Your search keyword '"Jonasson, My"' showing total 112 results

1. Acute nicotine exposure blocks aromatase in the limbic brain of healthy women : A [11C]cetrozole PET study

Author

Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, Comasco, Erika, Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, and Comasco, Erika

Abstract

Background: Of interest to women's mental health, a wealth of studies suggests sex differences in nicotine addiction and treatment response, but their psychoneuroendocrine underpinnings remain largely unknown. A pathway involving sex steroids could indeed be involved in the behavioural effects of nicotine, as it was found to inhibit aromatase in vitro and in vivo in rodents and non-human primates, respectively. Aromatase regulates the synthesis of oestrogens and, of relevance to addiction, is highly expressed in the limbic brain. Methods: The present study sought to investigate in vivo aromatase availability in relation to exposure to nicotine in healthy women. Structural magnetic resonance imaging and two [11C]cetrozole positron emission tomography (PET) scans were performed to assess the availability of aromatase before and after administration of nicotine. Gonadal hormones and cotinine levels were measured. Given the region-specific expression of aromatase, a ROI -based approach was employed to assess changes in [11C]cetrozole non-displaceable binding potential. Results: The highest availability of aromatase was found in the right and left thalamus. Upon nicotine exposure, [11C]cetrozole binding in the thalamus was acutely decreased bilaterally (Cohen's d =-0.99). In line, cotinine levels were negatively associated with aromatase availability in the thalamus, although as non-significant trend. Conclusions: These findings indicate acute blocking of aromatase availability by nicotine in the thalamic area. This suggests a new putative mechanism mediating the effects of nicotine on human behaviour, particularly relevant to sex differences in nicotine addiction.

Published

2023

2. Striatal dopamine transporter and receptor availability correlate with relative cerebral blood flow measured with [11C]PE2I, [18F]FE-PE2I and [11C]raclopride PET in healthy individuals

Author

Jonasson, My, Frick, Andreas, Fazio, Patrik, Hjorth, Olof, Danfors, Torsten, Axelsson, Jan, Appel, Lieuwe, Furmark, Tomas, Varrone, Andrea, Lubberink, Mark, Jonasson, My, Frick, Andreas, Fazio, Patrik, Hjorth, Olof, Danfors, Torsten, Axelsson, Jan, Appel, Lieuwe, Furmark, Tomas, Varrone, Andrea, and Lubberink, Mark

Abstract

The aim of this retrospective study was to investigate relationships between relative cerebral blood flow and striatal dopamine transporter and dopamine D2/3 availability in healthy subjects. The data comprised dynamic PET scans with two dopamine transporter tracers [11C]PE2I (n = 20) and [18F]FE-PE2I (n = 20) and the D2/3 tracer [11C]raclopride (n = 18). Subjects with a [11C]PE2I scan also underwent a dynamic scan with the serotonin transporter tracer [11C]DASB. Binding potential (BPND) and relative tracer delivery (R1) values were calculated on regional and voxel-level. Striatal R1 and BPND values were correlated, using either an MRI-based volume of interest (VOI) or an isocontour VOI based on the parametric BPND image. An inter-tracer comparison between [11C]PE2I BPND and [11C]DASB R1 was done on a VOI-level and simulations were performed to investigate whether the constraints of the modeling could cause correlation of the parameters. A positive association was found between BPND and R1 for all three dopamine tracers. A similar correlation was found for the inter-tracer correlation between [11C]PE2I BPND and [11C]DASB R1. Simulations showed that this relationship was not caused by cross-correlation between parameters in the kinetic model. In conclusion, these results suggest an association between resting-state striatal dopamine function and relative blood flow in healthy subjects.

Published

2023

3. Acute nicotine exposure blocks aromatase in the limbic brain of healthy women : A [11C]cetrozole PET study

Author

Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, Comasco, Erika, Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, and Comasco, Erika

Abstract

Background: Of interest to women's mental health, a wealth of studies suggests sex differences in nicotine addiction and treatment response, but their psychoneuroendocrine underpinnings remain largely unknown. A pathway involving sex steroids could indeed be involved in the behavioural effects of nicotine, as it was found to inhibit aromatase in vitro and in vivo in rodents and non-human primates, respectively. Aromatase regulates the synthesis of oestrogens and, of relevance to addiction, is highly expressed in the limbic brain. Methods: The present study sought to investigate in vivo aromatase availability in relation to exposure to nicotine in healthy women. Structural magnetic resonance imaging and two [11C]cetrozole positron emission tomography (PET) scans were performed to assess the availability of aromatase before and after administration of nicotine. Gonadal hormones and cotinine levels were measured. Given the region-specific expression of aromatase, a ROI -based approach was employed to assess changes in [11C]cetrozole non-displaceable binding potential. Results: The highest availability of aromatase was found in the right and left thalamus. Upon nicotine exposure, [11C]cetrozole binding in the thalamus was acutely decreased bilaterally (Cohen's d =-0.99). In line, cotinine levels were negatively associated with aromatase availability in the thalamus, although as non-significant trend. Conclusions: These findings indicate acute blocking of aromatase availability by nicotine in the thalamic area. This suggests a new putative mechanism mediating the effects of nicotine on human behaviour, particularly relevant to sex differences in nicotine addiction.

Published

2023

4. Acute nicotine exposure blocks aromatase in the limbic brain of healthy women : A [11C]cetrozole PET study

Author

Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, Comasco, Erika, Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, and Comasco, Erika

Abstract

Background: Of interest to women's mental health, a wealth of studies suggests sex differences in nicotine addiction and treatment response, but their psychoneuroendocrine underpinnings remain largely unknown. A pathway involving sex steroids could indeed be involved in the behavioural effects of nicotine, as it was found to inhibit aromatase in vitro and in vivo in rodents and non-human primates, respectively. Aromatase regulates the synthesis of oestrogens and, of relevance to addiction, is highly expressed in the limbic brain. Methods: The present study sought to investigate in vivo aromatase availability in relation to exposure to nicotine in healthy women. Structural magnetic resonance imaging and two [11C]cetrozole positron emission tomography (PET) scans were performed to assess the availability of aromatase before and after administration of nicotine. Gonadal hormones and cotinine levels were measured. Given the region-specific expression of aromatase, a ROI -based approach was employed to assess changes in [11C]cetrozole non-displaceable binding potential. Results: The highest availability of aromatase was found in the right and left thalamus. Upon nicotine exposure, [11C]cetrozole binding in the thalamus was acutely decreased bilaterally (Cohen's d =-0.99). In line, cotinine levels were negatively associated with aromatase availability in the thalamus, although as non-significant trend. Conclusions: These findings indicate acute blocking of aromatase availability by nicotine in the thalamic area. This suggests a new putative mechanism mediating the effects of nicotine on human behaviour, particularly relevant to sex differences in nicotine addiction.

