Search

Your search keyword '"Walterfang M"' showing total 457 results
Start Over Author "Walterfang M"
457 results on '"Walterfang M"'

2. Plasma neurofilament light in behavioural variant frontotemporal dementia compared to mood and psychotic disorders

Author

Eratne, D, Kang, M, Malpas, C, Simpson-Yap, S, Lewis, C, Dang, C, Grewal, J, Coe, A, Dobson, H, Keem, M, Chiu, W-H, Kalincik, T, Ooi, S, Darby, D, Brodtmann, A, Hansson, O, Janelidze, S, Blennow, K, Zetterberg, H, Walker, A, Dean, O, Berk, M, Wannan, C, Pantelis, C, Loi, SM, Walterfang, M, Berkovic, SF, Santillo, AF, Velakoulis, D, Eratne, D, Kang, M, Malpas, C, Simpson-Yap, S, Lewis, C, Dang, C, Grewal, J, Coe, A, Dobson, H, Keem, M, Chiu, W-H, Kalincik, T, Ooi, S, Darby, D, Brodtmann, A, Hansson, O, Janelidze, S, Blennow, K, Zetterberg, H, Walker, A, Dean, O, Berk, M, Wannan, C, Pantelis, C, Loi, SM, Walterfang, M, Berkovic, SF, Santillo, AF, and Velakoulis, D

Abstract

OBJECTIVE: Blood biomarkers of neuronal injury such as neurofilament light (NfL) show promise to improve diagnosis of neurodegenerative disorders and distinguish neurodegenerative from primary psychiatric disorders (PPD). This study investigated the diagnostic utility of plasma NfL to differentiate behavioural variant frontotemporal dementia (bvFTD, a neurodegenerative disorder commonly misdiagnosed initially as PPD), from PPD, and performance of large normative/reference data sets and models. METHODS: Plasma NfL was analysed in major depressive disorder (MDD, n = 42), bipolar affective disorder (BPAD, n = 121), treatment-resistant schizophrenia (TRS, n = 82), bvFTD (n = 22), and compared to the reference cohort (Control Group 2, n = 1926, using GAMLSS modelling), and age-matched controls (Control Group 1, n = 96, using general linear models). RESULTS: Large differences were seen between bvFTD (mean NfL 34.9 pg/mL) and all PPDs and controls (all < 11 pg/mL). NfL distinguished bvFTD from PPD with high accuracy, sensitivity (86%), and specificity (88%). GAMLSS models using reference Control Group 2 facilitated precision interpretation of individual levels, while performing equally to or outperforming models using local controls. Slightly higher NfL levels were found in BPAD, compared to controls and TRS. CONCLUSIONS: This study adds further evidence on the diagnostic utility of NfL to distinguish bvFTD from PPD of high clinical relevance to a bvFTD differential diagnosis, and includes the largest cohort of BPAD to date. Using large reference cohorts, GAMLSS modelling and the interactive Internet-based application we developed, may have important implications for future research and clinical translation. Studies are underway investigating utility of plasma NfL in diverse neurodegenerative and primary psychiatric conditions in real-world clinical settings.

Published
2024

3. Cerebrospinal fluid neurofilament light predicts longitudinal diagnostic change in patients with psychiatric and neurodegenerative disorders

Author

Kang, MJY, Eratne, D, Dobson, H, Malpas, CBB, Keem, M, Lewis, C, Grewal, J, Tsoukra, V, Dang, C, Mocellin, R, Kalincik, T, Santillo, AFF, Zetterberg, H, Blennow, K, Stehmann, C, Varghese, S, Li, Q-X, Masters, CLL, Collins, S, Berkovic, SF, Evans, A, Kelso, W, Farrand, S, Loi, SMM, Walterfang, M, Velakoulis, D, Kang, MJY, Eratne, D, Dobson, H, Malpas, CBB, Keem, M, Lewis, C, Grewal, J, Tsoukra, V, Dang, C, Mocellin, R, Kalincik, T, Santillo, AFF, Zetterberg, H, Blennow, K, Stehmann, C, Varghese, S, Li, Q-X, Masters, CLL, Collins, S, Berkovic, SF, Evans, A, Kelso, W, Farrand, S, Loi, SMM, Walterfang, M, and Velakoulis, D

Abstract

OBJECTIVE: People with neuropsychiatric symptoms often experience delay in accurate diagnosis. Although cerebrospinal fluid neurofilament light (CSF NfL) shows promise in distinguishing neurodegenerative disorders (ND) from psychiatric disorders (PSY), its accuracy in a diagnostically challenging cohort longitudinally is unknown. METHODS: We collected longitudinal diagnostic information (mean = 36 months) from patients assessed at a neuropsychiatry service, categorising diagnoses as ND/mild cognitive impairment/other neurological disorders (ND/MCI/other) and PSY. We pre-specified NfL > 582 pg/mL as indicative of ND/MCI/other. RESULTS: Diagnostic category changed from initial to final diagnosis for 23% (49/212) of patients. NfL predicted the final diagnostic category for 92% (22/24) of these and predicted final diagnostic category overall (ND/MCI/other vs. PSY) in 88% (187/212), compared to 77% (163/212) with clinical assessment alone. CONCLUSIONS: CSF NfL improved diagnostic accuracy, with potential to have led to earlier, accurate diagnosis in a real-world setting using a pre-specified cut-off, adding weight to translation of NfL into clinical practice.

Published
2024

4. Hippocampal morphology in Huntington's disease, implications for plasticity and pathogenesis: The IMAGE-HD study.

Author

Wilkes, FA, Jakabek, D, Walterfang, M, Velakoulis, D, Poudel, GR, Stout, JC, Chua, P, Egan, GF, Looi, JCL, Georgiou-Karistianis, N, Wilkes, FA, Jakabek, D, Walterfang, M, Velakoulis, D, Poudel, GR, Stout, JC, Chua, P, Egan, GF, Looi, JCL, and Georgiou-Karistianis, N

Abstract

While striatal changes in Huntington's Disease (HD) are well established, few studies have investigated changes in the hippocampus, a key neuronal hub. Using MRI scans obtained from the IMAGE-HD study, hippocampi were manually traced and then analysed with the Spherical Harmonic Point Distribution Method (SPHARM-PDM) in 36 individuals with presymptomatic-HD, 37 with early symptomatic-HD, and 36 healthy matched controls. There were no significant differences in overall hippocampal volume between groups. Interestingly we found decreased bilateral hippocampal volume in people with symptomatic-HD who took selective serotonin reuptake inhibitors compared to those who did not, despite no significant differences in anxiety, depressive symptoms, or motor incapacity between the two groups. In symptomatic-HD, there was also significant shape deflation in the right hippocampal head, showing the utility of using manual tracing and SPHARM-PDM to characterise subtle shape changes which may be missed by other methods. This study confirms previous findings of the lack of hippocampal volumetric differentiation in presymptomatic-HD and symptomatic-HD compared to controls. We also find novel shape and volume findings in those with symptomatic-HD, especially in relation to decreased hippocampal volume in those treated with SSRIs.

Published
2023

5. Carer burden and behavioral disturbance is similar between younger-onset Alzheimer's disease and behavioral variant frontotemporal dementia

Author

Kang, MJY, Farrand, S, Evans, A, Chiu, W-H, Eratne, D, Kelso, W, Walterfang, M, Velakoulis, D, Loi, SM, Kang, MJY, Farrand, S, Evans, A, Chiu, W-H, Eratne, D, Kelso, W, Walterfang, M, Velakoulis, D, and Loi, SM

Abstract

OBJECTIVES: Carer burden is common in younger-onset dementia (YOD), often due to the difficulty of navigating services often designed for older people with dementia. Compared to Alzheimer's disease (AD), the burden is reported to be higher in behavioral variant frontotemporal dementia (bvFTD). However, there is little literature comparing carer burden specifically in YOD. This study hypothesized that carer burden in bvFTD would be higher than in AD. DESIGN: Retrospective cross-sectional study. SETTING: Tertiary neuropsychiatry service in Victoria, Australia. PARTICIPANTS: Patient-carer dyads with YOD. MEASUREMENTS: We collected patient data, including behaviors using the Cambridge Behavioral Inventory-Revised (CBI-R). Carer burden was rated using the Zarit Burden Inventory-short version (ZBI-12). Descriptive statistics and Mann-Whitney U tests were used to analyze the data. RESULTS: Carers reported high burden (ZBI-12 mean score = 17.2, SD = 10.5), with no significant difference in burden between younger-onset AD and bvFTD. CBI-R stereotypic and motor behaviors, CBI-R everyday skills, and total NUCOG scores differed between the two groups. There was no significant difference in the rest of the CBI-R subcategories, including the behavior-related domains. CONCLUSION: Carers of YOD face high burden and are managing significant challenging behaviors. We found no difference in carer burden between younger-onset AD and bvFTD. This could be due to similarities in the two subtypes in terms of abnormal behavior, motivation, and self-care as measured on CBI-R, contrary to previous literature. Clinicians should screen for carer burden and associated factors including behavioral symptoms in YOD syndromes, as they may contribute to carer burden regardless of the type.

Published
2023

6. Investigation of Brain Iron in Niemann-Pick Type C: A 7T Quantitative Susceptibility Mapping Study

Author

Ravanfar, P, Syeda, WT, Rushmore, RJ, Moffat, B, Lyall, AE, Merritt, AH, Devenyi, GA, Chakravarty, MM, Desmond, P, Cropley, VL, Makris, N, Shenton, ME, Bush, AI, Velakoulis, D, Pantelis, C, Walterfang, M, Ravanfar, P, Syeda, WT, Rushmore, RJ, Moffat, B, Lyall, AE, Merritt, AH, Devenyi, GA, Chakravarty, MM, Desmond, P, Cropley, VL, Makris, N, Shenton, ME, Bush, AI, Velakoulis, D, Pantelis, C, and Walterfang, M

Abstract

BACKGROUND AND PURPOSE: While brain iron dysregulation has been observed in several neurodegenerative disorders, its association with the progressive neurodegeneration in Niemann-Pick type C is unknown. Systemic iron abnormalities have been reported in patients with Niemann-Pick type C and in animal models of Niemann-Pick type C. In this study, we examined brain iron using quantitative susceptibility mapping MR imaging in individuals with Niemann-Pick type C compared with healthy controls. MATERIALS AND METHODS: A cohort of 10 patients with adolescent- and adult-onset Niemann-Pick type C and 14 age- and sex-matched healthy controls underwent 7T brain MR imaging with T1 and quantitative susceptibility mapping acquisitions. A probing whole-brain voxelwise comparison of quantitative susceptibility mapping between groups was conducted. Mean quantitative susceptibility mapping in the ROIs (thalamus, hippocampus, putamen, caudate nucleus, and globus pallidus) was further compared. The correlations between regional volume, quantitative susceptibility mapping values, and clinical features, which included disease severity on the Iturriaga scale, cognitive function, and the Social and Occupational Functioning Assessment Scale, were explored as secondary analyses. RESULTS: We observed lower volume in the thalamus and voxel clusters of higher quantitative susceptibility mapping in the pulvinar nuclei bilaterally in patients with Niemann-Pick type C compared with the control group. In patients with Niemann-Pick type C, higher quantitative susceptibility mapping in the pulvinar nucleus clusters correlated with lower volume of the thalamus on both sides. Moreover, higher quantitative susceptibility mapping in the right pulvinar cluster was associated with greater disease severity. CONCLUSIONS: Our findings suggest iron deposition in the pulvinar nucleus in Niemann-Pick type C disease, which is associated with thalamic atrophy and disease severity. This preliminary evidence support

Published
2023

7. Selective perforant-pathway atrophy in Huntington disease: MRI analysis of hippocampal subfields

Author

Wibawa, P, Walterfang, M, Malpas, CBB, Glikmann-Johnston, Y, Poudel, G, Razi, A, Hannan, AJJ, Velakoulis, D, Georgiou-Karistianis, N, Wibawa, P, Walterfang, M, Malpas, CBB, Glikmann-Johnston, Y, Poudel, G, Razi, A, Hannan, AJJ, Velakoulis, D, and Georgiou-Karistianis, N

Abstract

INTRODUCTION: While individuals with Huntington disease (HD) show memory impairment that indicates hippocampal dysfunction, the available literature does not consistently identify structural evidence for involvement of the whole hippocampus but rather suggests that hippocampal atrophy may be confined to certain hippocampal subregions. METHODS: We processed T1-weighted MRI from IMAGE-HD study using FreeSurfer 7.0 and compared the volumes of the hippocampal subfields among 36 early motor symptomatic (symp-HD), 40 pre-symptomatic (pre-HD), and 36 healthy control individuals across three timepoints over 36 months. RESULTS: Mixed-model analyses revealed significantly lower subfield volumes in symp-HD, compared with pre-HD and control groups, in the subicular regions of the perforant-pathway: presubiculum, subiculum, dentate gyrus, tail, and right molecular layer. These adjoining subfields aggregated into a single principal component, which demonstrated an accelerated rate of atrophy in the symp-HD. Volumes between pre-HD and controls did not show any significant difference. In the combined HD groups, CAG repeat length and disease burden score were associated with presubiculum, molecular layer, tail, and perforant-pathway subfield volumes. Hippocampal left tail and perforant-pathway subfields were associated with motor onset in the pre-HD group. CONCLUSIONS: Hippocampal subfields atrophy in early symptomatic HD affects key regions of the perforant-pathway, which may implicate the distinctive memory impairment at this stage of illness. Their volumetric associations with genetic and clinical markers suggest the selective susceptibility of these subfields to mutant Huntingtin and disease progression.

