003

33. Stress-like responses to common procedures in individually and group-housed female rats.

Author

Sharp J, Zammit T, Azar T, and Lawson D

Subjects
Animal Husbandry, Animals, Behavior, Animal, Blood Pressure, Female, Handling, Psychological, Heart Rate, Rats, Social Isolation, Stress, Physiological physiopathology, Animals, Laboratory, Housing, Animal, Rats, Sprague-Dawley, Rodent Diseases physiopathology, Stress, Physiological veterinary
Abstract

The objective of this study was to assess the cardiovascular function and behavior of female Sprague-Dawley rats housed individually or with one or three cage mates under resting conditions and when subjected to common husbandry and experimental procedures and potentially stressful olfactory stimuli. Heart rate (HR) and mean arterial blood pressure (MAP) were assessed continuously by using radiotelemetry and are reported for the following periods: for 1 hour each day prior to any human interaction; for 12 h each day during the dark phase of the 12:12-h light: dark photoperiod; and for 2 h before and 3 h after acute husbandry and experimental procedures. Home-cage behaviors (sleeping, awake but not moving, moving, rearing, and grooming) were scored once each minute for 15 min before and 45 min after the acute procedures. Mean resting HR values in the mornings prior to human contact were significantly (P < 0.05) lower in rats housed four per cage than animals housed alone or with one cage mate, whereas MAP during this period was lowest in rats housed two per cage. Nocturnal HRs were highest in rats housed two per cage, whereas nocturnal MAP did not differ significantly between housing groups. When rats were subjected to acute husbandry and experimental procedures, HRs increased 80 to 180 beats per min (bpm) above a baseline of 300 to 325 bpm and were significantly (P < 0.05) increased for periods of 30 to 90 min after the procedures. MAP showed increases that were proportionately the same as those in HR. Group housing often, but not always, reduced these cardiovascular responses. Procedure-induced arousal behaviors occurred in all housing groups after the acute husbandry and experimental procedures, but the occurrence of these behaviors was less frequent and of shorter duration in group-housed rats than rats housed alone. In light of these results, we conclude that under resting conditions group housed rats were somewhat less stressed than were rats housed alone. Further, we conclude that common procedures induce significant stress-like responses in female rats, and the magnitude and duration of these responses are reduced by group housing.

Published
2003

34. Are "by-stander" female Sprague-Dawley rats affected by experimental procedures?

Author

Sharp J, Zammit T, Azar T, and Lawson D

Subjects
Animal Husbandry, Animals, Behavior, Animal, Blood Pressure, Female, Heart Rate, Housing, Animal, Population Density, Rats, Rats, Sprague-Dawley, Animal Experimentation, Animals, Laboratory, Rodent Diseases physiopathology, Stress, Physiological veterinary
Abstract

The objective of this study was to test the hypotheses that female rats are stressed by being in the same room as animals subjected to common husbandry and experimental procedures and that the level of stress is affected by housing density. Two commonly used indices of stress, heart rate (HR) and mean arterial blood pressure (MAP), were determined by using radiotelemetry for 2 h before and 3 h after rats witnessed the following procedures: decapitation, simulated decapitation, cage change, simulated cage change, restraint and subcutaneous injection, removal of rats to another room for injection, restraint and tail-vein injection, handling and weighing, and handling and vaginal lavage. In addition, home cage behaviors (sleeping, awake, moving, rearing, and grooming) were scored once each minute for 15 min before and 45 min after the procedures. Witnessing decapitation of six other rats induced small, but significant, increases in HR above undisturbed baseline values in animals housed alone, whereas responses in animals housed with one or three cage mates were slightly greater than those of rats housed alone. Witnessing a routine cage change induced significant increases in HR in rats which were equal to or greater than those induced by witnessing decapitations; however, housing density had little effect on the responses to cage change. HR did not significantly increase above baseline values in rats witnessing restraint and a subcutaneous or tail-vein injection of other rats or when witnessing other rats being handled and weighed. However, rats housed alone showed significant increases in HR when witnessing a vaginal lavage of other rats. Active behaviors (moving, rearing, grooming) in the home cage were significantly altered only in rats housed alone and then only when witnessing a cage change or a tail-vein injection. Considering primarily increased HR, we conclude that female Sprague-Dawley rats may be marginally stressed when present in the same room in which decapitation is being performed, but similar stress-like responses are induced by common husbandry and experimental procedures. Finally, group housing often, but not always, reduces the stress-like responses that can occur in female by-stander rats.