Published

2023

5. Striatal dopamine transporter and receptor availability correlate with relative cerebral blood flow measured with [11C]PE2I, [18F]FE-PE2I and [11C]raclopride PET in healthy individuals

Author

Jonasson, My, Frick, Andreas, Fazio, Patrik, Hjorth, Olof, Danfors, Torsten, Axelsson, Jan, Appel, Lieuwe, Furmark, Tomas, Varrone, Andrea, Lubberink, Mark, Jonasson, My, Frick, Andreas, Fazio, Patrik, Hjorth, Olof, Danfors, Torsten, Axelsson, Jan, Appel, Lieuwe, Furmark, Tomas, Varrone, Andrea, and Lubberink, Mark

Abstract

The aim of this retrospective study was to investigate relationships between relative cerebral blood flow and striatal dopamine transporter and dopamine D2/3 availability in healthy subjects. The data comprised dynamic PET scans with two dopamine transporter tracers [11C]PE2I (n = 20) and [18F]FE-PE2I (n = 20) and the D2/3 tracer [11C]raclopride (n = 18). Subjects with a [11C]PE2I scan also underwent a dynamic scan with the serotonin transporter tracer [11C]DASB. Binding potential (BPND) and relative tracer delivery (R1) values were calculated on regional and voxel-level. Striatal R1 and BPND values were correlated, using either an MRI-based volume of interest (VOI) or an isocontour VOI based on the parametric BPND image. An inter-tracer comparison between [11C]PE2I BPND and [11C]DASB R1 was done on a VOI-level and simulations were performed to investigate whether the constraints of the modeling could cause correlation of the parameters. A positive association was found between BPND and R1 for all three dopamine tracers. A similar correlation was found for the inter-tracer correlation between [11C]PE2I BPND and [11C]DASB R1. Simulations showed that this relationship was not caused by cross-correlation between parameters in the kinetic model. In conclusion, these results suggest an association between resting-state striatal dopamine function and relative blood flow in healthy subjects.

Published

2023

6. Acute nicotine exposure blocks aromatase in the limbic brain of healthy women : A [11C]cetrozole PET study

Author

Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, Comasco, Erika, Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, and Comasco, Erika

Abstract

Background: Of interest to women's mental health, a wealth of studies suggests sex differences in nicotine addiction and treatment response, but their psychoneuroendocrine underpinnings remain largely unknown. A pathway involving sex steroids could indeed be involved in the behavioural effects of nicotine, as it was found to inhibit aromatase in vitro and in vivo in rodents and non-human primates, respectively. Aromatase regulates the synthesis of oestrogens and, of relevance to addiction, is highly expressed in the limbic brain. Methods: The present study sought to investigate in vivo aromatase availability in relation to exposure to nicotine in healthy women. Structural magnetic resonance imaging and two [11C]cetrozole positron emission tomography (PET) scans were performed to assess the availability of aromatase before and after administration of nicotine. Gonadal hormones and cotinine levels were measured. Given the region-specific expression of aromatase, a ROI -based approach was employed to assess changes in [11C]cetrozole non-displaceable binding potential. Results: The highest availability of aromatase was found in the right and left thalamus. Upon nicotine exposure, [11C]cetrozole binding in the thalamus was acutely decreased bilaterally (Cohen's d =-0.99). In line, cotinine levels were negatively associated with aromatase availability in the thalamus, although as non-significant trend. Conclusions: These findings indicate acute blocking of aromatase availability by nicotine in the thalamic area. This suggests a new putative mechanism mediating the effects of nicotine on human behaviour, particularly relevant to sex differences in nicotine addiction.

Published

2023

7. Acute nicotine exposure blocks aromatase in the limbic brain of healthy women : A [11C]cetrozole PET study

Author

Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, Comasco, Erika, Dubol, Manon, Immenschuh, Jana, Jonasson, My, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Roslin, Sara, Wikström, Johan, Antoni, Gunnar, Watanabe, Yasuyoshi, Lubberink, Mark, Biegon, Anat, Sundström Poromaa, Inger, and Comasco, Erika

Abstract

Background: Of interest to women's mental health, a wealth of studies suggests sex differences in nicotine addiction and treatment response, but their psychoneuroendocrine underpinnings remain largely unknown. A pathway involving sex steroids could indeed be involved in the behavioural effects of nicotine, as it was found to inhibit aromatase in vitro and in vivo in rodents and non-human primates, respectively. Aromatase regulates the synthesis of oestrogens and, of relevance to addiction, is highly expressed in the limbic brain. Methods: The present study sought to investigate in vivo aromatase availability in relation to exposure to nicotine in healthy women. Structural magnetic resonance imaging and two [11C]cetrozole positron emission tomography (PET) scans were performed to assess the availability of aromatase before and after administration of nicotine. Gonadal hormones and cotinine levels were measured. Given the region-specific expression of aromatase, a ROI -based approach was employed to assess changes in [11C]cetrozole non-displaceable binding potential. Results: The highest availability of aromatase was found in the right and left thalamus. Upon nicotine exposure, [11C]cetrozole binding in the thalamus was acutely decreased bilaterally (Cohen's d =-0.99). In line, cotinine levels were negatively associated with aromatase availability in the thalamus, although as non-significant trend. Conclusions: These findings indicate acute blocking of aromatase availability by nicotine in the thalamic area. This suggests a new putative mechanism mediating the effects of nicotine on human behaviour, particularly relevant to sex differences in nicotine addiction.

Published

2023

8. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo.

Published

2022

9. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., De två första författarna delar förstaförfattarskapet.

Published

2022

10. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy.

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., Funding: Swedish Research Council; Swedish Brain Foundation; Riksbankens Jubileumsfond - the Swedish Foundation for Humanities and Social Sciences

Published

2022

11. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., De två första författarna delar förstaförfattarskapet.

Published

2022

12. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., De två första författarna delar förstaförfattarskapet.

Published

2022

13. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy.

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., Funding: Swedish Research Council; Swedish Brain Foundation; Riksbankens Jubileumsfond - the Swedish Foundation for Humanities and Social Sciences

Published

2022

14. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., De två första författarna delar förstaförfattarskapet.

Published

2022

15. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy.

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., Funding: Swedish Research Council; Swedish Brain Foundation; Riksbankens Jubileumsfond - the Swedish Foundation for Humanities and Social Sciences

Published

2022

16. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy.

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., Funding: Swedish Research Council; Swedish Brain Foundation; Riksbankens Jubileumsfond - the Swedish Foundation for Humanities and Social Sciences

Published

2022

17. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy.