Published
2023

8. Survival in Huntington's disease and other young-onset dementias

Author

Loi, SM, Tsoukra, P, Sun, E, Chen, Z, Wibawa, P, di Biase, M, Farrand, S, Eratne, D, Kelso, W, Evans, A, Walterfang, M, Velakoulis, D, Loi, SM, Tsoukra, P, Sun, E, Chen, Z, Wibawa, P, di Biase, M, Farrand, S, Eratne, D, Kelso, W, Evans, A, Walterfang, M, and Velakoulis, D

Abstract

OBJECTIVES: To compare survival and risk factors associated with mortality in common young-onset dementias (YOD) including Huntington's disease. METHODS: This retrospective cohort study included inpatients from an Australian specialist neuropsychiatry service, over 20 years. Dementia diagnoses were based on consensus criteria and Huntington's disease (HD) was confirmed genetically. Mortality and cause of death were determined using linkage to the Australian Institute of Health and Welfare National Death Index. RESULTS: There were 386 individuals with YOD included. The dementia types included frontotemporal dementia (FTD) (24.5%), HD (21.2%) and Alzheimer's disease (AD) (20.5%). 63% (n = 243) individuals had died. The longest median survival was for those who had HD, 18.8 years from symptom onset and with a reduced mortality risk compared to AD and FTD (hazard ratio 0.5). Overall, people with YOD had significantly increased mortality, of 5-8 times, compared to the general population. Females with a YOD had higher standardised mortality ratio compared to males (9.3 vs. 4.9) overall. The most frequent cause of death in those with HD was reported as HD, with other causes of death in the other YOD-subtypes related to dementia and mental/behavioural disorders. DISCUSSION: This is the first Australian study to investigate survival and risk factors of mortality in people with YOD. YOD has a significant risk of death compared to the general population. Our findings provide useful clinical information for people affected by YOD as well as future planning and service provision.

Published
2023

9. Comparison of the Accuracy of the 7-Item HADS Depression Subscale and 14-Item Total HADS for Screening for Major Depression: A Systematic Review and Individual Participant Data Meta-Analysis

Author

Wu, Y, Levis, B, Daray, FM, Ioannidis, JPA, Patten, SB, Cuijpers, P, Ziegelstein, RC, Gilbody, S, Fischer, FH, Fan, S, Sun, Y, He, C, Krishnan, A, Neupane, D, Bhandari, PM, Negeri, Z, Riehm, KE, Rice, DB, Azar, M, Yan, XW, Imran, M, Chiovitti, MJ, Boruff, JT, McMillan, D, Kloda, LA, Markham, S, Henry, M, Ismail, Z, Loiselle, CG, Mitchell, ND, Al-Adawi, S, Beck, KR, Beraldi, A, Bernstein, CN, Boye, B, Buel-Drabe, N, Bunevicius, A, Can, C, Carter, G, Chen, C-K, Cheung, G, Clover, K, Conroy, RM, Costa-Requena, G, Cukor, D, Dabscheck, E, De Souza, J, Downing, M, Feinstein, A, Ferentinos, PP, Flint, AJ, Gallagher, P, Gandy, M, Grassi, L, Haerter, M, Hernando, A, Jackson, ML, Jenewein, J, Jette, N, Juliao, M, Kjaergaard, M, Kohler, S, Konig, H-H, Krishna, LKR, Lee, Y, Loebner, M, Loosman, WL, Love, AW, Loewe, B, Malt, UF, Marrie, RA, Massardo, L, Matsuoka, Y, Mehnert, A, Michopoulos, I, Misery, L, Nelson, CJ, Ng, CG, O'Donnell, ML, O'Rourke, SJ, Ozturk, A, Pabst, A, Pasco, JA, Peceliuniene, J, Pintor, L, Ponsford, JL, Pulido, F, Quinn, TJ, Reme, SE, Reuter, K, Riedel-Heller, SG, Rooney, AG, Sanchez-Gonzalez, R, Saracino, RM, Schellekens, MPJ, Scherer, M, Schwarzbold, ML, Cankorur, VS, Sharpe, L, Sharpe, M, Simard, S, Singer, S, Stafford, L, Stone, J, Strobe, NA, Sultan, S, Teixeira, AL, Tiringer, I, Turner, A, Walker, J, Walterfang, M, Wang, L-J, Weyerer, SB, White, J, Wiese, B, Williams, LJ, Wong, L-Y, Benedetti, A, Thombsi, BD, Wu, Y, Levis, B, Daray, FM, Ioannidis, JPA, Patten, SB, Cuijpers, P, Ziegelstein, RC, Gilbody, S, Fischer, FH, Fan, S, Sun, Y, He, C, Krishnan, A, Neupane, D, Bhandari, PM, Negeri, Z, Riehm, KE, Rice, DB, Azar, M, Yan, XW, Imran, M, Chiovitti, MJ, Boruff, JT, McMillan, D, Kloda, LA, Markham, S, Henry, M, Ismail, Z, Loiselle, CG, Mitchell, ND, Al-Adawi, S, Beck, KR, Beraldi, A, Bernstein, CN, Boye, B, Buel-Drabe, N, Bunevicius, A, Can, C, Carter, G, Chen, C-K, Cheung, G, Clover, K, Conroy, RM, Costa-Requena, G, Cukor, D, Dabscheck, E, De Souza, J, Downing, M, Feinstein, A, Ferentinos, PP, Flint, AJ, Gallagher, P, Gandy, M, Grassi, L, Haerter, M, Hernando, A, Jackson, ML, Jenewein, J, Jette, N, Juliao, M, Kjaergaard, M, Kohler, S, Konig, H-H, Krishna, LKR, Lee, Y, Loebner, M, Loosman, WL, Love, AW, Loewe, B, Malt, UF, Marrie, RA, Massardo, L, Matsuoka, Y, Mehnert, A, Michopoulos, I, Misery, L, Nelson, CJ, Ng, CG, O'Donnell, ML, O'Rourke, SJ, Ozturk, A, Pabst, A, Pasco, JA, Peceliuniene, J, Pintor, L, Ponsford, JL, Pulido, F, Quinn, TJ, Reme, SE, Reuter, K, Riedel-Heller, SG, Rooney, AG, Sanchez-Gonzalez, R, Saracino, RM, Schellekens, MPJ, Scherer, M, Schwarzbold, ML, Cankorur, VS, Sharpe, L, Sharpe, M, Simard, S, Singer, S, Stafford, L, Stone, J, Strobe, NA, Sultan, S, Teixeira, AL, Tiringer, I, Turner, A, Walker, J, Walterfang, M, Wang, L-J, Weyerer, SB, White, J, Wiese, B, Williams, LJ, Wong, L-Y, Benedetti, A, and Thombsi, BD

Abstract

The seven-item Hospital Anxiety and Depression Scale Depression subscale (HADS-D) and the total score of the 14-item HADS (HADS-T) are both used for major depression screening. Compared to the HADS-D, the HADS-T includes anxiety items and requires more time to complete. We compared the screening accuracy of the HADS-D and HADS-T for major depression detection. We conducted an individual participant data meta-analysis and fit bivariate random effects models to assess diagnostic accuracy among participants with both HADS-D and HADS-T scores. We identified optimal cutoffs, estimated sensitivity and specificity with 95% confidence intervals, and compared screening accuracy across paired cutoffs via two-stage and individual-level models. We used a 0.05 equivalence margin to assess equivalency in sensitivity and specificity. 20,700 participants (2,285 major depression cases) from 98 studies were included. Cutoffs of ≥7 for the HADS-D (sensitivity 0.79 [0.75, 0.83], specificity 0.78 [0.75, 0.80]) and ≥15 for the HADS-T (sensitivity 0.79 [0.76, 0.82], specificity 0.81 [0.78, 0.83]) minimized the distance to the top-left corner of the receiver operating characteristic curve. Across all sets of paired cutoffs evaluated, differences of sensitivity between HADS-T and HADS-D ranged from -0.05 to 0.01 (0.00 at paired optimal cutoffs), and differences of specificity were within 0.03 for all cutoffs (0.02-0.03). The pattern was similar among outpatients, although the HADS-T was slightly (not nonequivalently) more specific among inpatients. The accuracy of HADS-T was equivalent to the HADS-D for detecting major depression. In most settings, the shorter HADS-D would be preferred. (PsycInfo Database Record (c) 2023 APA, all rights reserved).

Published
2023

10. Cerebrospinal fluid neurofilament light and cerebral atrophy in younger-onset dementia and primary psychiatric disorders

Author

Walia, N, Eratne, D, Loi, SM, Farrand, S, Li, Q-X, Malpas, CB, Varghese, S, Walterfang, M, Evans, AH, Parker, S, Collins, SJ, Masters, CL, Velakoulis, D, Walia, N, Eratne, D, Loi, SM, Farrand, S, Li, Q-X, Malpas, CB, Varghese, S, Walterfang, M, Evans, AH, Parker, S, Collins, SJ, Masters, CL, and Velakoulis, D

Abstract

BACKGROUND AND AIMS: Neurodegeneration underpins the pathological processes of younger-onset dementia (YOD) and has been implicated in primary psychiatric disorders (PSYs). Cerebrospinal fluid (CSF) neurofilament light (NfL) has been used to investigate neurodegeneration severity through correlation with structural brain changes in various conditions, but has seldom been evaluated in YOD and PSYs. METHODS: This retrospective study included patients with YOD or PSYs with magnetic resonance imaging (MRI) of the brain and CSF NfL analysis. Findings from brain MRI were analysed using automated volumetry (volBrain) to measure white matter (WM), grey matter (GM) and whole brain (WB) volumes expressed as percentages of total intracranial volume. Correlations between NfL and brain volume measurements were computed whilst adjusting for age. RESULTS: Seventy patients (47 with YOD and 23 with PSY) were identified. YOD types included Alzheimer disease and behavioural variant frontotemporal dementia. PSY included schizophrenia and major depressive disorder. MRI brain sequences were either fast spoiler gradient-echo (FSPGR) or magnetization-prepared rapid acquisition gradient-echo (MPRAGE). In the total cohort, higher NfL was associated with reduced WB in the FSPGR and MPRAGE sequences (r = -0.402 [95% confidence interval (CI), -0.593 to -0.147], P = 0.008 and r = -0.625 [95% CI, -0.828 to -0.395], P < 0.001, respectively). Higher NfL was related to reduced GM in FSPGR (r = 0.385 [95% CI, -0.649 to -0.014], P = 0.017) and reduced WM in MPRAGE (r = -0.650 [95% CI, -0.777 to -0.307], P < 0.001). Similar relationships were seen in YOD, but not in PSY. CONCLUSION: Higher CSF NfL is related to brain atrophy in YOD, further supporting its use as a nonspecific marker of neurodegeneration severity.

