Your search keyword '"Kretzschmar, Imogen"' showing total 8 results

1. Randomised controlled trial of the short-term effects of OROS-methylphenidate on ADHD symptoms and behavioural outcomes in young male prisoners with attention deficit hyperactivity disorder:CIAO-II study

Author

Asherson, Philip, Johansson, Lena, Holland, Rachel, Bedding, Megan, Forrester, Andrew, Laura, Gianulli, Ginsberg, Ylva, Howitt, Sheila, Kretzschmar, Imogen, Lawrie, Stephen, Marsh, Craig, Kelly, Caroline, Mansfield, Megan, McCafferty, Clare, Khan, Khuram, Muller-Sedgwick, Ulrich, Strang, John, Williamson, Grace, Wilson, Lauren, Young, Susan, Landau, Sabine, and Thomson, Lindsay

Subjects

mental disorders, behavioral disciplines and activities

Abstract

(237/300 words)Background: 20-30% of prisoners meet diagnostic criteria for attention-deficit/hyperactivity disorder (ADHD). Methylphenidate reduces ADHD symptoms but effects in prisoners are uncertain due to 16 comorbid mental health and substance use disorders. Aim: To estimate the efficacy of an Osmotic-Release-Oral-System methylphenidate (OROS-methylphenidate) in reducing ADHD symptoms in young adult prisoners with ADHD. Methods: An 8-week parallel arm, double-blind, randomised, placebo-controlled trial of OROS-methylphenidate versus placebo in male prisoners (aged 16-25) meeting DSM-5 criteria for ADHD. Primary outcome was ADHD symptoms at 8-weeks using the investigator rated Connors Adult ADHD Rating Scale (CAARS-O). Thirteen secondary outcome measures included emotional dysregulation, mind-wandering, violent attitudes, mental health symptoms, and prison officer and educational staff ratings of behaviour and aggression.Findings: Mean CAARS-O at 8 weeks in the OROS-methylphenidate arm was estimated to be reduced 26 by 0.57 points relative to the Placebo arm (95% CI: -2.41 to 3.56) and non-significant. The responder rate, defined as a 20% reduction in CAARS-O scores was 48.3% for the OROS-methylphenidate arm28 and 47.9% for the placebo arm. No statistically significant trial arm difference were detected for any of the secondary outcomes. Mean final titrated dose was 53.8 mg in the OROS-methylphenidate arm.Conclusions: ADHD symptoms did not respond to OROS-methylphenidate in young adult prisoners. The findings do not support routine treatment with OROS-methylphenidate in this population. Further research is needed to evaluate effects of higher average dosing and adherence to treatment, multimodal treatments, and preventative interventions in the community.Trial registration: EudraCT Number 2015-004271-78; ISRCTN16827947. Database lock 27th August 2019

Published

2022

2. Randomised controlled trial of the short-term effects of osmotic-release oral system methylphenidate on symptoms and behavioural outcomes in young male prisoners with attention deficit hyperactivity disorder: CIAO-II study

Author

Asherson, Philip J., primary, Johansson, Lena, additional, Holland, Rachel, additional, Bedding, Megan, additional, Forrester, Andrew, additional, Giannulli, Laura, additional, Ginsberg, Ylva, additional, Howitt, Sheila, additional, Kretzschmar, Imogen, additional, Lawrie, Stephen M., additional, Marsh, Craig, additional, Kelly, Caroline, additional, Mansfield, Megan, additional, McCafferty, Clare, additional, Khan, Khuram, additional, Müller-Sedgwick, Ulrich, additional, Strang, John, additional, Williamson, Grace, additional, Wilson, Lauren, additional, Young, Susan, additional, Landau, Sabine, additional, and Thomson, Lindsay D. G., additional

Published

2022

3. OROS-methylphenidate to reduce ADHD symptoms in male prisoners aged 16–25 years: a RCT

Author

Asherson, Philip, primary, Johansson, Lena, additional, Holland, Rachel, additional, Bedding, Megan, additional, Forrester, Andrew, additional, Giannulli, Laura, additional, Ginsberg, Ylva, additional, Howitt, Sheila, additional, Kretzschmar, Imogen, additional, Lawrie, Stephen, additional, Marsh, Craig, additional, Kelly, Caroline, additional, Mansfield, Megan, additional, McCafferty, Clare, additional, Khan, Khuram, additional, Müller-Sedgwick, Ulrich, additional, Strang, John, additional, Williamson, Grace, additional, Wilson, Lauren, additional, Young, Susan, additional, Landau, Sabine, additional, and Thomson, Lindsay, additional

Published

2022

4. Randomised controlled trial of the short-term effects of osmotic-release oral system methylphenidate on symptoms and behavioural outcomes in young male prisoners with attention deficit hyperactivity disorder: CIAO-II study.