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., Funding: Swedish Research Council; Swedish Brain Foundation; Riksbankens Jubileumsfond - the Swedish Foundation for Humanities and Social Sciences

Published

2022

18. Serotonin and dopamine transporter availability in social anxiety disorder after combined treatment with escitalopram and cognitive-behavioral therapy

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Engman, Jonas, Björkstrand, Johannes, Faria, Vanda, Alaie, Iman, Carlbring, Per, Andersson, Gerhard, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Reis, Margareta, Wahlstedt, Kurt, Fredrikson, Mats, and Furmark, Tomas

Abstract

Selective serotonin reuptake inhibitors (SSRIs) and internet-based cognitive behavioral therapy (ICBT) are recommended treatments of social anxiety disorder (SAD), and often combined, but their effects on monoaminergic signaling are not well understood. In this multi-tracer positron emission tomography (PET) study, 24 patients with SAD were randomized to treatment with escitalopram+ICBT or placebo+ICBT under double-blind conditions. Before and after 9 weeks of treatment, patients were examined with positron emission tomography and the radioligands [11C]DASB and [11C]PE2I, probing the serotonin (SERT) and dopamine (DAT) transporter proteins respectively. Both treatment combinations resulted in significant improvement as measured by the Liebowitz Social Anxiety Scale (LSAS). At baseline, SERT-DAT co-expression was high and, in the putamen and thalamus, co-expression showed positive associations with symptom severity. SERT-DAT co-expression was also predictive of treatment success, but predictor-outcome associations differed in direction between the treatments. After treatment, average SERT occupancy in the SSRI + ICBT group was >80%, with positive associations between symptom improvement and occupancy in the nucleus accumbens, putamen and anterior cingulate cortex. Following placebo+ICBT, SERT binding increased in the raphe nuclei. DAT binding increased in both groups in limbic and striatal areas, but relations with symptom improvement differed, being negative for SSRI + ICBT and positive for placebo + ICBT. Thus, serotonin-dopamine transporter co-expression exerts influence on symptom severity and remission rate in the treatment of social anxiety disorder. However, the monoamine transporters are modulated in dissimilar ways when cognitive-behavioral treatment is given concomitantly with either SSRI-medication or pill placebo., De två första författarna delar förstaförfattarskapet.

Published

2022

19. Expression and co-expression of serotonin and dopamine transporters in social anxiety disorder : a multitracer positron emission tomography study

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

Serotonin and dopamine are putatively involved in the etiology and treatment of anxiety disorders, but positron emission tomography (PET) studies probing the two neurotransmitters in the same individuals are lacking. The aim of this multitracer PET study was to evaluate the regional expression and co-expression of the transporter proteins for serotonin (SERT) and dopamine (DAT) in patients with social anxiety disorder (SAD). Voxel-wise binding potentials (BPND) for SERT and DAT were determined in 27 patients with SAD and 43 age- and sex-matched healthy controls, using the radioligands [11C]DASB (3-amino-4-(2-dimethylaminomethylphenylsulfanyl)-benzonitrile) and [11C]PE2I (N-(3-iodopro-2E-enyl)-2beta-carbomethoxy-3beta-(4'-methylphenyl)nortropane). Results showed that, within transmitter systems, SAD patients exhibited higher SERT binding in the nucleus accumbens while DAT availability in the amygdala, hippocampus, and putamen correlated positively with symptom severity. At a more lenient statistical threshold, SERT and DAT BPND were also higher in other striatal and limbic regions in patients, and correlated with symptom severity, whereas no brain region showed higher binding in healthy controls. Moreover, SERT/DAT co-expression was significantly higher in SAD patients in the amygdala, nucleus accumbens, caudate, putamen, and posterior ventral thalamus, while lower co-expression was noted in the dorsomedial thalamus. Follow-up logistic regression analysis confirmed that SAD diagnosis was significantly predicted by the statistical interaction between SERT and DAT availability, in the amygdala, putamen, and dorsomedial thalamus. Thus, SAD was associated with mainly increased expression and co-expression of the transporters for serotonin and dopamine in fear and reward-related brain regions. Resultant monoamine dysregulation may underlie SAD symptomatology and constitute a target for treatment.

Published

2021

20. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [11C]DASB and [11C]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response.

Published

2021

21. Expression and co-expression of serotonin and dopamine transporters in social anxiety disorder : a multitracer positron emission tomography study

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

Serotonin and dopamine are putatively involved in the etiology and treatment of anxiety disorders, but positron emission tomography (PET) studies probing the two neurotransmitters in the same individuals are lacking. The aim of this multitracer PET study was to evaluate the regional expression and co-expression of the transporter proteins for serotonin (SERT) and dopamine (DAT) in patients with social anxiety disorder (SAD). Voxel-wise binding potentials (BPND) for SERT and DAT were determined in 27 patients with SAD and 43 age- and sex-matched healthy controls, using the radioligands [11C]DASB (3-amino-4-(2-dimethylaminomethylphenylsulfanyl)-benzonitrile) and [11C]PE2I (N-(3-iodopro-2E-enyl)-2beta-carbomethoxy-3beta-(4'-methylphenyl)nortropane). Results showed that, within transmitter systems, SAD patients exhibited higher SERT binding in the nucleus accumbens while DAT availability in the amygdala, hippocampus, and putamen correlated positively with symptom severity. At a more lenient statistical threshold, SERT and DAT BPND were also higher in other striatal and limbic regions in patients, and correlated with symptom severity, whereas no brain region showed higher binding in healthy controls. Moreover, SERT/DAT co-expression was significantly higher in SAD patients in the amygdala, nucleus accumbens, caudate, putamen, and posterior ventral thalamus, while lower co-expression was noted in the dorsomedial thalamus. Follow-up logistic regression analysis confirmed that SAD diagnosis was significantly predicted by the statistical interaction between SERT and DAT availability, in the amygdala, putamen, and dorsomedial thalamus. Thus, SAD was associated with mainly increased expression and co-expression of the transporters for serotonin and dopamine in fear and reward-related brain regions. Resultant monoamine dysregulation may underlie SAD symptomatology and constitute a target for treatment.

Published

2021

22. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [C-11]DASB and [C-11]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response., Funding Agencies|Swedish Research CouncilSwedish Research CouncilEuropean Commission; Riksbankens Jubileumsfond-the Swedish Foundation for Humanities and Social Sciences; Kjell and Marta Beijer Foundation

Published

2021

23. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [11C]DASB and [11C]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response.

Published

2021

24. Expression and co-expression of serotonin and dopamine transporters in social anxiety disorder : a multitracer positron emission tomography study

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

Serotonin and dopamine are putatively involved in the etiology and treatment of anxiety disorders, but positron emission tomography (PET) studies probing the two neurotransmitters in the same individuals are lacking. The aim of this multitracer PET study was to evaluate the regional expression and co-expression of the transporter proteins for serotonin (SERT) and dopamine (DAT) in patients with social anxiety disorder (SAD). Voxel-wise binding potentials (BPND) for SERT and DAT were determined in 27 patients with SAD and 43 age- and sex-matched healthy controls, using the radioligands [11C]DASB (3-amino-4-(2-dimethylaminomethylphenylsulfanyl)-benzonitrile) and [11C]PE2I (N-(3-iodopro-2E-enyl)-2beta-carbomethoxy-3beta-(4'-methylphenyl)nortropane). Results showed that, within transmitter systems, SAD patients exhibited higher SERT binding in the nucleus accumbens while DAT availability in the amygdala, hippocampus, and putamen correlated positively with symptom severity. At a more lenient statistical threshold, SERT and DAT BPND were also higher in other striatal and limbic regions in patients, and correlated with symptom severity, whereas no brain region showed higher binding in healthy controls. Moreover, SERT/DAT co-expression was significantly higher in SAD patients in the amygdala, nucleus accumbens, caudate, putamen, and posterior ventral thalamus, while lower co-expression was noted in the dorsomedial thalamus. Follow-up logistic regression analysis confirmed that SAD diagnosis was significantly predicted by the statistical interaction between SERT and DAT availability, in the amygdala, putamen, and dorsomedial thalamus. Thus, SAD was associated with mainly increased expression and co-expression of the transporters for serotonin and dopamine in fear and reward-related brain regions. Resultant monoamine dysregulation may underlie SAD symptomatology and constitute a target for treatment.