Published
2023

13. BRINGING THE BENCH TO THE BEDSIDE: UPDATES ON THE MIND STUDY AND WHAT A ROUTINELY AVAILABLE SIMPLE BLOOD TEST FOR NEUROFILAMENT LIGHT WOULD MEAN AT THE CLINICAL COAL FACE FOR PATIENTS AND FAMILIES, PSYCHIATRISTS, NEUROLOGISTS, GERIATRICIANS AND GENERAL PRACTITIONERS

Author

Eratne, D, Lewis, C, Cadwallader, C, Kang, M, Keem, M, Santillo, A, Li, QX, Stehmann, C, Loi, SM, Walterfang, M, Watson, R, Yassi, N, Blennow, K, Zetterberg, H, Janelidze, S, Hansson, O, Berry-Kravitz, E, Brodtmann, A, Darby, D, Walker, A, Dean, O, Masters, CL, Collins, S, Berkovic, SF, Velakoulis, D, Eratne, D, Lewis, C, Cadwallader, C, Kang, M, Keem, M, Santillo, A, Li, QX, Stehmann, C, Loi, SM, Walterfang, M, Watson, R, Yassi, N, Blennow, K, Zetterberg, H, Janelidze, S, Hansson, O, Berry-Kravitz, E, Brodtmann, A, Darby, D, Walker, A, Dean, O, Masters, CL, Collins, S, Berkovic, SF, and Velakoulis, D

Published
2022

14. Cerebrospinal fluid neurofilament light chain differentiates behavioural variant frontotemporal dementia progressors from ‘phenocopy’ non‐progressors

Author

Keem, MH, Eratne, D, Lewis, C, Kang, M, Walterfang, M, Loi, SM, Kelso, W, Cadwallader, C, Berkovic, SF, Li, Q, Masters, CL, Collins, S, Santillo, A, Velakoulis, D, Keem, MH, Eratne, D, Lewis, C, Kang, M, Walterfang, M, Loi, SM, Kelso, W, Cadwallader, C, Berkovic, SF, Li, Q, Masters, CL, Collins, S, Santillo, A, and Velakoulis, D

Abstract

Background Distinguishing behavioural variant frontotemporal dementia (bvFTD) from non‐neurodegenerative ‘non‐progressor’, ‘phenocopy’ mimics of frontal lobe dysfunction, can be one of the most challenging clinical dilemmas. A biomarker of neuronal injury, neurofilament light chain (NfL), could reduce misdiagnosis and delay. Method Cerebrospinal fluid (CSF) NfL, amyloid beta 1‐42 (AB42), total and phosphorylated tau (T‐tau, P‐tau) levels were examined in patients with an initial diagnosis of bvFTD. Based on follow up information, patients were categorised as Progressors. Non‐Progressors were subtyped in to Phenocopy Non‐Progressors (non‐neurological/neurodegenerative final diagnosis), and Static Non‐Progressors (static deficits, not fully explained by non‐neurological/neurodegenerative causes). Result Forty‐three patients were included: 20 Progressors, 23 Non‐Progressors (15 Phenocopy, 8 Static), 20 controls. NfL concentrations were lower in Non‐Progressors (Non‐Progressors Mean, M=554pg/mL, 95%CI:[461, 675], Phenocopy Non‐Progressors M=459pg/mL, 95%CI:[385, 539], Static Non‐Progressors M=730pg/mL, 95%CI:[516, 940]), compared to bvFTD Progressors (M=2397pg/mL, 95%CI:[1607, 3332]). NfL distinguished Progressors from Non‐Progressors with the highest accuracy (area under the curve 0.92, 90%/87% sensitivity/specificity, 86%/91% positive/negative predictive value, 88% accuracy). Static Non‐Progressors tended to have higher T‐tau and P‐tau levels compared to Phenocopy Non‐Progressors. Conclusion This study demonstrated strong diagnostic utility of CSF NfL in distinguishing bvFTD from phenocopy non‐progressor variants, at baseline, with high accuracy, in a real‐world clinical setting. This has important clinical implications to improve outcomes for patients and clinicians facing this challenging clinical dilemma, as well as for healthcare services, and clinical trials. Further research is required to investigate heterogeneity within the non‐progressor group and potential d

Published
2022

15. Mortality in dementia is predicted by older age of onset and cognitive presentation.

Author

Loi S.M., Tsoukra P., Chen Z., Wibawa P., Mijuskovic T., Eratne D., Di Biase M.A., Evans A., Farrand S., Kelso W., Goh A.M.Y., Walterfang M., Velakoulis D., Loi S.M., Tsoukra P., Chen Z., Wibawa P., Mijuskovic T., Eratne D., Di Biase M.A., Evans A., Farrand S., Kelso W., Goh A.M.Y., Walterfang M., and Velakoulis D.

Abstract

Objectives: Survival information in dementia is important for future planning and service provision. There have been limited Australian data investigating survival duration and risk factors associated with mortality in younger-onset dementia. Method(s): This was a cross-sectional retrospective study investigating survival in inpatients with a diagnosis of dementia admitted to a tertiary neuropsychiatry service from 1991 to 2014. The Australian Institute of Health and Welfare National Death Index was used to obtain mortality information. Result(s): A total of 468 inpatients were identified, of which 75% had symptom onset at 65 years of age (defined as younger-onset dementia). Dementia was categorised into four subtypes, Alzheimer's dementia, frontotemporal dementia, vascular dementia and other dementias; 72% of the patients had died. Overall median survival duration was 10.6 years with no significant differences in duration within the dementia subtypes (p = 0.174). Survival in older-onset dementia (symptom onset at >65 years of age) was about half of that in younger-onset dementia (median survival 6.3 years compared to 12.7 years, respectively). Independent predictors of mortality were having older-onset dementia (hazard ratio: 3.2) and having initial presenting symptoms being cognitive in nature (hazard ratio: 1.5). Females with an older-onset dementia had longer survival compared to males with an older-onset dementia, and this was reversed for younger-onset dementia. Older-onset dementia and younger-onset dementia conferred 3 and 6 times, respectively, increased risk of death compared to the general population. Conclusion(s): This is the largest Australian study to date investigating survival and risk factors to mortality in dementia. We report important clinical information to patients with dementia and their families about prognosis which will assist with future planning. Our findings suggest that for both older-onset dementia and younger-onset dementia, 'new ons

Published
2022

16. Time to diagnosis in younger-onset dementia and the impact of a specialist diagnostic service.

Author

Loi S.M., Goh A.M.Y., Mocellin R., Malpas C.B., Parker S., Eratne D., Farrand S., Kelso W., Evans A., Walterfang M., Velakoulis D., Loi S.M., Goh A.M.Y., Mocellin R., Malpas C.B., Parker S., Eratne D., Farrand S., Kelso W., Evans A., Walterfang M., and Velakoulis D.

Abstract

Objectives: While early diagnosis of younger-onset dementia (YOD) is crucial in terms of accessing appropriate services and future planning, diagnostic delays are common. This study aims to identify predictors of delay to diagnosis in a large sample of people with YOD and to investigate the impact of a specialist YOD service on this time to diagnosis. Design(s): A retrospective cross-sectional study. Setting(s): The inpatient unit of a tertiary neuropsychiatry service in metropolitan Victoria, Australia. Participant(s): People diagnosed with a YOD. Measurements and methods: We investigated the following predictors using general linear modeling: demographics including sex and location, age at onset, dementia type, cognition, psychiatric diagnosis, and number of services consulted with prior to diagnosis. Result(s): A total of 242 inpatients were included. The mean time to diagnosis was 3.4 years. Significant predictors of delay included younger age at onset, dementia type other than Alzheimer's disease (AD) and behavioral-variant frontotemporal dementia (bvFTD), and increased number of services consulted. These predictors individually led to an increased diagnostic delay of approximately 19 days, 5 months, and 6 months, respectively. A specialized YOD service reduced time to diagnosis by 12 months. Conclusion(s): We found that younger age at onset, having a dementia which was not the most commonly occurring AD or bvFTD, and increasing number of services were significant predictors of diagnostic delay. A novel result was that a specialist YOD service may decrease diagnostic delay, highlighting the importance of such as service in reducing time to diagnosis as well as providing post-diagnostic support.Copyright ©

Published
2022

17. A phase 1b open-label study of sodium selenate as a disease-modifying treatment for possible behavioral variant frontotemporal dementia

Author

Vivash, L, Malpas, CB, Meletis, C, Gollant, M, Eratne, D, Li, Q-X, McDonald, S, O'Brien, WT, Brodtmann, A, Darby, D, Kyndt, C, Walterfang, M, Hovens, CM, Velakoulis, D, O'Brien, TJ, Vivash, L, Malpas, CB, Meletis, C, Gollant, M, Eratne, D, Li, Q-X, McDonald, S, O'Brien, WT, Brodtmann, A, Darby, D, Kyndt, C, Walterfang, M, Hovens, CM, Velakoulis, D, and O'Brien, TJ

Abstract

INTRODUCTION: Sodium selenate increases tau dephosphorylation through protein phosphatase 2 activation. Here we report an open-label Phase 1b study of sodium selenate as a disease-modifying treatment for behavioral variant frontotemporal dementia (bvFTD). METHODS: Twelve participants with bvFTD received sodium selenate (15 mg, three times a day) for 52 weeks. Safety assessments were carried out throughout the trial. Primary outcomes were frequency of adverse events (AEs), serious adverse events (SAEs), and discontinuations. Secondary outcomes of potential efficacy included cognitive and behavioral assessments, magnetic resonance imaging (MRI) whole brain volume, and cerebrospinal fluid (CSF) and blood total tau (t-tau), phosphorylated tau (p-tau), and neurofilament light (NfL) levels, which were measured at baseline and at week 52. RESULTS: Sodium selenate was safe and well tolerated. All participants completed the study, and the majority (64.7%) of reported AEs were mild. One SAE occurred, which was not treatment related. Small declines in MRI and cognitive and behavioral measures were observed over the treatment period. There was no evidence for change in CSF protein levels (t-tau, p-tau, or NfL). Further analysis showed two distinct groups when measuring disease progression markers over the course of the study-one (n = 4) with substantial brain atrophy (2.5% to 6.5% reduction) and cognitive and behavioral decline over the 12-month treatment period, and the second group (n = 7) with no detectable change in cognitive and behavioral measures and less brain atrophy (0.3% to 1.7% reduction). CONCLUSION: Sodium selenate is safe and well tolerated in patients with bvFTD. Randomized-controlled trials are warranted to investigate potential efficacy.

Published
2022

18. Midsagittal corpus callosal thickness and cognitive impairment in Parkinson's disease

Author

Owens-Walton, C, Adamson, C, Walterfang, M, Hall, S, Westen, D, Hansson, O, Shaw, M, Looi, JCL, Owens-Walton, C, Adamson, C, Walterfang, M, Hall, S, Westen, D, Hansson, O, Shaw, M, and Looi, JCL

Abstract

People diagnosed with Parkinson's disease (PD) can experience significant neuropsychiatric symptoms, including cognitive impairment and dementia, the neuroanatomical substrates of which are not fully characterised. Symptoms associated with cognitive impairment and dementia in PD may relate to direct structural changes to the corpus callosum via primary white matter pathology or as a secondary outcome due to the degeneration of cortical regions. Using magnetic resonance imaging, the corpus callosum can be investigated at the midsagittal plane, where it converges to a contiguous mass and is not intertwined with other tracts. The objective of this project was thus twofold: First, we investigated possible changes in the thickness of the midsagittal callosum and cortex in patients with PD with varying levels of cognitive impairment; and secondly, we investigated the relationship between the thickness of the midsagittal corpus callosum and the thickness of the cortex. Study participants included cognitively unimpaired PD participants (n = 35), PD participants with mild cognitive impairment (n = 22), PD participants with dementia (n = 17) and healthy controls (n = 27). We found thinning of the callosum in PD-related dementia compared with PD-related mild cognitive impairment and cognitively unimpaired PD participants. Regression analyses found thickness of the left medial orbitofrontal cortex to be positively correlated with thickness of the anterior callosum in PD-related mild cognitive impairment. This study suggests that a midsagittal thickness model can uncover changes to the corpus callosum in PD-related dementia, which occur in line with changes to the cortex in this advanced disease stage.

Published
2022

19. Risk factors to mortality and causes of death in frontotemporal dementia: An Australian perspective

Author

Loi, SM, Tsoukra, P, Chen, Z, Wibawa, P, Eratne, D, Kelso, W, Walterfang, M, Velakoulis, D, Loi, SM, Tsoukra, P, Chen, Z, Wibawa, P, Eratne, D, Kelso, W, Walterfang, M, and Velakoulis, D

Abstract

OBJECTIVES: Frontotemporal dementia (FTD) is a common cause of dementia in younger people. There is less information known about risk factors to mortality such as the type of symptom onset and cause of death in this group. METHOD: This was a retrospective file review of inpatients with FTD admitted to a tertiary neuropsychiatry unit located in Australia from 1992 to 2014. Mortality information including linkage of names and causes of death were obtained from the Australian Institute Health and Welfare National Death Index. RESULTS: One hundred inpatients were diagnosed with FTD, including behavioural-variant, language-variant FTDs and FTD-motor neuron disease (FTD-MND). Mean age was 52.8 years (SD = 10, range 31-76 years). Sixty-seven of them had died at linkage. Median survival of the sample was 10.5 years and FTD-MND had the shortest survival, 3.5 years. Increasing age of onset and FTD-MND were found to be significant predictors of association for mortality. Compared to the general population, having a FTD had an 8× increased risk of death. Females had double the standardised mortality ratio compared to males. DISCUSSION: This study provides important prognostic information for people diagnosed with FTD living in Australia. It highlights the importance of obtaining a definitive diagnosis as early as possible for future planning. More investigation into the relationship of symptom onset type and sex differences in FTD is required.

Published
2022

20. Carer burden and psychological distress in young-onset dementia: An Australian perspective

Author

Kang, M, Farrand, S, Walterfang, M, Velakoulis, D, Loi, SM, Evans, A, Kang, M, Farrand, S, Walterfang, M, Velakoulis, D, Loi, SM, and Evans, A

Abstract

OBJECTIVES: Carer burden in dementia is associated with poor outcomes, including early nursing home placement for people with dementia and psychological distress for their carers. Carers of people with young-onset dementia (YOD) are particularly vulnerable to carer burden. Yet they are often overlooked by clinicians as dementia services are generally designed for older people. We sought to estimate the rate of burden and psychological distress in carers of YOD at a state-wide tertiary service based in Australia. METHODS: We conducted a cross-sectional study examining 71 dyads from a Neuropsychiatry service. We collected patient demographic and clinical data including the Neuropsychiatry Unit Cognitive Assessment tool (NUCOG) and Mini-Mental State Examination (MMSE). Carer data, such as demographics and psychological distress, were obtained using Depression Anxiety Stress Scale 21 (DASS-21). Carer burden was rated using the Zarit Burden Inventory-short version (ZBI). RESULTS: Higher carer burden, measured using ZBI, was associated with longer duration of dementia and greater severity of overall cognitive impairment. Carers who felt burdened reported higher levels of stress, depression, and anxiety measured using DASS-21. Multiple linear regression analysis found carer burden was independently predicted by duration of dementia, total cognition score and carers experiencing psychological stress. DISCUSSION: We found that patient variables of dementia duration and cognitive impairment and carer variable of carer stress to be associated with carer burden. Poor executive function was associated with carer stress. Early identification and management of carer burden and psychological distress is important for outcomes. Ideally, this should be provided by a specialist YOD service.

