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5. Longitudinal clinical and functional outcome in distinct cognitive subgroups of first-episode psychosis:a cluster analysis

Author

Oomen, Priscilla P., Begemann, Marieke J. H., Brand, Bodyl A., de Haan, Lieuwe, Veling, Wim, Koops, Sanne, van Os, Jim, Smit, Filip, Bakker, P. Roberto, van Beveren, Nico, Boonstra, Nynke, Guloksuz, Sinan, Kikkert, Martijn, Lokkerbol, Joran, Marcelis, Machteld, Rosema, Bram-Sieben, de Beer, Franciska, Gangadin, Shiral S., Geraets, Chris N. W., van't Hag, Erna, Haveman, Yudith, van der Heijden, Inge, Voppel, Alban E., Willemse, Elske, van Amelsvoort, Therese, Bak, Maarten, Batalla, Albert, Been, Agaath, van den Bosch, Marinte, van den Brink, Truus, Faber, Gunnar, Grootens, Koen P., de Jonge, Martin, Knegtering, Rikus, Kurkamp, Jorg, Mahabir, Amrita, Pijnenborg, Gerdina H. M., Staring, Tonnie, Veen, Natalie, Veerman, Selene, Wiersma, Sybren, Graveland, Ellen, Hoornaar, Joelle, Sommer, Iris E. C., Oomen, Priscilla P., Begemann, Marieke J. H., Brand, Bodyl A., de Haan, Lieuwe, Veling, Wim, Koops, Sanne, van Os, Jim, Smit, Filip, Bakker, P. Roberto, van Beveren, Nico, Boonstra, Nynke, Guloksuz, Sinan, Kikkert, Martijn, Lokkerbol, Joran, Marcelis, Machteld, Rosema, Bram-Sieben, de Beer, Franciska, Gangadin, Shiral S., Geraets, Chris N. W., van't Hag, Erna, Haveman, Yudith, van der Heijden, Inge, Voppel, Alban E., Willemse, Elske, van Amelsvoort, Therese, Bak, Maarten, Batalla, Albert, Been, Agaath, van den Bosch, Marinte, van den Brink, Truus, Faber, Gunnar, Grootens, Koen P., de Jonge, Martin, Knegtering, Rikus, Kurkamp, Jorg, Mahabir, Amrita, Pijnenborg, Gerdina H. M., Staring, Tonnie, Veen, Natalie, Veerman, Selene, Wiersma, Sybren, Graveland, Ellen, Hoornaar, Joelle, and Sommer, Iris E. C.

Abstract

Background Cognitive deficits may be characteristic for only a subgroup of first-episode psychosis (FEP) and the link with clinical and functional outcomes is less profound than previously thought. This study aimed to identify cognitive subgroups in a large sample of FEP using a clustering approach with healthy controls as a reference group, subsequently linking cognitive subgroups to clinical and functional outcomes. Methods 204 FEP patients were included. Hierarchical cluster analysis was performed using baseline brief assessment of cognition in schizophrenia (BACS). Cognitive subgroups were compared to 40 controls and linked to longitudinal clinical and functional outcomes (PANSS, GAF, self-reported WHODAS 2.0) up to 12-month follow-up. Results Three distinct cognitive clusters emerged: relative to controls, we found one cluster with preserved cognition (n = 76), one moderately impaired cluster (n = 74) and one severely impaired cluster (n = 54). Patients with severely impaired cognition had more severe clinical symptoms at baseline, 6- and 12-month follow-up as compared to patients with preserved cognition. General functioning (GAF) in the severely impaired cluster was significantly lower than in those with preserved cognition at baseline and showed trend-level effects at 6- and 12-month follow-up. No significant differences in self-reported functional outcome (WHODAS 2.0) were present. Conclusions Current results demonstrate the existence of three distinct cognitive subgroups, corresponding with clinical outcome at baseline, 6- and 12-month follow-up. Importantly, the cognitively preserved subgroup was larger than the severely impaired group. Early identification of discrete cognitive profiles can offer valuable information about the clinical outcome but may not be relevant in predicting self-reported functional outcomes.