Published

2021

25. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [C-11]DASB and [C-11]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response., Funding Agencies|Swedish Research CouncilSwedish Research CouncilEuropean Commission; Riksbankens Jubileumsfond-the Swedish Foundation for Humanities and Social Sciences; Kjell and Marta Beijer Foundation

Published

2021

26. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [11C]DASB and [11C]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response.

Published

2021

27. Expression and co-expression of serotonin and dopamine transporters in social anxiety disorder : a multitracer positron emission tomography study

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

Serotonin and dopamine are putatively involved in the etiology and treatment of anxiety disorders, but positron emission tomography (PET) studies probing the two neurotransmitters in the same individuals are lacking. The aim of this multitracer PET study was to evaluate the regional expression and co-expression of the transporter proteins for serotonin (SERT) and dopamine (DAT) in patients with social anxiety disorder (SAD). Voxel-wise binding potentials (BPND) for SERT and DAT were determined in 27 patients with SAD and 43 age- and sex-matched healthy controls, using the radioligands [11C]DASB (3-amino-4-(2-dimethylaminomethylphenylsulfanyl)-benzonitrile) and [11C]PE2I (N-(3-iodopro-2E-enyl)-2beta-carbomethoxy-3beta-(4'-methylphenyl)nortropane). Results showed that, within transmitter systems, SAD patients exhibited higher SERT binding in the nucleus accumbens while DAT availability in the amygdala, hippocampus, and putamen correlated positively with symptom severity. At a more lenient statistical threshold, SERT and DAT BPND were also higher in other striatal and limbic regions in patients, and correlated with symptom severity, whereas no brain region showed higher binding in healthy controls. Moreover, SERT/DAT co-expression was significantly higher in SAD patients in the amygdala, nucleus accumbens, caudate, putamen, and posterior ventral thalamus, while lower co-expression was noted in the dorsomedial thalamus. Follow-up logistic regression analysis confirmed that SAD diagnosis was significantly predicted by the statistical interaction between SERT and DAT availability, in the amygdala, putamen, and dorsomedial thalamus. Thus, SAD was associated with mainly increased expression and co-expression of the transporters for serotonin and dopamine in fear and reward-related brain regions. Resultant monoamine dysregulation may underlie SAD symptomatology and constitute a target for treatment.

Published

2021

28. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [11C]DASB and [11C]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response.

Published

2021

29. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [C-11]DASB and [C-11]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response., Funding Agencies|Swedish Research CouncilSwedish Research CouncilEuropean Commission; Riksbankens Jubileumsfond-the Swedish Foundation for Humanities and Social Sciences; Kjell and Marta Beijer Foundation

Published

2021

30. Expression and co-expression of serotonin and dopamine transporters in social anxiety disorder : a multitracer positron emission tomography study

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N T, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

Serotonin and dopamine are putatively involved in the etiology and treatment of anxiety disorders, but positron emission tomography (PET) studies probing the two neurotransmitters in the same individuals are lacking. The aim of this multitracer PET study was to evaluate the regional expression and co-expression of the transporter proteins for serotonin (SERT) and dopamine (DAT) in patients with social anxiety disorder (SAD). Voxel-wise binding potentials (BPND) for SERT and DAT were determined in 27 patients with SAD and 43 age- and sex-matched healthy controls, using the radioligands [11C]DASB (3-amino-4-(2-dimethylaminomethylphenylsulfanyl)-benzonitrile) and [11C]PE2I (N-(3-iodopro-2E-enyl)-2beta-carbomethoxy-3beta-(4'-methylphenyl)nortropane). Results showed that, within transmitter systems, SAD patients exhibited higher SERT binding in the nucleus accumbens while DAT availability in the amygdala, hippocampus, and putamen correlated positively with symptom severity. At a more lenient statistical threshold, SERT and DAT BPND were also higher in other striatal and limbic regions in patients, and correlated with symptom severity, whereas no brain region showed higher binding in healthy controls. Moreover, SERT/DAT co-expression was significantly higher in SAD patients in the amygdala, nucleus accumbens, caudate, putamen, and posterior ventral thalamus, while lower co-expression was noted in the dorsomedial thalamus. Follow-up logistic regression analysis confirmed that SAD diagnosis was significantly predicted by the statistical interaction between SERT and DAT availability, in the amygdala, putamen, and dorsomedial thalamus. Thus, SAD was associated with mainly increased expression and co-expression of the transporters for serotonin and dopamine in fear and reward-related brain regions. Resultant monoamine dysregulation may underlie SAD symptomatology and constitute a target for treatment.

Published

2021

31. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [C-11]DASB and [C-11]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response., Funding Agencies|Swedish Research CouncilSwedish Research CouncilEuropean Commission; Riksbankens Jubileumsfond-the Swedish Foundation for Humanities and Social Sciences; Kjell and Marta Beijer Foundation

Published

2021

32. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof R., Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Mansson, Kristoffer N. T., Rosen, Jorgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [C-11]DASB and [C-11]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response., Funding Agencies|Swedish Research CouncilSwedish Research CouncilEuropean Commission; Riksbankens Jubileumsfond-the Swedish Foundation for Humanities and Social Sciences; Kjell and Marta Beijer Foundation

Published

2021

33. Expectancy effects on serotonin and dopamine transporters during SSRI treatment of social anxiety disorder : a randomized clinical trial

Author

Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, Furmark, Tomas, Hjorth, Olof, Frick, Andreas, Gingnell, Malin, Hoppe, Johanna M., Faria, Vanda, Hultberg, Sara, Alaie, Iman, Månsson, Kristoffer N. T., Rosén, Jörgen, Reis, Margareta, Wahlstedt, Kurt, Jonasson, My, Lubberink, Mark, Antoni, Gunnar, Fredrikson, Mats, and Furmark, Tomas

Abstract

It has been extensively debated whether selective serotonin reuptake inhibitors (SSRIs) are more efficacious than placebo in affective disorders, and it is not fully understood how SSRIs exert their beneficial effects. Along with serotonin transporter blockade, altered dopamine signaling and psychological factors may contribute. In this randomized clinical trial of participants with social anxiety disorder (SAD) we investigated how manipulation of verbally-induced expectancies, vital for placebo response, affect brain monoamine transporters and symptom improvement during SSRI treatment. Twenty-seven participants with SAD (17 men, 10 women), were randomized, to 9 weeks of overt or covert treatment with escitalopram 20 mg. The overt group received correct treatment information whereas the covert group was treated deceptively with escitalopram, described as an active placebo in a cover story. Before and after treatment, patients underwent positron emission tomography (PET) assessments with the [11C]DASB and [11C]PE2I radiotracers, probing brain serotonin (SERT) and dopamine (DAT) transporters. SAD symptoms were measured by the Liebowitz Social Anxiety Scale. Overt was superior to covert SSRI treatment, resulting in almost a fourfold higher rate of responders. PET results showed that SERT occupancy after treatment was unrelated to anxiety reduction and equally high in both groups. In contrast, DAT binding decreased in the right putamen, pallidum, and the left thalamus with overt SSRI treatment, and increased with covert treatment, resulting in significant group differences. DAT binding potential changes in these regions correlated negatively with symptom improvement. Findings support that the anxiolytic effects of SSRIs involve psychological factors contingent on dopaminergic neurotransmission while serotonin transporter blockade alone is insufficient for clinical response.