Published
2022

21. Clinical correlates of movement disorders in adult Niemann-Pick type C patients measured via a Personal KinetiGraph

Author

El-Masri, S, Malpas, CB, Evans, A, Walterfang, M, El-Masri, S, Malpas, CB, Evans, A, and Walterfang, M

Abstract

BACKGROUND: Niemann-Pick type C (NPC) is an autosomal recessive progressive neurodegenerative disorder caused by mutations in the NPC1 or NPC2 genes. Patients with this disorder have variable phenotypic presentations that often include neuropsychiatric manifestations, cognitive decline, and movement disorders. There is considerable interpatient variation in movement disorders, with limited quantitative measurements describing the movements observed. Objective measurements using wearable sensors provide clinically applicable monitoring of patients with Parkinson's disease, and hence may be utilized in patients with NPC. OBJECTIVE: To explore the relationship between objective measurements of movement obtained via the use of the Personal KinetiGraph (PKG) with the clinical information obtained via questionnaires and clinical rating tools of patients with Niemann-Pick type C. METHODS: Twelve patients with Niemann-Pick type C were recruited who wore the PKG for 6 days during regular activities. A 6-day output was provided by the manufacturer, which provided bradykinesia (BK) and dyskinesia (DK) scores. BK and DK scores were further divided into their interquartile ranges. A fluctuation score (FDS), percentage time immobile (PTI), and percent time with tremors (PTT) were also provided. Clinical assessments included Abnormal Involuntary Movement Scale (AIMS), Epworth Sleepiness Score (ESS), Falls, Neuropsychiatric Unit Assessment Tool (NUCOG), Parkinson's disease questionnaire (PDQ), and modified Unified Parkinson's Disease Rating Scale (UPDRS) which were performed over telehealth within 2 weeks of PKG use. Pearson's correlation analyses were utilized to explore the relationship between DK and BK quartiles and clinical measures. RESULTS: We found bradykinesia to be a feature among this cohort of patients, with a median BKS of 22.0 (7.4). Additionally, PTI scores were elevated at 4.9 (8.2) indicating elevated daytime sleepiness. Significant correlations were demonstrated b

Published
2022

22. Different Frequency of Heschl's Gyrus Duplication Patterns in Neuropsychiatric Disorders: An MRI Study in Bipolar and Major Depressive Disorders

Author

Takahashi, T, Sasabayashi, D, Yucel, M, Whittle, S, Lorenzetti, V, Walterfang, M, Suzuki, M, Pantelis, C, Malhi, GS, Allen, NB, Takahashi, T, Sasabayashi, D, Yucel, M, Whittle, S, Lorenzetti, V, Walterfang, M, Suzuki, M, Pantelis, C, Malhi, GS, and Allen, NB

Abstract

An increased prevalence of duplicated Heschl's gyrus (HG) has been repeatedly demonstrated in various stages of schizophrenia as a potential neurodevelopmental marker, but it remains unknown whether other neuropsychiatric disorders also exhibit this macroscopic brain feature. The present magnetic resonance imaging study aimed to examine the disease specificity of the established finding of altered HG patterns in schizophrenia by examining independent cohorts of bipolar disorder (BD) and major depressive disorder (MDD). Twenty-six BD patients had a significantly higher prevalence of HG duplication bilaterally compared to 24 age- and sex-matched controls, while their clinical characteristics (e.g., onset age, number of episodes, and medication) did not relate to HG patterns. No significant difference was found for the HG patterns between 56 MDD patients and 33 age- and sex-matched controls, but the patients with a single HG were characterized by more severe depressive/anxiety symptoms compared to those with a duplicated HG. Thus, in keeping with previous findings, the present study suggests that neurodevelopmental pathology associated with gyral formation of the HG during the late gestation period partly overlaps between schizophrenia and BD, but that HG patterns may make a somewhat distinct contribution to the phenomenology of MDD.

Published
2022

23. Huntington's disease: Mortality and risk factors in an Australian cohort

Author

Sun, E, Kang, M, Wibawa, P, Tsoukra, V, Chen, Z, Farrand, S, Eratne, D, Kelso, W, Evans, A, Walterfang, M, Velakoulis, D, Loi, SM, Sun, E, Kang, M, Wibawa, P, Tsoukra, V, Chen, Z, Farrand, S, Eratne, D, Kelso, W, Evans, A, Walterfang, M, Velakoulis, D, and Loi, SM

Abstract

INTRODUCTION: There has not been any examination of the risk factors associated with mortality in Huntington's Disease (HD) in an Australian cohort. METHOD: This retrospective study included inpatients admitted to a specialist neuropsychiatry service in Melbourne, Australia. HD status was based on genetic testing. Risk factors included age of onset, CAG repeat length and neuroimaging. Mortality data was acquired through the Australian Institute of Health and Welfare National Death Index. RESULTS: The cohort included 83 participants, with 44 (53%) deceased. The median age of death was 59 years and median survival was 18.8 years from onset age (median 41.0 years). CAG repeat length (median 44.0, IQR 42.5, 47.0) was inversely correlated with age of onset (r = -0.73) and age at death (r = -0.80) but was not correlated with mortality status. There was no difference in functional and cognitive assessments, nor brain volumes, in the alive group compared to the deceased group. There were more people who were alive who had a positive family history of a psychiatric condition (p = 0.006) or dementia (p = 0.009). Standardised mortality ratios demonstrated a 5.9× increased risk of death for those with HD compared to the general population. CONCLUSIONS: This is the first study to examine risk factors of mortality in HD in an Australian cohort. Median survival in our cohort is consistent with previous studies in HD, and markedly reduced compared to the general Australian population. CAG repeat length was not associated with mortality suggesting that non-genetic factors contribute to mortality status and warrant further investigation.

Published
2022

24. Cerebrospinal fluid neurofilament light chain differentiates primary psychiatric disorders from rapidly progressive, Alzheimer's disease and frontotemporal disorders in clinical settings

Author

Eratne, D, Loi, SM, Qiao-Xin, L, Stehmann, C, Malpas, CB, Santillo, A, Janelidze, S, Cadwallader, C, Walia, N, Ney, B, Lewis, V, Senesi, M, Fowler, C, McGlade, A, Varghese, S, Ravanfar, P, Kelso, W, Farrand, S, Keem, M, Kang, M, Goh, AMY, Dhiman, K, Gupta, V, Watson, R, Yassi, N, Kaylor-Hughes, C, Kanaan, R, Perucca, P, Dobson, H, Vivash, L, Ali, R, O'Brien, TJ, Hansson, O, Zetterberg, H, Blennow, K, Walterfang, M, Masters, CL, Berkovic, SF, Collins, S, Velakoulis, D, Eratne, D, Loi, SM, Qiao-Xin, L, Stehmann, C, Malpas, CB, Santillo, A, Janelidze, S, Cadwallader, C, Walia, N, Ney, B, Lewis, V, Senesi, M, Fowler, C, McGlade, A, Varghese, S, Ravanfar, P, Kelso, W, Farrand, S, Keem, M, Kang, M, Goh, AMY, Dhiman, K, Gupta, V, Watson, R, Yassi, N, Kaylor-Hughes, C, Kanaan, R, Perucca, P, Dobson, H, Vivash, L, Ali, R, O'Brien, TJ, Hansson, O, Zetterberg, H, Blennow, K, Walterfang, M, Masters, CL, Berkovic, SF, Collins, S, and Velakoulis, D

Abstract

INTRODUCTION: Many patients with cognitive and neuropsychiatric symptoms face diagnostic delay and misdiagnosis. We investigated whether cerebrospinal fluid (CSF) neurofilament light (NfL) and total-tau (t-tau) could assist in the clinical scenario of differentiating neurodegenerative (ND) from psychiatric disorders (PSY), and rapidly progressive disorders. METHODS: Biomarkers were examined in patients from specialist services (ND and PSY) and a national Creutzfeldt-Jakob registry (Creutzfeldt-Jakob disease [CJD] and rapidly progressive dementias/atypically rapid variants of common ND, RapidND). RESULTS: A total of 498 participants were included: 197 ND, 67 PSY, 161 CJD, 48 RapidND, and 20 controls. NfL was elevated in ND compared to PSY and controls, with highest levels in CJD and RapidND. NfL distinguished ND from PSY with 95%/78% positive/negative predictive value, 92%/87% sensitivity/specificity, 91% accuracy. NfL outperformed t-tau in most real-life clinical diagnostic dilemma scenarios, except distinguishing CJD from RapidND. DISCUSSION: We demonstrated strong generalizable evidence for the diagnostic utility of CSF NfL in differentiating ND from psychiatric disorders, with high accuracy.

Published
2022

25. Cerebrospinal fluid neurofilament light chain differentiates behavioural variant frontotemporal dementia progressors from non-progressors

Author

Eratne, D, Keem, M, Lewis, C, Kang, M, Walterfang, M, Farrand, S, Loi, S, Kelso, W, Cadwallader, C, Berkovic, SF, Li, Q-X, Masters, CL, Collins, S, Santillo, A, Velakoulis, D, Eratne, D, Keem, M, Lewis, C, Kang, M, Walterfang, M, Farrand, S, Loi, S, Kelso, W, Cadwallader, C, Berkovic, SF, Li, Q-X, Masters, CL, Collins, S, Santillo, A, and Velakoulis, D

Abstract

BACKGROUND: Distinguishing behavioural variant frontotemporal dementia (bvFTD) from non-neurodegenerative 'non-progressor' mimics of frontal lobe dysfunction, can be one of the most challenging clinical dilemmas. A biomarker of neuronal injury, neurofilament light chain (NfL), could reduce misdiagnosis and delay. METHODS: Cerebrospinal fluid (CSF) NfL, amyloid beta 1-42 (AB42), total and phosphorylated tau (T-tau, P-tau) levels were examined in patients with an initial diagnosis of bvFTD. Based on follow-up information, patients were categorised as Progressors or Non-Progressors: further subtyped into Non-Progressor Revised (non-neurological/neurodegenerative final diagnosis), and Non-Progressor Static (static deficits, not fully explained by non-neurological/neurodegenerative causes). RESULTS: Forty-three patients were included: 20 Progressors, 23 Non-Progressors (15 Non-Progressor Revised, 8 Non-Progressor Static), and 20 controls. NfL concentrations were lower in Non-Progressors (Non-Progressors Mean, M = 554 pg/mL, 95%CI:[461, 675], Non-Progressor Revised M = 459 pg/mL, 95%CI:[385, 539], and Non-Progressor Static M = 730 pg/mL, 95%CI:[516, 940]), compared to Progressors (M = 2397 pg/mL, 95%CI:[1607, 3332]). NfL distinguished Progressors from Non-Progressors with the highest accuracy (area under the curve 0.92, 90%/87% sensitivity/specificity, 86%/91% positive/negative predictive value, 88% accuracy). Non-Progressor Static tended to have higher T-tau and P-tau levels compared to Non-Progressor Revised Diagnoses. CONCLUSION: This study demonstrated strong diagnostic utility of CSF NfL to distinguish bvFTD from non-progressor variants, at baseline, with high accuracy, in a real-world clinical setting. This has important clinical implications, to improve outcomes for patients and clinicians facing this challenging clinical dilemma, healthcare services, and clinical trials. Further research is required to investigate heterogeneity within the non-progressor group and

Published
2022

26. Clinical impact of whole-genome sequencing in patients with early-onset dementia.

Author

Huq, AJ, Thompson, B, Bennett, MF, Bournazos, A, Bommireddipalli, S, Gorelik, A, Schultz, J, Sexton, A, Purvis, R, West, K, Cotter, M, Valente, G, Hughes, A, Riaz, M, Walsh, M, Farrand, S, Loi, SM, Kilpatrick, T, Brodtmann, A, Darby, D, Eratne, D, Walterfang, M, Delatycki, MB, Storey, E, Fahey, M, Cooper, S, Lacaze, P, Masters, CL, Velakoulis, D, Bahlo, M, James, PA, Winship, I, Huq, AJ, Thompson, B, Bennett, MF, Bournazos, A, Bommireddipalli, S, Gorelik, A, Schultz, J, Sexton, A, Purvis, R, West, K, Cotter, M, Valente, G, Hughes, A, Riaz, M, Walsh, M, Farrand, S, Loi, SM, Kilpatrick, T, Brodtmann, A, Darby, D, Eratne, D, Walterfang, M, Delatycki, MB, Storey, E, Fahey, M, Cooper, S, Lacaze, P, Masters, CL, Velakoulis, D, Bahlo, M, James, PA, and Winship, I

Abstract

BACKGROUND: In the clinical setting, identification of the genetic cause in patients with early-onset dementia (EOD) is challenging due to multiple types of genetic tests required to arrive at a diagnosis. Whole-genome sequencing (WGS) has the potential to serve as a single diagnostic platform, due to its superior ability to detect common, rare and structural genetic variation. METHODS: WGS analysis was performed in 50 patients with EOD. Point mutations, small insertions/deletions, as well as structural variants (SVs) and short tandem repeats (STRs), were analysed. An Alzheimer's disease (AD)-related polygenic risk score (PRS) was calculated in patients with AD. RESULTS: Clinical genetic diagnosis was achieved in 7 of 50 (14%) of the patients, with a further 8 patients (16%) found to have established risk factors which may have contributed to their EOD. Two pathogenic variants were identified through SV analysis. No expanded STRs were found in this study cohort, but a blinded analysis with a positive control identified a C9orf72 expansion accurately. Approximately 37% (7 of 19) of patients with AD had a PRS equivalent to >90th percentile risk. DISCUSSION: WGS acts as a single genetic test to identify different types of clinically relevant genetic variations in patients with EOD. WGS, if used as a first-line clinical diagnostic test, has the potential to increase the diagnostic yield and reduce time to diagnosis for EOD.