Author

Asherson, Philip J., Johansson, Lena, Holland, Rachel, Bedding, Megan, Forrester, Andrew, Giannulli, Laura, Ginsberg, Ylva, Howitt, Sheila, Kretzschmar, Imogen, Lawrie, Stephen M., Marsh, Craig, Kelly, Caroline, Mansfield, Megan, McCafferty, Clare, Khan, Khuram, Müller-Sedgwick, Ulrich, Strang, John, Williamson, Grace, Wilson, Lauren, and Young, Susan

Subjects

ATTENTION-deficit hyperactivity disorder, RANDOMIZED controlled trials, METHYLPHENIDATE, MENTAL illness, MIND-wandering, YOUNG adults

Abstract

Background: Research has shown that 20–30% of prisoners meet the diagnostic criteria for attention-deficit hyperactivity disorder (ADHD). Methylphenidate reduces ADHD symptoms, but effects in prisoners are uncertain because of comorbid mental health and substance use disorders. Aims: To estimate the efficacy of an osmotic-release oral system methylphenidate (OROS-methylphenidate) in reducing ADHD symptoms in young adult prisoners with ADHD. Method: We conducted an 8-week parallel-arm, double-blind, randomised placebo-controlled trial of OROS-methylphenidate versus placebo in male prisoners (aged 16–25 years) meeting the DSM-5 criteria for ADHD. Primary outcome was ADHD symptoms at 8 weeks, using the investigator-rated Connors Adult ADHD Rating Scale (CAARS-O). Thirteen secondary outcomes were measured, including emotional dysregulation, mind wandering, violent attitudes, mental health symptoms, and prison officer and educational staff ratings of behaviour and aggression. Results: In the OROS-methylphenidate arm, mean CAARS-O score at 8 weeks was estimated to be reduced by 0.57 points relative to the placebo arm (95% CI −2.41 to 3.56), and non-significant. The responder rate, defined as a 20% reduction in CAARS-O score, was 48.3% for the OROS-methylphenidate arm and 47.9% for the placebo arm. No statistically significant trial arm differences were detected for any of the secondary outcomes. Mean final titrated dose was 53.8 mg in the OROS-methylphenidate arm. Conclusions: ADHD symptoms did not respond to OROS-methylphenidate in young adult prisoners. The findings do not support routine treatment with OROS-methylphenidate in this population. Further research is needed to evaluate effects of higher average dosing and adherence to treatment, multi-modal treatments and preventative interventions in the community. [ABSTRACT FROM AUTHOR]

Published

2023

5. Randomised Controlled Trial of the Short-Term Effects of OROS-Methylphenidate on ADHD Symptoms and Behavioural Outcomes in Young Male Prisoners with Attention Deficit Hyperactivity Disorder (CIAO-II)

Author

Asherson, Philip, primary, Johansson, Lena, additional, Holland, R., additional, Bedding, Megan, additional, Forrester, A., additional, Giannulli, Laura, additional, Ginsberg, Ylva, additional, Howitt, Sheila, additional, Kretzschmar, Imogen, additional, Lawrie, Stephen, additional, Marsh, Craig, additional, Kelly, C., additional, Mansfield, Megan, additional, McCafferty, Clare, additional, Khan, K., additional, Muller-Sedgwick, Ulrich, additional, Strang, J., additional, Williamson, Grace, additional, Wilson, L., additional, Young, S., additional, Landau, Sabine, additional, and Thomson, Lindsay, additional

Published

2021

6. Mental health in the Republic of The Gambia

Author

Kretzschmar, Imogen, primary, Nyan, Ousman, additional, Mendy, Ann Marie, additional, and Janneh, Bamba, additional

Published

2012

7. An optimal trauma-informed pathway for PTSD, complex PTSD and other mental health and psychosocial impacts of trauma in prisons: an expert consensus statement.

Author

Crole-Rees, Clare, Tomlin, Jack, Kalebic, Natasha, Argent, Sarah, Berrington, Claudia, Chaplin, Edward, Davies, Jason, Hoskins, Matthew, James, Lucie, Jarrett, Manuela, John, Oliver, Jones, Lewis, Kothari, Radha, Kretzschmar, Imogen, MacManus, Deirdre, Martin, Michael, McKinnon, Iain, O'Connor, Gwen, Petrillo, Madeline, and Phillips, Marie

Subjects

*POST-traumatic stress disorder, *DISEASE prevalence, *TRAUMA-informed practice, *TRAUMA-informed care, *MENTAL health

Abstract

People in prisons have high levels of trauma exposure throughout their lives. Presentations are often complex, with a high prevalence of PTSD and CPTSD and other mental health comorbidities. Prisons themselves can be stressful and traumatising environments. There are challenges in the delivery of effective treatments for PTSD and CPTSD. There is a need for the development of effective clinical pathways for these conditions that are embedded within trauma-informed organisational approaches. Responding to this need, this report is the result of a multidisciplinary expert consensus meeting and review of the research literature on PTSD, CPTSD, associated comorbidities and optimal approaches to trauma-informed practice. The group consisted of 24 expert representatives from psychology, psychiatry, healthcare, academia, social care and Welsh Government. The meeting commenced with presentations on various aspects of the clinical pathway for PTSD and complex PTSD in prisons, and of applications of trauma-informed practice within prisons. Small sub-groups then provided practical recommendations and solutions relevant to their assigned topic. Findings were presented to all meeting attendees for another round of discussion and debate, until consensus was reached. The resulting recommendations provide guidance to improve identification, treatment and support for people living in prison who have experienced trauma. [ABSTRACT FROM AUTHOR]