Published

2021

34. Quantification of aromatase binding in the female human brain using [11 C]cetrozole positron emission tomography.

Author

Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, Comasco, Erika, Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, and Comasco, Erika

Abstract

Aromatase, the enzyme that in the brain converts testosterone and androstenedione to estradiol and estrone, respectively, is a putative key factor in psychoneuroendocrinology. In vivo assessment of aromatase was performed to evaluate tracer kinetic models and optimal scan duration, for quantitative analysis of the aromatase positron emission tomography (PET) ligand [11 C]cetrozole. Anatomical magnetic resonance and 90-min dynamic [11 C]cetrozole PET-CT scans were performed on healthy women. Volume of interest (VOI)-based analyses with a plasma-input function were performed using the single-tissue and two-tissue (2TCM) reversible compartment models and plasma-input Logan analysis. Additionally, the simplified reference tissue model (SRTM), Logan reference tissue model (LRTM), and standardized uptake volume ratio model, with cerebellum as reference region, were evaluated. Parametric images were generated and regionally averaged voxel values were compared with VOI-based analyses of the reference tissue models. The optimal reference model was used for evaluation of a decreased scan duration. Differences between the plasma-input- and reference tissue-based methods and comparisons between scan durations were assessed by linear regression. The [11 C]cetrozole time-activity curves were best described by the 2TCM. SRTM nondisplaceable binding potential (BPND ), with cerebellum as reference region, can be used to estimate [11 C]cetrozole binding and generated robust and quantitatively accurate results for a reduced scan duration of 60 min. Receptor parametric mapping, a basis function implementation of SRTM, as well as LRTM, produced quantitatively accurate parametric images, showing BPND at the voxel level. As PET tracer, [11 C]cetrozole can be employed for relatively short brain scans to measure aromatase binding using a reference tissue-based approach.

Published

2020

35. Quantification of aromatase binding in the female human brain using [11 C]cetrozole positron emission tomography.

Author

Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, Comasco, Erika, Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, and Comasco, Erika

Abstract

Aromatase, the enzyme that in the brain converts testosterone and androstenedione to estradiol and estrone, respectively, is a putative key factor in psychoneuroendocrinology. In vivo assessment of aromatase was performed to evaluate tracer kinetic models and optimal scan duration, for quantitative analysis of the aromatase positron emission tomography (PET) ligand [11 C]cetrozole. Anatomical magnetic resonance and 90-min dynamic [11 C]cetrozole PET-CT scans were performed on healthy women. Volume of interest (VOI)-based analyses with a plasma-input function were performed using the single-tissue and two-tissue (2TCM) reversible compartment models and plasma-input Logan analysis. Additionally, the simplified reference tissue model (SRTM), Logan reference tissue model (LRTM), and standardized uptake volume ratio model, with cerebellum as reference region, were evaluated. Parametric images were generated and regionally averaged voxel values were compared with VOI-based analyses of the reference tissue models. The optimal reference model was used for evaluation of a decreased scan duration. Differences between the plasma-input- and reference tissue-based methods and comparisons between scan durations were assessed by linear regression. The [11 C]cetrozole time-activity curves were best described by the 2TCM. SRTM nondisplaceable binding potential (BPND ), with cerebellum as reference region, can be used to estimate [11 C]cetrozole binding and generated robust and quantitatively accurate results for a reduced scan duration of 60 min. Receptor parametric mapping, a basis function implementation of SRTM, as well as LRTM, produced quantitatively accurate parametric images, showing BPND at the voxel level. As PET tracer, [11 C]cetrozole can be employed for relatively short brain scans to measure aromatase binding using a reference tissue-based approach.

Published

2020

36. Quantification of aromatase binding in the female human brain using [11 C]cetrozole positron emission tomography.

Author

Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, Comasco, Erika, Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, and Comasco, Erika

Abstract

Aromatase, the enzyme that in the brain converts testosterone and androstenedione to estradiol and estrone, respectively, is a putative key factor in psychoneuroendocrinology. In vivo assessment of aromatase was performed to evaluate tracer kinetic models and optimal scan duration, for quantitative analysis of the aromatase positron emission tomography (PET) ligand [11 C]cetrozole. Anatomical magnetic resonance and 90-min dynamic [11 C]cetrozole PET-CT scans were performed on healthy women. Volume of interest (VOI)-based analyses with a plasma-input function were performed using the single-tissue and two-tissue (2TCM) reversible compartment models and plasma-input Logan analysis. Additionally, the simplified reference tissue model (SRTM), Logan reference tissue model (LRTM), and standardized uptake volume ratio model, with cerebellum as reference region, were evaluated. Parametric images were generated and regionally averaged voxel values were compared with VOI-based analyses of the reference tissue models. The optimal reference model was used for evaluation of a decreased scan duration. Differences between the plasma-input- and reference tissue-based methods and comparisons between scan durations were assessed by linear regression. The [11 C]cetrozole time-activity curves were best described by the 2TCM. SRTM nondisplaceable binding potential (BPND ), with cerebellum as reference region, can be used to estimate [11 C]cetrozole binding and generated robust and quantitatively accurate results for a reduced scan duration of 60 min. Receptor parametric mapping, a basis function implementation of SRTM, as well as LRTM, produced quantitatively accurate parametric images, showing BPND at the voxel level. As PET tracer, [11 C]cetrozole can be employed for relatively short brain scans to measure aromatase binding using a reference tissue-based approach.

Published

2020

37. Quantification of aromatase binding in the female human brain using [11 C]cetrozole positron emission tomography.

Author

Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, Comasco, Erika, Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, and Comasco, Erika

Abstract

Aromatase, the enzyme that in the brain converts testosterone and androstenedione to estradiol and estrone, respectively, is a putative key factor in psychoneuroendocrinology. In vivo assessment of aromatase was performed to evaluate tracer kinetic models and optimal scan duration, for quantitative analysis of the aromatase positron emission tomography (PET) ligand [11 C]cetrozole. Anatomical magnetic resonance and 90-min dynamic [11 C]cetrozole PET-CT scans were performed on healthy women. Volume of interest (VOI)-based analyses with a plasma-input function were performed using the single-tissue and two-tissue (2TCM) reversible compartment models and plasma-input Logan analysis. Additionally, the simplified reference tissue model (SRTM), Logan reference tissue model (LRTM), and standardized uptake volume ratio model, with cerebellum as reference region, were evaluated. Parametric images were generated and regionally averaged voxel values were compared with VOI-based analyses of the reference tissue models. The optimal reference model was used for evaluation of a decreased scan duration. Differences between the plasma-input- and reference tissue-based methods and comparisons between scan durations were assessed by linear regression. The [11 C]cetrozole time-activity curves were best described by the 2TCM. SRTM nondisplaceable binding potential (BPND ), with cerebellum as reference region, can be used to estimate [11 C]cetrozole binding and generated robust and quantitatively accurate results for a reduced scan duration of 60 min. Receptor parametric mapping, a basis function implementation of SRTM, as well as LRTM, produced quantitatively accurate parametric images, showing BPND at the voxel level. As PET tracer, [11 C]cetrozole can be employed for relatively short brain scans to measure aromatase binding using a reference tissue-based approach.