Published
2003

35. Does witnessing experimental procedures produce stress in male rats?

Author

Sharp J, Zammit T, Azar T, and Lawson D

Subjects
Animals, Autopsy, Euthanasia, Housing, Animal, Injections, Male, Photic Stimulation, Rats, Rats, Sprague-Dawley, Restraint, Physical, Specific Pathogen-Free Organisms, Time Factors, Animal Husbandry methods, Blood Pressure physiology, Heart Rate physiology, Stress, Physiological physiopathology, Vision, Ocular
Abstract

The objective of this study was to test the hypotheses that male rats are stressed by being in the same room as animals subjected to common husbandry and experimental procedures and that the level of stress is affected by housing density. Two commonly used indices of stress, heart rate (HR) and mean arterial blood pressure (MAP), were determined by using radiotelemetry for 2 h before and 3 h after rats witnessed the following procedures: decapitation, decapitation and necropsy, cage change, restraint and subcutaneous injection, and restraint and tail-vein injection. In addition, home cage behaviors (sleeping, awake, moving, rearing, and grooming) were scored once each minute for 15 min before and 45 min after the procedures. Witnessing decapitation or decapitation and necropsy of 6 other rats induced small, but significant, increases in HR and MAP in animals housed alone, whereas responses in animals housed with one or three cagemates were more transient or not significant. Witnessing a routine cage change also induced small increases in HR and MAP in rats housed alone or with one cagemate, but HR and MAP decreased in rats housed four per cage. HR and MAP did not change in rats witnessing restraint and a subcutaneous injection of other rats, but these indices were transiently increased when rats witnessed animals being restrained in a rodent restrainer and given a tail-vein injection. Home cage behaviors were significantly altered only in rats witnessing decapitation and necropsy and then only in rats housed alone. We conclude that male Sprague-Dawley rats are not significantly stressed when present in the same room in which decapitation or other common experimental procedures are being performed, especially when the animals are housed with cagemates.

Published
2002

36. Recovery from carotid artery catheterization performed under various anesthetics in male, Sprague-Dawley rats.

Author

Lawson DM, Duke JL, Zammit TG, Collins HL, and DiCarlo SE

Subjects
Anesthesia methods, Animals, Blood Pressure, Body Weight, Catheterization adverse effects, Eating, Heart Rate, Male, Rats, Rats, Sprague-Dawley, Time Factors, Anesthesia veterinary, Carotid Arteries, Catheterization methods
Abstract

This study was designed to determine the time to recovery from carotid artery catheterization using multiple criteria and to compare recovery times between three common anesthetics. Male Sprague-Dawley rats, chronically instrumented with radio-telemetry transmitters, were anesthetized with sodium pentobarbital, halothane or a mixture of ketamine, xylazine and acepromazine before an indwelling catheter was placed in the carotid artery. The procedure was completed in less than 15 min. Changes in body weight, food and water consumption, blood pressure, heart rate and activity were used to determine recovery. As judged by recovery of body weight, animals anesthetized with each of the anesthetics recovered by the 4th day after catheterization. Food and water consumption normalized by 1-2 days after surgery. Heart rates and blood pressures during the light phase of the photoperiod were significantly increased for 2 days by all anesthetics. During the dark phase of the photoperiod, heart rates and blood pressures were not significantly affected by pentobarbital or halothane anesthesia, but were significantly decreased and increased respectively on the night immediately following surgery in the ketamine / xylazine / acepromazine-anesthetized rats. Delayed elevations of heart rate were observed in pentobarbital and halothane anesthetized rats on days and/or nights 5 and 6 post surgery. Animal activity patterns during the light phase of the photoperiod were not affected by pentobarbital or halothane, but were increased by ketamine 2 days after surgery. During the dark phase, halothane transiently reduced activity whereas ketamine-anesthetized rats showed reduced activity for 4 nights post surgery. These studies show that recovery depends on the criteria selected and the anesthetic used, but, in general, 2-4 days were required for recovery from this relatively simple procedure.

Published
2001

37. The effects of routine cage-changing on cardiovascular and behavioral parameters in male Sprague-Dawley rats.

Author

Duke JL, Zammit TG, and Lawson DM

Subjects
Animals, Behavior, Animal, Blood Pressure, Confounding Factors, Epidemiologic, Heart Rate, Male, Rats, Animal Husbandry, Housing, Animal, Rats, Sprague-Dawley, Stress, Psychological
Abstract

The objective of this study was to determine whether the blood pressure and heart rate of adult male Sprague-Dawley rats are affected by the routine animal husbandry procedure of moving animals to clean cages. Cardiovascular parameters were obtained by using radiotelemetry; behavior in the home cage also was evaluated. Each rat had a radiotelemetry transmitter implanted in the peritoneal cavity, with the attached catheter placed in the femoral artery. After a 7- to 9-day recovery period, half of the rats were moved to clean cages with fresh wood-chip bedding; the other animals were left undisturbed. Systolic, diastolic, and mean arterial blood pressures; heart rate; and cage behavior (movement, rearing, grooming) increased promptly and significantly when animals were placed in clean cages. These cardiovascular and behavioral responses lasted for 45 to 60 min. Those animals not moved to clean cages but present in the animal room when this procedure was done did not show significant increases in blood pressure, heart rate, or activity. When rats were moved to clean cages that contained new bedding plus a small quantity of the soiled bedding from their previous cage, the cardiovascular and behavioral responses were similar to those of animals exposed to completely fresh bedding. The responses of rats being moved to new cages did not diminish between the first and fourth weekly cage change. Rats whose cages were not changed for 2 weeks showed small, but significant, increases in cardiovascular and behavioral responses above the responses in animals with weekly cage changes. We conclude that ordinary animal husbandry procedures such as moving rats to a clean cage can induce transient, but significant, cardiovascular and behavioral changes. Investigators and animal care staff should recognize that such routine procedures could confound experiments conducted shortly thereafter.

Published
2001

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