Plasma neurofilament light chain protein is not increased in treatment-resistant schizophrenia and first-degree relatives

On behalf of The MiND Study Group

doi:10.1177/00048674211058684

Plasma neurofilament light chain protein is not increased in treatment-resistant schizophrenia and first-degree relatives

On behalf of The MiND Study Group

Research output: Contribution to journal › Article › peer-review

15 Citations (Scopus)

Abstract

Objective: Schizophrenia, a complex psychiatric disorder, is often associated with cognitive, neurological and neuroimaging abnormalities. The processes underlying these abnormalities, and whether a subset of people with schizophrenia have a neuroprogressive or neurodegenerative component to schizophrenia, remain largely unknown. Examining fluid biomarkers of diverse types of neuronal damage could increase our understanding of these processes, as well as potentially provide clinically useful biomarkers, for example with assisting with differentiation from progressive neurodegenerative disorders such as Alzheimer and frontotemporal dementias. Methods: This study measured plasma neurofilament light chain protein (NfL) using ultrasensitive Simoa technology, to investigate the degree of neuronal injury in a well-characterised cohort of people with treatment-resistant schizophrenia on clozapine (n = 82), compared to first-degree relatives (an at-risk group, n = 37), people with schizophrenia not treated with clozapine (n = 13), and age- and sex-matched controls (n = 59). Results: We found no differences in NfL levels between treatment-resistant schizophrenia (mean NfL, M = 6.3 pg/mL, 95% confidence interval: [5.5, 7.2]), first-degree relatives (siblings, M = 6.7 pg/mL, 95% confidence interval: [5.2, 8.2]; parents, M after adjusting for age = 6.7 pg/mL, 95% confidence interval: [4.7, 8.8]), controls (M = 5.8 pg/mL, 95% confidence interval: [5.3, 6.3]) and not treated with clozapine (M = 4.9 pg/mL, 95% confidence interval: [4.0, 5.8]). Exploratory, hypothesis-generating analyses found weak correlations in treatment-resistant schizophrenia, between NfL and clozapine levels (Spearman’s r = 0.258, 95% confidence interval: [0.034, 0.457]), dyslipidaemia (r = 0.280, 95% confidence interval: [0.064, 0.470]) and a negative correlation with weight (r = −0.305, 95% confidence interval: [−0.504, −0.076]). Conclusion: Treatment-resistant schizophrenia does not appear to be associated with neuronal, particularly axonal degeneration. Further studies are warranted to investigate the utility of NfL to differentiate treatment-resistant schizophrenia from neurodegenerative disorders such as behavioural variant frontotemporal dementia, and to explore NfL in other stages of schizophrenia such as the prodome and first episode.

Original language	English
Number of pages	1
Journal	Australian and New Zealand Journal of Psychiatry
Early online date	17 Nov 2021
DOIs	https://doi.org/10.1177/00048674211058684
Publication status	E-pub ahead of print - 17 Nov 2021

Keywords

biomarker
diagnosis
neurofilament
Schizophrenia
treatment-resistant

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1177/00048674211058684

Cite this

@article{4702e1aa7ba94a188b746689db75af1c,

title = "Plasma neurofilament light chain protein is not increased in treatment-resistant schizophrenia and first-degree relatives",