Published

2020

38. Quantification of aromatase binding in the female human brain using [11 C]cetrozole positron emission tomography.

Author

Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, Comasco, Erika, Jonasson, My, Nordeman, Patrik, Eriksson, Jonas, Wilking, Helena, Wikström, Johan, Takahashi, Kayo, Niwa, Takashi, Hosoya, Takamitsu, Watanabe, Yasuyoshi, Antoni, Gunnar, Sundström Poromaa, Inger, Lubberink, Mark, and Comasco, Erika

Abstract

Aromatase, the enzyme that in the brain converts testosterone and androstenedione to estradiol and estrone, respectively, is a putative key factor in psychoneuroendocrinology. In vivo assessment of aromatase was performed to evaluate tracer kinetic models and optimal scan duration, for quantitative analysis of the aromatase positron emission tomography (PET) ligand [11 C]cetrozole. Anatomical magnetic resonance and 90-min dynamic [11 C]cetrozole PET-CT scans were performed on healthy women. Volume of interest (VOI)-based analyses with a plasma-input function were performed using the single-tissue and two-tissue (2TCM) reversible compartment models and plasma-input Logan analysis. Additionally, the simplified reference tissue model (SRTM), Logan reference tissue model (LRTM), and standardized uptake volume ratio model, with cerebellum as reference region, were evaluated. Parametric images were generated and regionally averaged voxel values were compared with VOI-based analyses of the reference tissue models. The optimal reference model was used for evaluation of a decreased scan duration. Differences between the plasma-input- and reference tissue-based methods and comparisons between scan durations were assessed by linear regression. The [11 C]cetrozole time-activity curves were best described by the 2TCM. SRTM nondisplaceable binding potential (BPND ), with cerebellum as reference region, can be used to estimate [11 C]cetrozole binding and generated robust and quantitatively accurate results for a reduced scan duration of 60 min. Receptor parametric mapping, a basis function implementation of SRTM, as well as LRTM, produced quantitatively accurate parametric images, showing BPND at the voxel level. As PET tracer, [11 C]cetrozole can be employed for relatively short brain scans to measure aromatase binding using a reference tissue-based approach.

Published

2020

39. Optimal timing of tau pathology imaging and automatic extraction of a reference region using dynamic [18F]THK5317 PET

Author

Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, Lubberink, Mark, Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, and Lubberink, Mark

Abstract

[F-18]THK5317 is a PET tracer for in-vivo imaging of tau associated with Alzheimer's disease (AD). This work aimed to evaluate optimal timing for standardized uptake value ratio (SUVR) measures with [F-18]THK5317 and automated generation of SUVR-1 and relative cerebral blood flow (R-1) parametric images. Nine AD patients and nine controls underwent 90 min [F-18]THK5317 scans. SUVR-1 was calculated at transient equilibrium (TE) and for seven different 20 min intervals and compared with distribution volume ratio (DVR; reference Logan). Cerebellar grey matter (MRI) was used as reference region. A supervised cluster analysis (SVCA) method was implemented to automatically generate a reference region, directly from the dynamic PET volume without the need of a structural MRI scan, for computation of SUVR-1 and R-1 images for a scan duration matching the optimal timing. TE was reached first in putamen, frontal- and parietal cortex at 22 +/- 4 min for AD patients and in putamen at 20 +/- 0 min in controls. Over all regions and subjects, SUVR20-40-1 correlated best with DVR-1, R-2 = 0.97. High correlation was found between values generated using MRI- and SVCA-based reference (R-2 = 0.93 for SUVR20-40-1; R-2 = 0.94 for R-1). SUVR20-40 allows for accurate semi-quantitative assessment of tau pathology and SVCA may be used to obtain a reference region for calculation of both SUVR-1 and R-1 with 40 min scan duration.

Published

2019

40. Optimal timing of tau pathology imaging and automatic extraction of a reference region using dynamic [18F]THK5317 PET

Author

Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, Lubberink, Mark, Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, and Lubberink, Mark

Abstract

[F-18]THK5317 is a PET tracer for in-vivo imaging of tau associated with Alzheimer's disease (AD). This work aimed to evaluate optimal timing for standardized uptake value ratio (SUVR) measures with [F-18]THK5317 and automated generation of SUVR-1 and relative cerebral blood flow (R-1) parametric images. Nine AD patients and nine controls underwent 90 min [F-18]THK5317 scans. SUVR-1 was calculated at transient equilibrium (TE) and for seven different 20 min intervals and compared with distribution volume ratio (DVR; reference Logan). Cerebellar grey matter (MRI) was used as reference region. A supervised cluster analysis (SVCA) method was implemented to automatically generate a reference region, directly from the dynamic PET volume without the need of a structural MRI scan, for computation of SUVR-1 and R-1 images for a scan duration matching the optimal timing. TE was reached first in putamen, frontal- and parietal cortex at 22 +/- 4 min for AD patients and in putamen at 20 +/- 0 min in controls. Over all regions and subjects, SUVR20-40-1 correlated best with DVR-1, R-2 = 0.97. High correlation was found between values generated using MRI- and SVCA-based reference (R-2 = 0.93 for SUVR20-40-1; R-2 = 0.94 for R-1). SUVR20-40 allows for accurate semi-quantitative assessment of tau pathology and SVCA may be used to obtain a reference region for calculation of both SUVR-1 and R-1 with 40 min scan duration.

Published

2019

41. Optimal timing of tau pathology imaging and automatic extraction of a reference region using dynamic [18F]THK5317 PET

Author

Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, Lubberink, Mark, Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, and Lubberink, Mark

Abstract

[F-18]THK5317 is a PET tracer for in-vivo imaging of tau associated with Alzheimer's disease (AD). This work aimed to evaluate optimal timing for standardized uptake value ratio (SUVR) measures with [F-18]THK5317 and automated generation of SUVR-1 and relative cerebral blood flow (R-1) parametric images. Nine AD patients and nine controls underwent 90 min [F-18]THK5317 scans. SUVR-1 was calculated at transient equilibrium (TE) and for seven different 20 min intervals and compared with distribution volume ratio (DVR; reference Logan). Cerebellar grey matter (MRI) was used as reference region. A supervised cluster analysis (SVCA) method was implemented to automatically generate a reference region, directly from the dynamic PET volume without the need of a structural MRI scan, for computation of SUVR-1 and R-1 images for a scan duration matching the optimal timing. TE was reached first in putamen, frontal- and parietal cortex at 22 +/- 4 min for AD patients and in putamen at 20 +/- 0 min in controls. Over all regions and subjects, SUVR20-40-1 correlated best with DVR-1, R-2 = 0.97. High correlation was found between values generated using MRI- and SVCA-based reference (R-2 = 0.93 for SUVR20-40-1; R-2 = 0.94 for R-1). SUVR20-40 allows for accurate semi-quantitative assessment of tau pathology and SVCA may be used to obtain a reference region for calculation of both SUVR-1 and R-1 with 40 min scan duration.