Published
2022

28. Odor Identification Testing Can Assist in the Clinical Distinction between Psychiatric Disorders and Neurological/Neurodegenerative Disorders

Author

Pachi, I. Evans, A.H. Loi, S.M. Eratne, D. Malpas, C.B. Walterfang, M. Farrand, S. Kelso, W. Stefanis, L. Velakoulis, D.

Abstract

Background/Objectives: The aim was to identify whether performance on olfactory identification can distinguish neurological/neurodegenerative disorders (NNDs) from primary psychiatric disorders (PPDs). Methods: This is a cross-sectional retrospective study of inpatients assessed in Neuropsychiatry, Royal Melbourne Hospital. Data extracted from the admission records included: demographics, tobacco use, medical comorbidities, cognitive function using the Neuropsychiatry Unit Cognitive Assessment Tool (NUCOG), and odor identification using the Sniffin' Sticks Screening 12 test. The final diagnosis for patients was informed by established diagnostic criteria. Results: A total 121 patients were included. Eighty-eight patients (73%) were diagnosed with neurological or neurodegenerative disease, including Alzheimers dementia, frontotemporal dementia, Lewy body parkinsonian-related dementias (Parkinson disease, multiple system atrophy, dementia with Lewy bodies) and other neurological causes of dementia; 33 patients (27%) were diagnosed with PPDs (including mood and psychotic disorders). Patients who scored ≤8 on the Sniffin' Sticks Screening 12 test were more likely to have NND than PPD, even after adjustment for age, sex and tobacco use (P=0.009, adjusted odds ratios=3.85, 95% confidence interval=1.40-10.62). Receiver operating characteristic curve analyses demonstrated that a score of ≤8 differentiated NND from PPD with sensitivity of 57% and specificity of 73% (receiver operating characteristic area under the curve of 0.67, P=0.004). Conclusions: Patients with neuropsychiatric difficulties who score 8 or less on Sniffin' Sticks are more likely to have a neurodegenerative illness. A cut-off score of 8 is potentially a "red flag" for clinicians faced with the diagnostic question of PPD versus NND. © 2021 Lippincott Williams and Wilkins. All rights reserved.

Published
2021

29. The diagnostic challenge among young onset dementia syndromes and primary psychiatric diseases: Results of a retrospective, 20‐year cross‐sectional study

Author

Tsoukra, P, Velakoulis, D, Wibawa, P, Malpas, CB, Walterfang, M, Evans, AH, Farrand, S, Kelso, W, Eratne, D, Loi, SM, Tsoukra, P, Velakoulis, D, Wibawa, P, Malpas, CB, Walterfang, M, Evans, AH, Farrand, S, Kelso, W, Eratne, D, and Loi, SM

Abstract

Background Distinguishing a dementia syndrome from a primary psychiatric disease in younger patients can be challenging and may lead to diagnostic change over time. The aim of this study was to examine diagnostic stability in a cohort of patients with younger‐onset neurocognitive disorders. Method We retrospectively reviewed records of patients that were admitted to our unit between 2000 and 2019, were followed‐up for ≥12 months and received a diagnosis of young onset dementia at any time point. Initial diagnosis included Alzheimer disease (AD)‐type dementia (n= 30), frontotemporal dementia (FTD) syndromes (n=44), vascular dementia (VaD, n=7), mild cognitive impairment (MCI, n= 10), primary psychiatric diseases (n=6) and other conditions such as Lewy Body Dementia (n=30). Result In a total of n=127 patients, 49 (39%) changed their initial diagnoses during follow‐up. Behavioural variant FTD (bvFTD) was the least stable diagnosis, followed by dementia not otherwise specified and MCI. Compared to patients with a stable diagnosis, those who changed exhibited: a higher cognitive score at baseline, a longer follow‐up period, greater delay to final diagnosis, and no family history of dementia. Patients switching from a neurodegenerative to a psychiatric diagnosis more likely had a long psychiatric history, while those changing from a psychiatric to a neurodegenerative diagnosis had a recent manifestation of psychiatric symptoms. Conclusion Misdiagnosis in younger patients with neurocognitive disorders is not uncommon, especially in cases of behavioural variant FTD. Late‐onset psychiatric symptoms may be the harbinger to a neurodegenerative disease. Close follow‐up and monitoring of these patients are necessary.

Published
2021

30. Mortality in FTD: An Australian perspective.

Author

Loi, SM, Chen, B, Tsoukra, P, Eratne, D, Wibawa, P, Farrand, S, Kelso, W, Evans, AH, Walterfang, M, Velakoulis, D, Loi, SM, Chen, B, Tsoukra, P, Eratne, D, Wibawa, P, Farrand, S, Kelso, W, Evans, AH, Walterfang, M, and Velakoulis, D

Abstract

THEME: Clinical manifestations TOPIC: Neuropsychiatry & beh neurology SUBTOPIC: Neuropsychiatry BACKGROUND: Survival duration in frontotemporal dementia (FTD) remains inconsistent, depending on the clinical phenotype with different risk factors identified. Risk factors to mortality include the FTD-MND presentation, a genetic predisposition (Agarwal S et al. 2019), deficits in neuropsychological tests, imaging changes (Agarwal et al. 2019; Hodges et al. 2003) and non-tau pathology (Roberson et al. 2005; Hodges et al. 2003). We aimed to identify survival duration and cause of death in this group. METHOD: All inpatients admitted to Neuropsychiatry, based at the Royal Melbourne Hospital, in metropolitan Australia from 1992 - 2014, who were diagnosed with probably FTD of any subtype were included. Linkage data was obtained by the Australian Institute of Health and Welfare (AIHW). We reviewed their clinical information including demographics, age of symptom onset, type of presenting symptom, neuroimaging and diagnosis. RESULT: Of the 528 individual inpatients identified with a dementia, there were n=100 who had a diagnosis of probable FTD. There were n=76 who had a behavioural-variant FTD (bv-FTD), n=14 who had a language-variant FTD (lang-FTD) and n=10 who had FTD-MND. 67% of the group had died. Overall median duration of survival was 10.5 years (95% CI 7.9, 12.2). There were no differences in age of death nor age onset between the three FTD-subtypes (p=0.479, p=0.289, respectively). As expected, there were significant differences in the median survival duration of the three FTD subtypes, with FTD-MND having the shortest duration (p=0.004). Causes of death based on ICD-10 were predominantly dementia-related (26.3% Other degenerative diseases of nervous system; 17.5% unspecified dementia) but also included acute myocardial infarction (7%) and alcohol-related (7%). Standardised mortality ratios (SMRs) revealed that compared to population norms, people with FTD had 8x morta

Published
2021

31. Plasma neurofilament light chain and phosphorylated tau 181 in neurodegenerative and psychiatric disorders: moving closer towards a simple diagnostic test like a 'C‐reactive protein' for the brain?

Author

Eratne, D, Santillo, A, Li, Q, Kang, M, Keem, M, Lewis, C, Loi, SM, Walterfang, M, Hansson, O, Janelidze, S, Yassi, N, Watson, R, Berkovic, SF, Masters, CL, Collins, S, Velakoulis, D, Eratne, D, Santillo, A, Li, Q, Kang, M, Keem, M, Lewis, C, Loi, SM, Walterfang, M, Hansson, O, Janelidze, S, Yassi, N, Watson, R, Berkovic, SF, Masters, CL, Collins, S, and Velakoulis, D

Abstract

Background Accurate, timely diagnosis of neurodegenerative disorders, in particular distinguishing primary psychiatric from neurological disorders and in younger people, can be challenging. There is a need for biomarkers to reduce the diagnostic odyssey and improve outcomes. Neurofilament light (NfL) has shown promise as a diagnostic biomarker in a wide range of disorders. Our Markers in Neuropsychiatric Disorders (MiND) Study builds on our pilot (Eratne et al, ANZJP, 2020), to explore the diagnostic and broader utility of plasma and cerebrospinal fluid (CSF) NfL and other novel markers such as phosphorylated tau 181 (p‐tau181), in a broad range of psychiatric and neurodegenerative/neurological disorders, with a view of translation into routine clinical practice. Methods We assessed plasma and/or CSF NfL and p‐tau181 concentrations in broad cohorts, including: patients assessed for neurocognitive/psychiatric symptoms at Neuropsychiatry and Melbourne Young‐Onset Dementia services and other services, in a wide range of disorders including Alzheimer disease, frontotemporal dementia, schizophrenia, bipolar disorder, depression, Niemann‐Pick Type C, epilepsy, functional neurological disorders. The most recent primary consensus diagnosis informed by established diagnostic criteria was categorised: primary psychiatric disorder (PPD), neurodegenerative/neurological disorder (ND), or healthy controls (HC). Results Findings from over 500 patients/participants will be presented, which indicate that CSF and plasma NfL levels are significantly elevated in a broad range of ND compared to a broad range of PPD, and HC, and bvFTD progressors from phenocopy syndromes, differentiating with areas under the curve of >0.90, sensitivity and specificity >90%. Plasma P‐tau181 levels distinguished Alzheimer disease (mainly younger sporadic), compared to other neurodegenerative disorders, with AUC 0.90, 90% sensitivity and specificity. As recruitment, sample analysis, data coll

Published
2021

32. Characterization of Dysphagia and Longitudinal Changes in Swallowing Function in Adults with Niemann-Pick Disease Type C Treated with Miglustat.

Author

Lewis C., Keage M., Watanabe M., Schubiger D., Velakoulis D., Walterfang M., Vogel A.P., Lewis C., Keage M., Watanabe M., Schubiger D., Velakoulis D., Walterfang M., and Vogel A.P.

Abstract

Niemann-Pick disease type C (NPC) is a rare, autosomal recessive neurodegenerative disease, characterized by progressive psychiatric and neurological deficits. Neurological symptoms include cognitive decline and dysphagia. Aspiration pneumonia secondary to dysphagia is a leading cause of death in NPC. Miglustat is currently the only approved disease-specific treatment shown to be effective in stabilizing neurological symptoms. Miglustat has previously been reported to halt or improve early dysphagia and cognitive symptoms. Here we examine the characteristics of dysphagia, the relationship between dysphagia and the presence of cognitive impairment, and longitudinal changes in swallowing function during miglustat treatment in adult-and-adolescent-onset NPC. Retrospective analysis of videofluoroscopic swallow studies (VFSS) was completed for ten adults with NPC (mean age 28.44 years +/- 9.34 years). Participants were recruited through the Royal Melbourne Hospital in Australia between 2008 and 2015. The Bethlehem Swallowing Scale and the Penetration-Aspiration Scale were used to quantify VFSS data. Dysphagia was present in 90% of participants at baseline with reduced lingual function and a delayed swallowing reflex as the most common symptoms. Swallow impairment appeared to stabilize during miglustat therapy for periods up to 66 months, with no significant changes in scores (p > 0.05). Data were in accordance with the literature and support the use of miglustat as an efficacious treatment for reducing swallowing impairment and stabilizing cognitive function. Findings provide detailed information on the impairments experienced by patients, give context to events leading to aspiration in NPC and, importantly, inform how management of dysphagia can complement pharmaceutical treatment.Copyright © 2020, Springer Science+Business Media, LLC, part of Springer Nature.