Published
2023

6. Longitudinal clinical and functional outcome in distinct cognitive subgroups of first-episode psychosis: a cluster analysis

Author

Onderzoeksgroep 2, Brain, Hersenen-Medisch 1, Oomen, Priscilla P, Begemann, Marieke J H, Brand, Bodyl A, de Haan, Lieuwe, Veling, Wim, Koops, Sanne, van Os, Jim, Smit, Filip, Bakker, P Roberto, van Beveren, Nico, Boonstra, Nynke, Gülöksüz, Sinan, Kikkert, Martijn, Lokkerbol, Joran, Marcelis, Machteld, Rosema, Bram-Sieben, de Beer, Franciska, Gangadin, Shiral S, Geraets, Chris N W, van 't Hag, Erna, Haveman, Yudith, van der Heijden, Inge, Voppel, Alban E, Willemse, Elske, van Amelsvoort, Therese, Bak, Maarten, Batalla, Albert, Been, Agaath, van den Bosch, Marinte, van den Brink, Truus, Faber, Gunnar, Grootens, Koen P, de Jonge, Martin, Knegtering, Rikus, Kurkamp, Jörg, Mahabir, Amrita, Pijnenborg, Gerdina H M, Staring, Tonnie, Veen, Natalie, Veerman, Selene, Wiersma, Sybren, Graveland, Ellen, Hoornaar, Joelle, Sommer, Iris E C, Onderzoeksgroep 2, Brain, Hersenen-Medisch 1, Oomen, Priscilla P, Begemann, Marieke J H, Brand, Bodyl A, de Haan, Lieuwe, Veling, Wim, Koops, Sanne, van Os, Jim, Smit, Filip, Bakker, P Roberto, van Beveren, Nico, Boonstra, Nynke, Gülöksüz, Sinan, Kikkert, Martijn, Lokkerbol, Joran, Marcelis, Machteld, Rosema, Bram-Sieben, de Beer, Franciska, Gangadin, Shiral S, Geraets, Chris N W, van 't Hag, Erna, Haveman, Yudith, van der Heijden, Inge, Voppel, Alban E, Willemse, Elske, van Amelsvoort, Therese, Bak, Maarten, Batalla, Albert, Been, Agaath, van den Bosch, Marinte, van den Brink, Truus, Faber, Gunnar, Grootens, Koen P, de Jonge, Martin, Knegtering, Rikus, Kurkamp, Jörg, Mahabir, Amrita, Pijnenborg, Gerdina H M, Staring, Tonnie, Veen, Natalie, Veerman, Selene, Wiersma, Sybren, Graveland, Ellen, Hoornaar, Joelle, and Sommer, Iris E C

Published
2023

7. Longitudinal clinical and functional outcome in distinct cognitive subgroups of first-episode psychosis: a cluster analysis.

Author

Oomen, Priscilla P., Begemann, Marieke J. H., Brand, Bodyl A., de Haan, Lieuwe, Veling, Wim, Koops, Sanne, van Os, Jim, Smit, Filip, Bakker, P. Roberto, van Beveren, Nico, Boonstra, Nynke, Gülöksüz, Sinan, Kikkert, Martijn, Lokkerbol, Joran, Marcelis, Machteld, Rosema, Bram-Sieben, de Beer, Franciska, Gangadin, Shiral S., Geraets, Chris N. W., and van 't Hag, Erna

Subjects
COGNITION disorders, PSYCHOSES, FUNCTIONAL status, SCHIZOPHRENIA, SELF-evaluation, TREATMENT effectiveness, COMPARATIVE studies, DESCRIPTIVE statistics, CLUSTER analysis (Statistics), LONGITUDINAL method
Abstract

Background: Cognitive deficits may be characteristic for only a subgroup of first-episode psychosis (FEP) and the link with clinical and functional outcomes is less profound than previously thought. This study aimed to identify cognitive subgroups in a large sample of FEP using a clustering approach with healthy controls as a reference group, subsequently linking cognitive subgroups to clinical and functional outcomes. Methods: 204 FEP patients were included. Hierarchical cluster analysis was performed using baseline brief assessment of cognition in schizophrenia (BACS). Cognitive subgroups were compared to 40 controls and linked to longitudinal clinical and functional outcomes (PANSS, GAF, self-reported WHODAS 2.0) up to 12-month follow-up. Results: Three distinct cognitive clusters emerged: relative to controls, we found one cluster with preserved cognition (n = 76), one moderately impaired cluster (n = 74) and one severely impaired cluster (n = 54). Patients with severely impaired cognition had more severe clinical symptoms at baseline, 6- and 12-month follow-up as compared to patients with preserved cognition. General functioning (GAF) in the severely impaired cluster was significantly lower than in those with preserved cognition at baseline and showed trend-level effects at 6- and 12-month follow-up. No significant differences in self-reported functional outcome (WHODAS 2.0) were present. Conclusions: Current results demonstrate the existence of three distinct cognitive subgroups, corresponding with clinical outcome at baseline, 6- and 12-month follow-up. Importantly, the cognitively preserved subgroup was larger than the severely impaired group. Early identification of discrete cognitive profiles can offer valuable information about the clinical outcome but may not be relevant in predicting self-reported functional outcomes. [ABSTRACT FROM AUTHOR]