Published

2019

42. Optimal timing of tau pathology imaging and automatic extraction of a reference region using dynamic [18F]THK5317 PET

Author

Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, Lubberink, Mark, Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, and Lubberink, Mark

Abstract

[F-18]THK5317 is a PET tracer for in-vivo imaging of tau associated with Alzheimer's disease (AD). This work aimed to evaluate optimal timing for standardized uptake value ratio (SUVR) measures with [F-18]THK5317 and automated generation of SUVR-1 and relative cerebral blood flow (R-1) parametric images. Nine AD patients and nine controls underwent 90 min [F-18]THK5317 scans. SUVR-1 was calculated at transient equilibrium (TE) and for seven different 20 min intervals and compared with distribution volume ratio (DVR; reference Logan). Cerebellar grey matter (MRI) was used as reference region. A supervised cluster analysis (SVCA) method was implemented to automatically generate a reference region, directly from the dynamic PET volume without the need of a structural MRI scan, for computation of SUVR-1 and R-1 images for a scan duration matching the optimal timing. TE was reached first in putamen, frontal- and parietal cortex at 22 +/- 4 min for AD patients and in putamen at 20 +/- 0 min in controls. Over all regions and subjects, SUVR20-40-1 correlated best with DVR-1, R-2 = 0.97. High correlation was found between values generated using MRI- and SVCA-based reference (R-2 = 0.93 for SUVR20-40-1; R-2 = 0.94 for R-1). SUVR20-40 allows for accurate semi-quantitative assessment of tau pathology and SVCA may be used to obtain a reference region for calculation of both SUVR-1 and R-1 with 40 min scan duration.

Published

2019

43. Optimal timing of tau pathology imaging and automatic extraction of a reference region using dynamic [18F]THK5317 PET

Author

Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, Lubberink, Mark, Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, and Lubberink, Mark

Abstract

[F-18]THK5317 is a PET tracer for in-vivo imaging of tau associated with Alzheimer's disease (AD). This work aimed to evaluate optimal timing for standardized uptake value ratio (SUVR) measures with [F-18]THK5317 and automated generation of SUVR-1 and relative cerebral blood flow (R-1) parametric images. Nine AD patients and nine controls underwent 90 min [F-18]THK5317 scans. SUVR-1 was calculated at transient equilibrium (TE) and for seven different 20 min intervals and compared with distribution volume ratio (DVR; reference Logan). Cerebellar grey matter (MRI) was used as reference region. A supervised cluster analysis (SVCA) method was implemented to automatically generate a reference region, directly from the dynamic PET volume without the need of a structural MRI scan, for computation of SUVR-1 and R-1 images for a scan duration matching the optimal timing. TE was reached first in putamen, frontal- and parietal cortex at 22 +/- 4 min for AD patients and in putamen at 20 +/- 0 min in controls. Over all regions and subjects, SUVR20-40-1 correlated best with DVR-1, R-2 = 0.97. High correlation was found between values generated using MRI- and SVCA-based reference (R-2 = 0.93 for SUVR20-40-1; R-2 = 0.94 for R-1). SUVR20-40 allows for accurate semi-quantitative assessment of tau pathology and SVCA may be used to obtain a reference region for calculation of both SUVR-1 and R-1 with 40 min scan duration.

Published

2019

44. Optimal timing of tau pathology imaging and automatic extraction of a reference region using dynamic [18F]THK5317 PET

Author

Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, Lubberink, Mark, Jonasson, My, Wall, Anders, Chiotis, Konstantinos, Leuzy, Antoine, Eriksson, Jonas, Antoni, Gunnar, Nordberg, Agneta, and Lubberink, Mark

Abstract

[F-18]THK5317 is a PET tracer for in-vivo imaging of tau associated with Alzheimer's disease (AD). This work aimed to evaluate optimal timing for standardized uptake value ratio (SUVR) measures with [F-18]THK5317 and automated generation of SUVR-1 and relative cerebral blood flow (R-1) parametric images. Nine AD patients and nine controls underwent 90 min [F-18]THK5317 scans. SUVR-1 was calculated at transient equilibrium (TE) and for seven different 20 min intervals and compared with distribution volume ratio (DVR; reference Logan). Cerebellar grey matter (MRI) was used as reference region. A supervised cluster analysis (SVCA) method was implemented to automatically generate a reference region, directly from the dynamic PET volume without the need of a structural MRI scan, for computation of SUVR-1 and R-1 images for a scan duration matching the optimal timing. TE was reached first in putamen, frontal- and parietal cortex at 22 +/- 4 min for AD patients and in putamen at 20 +/- 0 min in controls. Over all regions and subjects, SUVR20-40-1 correlated best with DVR-1, R-2 = 0.97. High correlation was found between values generated using MRI- and SVCA-based reference (R-2 = 0.93 for SUVR20-40-1; R-2 = 0.94 for R-1). SUVR20-40 allows for accurate semi-quantitative assessment of tau pathology and SVCA may be used to obtain a reference region for calculation of both SUVR-1 and R-1 with 40 min scan duration.

Published

2019

45. Differential diagnosis of patients with parkinsonian syndrome using multilinear regression to disease-specific C-11-PE2I-PET templates and classification tree learning

Author

Lubberink, Mark, Widström, Charles, Jonasson, My, Appel, Lieuwe, Fällmar, David, Nyholm, Dag, Sörensen, Jens, Danfors, Torsten, Lubberink, Mark, Widström, Charles, Jonasson, My, Appel, Lieuwe, Fällmar, David, Nyholm, Dag, Sörensen, Jens, and Danfors, Torsten

Published

2018

46. Blood Flow Dependence of Early [C-11]PE2I and [F-18]FE-PE2I PET SUVR Measurements Used In the Differential Diagnosis of Parkinsonian Disorders

Author

Jonasson, My, Langaas, G., Appel, Lieuwe, Danfors, Torsten, Fazio, P., Lubberink, Mark, Varrone, A., Jonasson, My, Langaas, G., Appel, Lieuwe, Danfors, Torsten, Fazio, P., Lubberink, Mark, and Varrone, A.