Published
2021

33. A cross-sectional, prospective ocular motor study in 72 patients with Niemann-Pick disease type C

Author

Bremova-Ertl, T, Abel, Larry, Walterfang, M, Salsano, E, Ardissone, A, Malinová, V, Kolníková, M, Gascón Bayarri, J, Reza Tavasoli, A, Reza Ashrafi, M, Amraoui, Y, Mengel, E, Kolb, SA, Brecht, A, Bardins, S, Strupp, M, Bremova-Ertl, T, Abel, Larry, Walterfang, M, Salsano, E, Ardissone, A, Malinová, V, Kolníková, M, Gascón Bayarri, J, Reza Tavasoli, A, Reza Ashrafi, M, Amraoui, Y, Mengel, E, Kolb, SA, Brecht, A, Bardins, S, and Strupp, M

Published
2021

34. A 10 year retrospective cohort study of inpatients with younger-onset dementia

Author

Loi, SM, Eratne, D, Goh, AMY, Wibawa, P, Farrand, S, Kelso, W, Evans, A, Watson, R, Walterfang, M, Velakoulis, D, Loi, SM, Eratne, D, Goh, AMY, Wibawa, P, Farrand, S, Kelso, W, Evans, A, Watson, R, Walterfang, M, and Velakoulis, D

Abstract

OBJECTIVES: Younger-onset dementia (YOD) refers to a dementia where symptom onset occurs when the patient is less than 65 years of age. YOD is far less common than late-onset dementia (occurring when patients are over 65 years old) and more challenging to diagnose due to its heterogeneous presentation. There have been relatively few studies describing demographic and diagnostic characteristics of patients with YOD in the community, particularly with follow-up information. METHODS: A retrospective cohort study was performed of inpatients admitted to a tertiary neuropsychiatry service, located in metropolitan Victoria, Australia, from 2009 to 2019. Inpatients with a YOD diagnosis were identified and data regarding diagnosis, demographics and investigations were obtained. RESULTS: There were 849 individual inpatients who were admitted to the service in the 10-year period and received comprehensive assessment. There were 306 individuals who received a YOD diagnosis, using contemporaneous diagnostic criteria (frequency 36%). The most common diagnoses were Alzheimer's disease (24.2%), frontotemporal dementia (23.1%), Huntington's disease (16.7%) and vascular dementia (7.8%). More than half of these inpatients were followed up and 6.5% had a diagnostic change when reviewed. CONCLUSIONS: This study reports on the largest cohort of YOD to date, with diagnostic breakdown similar to previous retrospective file reviews. The neuropsychiatry service is funded to follow-up its patients, thus allowing re-assessment and continuity of care. While there are limitations in this study such as the lack of neuropathological outcomes, the findings emphasise the strengths of follow-up and appropriate service provision for these patients.

Published
2021

35. The effect of improved dietary control on cognitive and psychiatric functioning in adults with phenylketonuria: the ReDAPT study

Author

Burgess, NM, Kelso, W, Malpas, CB, Winton-Brown, T, Fazio, T, Panetta, J, De Jong, G, Neath, J, Atherton, S, Velakoulis, D, Walterfang, M, Burgess, NM, Kelso, W, Malpas, CB, Winton-Brown, T, Fazio, T, Panetta, J, De Jong, G, Neath, J, Atherton, S, Velakoulis, D, and Walterfang, M

Abstract

BACKGROUND: Phenylketonuria (PKU) is an autosomal recessive inherited disorder characterised by a deficiency in phenylalanine hydroxylase. Untreated, PKU is associated with a wide range of cognitive and psychiatric sequelae. Contemporary management guidelines recommend lifetime dietary control of phenylalanine (Phe) levels, however many individuals who discontinue dietary control subsequently suffer symptoms of anxiety, depression and disturbances to cognition. We undertook a prospective cohort study of patients with early-treated phenylketonuria who had ceased dietary control to test the hypothesis that resumption of dietary control of PKU is associated with improvements in measures of psychiatric morbidity and cognitive functioning. METHODS: We re-initiated dietary control for early-treated patients with PKU and monitored cognitive and psychiatric outcomes over a twelve-month period. Assessments included objective cognitive function (measured by cognitive proficiency index (CPI)), anxiety and depression scales. General linear mixed model (GLMM) analyses were performed to assess change in psychometric variables from baseline over twelve months after resumption of dietary control. RESULTS: A total of nine patients were recruited. Mean age was 33 years (SD = 8.75), five were female. Mean time off dietary control was 19.1 years (SD = 11.3), and mean baseline phenylalanine (Phe) levels were 1108 µmol/L (SD = 293). GLMM analysis demonstrated a positive relationship between CPI and time on diet (b = 0.56 [95% CI = 0.17, 0.95]). Age, time off diet, Phe levels and depression scores were not associated with cognitive function. There was a negative relationship between time on diet and anxiety (b = - 0.88 95% CI = [- 1.26, - 0.50]) and depression ratings (b = - 0.61, 95% CI = [- 0.95, - 0.26]). CONCLUSIONS: This study demonstrated improvements in cognitive function, anxiety, and depression ratings associated with resumption of dietary control of PKU. Raw Phe levels were not

Published
2021

38. Probability of major depression classification based on the SCID, CIDI, and MINI diagnostic interviews: A synthesis of three individual participant data meta-analyses

Author

Wu, Y. Levis, B. Ioannidis, J.P.A. Benedetti, A. Thombs, B.D. Sun, Y. He, C. Krishnan, A. Bhandari, P.M. Neupane, D. Negeri, Z. Imran, M. Rice, D.B. Riehm, K.E. Saadat, N. Azar, M. Levis, A.W. Sanchez, T.A. Chiovitti, M.J. Yan, X.W. Boruff, J. Kloda, L.A. Cuijpers, P. Gilbody, S. McMillan, D. Patten, S.B. Shrier, I. Ziegelstein, R.C. Comeau, L. Mitchell, N.D. Tonelli, M. Vigod, S.N. Henry, M. Ismail, Z. Loiselle, C.G. Akena, D.H. Al-Adawi, S. Alamri, S.H. Alvarado, R. Alvarado-Esquivel, C. Amtmann, D. Arroll, B. Ayalon, L. Bakare, M.O. Baradaran, H.R. Barnes, J. Bavle, A.D. Beck, C.T. Beraldi, A. Bernstein, C.N. Bhana, A. Bindt, C. Bombardier, C.H. Boyce, P.M. Büel-Drabe, N. Buji, R.I. Bunevicius, A. Butnoriene, J. Bunevicius, R. Butterworth, P. Carter, G. Chagas, M.H. Chan, J.C.N. Chan, L.F. Chaudron, L.H. Chen, C.-K. Cholera, R. Clover, K. Conroy, R.M. Conway, A. Conwell, Y. Correa, H. Castro E Couto, T. Cukor, D. Dabscheck, E. Daray, F.M. De Figueiredo, F.P. De Man-Van Ginkel, J.M. Diez-Quevedo, C. Douven, E. Downing, M.G. Eapen, V. Fann, J.R. Feinstein, A. Ferentinos, P.P. Fernandes, M. Field, S. Figueiredo, B. Fischer, F.H. Fisher, J.R.W. Flint, A.J. Fujimori, M. Fung, D.S.S. Gallagher, P. Gandy, M. Garcia-Esteve, L. Garman, E.C. Gelaye, B. Gholizadeh, L. Giardinelli, L. Gibson, L.J. Goodyear-Smith, F. Grassi, L. Green, E.P. Greeno, C.G. Hall, B.J. Hantsoo, L. Haroz, E.E. Harter, M. Hegerl, U. Helle, N. Hides, L. Hobfoll, S.E. Honikman, S. Howard, L.M. Hudson, M. Hyphantis, T. Inagaki, M. Jenewein, J. Jeon, H.J. Jette, N. Keller, M. Khalifa, D.S. Khamseh, M.E. Kiely, K.M. Kim, S.-W. Kjargaard, M. Kohler, S. Kohlhoff, J. Kohrt, B.A. Kozinszky, Z. Kusminskas, L. Kwan, Y. Lamers, F. Lara, M.A. Lelli, L. Leonardou, A.A. Levin-Aspenson, H.F. Lotrakul, M. Loureiro, S.R. Lowe, B. Luitel, N.P. Lund, C. Maes, M. Marrie, R.A. Marsh, L. Martin-Santos, R. Marx, B.P. Massardo, L. Matsuoka, Y. Mehner, A. Meuti, V. Michopoulos, I. Misery, L. Sidik, S.M. Munhoz, T.N. Muramatsu, K. Radoš, S.N. Nakku, J.E.M. Navarrete, L. Garcia, P.N. Navines, R. Nishi, D. O'Donnell, M.L. Luwa E-Andjafono, D.O. Osório, F.L. Öztürk, A. Peceliuniene, J. Pence, B.W. Persoons, P. Picardi, A. Pintor, L. Ponsford, J.L. Pugh, S.L. Quinn, T.J. Rancans, E. Rathod, S.D. Reme, S.E. Reuter, K. Robertson-Blackmore, E. Rochat, T.J. Rooney, A.G. Rowe, H.J. Sánchez-González, R. Santos, I.S. Schram, M.T. Schwarzbold, M.L. Cankorur, V.S. Shaaban, J. Sharpe, L. Shinn, E.H. Sidebottom, A. Simard, S. Simning, A. Singer, S. Siu, B.W.M. Skalkidou, A. Spangenberg, L. Stafford, L. Stein, A. Stewart, R.C. Stone, J. Su, K.-P. Sultan, S. Sundström-Poromaa, I. Sung, S.C. Suzuki, K. Tadinac, M. Tan, P.L.L. Tandon, S.D. Taylor-Rowan, M. Teixeira, A.L. Tendais, I. Thiagayson, P. Tiringer, I. Töreki, A. Torres-Giménez, A. Tran, T.D. Trevillion, K. Tung, K.-Y. Turner, A. Turner, K. Van Der Feltz-Cornelis, C.M. Van Heyningen, T. Van Weert, H.C. Vega-Dienstmaier, J.M. Vöhringer, P.A. Wagner, L.I. Walterfang, M. Wang, J.L. Wang, W. Wang, L.-J. White, J. Wong, D.K. Wynter, K. Yamada, M. Yonkers, K.A. Zeng, Q.Z. Zhang, Y. DEPRESsion Screening Data (DEPRESSD) Collaboration

Abstract

Introduction: Three previous individual participant data meta-analyses (IPDMAs) reported that, compared to the Structured Clinical Interview for the DSM (SCID), alternative reference standards, primarily the Composite International Diagnostic Interview (CIDI) and the Mini International Neuropsychiatric Interview (MINI), tended to misclassify major depression status, when controlling for depression symptom severity. However, there was an important lack of precision in the results. Objective: To compare the odds of the major depression classification based on the SCID, CIDI, and MINI. Methods: We included and standardized data from 3 IPDMA databases. For each IPDMA, separately, we fitted binomial generalized linear mixed models to compare the adjusted odds ratios (aORs) of major depression classification, controlling for symptom severity and characteristics of participants, and the interaction between interview and symptom severity. Next, we synthesized results using a DerSimonian-Laird random-effects meta-analysis. Results: In total, 69,405 participants (7,574 [11%] with major depression) from 212 studies were included. Controlling for symptom severity and participant characteristics, the MINI (74 studies; 25,749 participants) classified major depression more often than the SCID (108 studies; 21,953 participants; aOR 1.46; 95% confidence interval [CI] 1.11-1.92]). Classification odds for the CIDI (30 studies; 21,703 participants) and the SCID did not differ overall (aOR 1.19; 95% CI 0.79-1.75); however, as screening scores increased, the aOR increased less for the CIDI than the SCID (interaction aOR 0.64; 95% CI 0.52-0.80). Conclusions: Compared to the SCID, the MINI classified major depression more often. The odds of the depression classification with the CIDI increased less as symptom levels increased. Interpretation of research that uses diagnostic interviews to classify depression should consider the interview characteristics. © 2020

Published
2020

39. Depression prevalence using the HADS-D compared to SCID major depression classification: An individual participant data meta-analysis

Author

Brehaut, E. Neupane, D. Levis, B. Wu, Y. Sun, Y. Krishnan, A. He, C. Bhandari, P.M. Negeri, Z. Riehm, K.E. Rice, D.B. Azar, M. Yan, X.W. Imran, M. Chiovitti, M.J. Saadat, N. Cuijpers, P. Ioannidis, J.P.A. Markham, S. Patten, S.B. Ziegelstein, R.C. Henry, M. Ismail, Z. Loiselle, C.G. Mitchell, N.D. Tonelli, M. Boruff, J.T. Kloda, L.A. Beraldi, A. Braeken, A.P.B.M. Carter, G. Clover, K. Conroy, R.M. Cukor, D. da Rocha e Silva, C.E. De Souza, J. Downing, M.G. Feinstein, A. Ferentinos, P.P. Fischer, F.H. Flint, A.J. Fujimori, M. Gallagher, P. Goebel, S. Jetté, N. Julião, M. Keller, M. Kjærgaard, M. Love, A.W. Löwe, B. Martin-Santos, R. Michopoulos, I. Navines, R. O'Rourke, S.J. Öztürk, A. Pintor, L. Ponsford, J.L. Rooney, A.G. Sánchez-González, R. Schwarzbold, M.L. Sharpe, M. Simard, S. Singer, S. Stone, J. Tung, K.-Y. Turner, A. Walker, J. Walterfang, M. White, J. Benedetti, A. Thombs, B.D.