Published
2023
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9. Longitudinal clinical and functional outcome in distinct cognitive subgroups of first-episode psychosis: a cluster analysis

Author

Oomen, Priscilla P., primary, Begemann, Marieke J. H., additional, Brand, Bodyl A., additional, de Haan, Lieuwe, additional, Veling, Wim, additional, Koops, Sanne, additional, van Os, Jim, additional, Smit, Filip, additional, Bakker, P. Roberto, additional, van Beveren, Nico, additional, Boonstra, Nynke, additional, Gülöksüz, Sinan, additional, Kikkert, Martijn, additional, Lokkerbol, Joran, additional, Marcelis, Machteld, additional, Rosema, Bram-Sieben, additional, de Beer, Franciska, additional, Gangadin, Shiral S., additional, Geraets, Chris N. W., additional, van ‘t Hag, Erna, additional, Haveman, Yudith, additional, van der Heijden, Inge, additional, Voppel, Alban E., additional, Willemse, Elske, additional, van Amelsvoort, Therese, additional, Bak, Maarten, additional, Batalla, Albert, additional, Been, Agaath, additional, van den Bosch, Marinte, additional, van den Brink, Truus, additional, Faber, Gunnar, additional, Grootens, Koen P., additional, de Jonge, Martin, additional, Knegtering, Rikus, additional, Kurkamp, Jörg, additional, Mahabir, Amrita, additional, Pijnenborg, Gerdina H. M., additional, Staring, Tonnie, additional, Veen, Natalie, additional, Veerman, Selene, additional, Wiersma, Sybren, additional, Graveland, Ellen, additional, Hoornaar, Joelle, additional, and Sommer, Iris E. C., additional

Published
2021
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10. Antipsychotic medication for women with schizophrenia spectrum disorders.

Author

Brand, Bodyl A., Haveman, Yudith R. A., de Beer, Franciska, de Boer, Janna N., Dazzan, Paola, and Sommer, Iris E. C.

Subjects
DRUG therapy for schizophrenia, DRUG efficacy, PERIMENOPAUSE, DRUG tolerance, QUETIAPINE, MENSTRUATION, SEX distribution, OLANZAPINE, POSTMENOPAUSE, ANTIPSYCHOTIC agents, WOMEN'S health, PHARMACODYNAMICS
Abstract

There are significant differences between men and women in the efficacy and tolerability of antipsychotic drugs. Here, we provide a comprehensive overview of what is currently known about the pharmacokinetics and pharmacodynamics of antipsychotics in women with schizophrenia spectrum disorders (SSDs) and translate these insights into considerations for clinical practice. Slower drug absorption, metabolism and excretion in women all lead to higher plasma levels, which increase the risk for side-effects. Moreover, women reach higher dopamine receptor occupancy compared to men at similar serum levels, since oestrogens increase dopamine sensitivity. As current treatment guidelines are based on studies predominantly conducted in men, women are likely to be overmedicated by default. The risk of overmedicating generally increases when sex hormone levels are high (e.g. during ovulation and gestation), whereas higher doses may be required during low-hormonal phases (e.g. during menstruation and menopause). For premenopausal women, with the exceptions of quetiapine and lurasidone, doses of antipsychotics should be lower with largest adjustments required for olanzapine. Clinicians should be wary of side-effects that are particularly harmful in women, such as hyperprolactinaemia which can cause oestrogen deficiency and metabolic symptoms that may cause cardiovascular diseases. Given the protective effects of oestrogens on the course of SSD, oestrogen replacement therapy should be considered for postmenopausal patients, who are more vulnerable to side-effects and yet require higher dosages of most antipsychotics to reach similar efficacy. In conclusion, there is a need for tailored, female-specific prescription guidelines, which take into account adjustments required across different phases of life. [ABSTRACT FROM AUTHOR]

Published
2022
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12. Evaluation of selected dye compounds as inhibitors of monoamine oxidase

Author

De Beer, Franciska, Petzer, A., Petzer, J.P., 12264954 - Petzer, Anél (Supervisor), 10727388 - Petzer, Jacobus Petrus (Supervisor), and 12264954 - Petzer, Anél (Supervisor)||10727388 - Petzer, Jacobus Petrus (Supervisor)