abstract = "Objective: Schizophrenia, a complex psychiatric disorder, is often associated with cognitive, neurological and neuroimaging abnormalities. The processes underlying these abnormalities, and whether a subset of people with schizophrenia have a neuroprogressive or neurodegenerative component to schizophrenia, remain largely unknown. Examining fluid biomarkers of diverse types of neuronal damage could increase our understanding of these processes, as well as potentially provide clinically useful biomarkers, for example with assisting with differentiation from progressive neurodegenerative disorders such as Alzheimer and frontotemporal dementias. Methods: This study measured plasma neurofilament light chain protein (NfL) using ultrasensitive Simoa technology, to investigate the degree of neuronal injury in a well-characterised cohort of people with treatment-resistant schizophrenia on clozapine (n = 82), compared to first-degree relatives (an at-risk group, n = 37), people with schizophrenia not treated with clozapine (n = 13), and age- and sex-matched controls (n = 59). Results: We found no differences in NfL levels between treatment-resistant schizophrenia (mean NfL, M = 6.3 pg/mL, 95% confidence interval: [5.5, 7.2]), first-degree relatives (siblings, M = 6.7 pg/mL, 95% confidence interval: [5.2, 8.2]; parents, M after adjusting for age = 6.7 pg/mL, 95% confidence interval: [4.7, 8.8]), controls (M = 5.8 pg/mL, 95% confidence interval: [5.3, 6.3]) and not treated with clozapine (M = 4.9 pg/mL, 95% confidence interval: [4.0, 5.8]). Exploratory, hypothesis-generating analyses found weak correlations in treatment-resistant schizophrenia, between NfL and clozapine levels (Spearman{\textquoteright}s r = 0.258, 95% confidence interval: [0.034, 0.457]), dyslipidaemia (r = 0.280, 95% confidence interval: [0.064, 0.470]) and a negative correlation with weight (r = −0.305, 95% confidence interval: [−0.504, −0.076]). Conclusion: Treatment-resistant schizophrenia does not appear to be associated with neuronal, particularly axonal degeneration. Further studies are warranted to investigate the utility of NfL to differentiate treatment-resistant schizophrenia from neurodegenerative disorders such as behavioural variant frontotemporal dementia, and to explore NfL in other stages of schizophrenia such as the prodome and first episode.",

keywords = "biomarker, diagnosis, neurofilament, Schizophrenia, treatment-resistant",

author = "{On behalf of The MiND Study Group} and Dhamidhu Eratne and Shorena Janelidze and Malpas, {Charles B.} and Samantha Loi and Mark Walterfang and Antonia Merritt and Ibrahima Diouf and Kaj Blennow and Henrik Zetterberg and Brandon Cilia and Cassandra Wannan and Chad Bousman and Ian Everall and Andrew Zalesky and Mahesh Jayaram and Naveen Thomas and Berkovic, {Samuel F.} and Oskar Hansson and Dennis Velakoulis and Christos Pantelis and Alexander Santillo and Li, {Qiao Xin} and Christiane Stehmann and Claire Cadwallader and Christopher Fowler and Parsa Ravanfar and Sarah Farrand and Michael Keem and Matthew Kang and Rosie Watson and Nawaf Yassi and Cath Kaylor-Hughes and Richard Kanaan and Piero Perucca and Lucy Vivash and Rashida Ali and O{\textquoteright}Brien, {Terence J.} and Masters, {Colin L.} and Steven Collins and Wendy Kelso and Andrew Evans and Anna King and Patrick Kwan and Jane Gunn and Ilias Goranitis and Tianxin Pan and Courtney Lewis and Tomas Kalincik",

