Possible selves in early psychosis : the role of the self-concept in adjustment to severe mental illness

Day, Michael

January 1999

No description available.

150

Psychotic

Schizoaffective disorder in an acute psychiatric unit: profile of users and agreement of diagnosis with operational criteria (OPCRIT)

Singh, Ryola Rangi

08 April 2014

Schizoaffective Disorder remains poorly understood. Experts still disagree on whether it is a discrete disorder; whether it exists on a spectrum between Bipolar Disorder and Schizophrenia or whether it even exists. Objectives: The study aimed to describe the demographic, clinical and treatment profile of mental health care users (MHCUs) diagnosed with Schizoaffective Disorder at a regional hospital (Helen Joseph Hospital) in Johannesburg, Gauteng. It also aimed to determine the degree of agreement between the clinicians‟ diagnosis and Operational Criteria (OPCRIT). Methods: All MHCUs at Helen Joseph Hospital psychiatric unit with a discharge diagnosis of Schizoaffective Disorder between January 2004 and December 2010 were included. The demographic, clinical and treatment profiles as well as data required for OPCRIT were extracted from hospital records and discharge summaries. Results: The main findings were that most MHCUs diagnosed with Schizoaffective Disorder were female with a mean age of illness onset of 25 years; had impaired social, occupational and interpersonal functioning; had a family history of mood disorders; were non-adherent on admission and were treated with at least 1 antipsychotic and 1 mood stabiliser. Also, there was no agreement between the clinicians‟ diagnosis and OPCRIT. Conclusion: More rigorous research is needed to accurately describe the profile of MHCUs diagnosed with Schizoaffective Disorder to improve understanding and management of their condition.

Psychotic Disorders

Cognitive therapy and recovery from acute psychosis : a randomised controlled trial

Drury, Valerie

January 1999

No description available.

150

Psychotic disorders

The neuropsychology and functional anatomy of verbal fluency in the major psychoses

Dixon, Tracy Anne

January 2000

No description available.

610

Schizophrenia; Psychotic illness

Distribution and regulation of neuropeptide Y and its receptors in the human and rat brain : role in affective disorders /

Caberlotto, Laura,

January 1900

Diss. (sammanfattning) Stockholm : Karol. inst. / Härtill 7 uppsatser.

State and trait measures in the affective disorders /

Svanborg, Pär,

January 1900

Diss. (sammanfattning) Stockholm : Karol. inst. / Härtill 6 uppsatser.

Mortality in schizophrenia and affective disorder /

Ösby, Urban,

January 1900

Diss. (sammanfattning) Stockholm : Karol. inst. / Härtill 5 uppsatser.

Evaluating clinicians’ differential diagnostic decisions for ICD-11 psychotic disorders

Peterson, Destiny Lynn

09 May 2015

The ICD is currently under revision and this study is the first phase of the electronic field trials for ICD-11 for psychotic disorders. The present study compared ICD-10 and ICD-11 with regards to changes made to the diagnostic guidelines and changes amongst specific disorders. Of specific interest was clinicians’ ability to accurately diagnose disorders that can present with overlapping features. We found that both diagnostic systems were accurate in differentiating disorders that have the potential to be easily confused. For some of the diagnostic guidelines that were undergoing substantial changes from ICD-10 to ICD-11, we did find improvements in the proposed guidelines. Subsequent studies will expand on our findings prior to the release of ICD-11. However, based on our initial findings, the proposed changes do appear to be increasing clinical utility of the diagnostic guidelines.

diagnosis

ICD

psychotic disorders

The impact of adolescence initiated alcohol and cannabis abuse/ dependence on the level of activity participation in adult males suffering from a pyschotic disorder

Wolhuter, Kristyn Ashleigh

January 2014

A research report submitted to the Faculty of Health Sciences, University of the Witwatersrand, Johannesburg, in partial fulfilment of the requirements for the degree of Master of Science in Occupational Therapy Johannesburg, 2014. / Background: Individuals suffering from both a psychotic disorder and a substance abuse disorder have shown to have poorer occupational outcomes. This study aimed at determining the exact consequences of substance abuse on occupational performance in order to tailor more specific treatment interventions in the future. Methodology: A non-experimental design and observational study was used. This involved a once off occupational therapy assessment using the Activity Participation Outcome Measure (APOM) as the recoding tool. The participants were divided into three groups: Alcohol abuse, cannabis abuse and no substance abuse. Methodology: A non-experimental design and observational study was used. This involved a once off occupational therapy assessment using the Activity Participation Outcome Measure (APOM) as the recoding tool. The participants were divided into three groups: Alcohol abuse, cannabis abuse and no substance abuse. Results: A statistically significant difference was noted between the alcohol and cannabis groups. The alcohol group achieved a higher level of activity participation in all eight APOM domains (Role performance, life skills, communication, motivation, process skills, self esteem, balanced lifestyle, and affect). The no substance abuse group (individuals diagnosed with schizophrenia) showed the lowest level of activity participation. Conclusion: Cannabis adolescent abuse/dependence appears to have a more negative impact on activity participation when compared to alcohol abuse.