Subjects
Darrow red, Methylene blue, Monoamine oxidase, Parkinson’s disease, Acridine orange, Oxazine 170, Alzheimer’s disease, Serotonin toxicity, Inhibition
Abstract

MSc (Pharmaceutical Chemistry), North-West University, Potchefstroom Campus Parkinson’s disease (PD) and Alzheimer’s disease (AD) are neurodegenerative diseases that significantly impact the quality of life of patients. The pathology of Parkinson’s disease is characterised by neuronal death of the nigrostriatal dopaminergic nerve terminals as well as the formation of Lewy bodies. The activity of monoamine oxidase (MAO) B increases in patients diagnosed with Parkinson’s diseases as they age resulting in oxidative stress, which in turn may lead to mitochondrial dysfunction as well as protein aggregation and misfolding. The pathology of Alzheimer’s disease includes the formation of amyloid plaques and neurofibrillary tangles (NFT). The aetiologies of these neurodegenerative diseases are still unknown. Current treatments are based on the presenting pathogenesis and symptoms of the respective diseases. Therefore, there is no treatment that stops or reverses neurodegeneration in Parkinson’s disease and Alzheimer’s disease and current treatment focuses on alleviating the symptoms. The MAO enzyme is involved in the pathogenesis of Parkinson’s disease and Alzheimer’s disease. MAO metabolises various neurotransmitters including noradrenaline (NA), dopamine (DA) and serotonin (5-HT). MAO is implicated in several neurodegenerative diseases due to the generation of reactive oxygen species (ROS) and participation in key pathological pathways. Monoamine oxidase type B (MAO-B) inhibition can be beneficial for the treatment of Parkinson’s diseases as well as Alzheimer’s disease. The current use of monoamine oxidase type A (MAO-A) inhibitors to treat depression is well documented. It is important to note that potent MAO-A inhibitors and serotonergic drugs should not be administered together as this can possibly induce serotonin toxicity. Caution should also be exercised with the use of potent irreversible inhibitors of MAO-A as they present with a higher occurrence of the “cheese reaction”. The dye compound methylene blue (MB), has shown promise as a therapeutic agent in studies conducted on Alzheimer’s disease and depression. Of particular interest is the ability of methylene blue to inhibit MAO. It was found that methylene blue as well as azure B, the major metabolite of methylene blue, potently inhibit MAO-A. It was also found that certain structural analogues of methylene blue also are good potency MAO-A inhibitors. For example, the dye compounds cresyl violet (IC50 = 0.0037 μM), Nile blue (IC50 = 0.0077 μM) and 1,9-dimethyl methylene blue (DMMB) (IC50 = 0.018 μM) are high potency MAO-A inhibitors. Due to the high potency MAO-A inhibition associated with these dye compounds, the present study investigated 22 commercially available dyes, that are similar in structure to methylene blue, as potential human MAO-A and MAO-B inhibitors. The inhibition potencies of the selected 22 dye compounds were determined by using recombinant human MAO-A and MAO-B enzymes. The IC50 values of the dyes were determined and were used as a measure of inhibition potency. Based on the IC50 values, acridine orange, oxazine 170 and Darrow red were identified as the highest potency inhibitors of this study. These compounds were subjected to further studies to determine the reversibility and mode of inhibition by means of dialysis and the construction of Lineweaver-Burk plots, respectively. It was found that acridine orange is a competitive and reversible inhibitor specific for MAO-A (IC50 = 0.017 μM). Oxazine 170 was identified as a competitive and reversible inhibitor specific for MAO-B (IC50 = 0.0065 μM). Darrow red exhibited competitive and reversible inhibition of MAO with specificity for neither of the isoforms (MAO-A, IC50 = 0.059 μM; MAO-B, IC50 = 0.065 μM). When compared to methylene blue (MAO-A, IC50 = 0.07 μM; MAO-B, IC50 = 4.37 μM), acridine orange and Darrow red exhibited more potent inhibition of MAO-A. The MAO-B inhibition potencies of oxazine 170 and Darrow red were also found to be higher than that of methylene blue. In conclusion, the MAO isoforms are implicated in the pathology of neurodegenerative and neuropsychiatric diseases such as Alzheimer’s disease, Parkinson’s disease and depression. Therefore, MAO is a viable and important target for possible medical intervention and drug treatments. The results of this study confirmed that some of the dye compounds evaluated in this study possess similar activity profiles to methylene blue. This can be explained by the structural similarity of the dye compounds with methylene blue. The dye compounds identified in this study can therefore be further investigated for possible preclinical development and be used as possible lead compounds to design future MAO inhibitors. Masters