note = "Funding Information: The authors acknowledge the financial support of the CRC for Mental Health. The Cooperative Research Centre (CRC) programme is an Australian Government Initiative. The authors wish to acknowledge the CRC Scientific Advisory Committee, in addition to the contributions of study participants, clinicians at recruitment services, staff at the Murdoch Children{\textquoteright}s Research Institute, staff at the Australian Imaging, Biomarkers and Lifestyle Flagship Study of Aging, and research staff at the Melbourne Neuropsychiatry Centre, including coordinators Merritt, A., Phassouliotis, C., and research assistants, Burnside, A., Cross, H., Gale, S., and Tahtalian, S. Participants for this study were sourced, in part, through the Australian Schizophrenia Research Bank (ASRB), which is supported by the National Health and Medical Research Council of Australia (Enabling Grant N. 386500), the Pratt Foundation, Ramsay Health Care, the Viertel Charitable Foundation and the Schizophrenia Research Institute. We thank the Chief Investigators and ASRB Manager: Carr, V., Schall, U., Scott, R., Jablensky, A., Mowry, B., Michie, P., Catts, S., Henskens, F., Pantelis, C., Loughland, C. We acknowledge the help of Jason Bridge for ASRB database queries. The authors are grateful for assistance from Brett Trounson and Dr Christopher Fowler and the team at The Florey Oak St Biobank. Finally, the authors would like to thank all the participants and their families. The corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication. Funding Information: The author(s) disclosed receipt of the following financial support for the research, authorship and/or publication of this article: C.P. was supported by a National Health and Medical Research Council (NHMRC) Senior Principal Research Fellowship (1105825) and an NHMRC L3 Investigator Grant (1196508). Funding to A.S. was provided by Swedish federal government under the ALF agreement, Lund University, the Fredrik and Ingrid Thuring, Ellen and Henrik Sj{\"o}bring and the Fromma Foundation for medical research. H.Z. is a Wallenberg Scholar supported by grants from the Swedish Research Council (#2018-02532), the European Research Council (#681712), Swedish State Support for Clinical Research (#ALFGBG-720931), the Alzheimer Drug Discovery Foundation (ADDF), USA (#201809-2016862), the AD Strategic Fund and the Alzheimer{\textquoteright}s Association (#ADSF-21-831376C, #ADSF-21-831381C and #ADSF-21-831377C), the Olav Thon Foundation, the Erling-Persson Family Foundation, Stiftelsen f{\"o}r Gamla Tj{\"a}narinnor, Hj{\"a}rnfonden, Sweden (#FO2019-0228), the European Union{\textquoteright}s Horizon 2020 research and innovation programme under the Marie Sk{\l}odowska-Curie grant agreement No 860197 (MIRIADE), and the UK Dementia Research Institute at UCL. This Study was also supported by: MACH MRFF RART 2.2, and Psychiatry and Rehabilitation Division, Region Sk{\aa}ne, Sweden. The role of these funding sources was to support research study staff and biosample analyses. Publisher Copyright: {\textcopyright} The Royal Australian and New Zealand College of Psychiatrists 2021.",

year = "2021",

month = nov,

day = "17",

doi = "10.1177/00048674211058684",

language = "English",

journal = "Australian and New Zealand Journal of Psychiatry",

issn = "0004-8674",

publisher = "SAGE Publications Ltd",

}

TY - JOUR

T1 - Plasma neurofilament light chain protein is not increased in treatment-resistant schizophrenia and first-degree relatives

AU - On behalf of The MiND Study Group

AU - Eratne, Dhamidhu

AU - Janelidze, Shorena

AU - Malpas, Charles B.

AU - Loi, Samantha

AU - Walterfang, Mark

AU - Merritt, Antonia

AU - Diouf, Ibrahima

AU - Blennow, Kaj

AU - Zetterberg, Henrik

AU - Cilia, Brandon

AU - Wannan, Cassandra

AU - Bousman, Chad

AU - Everall, Ian

AU - Zalesky, Andrew

AU - Jayaram, Mahesh

AU - Thomas, Naveen

AU - Berkovic, Samuel F.

AU - Hansson, Oskar

AU - Velakoulis, Dennis

AU - Pantelis, Christos

AU - Santillo, Alexander

AU - Li, Qiao Xin

AU - Stehmann, Christiane

AU - Cadwallader, Claire

AU - Fowler, Christopher

AU - Ravanfar, Parsa

AU - Farrand, Sarah

AU - Keem, Michael

AU - Kang, Matthew

AU - Watson, Rosie

AU - Yassi, Nawaf

AU - Kaylor-Hughes, Cath

AU - Kanaan, Richard

AU - Perucca, Piero

AU - Vivash, Lucy

AU - Ali, Rashida

AU - O’Brien, Terence J.

AU - Masters, Colin L.