Abstract

Objectives: Validated diagnostic interviews are required to classify depression status and estimate prevalence of disorder, but screening tools are often used instead. We used individual participant data meta-analysis to compare prevalence based on standard Hospital Anxiety and Depression Scale – depression subscale (HADS-D) cutoffs of ≥8 and ≥11 versus Structured Clinical Interview for DSM (SCID) major depression and determined if an alternative HADS-D cutoff could more accurately estimate prevalence. Methods: We searched Medline, Medline In-Process & Other Non-Indexed Citations via Ovid, PsycINFO, and Web of Science (inception-July 11, 2016) for studies comparing HADS-D scores to SCID major depression status. Pooled prevalence and pooled differences in prevalence for HADS-D cutoffs versus SCID major depression were estimated. Results: 6005 participants (689 SCID major depression cases) from 41 primary studies were included. Pooled prevalence was 24.5% (95% Confidence Interval (CI): 20.5%, 29.0%) for HADS-D ≥8, 10.7% (95% CI: 8.3%, 13.8%) for HADS-D ≥11, and 11.6% (95% CI: 9.2%, 14.6%) for SCID major depression. HADS-D ≥11 was closest to SCID major depression prevalence, but the 95% prediction interval for the difference that could be expected for HADS-D ≥11 versus SCID in a new study was −21.1% to 19.5%. Conclusions: HADS-D ≥8 substantially overestimates depression prevalence. Of all possible cutoff thresholds, HADS-D ≥11 was closest to the SCID, but there was substantial heterogeneity in the difference between HADS-D ≥11 and SCID-based estimates. HADS-D should not be used as a substitute for a validated diagnostic interview. © 2020 Elsevier Inc.

Published
2020

40. Probability of major depression diagnostic classification based on the SCID, CIDI and MINI diagnostic interviews controlling for Hospital Anxiety and Depression Scale – Depression subscale scores: An individual participant data meta-analysis of 73 primary studies

Author

Wu, Y. Levis, B. Sun, Y. Krishnan, A. He, C. Riehm, K.E. Rice, D.B. Azar, M. Yan, X.W. Neupane, D. Bhandari, P.M. Imran, M. Chiovitti, M.J. Saadat, N. Boruff, J.T. Cuijpers, P. Gilbody, S. McMillan, D. Ioannidis, J.P.A. Kloda, L.A. Patten, S.B. Shrier, I. Ziegelstein, R.C. Henry, M. Ismail, Z. Loiselle, C.G. Mitchell, N.D. Tonelli, M. Al-Adawi, S. Beraldi, A. Braeken, A.P.B.M. Büel-Drabe, N. Bunevicius, A. Carter, G. Chen, C.-K. Cheung, G. Clover, K. Conroy, R.M. Cukor, D. da Rocha e Silva, C.E. Dabscheck, E. Daray, F.M. Douven, E. Downing, M.G. Feinstein, A. Ferentinos, P.P. Fischer, F.H. Flint, A.J. Fujimori, M. Gallagher, P. Gandy, M. Goebel, S. Grassi, L. Härter, M. Jenewein, J. Jetté, N. Julião, M. Kim, J.-M. Kim, S.-W. Kjærgaard, M. Köhler, S. Loosman, W.L. Löwe, B. Martin-Santos, R. Massardo, L. Matsuoka, Y. Mehnert, A. Michopoulos, I. Misery, L. Navines, R. O'Donnell, M.L. Öztürk, A. Peceliuniene, J. Pintor, L. Ponsford, J.L. Quinn, T.J. Reme, S.E. Reuter, K. Rooney, A.G. Sánchez-González, R. Schwarzbold, M.L. Senturk Cankorur, V. Shaaban, J. Sharpe, L. Sharpe, M. Simard, S. Singer, S. Stafford, L. Stone, J. Sultan, S. Teixeira, A.L. Tiringer, I. Turner, A. Walker, J. Walterfang, M. Wang, L.-J. White, J. Wong, D.K. Benedetti, A. Thombs, B.D.

Abstract

Objective: Two previous individual participant data meta-analyses (IPDMAs) found that different diagnostic interviews classify different proportions of people as having major depression overall or by symptom levels. We compared the odds of major depression classification across diagnostic interviews among studies that administered the Depression subscale of the Hospital Anxiety and Depression Scale (HADS-D). Methods: Data accrued for an IPDMA on HADS-D diagnostic accuracy were analysed. We fit binomial generalized linear mixed models to compare odds of major depression classification for the Structured Clinical Interview for DSM (SCID), Composite International Diagnostic Interview (CIDI), and Mini International Neuropsychiatric Interview (MINI), controlling for HADS-D scores and participant characteristics with and without an interaction term between interview and HADS-D scores. Results: There were 15,856 participants (1942 [12%] with major depression) from 73 studies, including 15,335 (97%) non-psychiatric medical patients, 164 (1%) partners of medical patients, and 357 (2%) healthy adults. The MINI (27 studies, 7345 participants, 1066 major depression cases) classified participants as having major depression more often than the CIDI (10 studies, 3023 participants, 269 cases) (adjusted odds ratio [aOR] = 1.70 (0.84, 3.43)) and the semi-structured SCID (36 studies, 5488 participants, 607 cases) (aOR = 1.52 (1.01, 2.30)). The odds ratio for major depression classification with the CIDI was less likely to increase as HADS-D scores increased than for the SCID (interaction aOR = 0.92 (0.88, 0.96)). Conclusion: Compared to the SCID, the MINI may diagnose more participants as having major depression, and the CIDI may be less responsive to symptom severity. © 2019 Elsevier Inc.

Published
2020

41. Time to diagnosis in younger-onset dementia and the impact of a specialist diagnostic service.

Author

Farrand S., Kelso W., Velakoulis D., Walterfang M., Evans A., Loi S.M., Goh A.M.Y., Mocellin R., Malpas C.B., Parker S., Eratne D., Farrand S., Kelso W., Velakoulis D., Walterfang M., Evans A., Loi S.M., Goh A.M.Y., Mocellin R., Malpas C.B., Parker S., and Eratne D.

Abstract

Objectives:While early diagnosis of younger-onset dementia (YOD) is crucial in terms of accessing appropriate services and future planning, diagnostic delays are common. This study aims to identify predictors of delay to diagnosis in a large sample of people with YOD and to investigate the impact of a specialist YOD service on this time to diagnosis. Design(s):A retrospective cross-sectional study. Setting(s):The inpatient unit of a tertiary neuropsychiatry service in metropolitan Victoria, Australia. Participant(s):People diagnosed with a YOD.Measurements and methods:We investigated the following predictors using general linear modeling: demographics including sex and location, age at onset, dementia type, cognition, psychiatric diagnosis, and number of services consulted with prior to diagnosis. Result(s):A total of 242 inpatients were included. The mean time to diagnosis was 3.4 years. Significant predictors of delay included younger age at onset, dementia type other than Alzheimer's disease (AD) and behavioral-variant frontotemporal dementia (bvFTD), and increased number of services consulted. These predictors individually led to an increased diagnostic delay of approximately 19 days, 5 months, and 6 months, respectively. A specialized YOD service reduced time to diagnosis by 12 months. Conclusion(s):We found that younger age at onset, having a dementia which was not the most commonly occurring AD or bvFTD, and increasing number of services were significant predictors of diagnostic delay. A novel result was that a specialist YOD service may decrease diagnostic delay, highlighting the importance of such as service in reducing time to diagnosis as well as providing post-diagnostic support. Copyright © International Psychogeriatric Association 2020.

Published
2020

42. The disappearance of white matter in an adult-onset disease: a case report

Author

Ho, CSH, Mangelsdorf, S, Walterfang, M, Ho, CSH, Mangelsdorf, S, and Walterfang, M

Abstract

BACKGROUND: Vanishing white matter disease (VWMD) is one of the most prevalent hereditary white matter diseases in childhood, but it is increasingly recognised in adulthood with high phenotypic variation and severity. CASE PRESENTATION: We report a case of an adult female presenting with emotional lability and cognitive impairment, in addition to progressive dystonia, ataxia, postural instability and recurrent falls. Magnetic resonance imaging (MRI) of the brain and genetic testing confirmed the diagnosis of VWMD. CONCLUSIONS: VWMD has a broad clinical presentation in adulthood, and the age at onset of symptoms is one of its most important prognostic factors. It is crucial to recognize the pathognomonic MRI patterns and consider VWMD as a differential diagnosis when assessing patients presenting with psychiatric, cognitive and non-specific neurological symptoms.

Published
2020

43. Probability of major depression diagnostic classification based on the SCID, CIDI and MINI diagnostic interviews controlling for Hospital Anxiety and Depression Scale - Depression subscale scores: An individual participant data meta-analysis of 73 primary studies

Author

Wu, Y, Levis, B, Sun, Y, Krishnan, A, He, C, Riehm, KE, Rice, DB, Azar, M, Yan, XW, Neupane, D, Bhandari, PM, Imran, M, Chiovitti, MJ, Saadat, N, Boruff, JT, Cuijpers, P, Gilbody, S, McMillan, D, Ioannidis, JPA, Kloda, LA, Patten, SB, Shrier, I, Ziegelstein, RC, Henry, M, Ismail, Z, Loiselle, CG, Mitchell, ND, Tonelli, M, Al-Adawi, S, Beraldi, A, Braeken, APBM, Bueel-Drabe, N, Bunevicius, A, Carter, G, Chen, C-K, Cheung, G, Clover, K, Conroy, RM, Cukor, D, Rocha e Silva, CE, Dabscheck, E, Daray, FM, Douven, E, Downing, MG, Feinstein, A, Ferentinos, PP, Fischer, FH, Flint, AJ, Fujimori, M, Gallagher, P, Gandy, M, Goebel, S, Grassi, L, Haerter, M, Jenewein, J, Jette, N, Juliao, M, Kim, J-M, Kim, S-W, Kjaergaard, M, Kohler, S, Loosman, WL, Loewe, B, Martin-Santos, R, Massardo, L, Matsuoka, Y, Mehnert, A, Michopoulos, I, Misery, L, Navines, R, O'Donnell, ML, Ozturk, A, Peceliuniene, J, Pintor, L, Ponsford, JL, Quinn, TJ, Reme, SE, Reuter, K, Rooney, AG, Sanchez-Gonzalez, R, Schwarzbold, ML, Cankorur, VS, Shaaban, J, Sharpe, L, Sharpe, M, Simard, S, Singer, S, Stafford, L, Stone, J, Sultan, S, Teixeira, AL, Tiringer, I, Turner, A, Walker, J, Walterfang, M, Wang, L-J, White, J, Wong, DK, Benedetti, A, Thombs, BD, Wu, Y, Levis, B, Sun, Y, Krishnan, A, He, C, Riehm, KE, Rice, DB, Azar, M, Yan, XW, Neupane, D, Bhandari, PM, Imran, M, Chiovitti, MJ, Saadat, N, Boruff, JT, Cuijpers, P, Gilbody, S, McMillan, D, Ioannidis, JPA, Kloda, LA, Patten, SB, Shrier, I, Ziegelstein, RC, Henry, M, Ismail, Z, Loiselle, CG, Mitchell, ND, Tonelli, M, Al-Adawi, S, Beraldi, A, Braeken, APBM, Bueel-Drabe, N, Bunevicius, A, Carter, G, Chen, C-K, Cheung, G, Clover, K, Conroy, RM, Cukor, D, Rocha e Silva, CE, Dabscheck, E, Daray, FM, Douven, E, Downing, MG, Feinstein, A, Ferentinos, PP, Fischer, FH, Flint, AJ, Fujimori, M, Gallagher, P, Gandy, M, Goebel, S, Grassi, L, Haerter, M, Jenewein, J, Jette, N, Juliao, M, Kim, J-M, Kim, S-W, Kjaergaard, M, Kohler, S, Loosman, WL, Loewe, B, Martin-Santos, R, Massardo, L, Matsuoka, Y, Mehnert, A, Michopoulos, I, Misery, L, Navines, R, O'Donnell, ML, Ozturk, A, Peceliuniene, J, Pintor, L, Ponsford, JL, Quinn, TJ, Reme, SE, Reuter, K, Rooney, AG, Sanchez-Gonzalez, R, Schwarzbold, ML, Cankorur, VS, Shaaban, J, Sharpe, L, Sharpe, M, Simard, S, Singer, S, Stafford, L, Stone, J, Sultan, S, Teixeira, AL, Tiringer, I, Turner, A, Walker, J, Walterfang, M, Wang, L-J, White, J, Wong, DK, Benedetti, A, and Thombs, BD

Abstract

OBJECTIVE: Two previous individual participant data meta-analyses (IPDMAs) found that different diagnostic interviews classify different proportions of people as having major depression overall or by symptom levels. We compared the odds of major depression classification across diagnostic interviews among studies that administered the Depression subscale of the Hospital Anxiety and Depression Scale (HADS-D). METHODS: Data accrued for an IPDMA on HADS-D diagnostic accuracy were analysed. We fit binomial generalized linear mixed models to compare odds of major depression classification for the Structured Clinical Interview for DSM (SCID), Composite International Diagnostic Interview (CIDI), and Mini International Neuropsychiatric Interview (MINI), controlling for HADS-D scores and participant characteristics with and without an interaction term between interview and HADS-D scores. RESULTS: There were 15,856 participants (1942 [12%] with major depression) from 73 studies, including 15,335 (97%) non-psychiatric medical patients, 164 (1%) partners of medical patients, and 357 (2%) healthy adults. The MINI (27 studies, 7345 participants, 1066 major depression cases) classified participants as having major depression more often than the CIDI (10 studies, 3023 participants, 269 cases) (adjusted odds ratio [aOR] = 1.70 (0.84, 3.43)) and the semi-structured SCID (36 studies, 5488 participants, 607 cases) (aOR = 1.52 (1.01, 2.30)). The odds ratio for major depression classification with the CIDI was less likely to increase as HADS-D scores increased than for the SCID (interaction aOR = 0.92 (0.88, 0.96)). CONCLUSION: Compared to the SCID, the MINI may diagnose more participants as having major depression, and the CIDI may be less responsive to symptom severity.