Published

2018

47. Association between amygdala neurokinin-1 receptor availability and anxiety-related personality traits

Author

Motilla Hoppe, Johanna, Frick, Andreas, Åhs, Fredrik, Linnman, Clas, Appel, Lieuwe, Jonasson, My, Lubberink, Mark, Långström, Bengt, Frans, Örjan, von Knorring, Lars, Fredriksson, M, Furmark, Tomas, Motilla Hoppe, Johanna, Frick, Andreas, Åhs, Fredrik, Linnman, Clas, Appel, Lieuwe, Jonasson, My, Lubberink, Mark, Långström, Bengt, Frans, Örjan, von Knorring, Lars, Fredriksson, M, and Furmark, Tomas

Abstract

Animal studies indicate that substance P (SP) and its preferred neurokinin-1 (NK1) receptor modulate stress and anxiety-related behavior. Alterations in the SP-NK1 system have also been observed in human anxiety disorders, yet little is known about the relation between this system and individual differences in personality traits associated with anxiety propensity and approach-avoidance behavior, including trait anxiety, neuroticism, and extraversion. Exploring this relation could provide important insights into the neurobiological underpinnings of human anxiety and the etiology of anxiety disorders, as anxious traits are associated with increased susceptibility to develop psychopathological conditions. Here we examined the relationship between central NK1 receptor availability and self-rated measures of trait anxiety, neuroticism, and extraversion. The amygdala was chosen as the primary region of interest since this structure has been suggested to mediate the effect of the SP-NK1 system on anxiety. Anxious traits and NK1 receptor availability, determined with positron emission tomography and the radiotracer [11C]GR205171, were measured in 17 healthy individuals. Voxel-wise analyses showed a significant positive correlation between bilateral amygdala NK1 receptor availability and trait anxiety, and a trend in similar direction was observed for neuroticism. Conversely, extraversion was found to be negatively associated with amygdala NK1 receptor availability. Extraversion also correlated negatively with the NK1 measure in the cuneus/precuneus and fusiform gyrus according to exploratory whole-brain analyses. In conclusion, our findings indicate that amygdala NK1 receptor availability is associated with anxiety-related personality traits in healthy subjects, consistent with a modulatory role for the SP-NK1 system in human anxiety.

Published

2018

48. Longitudinal changes of tau PET imaging in relation to hypometabolism in prodromal and Alzheimer's disease dementia

Author

Chiotis, K, Saint-Aubert, L, Rodriguez-Vieitez, E, Leuzy, A, Almkvist, O, Savitcheva, I, Jonasson, My, Lubberink, Mark, Wall, Anders, Antoni, Gunnar, Nordberg, A, Chiotis, K, Saint-Aubert, L, Rodriguez-Vieitez, E, Leuzy, A, Almkvist, O, Savitcheva, I, Jonasson, My, Lubberink, Mark, Wall, Anders, Antoni, Gunnar, and Nordberg, A

Abstract

The development of tau-specific positron emission tomography (PET) tracers allows imaging in vivo the regional load of tau pathology in Alzheimer's disease (AD) and other tauopathies. Eighteen patients with baseline investigations enroled in a 17-month follow-up study, including 16 with AD (10 had mild cognitive impairment and a positive amyloid PET scan, that is, prodromal AD, and six had AD dementia) and two with corticobasal syndrome. All patients underwent PET scans with [(18)F]THK5317 (tau deposition) and [(18)F]FDG (glucose metabolism) at baseline and follow-up, neuropsychological assessment at baseline and follow-up and a scan with [(11)C]PIB (amyloid-β deposition) at baseline only. At a group level, patients with AD (prodromal or dementia) showed unchanged [(18)F]THK5317 retention over time, in contrast to significant decreases in [(18)F]FDG uptake in temporoparietal areas. The pattern of changes in [(18)F]THK5317 retention was heterogeneous across all patients, with qualitative differences both between the two AD groups (prodromal and dementia) and among individual patients. High [(18)F]THK5317 retention was significantly associated over time with low episodic memory encoding scores, while low [(18)F]FDG uptake was significantly associated over time with both low global cognition and episodic memory encoding scores. Both patients with corticobasal syndrome had a negative [(11)C]PIB scan, high [(18)F]THK5317 retention with a different regional distribution from that in AD, and a homogeneous pattern of increased [(18)F]THK5317 retention in the basal ganglia over time. These findings highlight the heterogeneous propagation of tau pathology among patients with symptomatic AD, in contrast to the homogeneous changes seen in glucose metabolism, which better tracked clinical progression.Molecular Psychiatry advance online publication, 16 May 2017; doi:10.1038/mp.2017.108.

Published

2018

49. Longitudinal uncoupling of cerebral perfusion, glucose metabolism, and tau deposition in Alzheimer's disease.

Author

Leuzy, Antoine, Rodriguez-Vieitez, Elena, Saint-Aubert, Laure, Chiotis, Konstantinos, Almkvist, Ove, Savitcheva, Irina, Jonasson, My, Lubberink, Mark, Wall, Anders, Antoni, Gunnar, Nordberg, Agneta, Leuzy, Antoine, Rodriguez-Vieitez, Elena, Saint-Aubert, Laure, Chiotis, Konstantinos, Almkvist, Ove, Savitcheva, Irina, Jonasson, My, Lubberink, Mark, Wall, Anders, Antoni, Gunnar, and Nordberg, Agneta

Abstract

INTRODUCTION: Cross-sectional findings using the tau tracer [18F]THK5317 (THK5317) have shown that [18F]fluorodeoxyglucose (FDG) positron emission tomography data can be approximated using perfusion measures (early-frame standardized uptake value ratio; ratio of tracer delivery in target to reference regions). In this way, a single positron emission tomography study can provide both functional and molecular information. METHODS: We included 16 patients with Alzheimer's disease who completed follow-up THK5317 and FDG studies 17 months after baseline investigations. Linear mixed-effects models and annual percentage change maps were used to examine longitudinal change. RESULTS: Limited spatial overlap was observed between areas showing declines in THK5317 perfusion measures and FDG. Minimal overlap was seen between areas showing functional change and those showing increased retention of THK5317. DISCUSSION: Our findings suggest a spatiotemporal offset between functional changes and tau pathology and a partial uncoupling between perfusion and metabolism, possibly as a function of Alzheimer's disease severity.

Published

2018

50. Towards Clinical Implementation of Dynamic Positron Emission Tomography in Neurodegenerative Diseases

Author

Jonasson, My and Jonasson, My

Abstract

Alzheimer’s disease (AD) and Parkinson’s disease (PD) are the two most common neurodegenerative disorders worldwide. Positron emission tomography (PET), together with suitable biomarkers, can aid in the clin-ical evaluation as well as in research investigations of these diseases. Straightforward and quantitative assessments of the parameters of inter-est estimated on a voxel-level, as parametric images, are possible when PET data is acquired over time. Prerequisites to facilitate clinical use of dynamic PET are simplified analysis methods and scan protocols suita-ble for clinical routine. The aim of this thesis was to validate simplified analysis methods, suitable for clinical use, for quantification of dopamine transporter (DAT) availability in patients with parkinsonism using [11C]PE2I PET and tau accumulation in AD patients with [18F]THK5317 PET. The included subjects comprised of both healthy controls and pa-tients with parkinsonism, AD or mild cognitive impairment and each subject underwent a dynamic PET scan with either [11C]PE2I or [18F]THK5317. Models for quantitative voxel-based analysis, resulting in parametric images of tracer binding and overall brain function, were validated in both patients and controls. These parametric methods were compared to region-based values acquired using both plasma- and refer-ence-input models. Clinically feasible scan durations were evaluated for both [11C]PE2I and [18F]THK5317, and a clustering method to obtain a reference time activity curve directly from the dynamic PET data was validated. Furthermore, images of DAT availability and overall brain functional activity, generated from one single dynamic [11C]PE2I PET scan, were compared to a dual-scan approach using [123I]FP-CIT single photon emission computed tomography (SPECT) and [18F]FDG PET, for differential diagnosis of patient with parkinsonism. Study I-III supply valuable information on the feasibility of dynamic [11C]PE2I in a clinical setting for differential diagn

Published

2018