Published

2024

8. OROS-methylphenidate to reduce ADHD symptoms in male prisoners aged 16–25 years: a RCT

Author

Asherson P, Johansson L, Holland R, Bedding M, Forrester A, Giannulli L, Ginsberg Y, Howitt S, Kretzschmar I, Lawrie S, Marsh C, Kelly C, Mansfield M, McCafferty C, Khan K, Müller-Sedgwick U, Strang J, Williamson G, Wilson L, Young S, Landau S, and Thomson L

Abstract

Background: It is estimated that 20–30% of prisoners meet diagnostic criteria for attention deficit hyperactivity disorder (ADHD). Methylphenidate reduces ADHD symptoms, but its effect among prisoners remains uncertain., Objectives: The primary objective was to estimate the efficacy of osmotic release oral system (OROS) methylphenidate in reducing ADHD symptoms in male prisoners aged 16–25 years who met diagnostic criteria for ADHD. Secondary objectives investigated change for associated clinical and behavioural problems and the role of ADHD symptoms in mediating change in behaviour., Design: A Phase IV, 8-week, parallel-arm, double-blind, randomised, placebo-controlled trial of OROS-methylphenidate, compared with placebo, in young male adult prisoners with ADHD. Participants were randomised in a 1 : 1 ratio of OROS-methylphenidate to placebo, stratified by prison., Setting: Participants were recruited from Her Majesty’s Prison and Young Offender Institution Isis (London, England) and Her Majesty’s Young Offender Institution Polmont (Falkirk, Scotland)., Participants: The participants were 200 male prisoners with ADHD aged 16–25 years who met the diagnostic criteria for ADHD. Exclusion criteria included moderate or severe learning disability; serious risk of violence to researchers; current major depression, psychosis, mania or hypomania, or a past history of bipolar disorder or schizophrenia; and drug-seeking behaviour that was of sufficient severity to affect the titration protocol., Intervention: The intervention was overencapsulated OROS-methylphenidate (18 mg) or placebo capsules. Trial medication was titrated weekly for 5 weeks against symptom reduction and adverse effects to a final dose of one to four capsules per day, followed by a stable dose for 3 weeks., Main Outcome Measures: The primary outcome was ADHD symptoms at 8 weeks using the investigator-rated Conners’ Adult ADHD Rating Scale-Observer. There were 13 secondary outcomes, including measures of emotional dysregulation, general psychopathology, reports of behaviour by prison staff and engagement with educational activities., Results: For the primary outcome, the estimated improvement between the OROS-methylphenidate and placebo arms was 0.57 points on the Conners’ Adult ADHD Rating Scale-Observer (95% confidence interval –2.41 to 3.56) at 8 weeks, with a standardised effect size of 0.06. The difference was not statistically significant and was smaller than the difference the trial was powered to detect. Responder rate, defined as a 20% reduction in the Conners’ Adult ADHD Rating Scale-Observer score, was 48.3% for the OROS-methylphenidate arm and 47.9% for the placebo arm. None of the 13 secondary outcomes that could be formally compared between the trial arms showed a significant effect and no mediators of change in behaviour were identified., Limitations: Low adherence to trial medication and low medication dose might have affected the results., Conclusion: OROS-methylphenidate was not found to have an effect, compared with placebo, on the primary and secondary outcomes investigated. The findings indicate that ADHD symptoms do not respond to a standard treatment for ADHD following titration to low doses in young adults in prison. The findings do not support the routine treatment with OROS-methylphenidate of young adult prisoners meeting diagnostic criteria for ADHD., Future Research: Investigations of adequate, maintained dosing, non-pharmacological interventions and community studies are suggested., Trial Registration: This trial is registered as ISRCTN16827947 and EudraCT 2015-004271-78., Funding: This project was funded by the Efficacy and Mechanism Evaluation (EME) programme, a MRC and National Institute for Health and Care Research (NIHR) partnership. Janssen-Cilag Ltd supplied OROS-MPH (Concerta-XL). This will be published in full in Efficacy and Mechanism Evaluation ; Vol. 9, No. 6. See the NIHR Journals Library website for further project information., (Copyright © 2022 Asherson et al. This work was produced by Asherson et al. under the terms of a commissioning contract issued by the Secretary of State for Health and Social Care. This is an Open Access publication distributed under the terms of the Creative Commons Attribution CC BY 4.0 licence, which permits unrestricted use, distribution, reproduction and adaption in any medium and for any purpose provided that it is properly attributed. See: https://creativecommons.org/licenses/by/4.0/. For attribution the title, original author(s), the publication source – NIHR Journals Library, and the DOI of the publication must be cited.)

Published

2022