Marijuana Abuse

Alcoholism

Psychotic Disorders

A dual oral intestinal film for pulsatile release of a mood stabilizing agent in the treatment of schizoaffective disorder

Hoosain, Famida Ghulam

January 2016

A thesis submitted to the Faculty of Health Sciences, University of the Witwatersrand, Johannesburg, in fulfilment of the requirements for the degree of Doctor of Philosophy Johannesburg, 2016 / Oral drug delivery is acknowledged by many as the idyllic method of drug delivery due to its versatility and convenience of administration. Nevertheless, the bioavailability of drugs delivered via the oral route remains disputed. Classically, conventional marketed drug delivery systems release drugs in inconstant and unpredictable manners, leading to sub-therapeutic and in some cases toxic drug doses. Consequently, patient compliance is compromised, in turn having an effect on the success of the therapeutic intervention in question. One such limitation occurs in the treatment of Schizophrenia, with patients unable to comply with treatment due to multiple administration requirements. Sulpiride, an antipsychotic agent, displays notable efficiency in reducing both positive and negative symptoms of Schizophrenia. However, sulpiride has a low bioavailability and thus therapy requires the use of large doses, and hence multiple administrations. In addition, a large percentage of Schizophrenic patients present with concomitant mood disorders, namely ‘Schizoaffective’ disorder, which further necessitates the use of mood stabilizing agents. As a result, patients end up with a huge pill burden and are unable to comply with therapy and this leads to reduced clinical outcomes. A dual layered, xerogel-bioadhesive intestinal patch drug delivery system (ODLS) was thus designed, formulated, and evaluated for the site-specific delivery of two bioactives in the treatment of Schizophrenia with concomitant mood disorders in a time controlled-idiosyncratic manner. Ultimately easing compliance to complicated treatment regimens, enhancing bioavailability and improving patient compliance. The ODLS essentially comprises of a bi-layered tablet, layer one comprised of a sustained release semi-interpenetrating polymer network (s-IPN) xerogel and a layer two of embedded pulsatile release bioadhesive intestinal patches, with the system as a whole enteric coated for protection. Intestinal patches encompassed in layer two are fabricated of a backing layer, a drug loaded layer, a mucoadhesive layer, and a mucus cleaving layer. The ODLS employs a combination of sustained and pulsatile drug release mechanisms, in addition to intestinal retentive mechanisms. Furthermore, the system physically protects the drug delivery system from acidic or proteolytic degradation within the human gastro-intestinal tract. The present study utilized the use of bioadhesion for site-specific and gastro retentive drug delivery, with crosslinking being employed for rate-modulated drug delivery. Sulpiride and sodium valproate were selected as model drugs for the sustained release xerogel layer and the pulsatile bioadhesive patch layer respectively in this study as sulpiride is an antipsychotic with low bioavailability yet good antipsychotic activity and sodium valproate is the mainstay drug treatment for mood disorders in schizophrenia. Therefore, sulpiride would profit from the sustained release as it would improve bioavailability and hence patient compliance, whereas sodium valproate would benefit from the pulsatile release so as to avoid the well-known resistance to therapy due to prolonged exposure to drug. Thus these drugs would gain benefit from the site-specific controlled drug delivery offered by the ODLS. The primary aim of the sustained release s-IPN xerogel was to ensure delayed release of drug over 24 hours thus decreasing the need for multiple administrations and to maintain a steady state drug concentration. Film casting, a versatile technique was utilized in the fabrication of polymeric films to develop the bioadhesive intestinal patches. Preliminary in vitro investigations led to identification of a combination of polymers and crosslinking agent best suited to develop the system. A central composite design was employed for system optimization. The xerogel layer demonstrated that zero-order drug release was achieved after the crosslinking procedure. Delayed drug release fundamentally decreases the number of doses required daily and thus patient compliance and clinical efficacy is improved. The pulsatile release layer displayed distinct triphasic drug release after assembly of the intestinal patches, pulsatile release of drugs fundamentally reduced resistance to drug therapy as well as reducing pill burden. Furthermore, in vitro analysis of the ODLS showed that the xerogel layer behaved superiorly in terms of controlling drug delivery in a site-specific and prolonged fashion in comparison to a marketed gold standard. There exists no gold standard for pulsatile delivery of sodium valproate hence the pulsatile layer was tested against the marketed standard administered as a single dose. In vitro findings were substantiated by in vivo analysis in a white pig model. Results indicated that the systemic bioavailability of sulpiride was higher than the gold standard and drug release was prolonged in a zero-order fashion over 24 hours. Sodium valproate released in a triphasic manner over 24 hours thus reducing the risk of treatment resistance and decreased pill burden. To summarize, the ODLS was able to overcome the many challenges associated with oral drug delivery in schizoaffective disorder, by simplification of complicated treatment regimens, and hence improving bioavailability of drug delivery orally. The benefits associated with oral drug delivery have evidently been exploited by the present study, producing a versatile drug delivery system which can successfully deliver two bioactives simultaneously via individualistic release patterns, thus treating both conditions with a single oral dosage form with a single daily administration. / MT2016

Psychotic Disorders

Drug Delivery Systems