AU - Collins, Steven

AU - Kelso, Wendy

AU - Evans, Andrew

AU - King, Anna

AU - Kwan, Patrick

AU - Gunn, Jane

AU - Goranitis, Ilias

AU - Pan, Tianxin

AU - Lewis, Courtney

AU - Kalincik, Tomas

N1 - Funding Information: The authors acknowledge the financial support of the CRC for Mental Health. The Cooperative Research Centre (CRC) programme is an Australian Government Initiative. The authors wish to acknowledge the CRC Scientific Advisory Committee, in addition to the contributions of study participants, clinicians at recruitment services, staff at the Murdoch Children’s Research Institute, staff at the Australian Imaging, Biomarkers and Lifestyle Flagship Study of Aging, and research staff at the Melbourne Neuropsychiatry Centre, including coordinators Merritt, A., Phassouliotis, C., and research assistants, Burnside, A., Cross, H., Gale, S., and Tahtalian, S. Participants for this study were sourced, in part, through the Australian Schizophrenia Research Bank (ASRB), which is supported by the National Health and Medical Research Council of Australia (Enabling Grant N. 386500), the Pratt Foundation, Ramsay Health Care, the Viertel Charitable Foundation and the Schizophrenia Research Institute. We thank the Chief Investigators and ASRB Manager: Carr, V., Schall, U., Scott, R., Jablensky, A., Mowry, B., Michie, P., Catts, S., Henskens, F., Pantelis, C., Loughland, C. We acknowledge the help of Jason Bridge for ASRB database queries. The authors are grateful for assistance from Brett Trounson and Dr Christopher Fowler and the team at The Florey Oak St Biobank. Finally, the authors would like to thank all the participants and their families. The corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication. Funding Information: The author(s) disclosed receipt of the following financial support for the research, authorship and/or publication of this article: C.P. was supported by a National Health and Medical Research Council (NHMRC) Senior Principal Research Fellowship (1105825) and an NHMRC L3 Investigator Grant (1196508). Funding to A.S. was provided by Swedish federal government under the ALF agreement, Lund University, the Fredrik and Ingrid Thuring, Ellen and Henrik Sjöbring and the Fromma Foundation for medical research. H.Z. is a Wallenberg Scholar supported by grants from the Swedish Research Council (#2018-02532), the European Research Council (#681712), Swedish State Support for Clinical Research (#ALFGBG-720931), the Alzheimer Drug Discovery Foundation (ADDF), USA (#201809-2016862), the AD Strategic Fund and the Alzheimer’s Association (#ADSF-21-831376C, #ADSF-21-831381C and #ADSF-21-831377C), the Olav Thon Foundation, the Erling-Persson Family Foundation, Stiftelsen för Gamla Tjänarinnor, Hjärnfonden, Sweden (#FO2019-0228), the European Union’s Horizon 2020 research and innovation programme under the Marie Skłodowska-Curie grant agreement No 860197 (MIRIADE), and the UK Dementia Research Institute at UCL. This Study was also supported by: MACH MRFF RART 2.2, and Psychiatry and Rehabilitation Division, Region Skåne, Sweden. The role of these funding sources was to support research study staff and biosample analyses. Publisher Copyright: © The Royal Australian and New Zealand College of Psychiatrists 2021.

PY - 2021/11/17

Y1 - 2021/11/17

N2 - Objective: Schizophrenia, a complex psychiatric disorder, is often associated with cognitive, neurological and neuroimaging abnormalities. The processes underlying these abnormalities, and whether a subset of people with schizophrenia have a neuroprogressive or neurodegenerative component to schizophrenia, remain largely unknown. Examining fluid biomarkers of diverse types of neuronal damage could increase our understanding of these processes, as well as potentially provide clinically useful biomarkers, for example with assisting with differentiation from progressive neurodegenerative disorders such as Alzheimer and frontotemporal dementias. Methods: This study measured plasma neurofilament light chain protein (NfL) using ultrasensitive Simoa technology, to investigate the degree of neuronal injury in a well-characterised cohort of people with treatment-resistant schizophrenia on clozapine (n = 82), compared to first-degree relatives (an at-risk group, n = 37), people with schizophrenia not treated with clozapine (n = 13), and age- and sex-matched controls (n = 59). Results: We found no differences in NfL levels between treatment-resistant schizophrenia (mean NfL, M = 6.3 pg/mL, 95% confidence interval: [5.5, 7.2]), first-degree relatives (siblings, M = 6.7 pg/mL, 95% confidence interval: [5.2, 8.2]; parents, M after adjusting for age = 6.7 pg/mL, 95% confidence interval: [4.7, 8.8]), controls (M = 5.8 pg/mL, 95% confidence interval: [5.3, 6.3]) and not treated with clozapine (M = 4.9 pg/mL, 95% confidence interval: [4.0, 5.8]). Exploratory, hypothesis-generating analyses found weak correlations in treatment-resistant schizophrenia, between NfL and clozapine levels (Spearman’s r = 0.258, 95% confidence interval: [0.034, 0.457]), dyslipidaemia (r = 0.280, 95% confidence interval: [0.064, 0.470]) and a negative correlation with weight (r = −0.305, 95% confidence interval: [−0.504, −0.076]). Conclusion: Treatment-resistant schizophrenia does not appear to be associated with neuronal, particularly axonal degeneration. Further studies are warranted to investigate the utility of NfL to differentiate treatment-resistant schizophrenia from neurodegenerative disorders such as behavioural variant frontotemporal dementia, and to explore NfL in other stages of schizophrenia such as the prodome and first episode.