Published
2019

13. Monoamine oxidase inhibition by selected dye compounds

Author

10727388 - Petzer, Jacobus Petrus, 12264954 - Petzer, Anél, De Beer, Franciska, Petzer, Jacobus P., Petzer, Anél, 10727388 - Petzer, Jacobus Petrus, 12264954 - Petzer, Anél, De Beer, Franciska, Petzer, Jacobus P., and Petzer, Anél

Abstract

Monoamine oxidase (MAO) is an important drug target as the MAO isoforms play key roles in neurodegenerative disorders such as Alzheimer's disease and Parkinson's disease, as well as in neuropsychiatric diseases such as depression. Methylene blue is an inhibitor of MAO‐A, while azure B, the major metabolite of methylene blue, and various other structural analogues retain the ability to inhibit MAO‐A. Based on this, the present study evaluated 22 dyes, many of which are structurally related to methylene blue, as potential inhibitors of human MAO‐A and MAO‐B. The results highlighted three dye compounds as good potency competitive and reversible MAO inhibitors, and which exhibit higher MAO inhibition than methylene blue: acridine orange, oxazine 170 and Darrow red. Acridine orange was found to be a MAO‐A specific inhibitor (IC50 = 0.017 μM), whereas oxazine 170 is a MAO‐B specific inhibitor (IC50 = 0.0065 μM). Darrow red was found to be a non‐specific MAO inhibitor (MAO‐A, IC50 = 0.059 μM; MAO‐B, IC50 = 0.065 μM). These compounds may be advanced for further testing and preclinical development, or be used as possible lead compounds for the future design of MAO inhibitors

Published
2019

14. Monoamine oxidase inhibition by selected dye compounds.

Author

de Beer, Franciska, Petzer, Jacobus P., and Petzer, Anél

Subjects
*MONOAMINE oxidase, *METHYLENE blue, *PARKINSON'S disease, *ACRIDINE orange, *OXAZINES, *ALZHEIMER'S disease
Abstract

Monoamine oxidase (MAO) is an important drug target as the MAO isoforms play key roles in neurodegenerative disorders such as Alzheimer's disease and Parkinson's disease, as well as in neuropsychiatric diseases such as depression. Methylene blue is an inhibitor of MAO‐A, while azure B, the major metabolite of methylene blue, and various other structural analogues retain the ability to inhibit MAO‐A. Based on this, the present study evaluated 22 dyes, many of which are structurally related to methylene blue, as potential inhibitors of human MAO‐A and MAO‐B. The results highlighted three dye compounds as good potency competitive and reversible MAO inhibitors, and which exhibit higher MAO inhibition than methylene blue: acridine orange, oxazine 170 and Darrow red. Acridine orange was found to be a MAO‐A specific inhibitor (IC50 = 0.017 μM), whereas oxazine 170 is a MAO‐B specific inhibitor (IC50 = 0.0065 μM). Darrow red was found to be a non‐specific MAO inhibitor (MAO‐A, IC50 = 0.059 μM; MAO‐B, IC50 = 0.065 μM). These compounds may be advanced for further testing and preclinical development, or be used as possible lead compounds for the future design of MAO inhibitors. [ABSTRACT FROM AUTHOR]

Published
2020
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15. [Antipsychotic medication after a first episode of psychosis: taper or continue?]

Author

de Haan L, Gangadin SS, de Beer F, Djordjevic M, Begemann MJH, and Sommer IEC

Subjects
Humans, Male, Young Adult, Decision Making, Shared, Dissent and Disputes, Antipsychotic Agents adverse effects, Psychotic Disorders drug therapy
Abstract

In this paper we discuss the risks and benefits of discontinuing antipsychotic medication within one year after remission of a first episode of psychosis. We start with a fictional case report of a 21-year-old man, who was diagnosed with schizophreniform disorder four months earlier. While symptoms responded well to a daily dose of 10 mg ariprazole, he experienced side effects (tiredness and mild hypersomnia). Three months after symptom remission, he expressed the wish to discontinue his medication. How should psychiatrists respond to his wish? To answer that, we briefly summarize relevant evidence and discuss arguments for the different therapeutic approaches, i.e., maintaining vs. tapering antipsychotic medication, based on specific patient characteristics. Recommendations from the current Dutch guidelines are complemented with personal experience and considerations in finding the optimal balance between side effects, relapse risk, stigma and acceptance of mental health problems, while incorporating the principles of shared decision-making.

Published
2023

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