AB - Objective: Schizophrenia, a complex psychiatric disorder, is often associated with cognitive, neurological and neuroimaging abnormalities. The processes underlying these abnormalities, and whether a subset of people with schizophrenia have a neuroprogressive or neurodegenerative component to schizophrenia, remain largely unknown. Examining fluid biomarkers of diverse types of neuronal damage could increase our understanding of these processes, as well as potentially provide clinically useful biomarkers, for example with assisting with differentiation from progressive neurodegenerative disorders such as Alzheimer and frontotemporal dementias. Methods: This study measured plasma neurofilament light chain protein (NfL) using ultrasensitive Simoa technology, to investigate the degree of neuronal injury in a well-characterised cohort of people with treatment-resistant schizophrenia on clozapine (n = 82), compared to first-degree relatives (an at-risk group, n = 37), people with schizophrenia not treated with clozapine (n = 13), and age- and sex-matched controls (n = 59). Results: We found no differences in NfL levels between treatment-resistant schizophrenia (mean NfL, M = 6.3 pg/mL, 95% confidence interval: [5.5, 7.2]), first-degree relatives (siblings, M = 6.7 pg/mL, 95% confidence interval: [5.2, 8.2]; parents, M after adjusting for age = 6.7 pg/mL, 95% confidence interval: [4.7, 8.8]), controls (M = 5.8 pg/mL, 95% confidence interval: [5.3, 6.3]) and not treated with clozapine (M = 4.9 pg/mL, 95% confidence interval: [4.0, 5.8]). Exploratory, hypothesis-generating analyses found weak correlations in treatment-resistant schizophrenia, between NfL and clozapine levels (Spearman’s r = 0.258, 95% confidence interval: [0.034, 0.457]), dyslipidaemia (r = 0.280, 95% confidence interval: [0.064, 0.470]) and a negative correlation with weight (r = −0.305, 95% confidence interval: [−0.504, −0.076]). Conclusion: Treatment-resistant schizophrenia does not appear to be associated with neuronal, particularly axonal degeneration. Further studies are warranted to investigate the utility of NfL to differentiate treatment-resistant schizophrenia from neurodegenerative disorders such as behavioural variant frontotemporal dementia, and to explore NfL in other stages of schizophrenia such as the prodome and first episode.

KW - biomarker

KW - diagnosis

KW - neurofilament

KW - Schizophrenia

KW - treatment-resistant

UR - http://www.scopus.com/inward/record.url?scp=85119493569&partnerID=8YFLogxK

U2 - 10.1177/00048674211058684

DO - 10.1177/00048674211058684

M3 - Article

AN - SCOPUS:85119493569

SN - 0004-8674

JO - Australian and New Zealand Journal of Psychiatry

JF - Australian and New Zealand Journal of Psychiatry

ER -

Plasma neurofilament light chain protein is not increased in treatment-resistant schizophrenia and first-degree relatives

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Keywords

UN SDGs

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