Published
2020

44. Use of olanzapine to treat agitation in traumatic brain injury: study protocol for a randomised controlled trial

Author

Phyland, RK, McKay, A, Olver, J, Walterfang, M, Hopwood, M, Hicks, AJ, Mortimer, D, Ponsford, JL, Phyland, RK, McKay, A, Olver, J, Walterfang, M, Hopwood, M, Hicks, AJ, Mortimer, D, and Ponsford, JL

Abstract

BACKGROUND: Agitation is common in the early stages of recovery from traumatic brain injury (TBI), when patients are in post-traumatic amnesia (PTA). Agitation is associated with risk of harm to patients and caregivers. Recent guidelines recommend that agitation during PTA is managed using environmental modifications. Agitation is also frequently treated pharmacologically, with the use of atypical antipsychotics such as olanzapine among the most common. This is despite a lack of well-designed studies to support the use of antipsychotics within this context. This study will be a double-blind, placebo-controlled randomised controlled trial. We will examine the efficacy, safety, cost-effectiveness and outcomes associated with the use of olanzapine for reducing agitation in patients in PTA following TBI over and above recommended environmental management. METHODS: Fifty-eight TBI rehabilitation inpatients who are in PTA and are agitated will receive olanzapine or placebo for the duration of PTA. All participants will additionally receive optimal environmental management for agitation. Measures of agitation, PTA and health will be undertaken at baseline. Treatment administration will begin at a dose of 5 mg daily and may be escalated to a maximum dose of 20 mg per day. Throughout the treatment period, agitation and PTA will be measured daily, and adverse events monitored weekly. Efficacy will be assessed by treatment group comparison of average Agitated Behaviour Scale scores during PTA. Participants will cease treatment upon emergence from PTA. Agitation levels will continue to be monitored for a further 2 weeks, post-treatment measures of health will be undertaken and cognitive and functional status will be assessed. Level of agitation and functional health will be assessed at hospital discharge. At 3 months post-discharge, functional outcomes and health service utilisation will be measured. DISCUSSION: This trial will provide crucial evidence to inform the management

Published
2020

45. Pineal Gland Volume in Major Depressive and Bipolar Disorders

Author

Takahashi, T, Sasabayashi, D, Yucel, M, Whittle, S, Lorenzetti, V, Walterfang, M, Suzuki, M, Pantelis, C, Malhi, GS, Allen, NB, Takahashi, T, Sasabayashi, D, Yucel, M, Whittle, S, Lorenzetti, V, Walterfang, M, Suzuki, M, Pantelis, C, Malhi, GS, and Allen, NB

Abstract

Abnormal melatonin secretion has been demonstrated in patients with affective disorders such as major depressive disorder (MDD) and bipolar disorder (BD). However, magnetic resonance imaging (MRI) studies that previously investigated the volume of the pineal gland, which regulates circadian rhythms by secreting melatonin, in these patients reported inconsistent findings. The present study employed MRI to examine pineal gland volumes and pineal cyst prevalence in 56 MDD patients (29 currently depressed and 27 remitted patients), 26 BD patients, and matched controls (33 for MDD and 24 for BD). Pineal volumes and cyst prevalence in the current MDD, remitted MDD, and BD groups did not significantly differ from those of the healthy controls. However, pineal gland volumes were significantly smaller in the current MDD subgroup of non-melancholic depression than in the melancholic MDD subgroup. Interestingly, pineal volumes correlated negatively with the severity of loss of interest in the current MDD group. Medication and the number of affective episodes were not associated with pineal volumes in the MDD or BD group. While these results do not suggest that pineal volumes reflect abnormal melatonin secretion in affective disorders, they do point to the possibility that pineal abnormalities are associated with clinical subtypes of MDD and its symptomatology.

Published
2020

46. Depression prevalence using the HADS-D compared to SCID major depression classification: An individual participant data meta-analysis

Author

Brehaut, E, Neupane, D, Levis, B, Wu, Y, Sun, Y, Krishnan, A, He, C, Bhandari, PM, Negeri, Z, Riehm, KE, Rice, DB, Azar, M, Yan, XW, Imran, M, Chiovitti, MJ, Saadat, N, Cuijpers, P, Ioannidis, JPA, Markham, S, Patten, SB, Ziegelstein, RC, Henry, M, Ismail, Z, Loiselle, CG, Mitchell, ND, Tonelli, M, Boruff, JT, Kloda, LA, Beraldi, A, Braeken, APBM, Carter, G, Clover, K, Conroy, RM, Cukor, D, da Rocha E Silva, CE, De Souza, J, Downing, MG, Feinstein, A, Ferentinos, PP, Fischer, FH, Flint, AJ, Fujimori, M, Gallagher, P, Goebel, S, Jette, N, Juliao, M, Keller, M, Kjaergaard, M, Love, AW, Loewe, B, Martin-Santos, R, Michopoulos, I, Navines, R, O'Rourke, SJ, Ozturk, A, Pintor, L, Ponsford, JL, Rooney, AG, Sanchez-Gonzalez, R, Schwarzbold, ML, Sharpe, M, Simard, S, Singer, S, Stone, J, Tung, K-Y, Turner, A, Walker, J, Walterfang, M, White, J, Benedetti, A, Thombs, BD, Brehaut, E, Neupane, D, Levis, B, Wu, Y, Sun, Y, Krishnan, A, He, C, Bhandari, PM, Negeri, Z, Riehm, KE, Rice, DB, Azar, M, Yan, XW, Imran, M, Chiovitti, MJ, Saadat, N, Cuijpers, P, Ioannidis, JPA, Markham, S, Patten, SB, Ziegelstein, RC, Henry, M, Ismail, Z, Loiselle, CG, Mitchell, ND, Tonelli, M, Boruff, JT, Kloda, LA, Beraldi, A, Braeken, APBM, Carter, G, Clover, K, Conroy, RM, Cukor, D, da Rocha E Silva, CE, De Souza, J, Downing, MG, Feinstein, A, Ferentinos, PP, Fischer, FH, Flint, AJ, Fujimori, M, Gallagher, P, Goebel, S, Jette, N, Juliao, M, Keller, M, Kjaergaard, M, Love, AW, Loewe, B, Martin-Santos, R, Michopoulos, I, Navines, R, O'Rourke, SJ, Ozturk, A, Pintor, L, Ponsford, JL, Rooney, AG, Sanchez-Gonzalez, R, Schwarzbold, ML, Sharpe, M, Simard, S, Singer, S, Stone, J, Tung, K-Y, Turner, A, Walker, J, Walterfang, M, White, J, Benedetti, A, and Thombs, BD

Abstract

OBJECTIVES: Validated diagnostic interviews are required to classify depression status and estimate prevalence of disorder, but screening tools are often used instead. We used individual participant data meta-analysis to compare prevalence based on standard Hospital Anxiety and Depression Scale - depression subscale (HADS-D) cutoffs of ≥8 and ≥11 versus Structured Clinical Interview for DSM (SCID) major depression and determined if an alternative HADS-D cutoff could more accurately estimate prevalence. METHODS: We searched Medline, Medline In-Process & Other Non-Indexed Citations via Ovid, PsycINFO, and Web of Science (inception-July 11, 2016) for studies comparing HADS-D scores to SCID major depression status. Pooled prevalence and pooled differences in prevalence for HADS-D cutoffs versus SCID major depression were estimated. RESULTS: 6005 participants (689 SCID major depression cases) from 41 primary studies were included. Pooled prevalence was 24.5% (95% Confidence Interval (CI): 20.5%, 29.0%) for HADS-D ≥8, 10.7% (95% CI: 8.3%, 13.8%) for HADS-D ≥11, and 11.6% (95% CI: 9.2%, 14.6%) for SCID major depression. HADS-D ≥11 was closest to SCID major depression prevalence, but the 95% prediction interval for the difference that could be expected for HADS-D ≥11 versus SCID in a new study was -21.1% to 19.5%. CONCLUSIONS: HADS-D ≥8 substantially overestimates depression prevalence. Of all possible cutoff thresholds, HADS-D ≥11 was closest to the SCID, but there was substantial heterogeneity in the difference between HADS-D ≥11 and SCID-based estimates. HADS-D should not be used as a substitute for a validated diagnostic interview.

Published
2020

47. A study protocol for a phase II randomised, double-blind, placebo-controlled trial of sodium selenate as a disease-modifying treatment for behavioural variant frontotemporal dementia

Author

Vivash, L, Malpas, CB, Churilov, L, Walterfang, M, Brodtmann, A, Piguet, O, Ahmed, RM, Bush, A, Hovens, CM, Kalincik, T, Darby, D, Velakoulis, D, O'Brien, TJ, Vivash, L, Malpas, CB, Churilov, L, Walterfang, M, Brodtmann, A, Piguet, O, Ahmed, RM, Bush, A, Hovens, CM, Kalincik, T, Darby, D, Velakoulis, D, and O'Brien, TJ

Abstract

INTRODUCTION: Behavioural variant frontotemporal dementia (bvFTD) is a neurodegenerative disorder often neuropathologically associated with the accumulation of abnormally hyperphosphorylated tau, for which there is currently no disease-modifying treatment. Previous work by our group has shown sodium selenate upregulates the activity of protein phosphatase 2 in the brain, increasing the rate of tau dephosphorylation. The objective of this study is to evaluate the efficacy and safety of sodium selenate as a disease-modifying treatment for bvFTD. METHODS AND ANALYSIS: This will be a multisite, phase IIb, double-blind placebo-controlled trial of sodium selenate. One hundred and twenty participants will be enrolled across 4 Australian academic hospitals. Following screening eligible participants will be randomised (1:1) to sodium selenate (15 mg three times a day) or placebo for 52 weeks. Participants will have regular safety and efficacy visits throughout the study period. The primary study outcome will be percentage brain volume change (PBVC) as measured on MRI over 52 weeks of treatment. This will be analysed with a general linear model (analysis of covariance (ANCOVA)) with the PBVC as an output, the treatment as an input and the baseline brain volume as covariate for adjustment purposes. Secondary outcomes include safety and tolerability measures, and efficacy measures; change in cerebrospinal fluid total-tau, Addenbrooke's Cognitive Examination-III and Cambridge Behavioural Inventory-Revised scores over the 52 weeks of treatment. These will also be analysed with ANCOVA where the corresponding baseline measure will be incorporated in the model. Additional exploratory outcomes will include other imaging, cognitive and biospecimen analyses. ETHICS AND DISSEMINATION: The study was approved by the Human Research and Ethics Committee of the lead site as part of the Australian Multisite Ethics approval system. The results of the study will be presented at national and int

Published
2020

48. Imaging of neuroinflammation in adult Niemann-Pick type C disease: a cross-sectional study

Author

Walterfang, M, Di Biase, MA, Cropley, VL, Scott, AM, O'Keefe, G, Velakoulis, D, Pathmaraj, K, Ackermann, U, Pantelis, C, Walterfang, M, Di Biase, MA, Cropley, VL, Scott, AM, O'Keefe, G, Velakoulis, D, Pathmaraj, K, Ackermann, U, and Pantelis, C

Abstract

Objective: To test the hypothesis that neuroinflammation is a key process in adult Niemann-Pick type C (NPC) disease, we undertook PET scanning utilizing a ligand binding activated microglia on 9 patients and 9 age- and sex-matched controls. Method: We scanned all participants with the PET radioligand 11C-(R)-PK-11195 and undertook structural MRI to measure gray matter volume and white matter fractional anisotropy (FA). Results: We found increased binding of 11C-(R)-PK-11195 in total white matter compared to controls (p < 0.01), but not in gray matter regions, and this did not correlate with illness severity or duration. Gray matter was reduced in the thalamus (p < 0.0001) in patients, who also showed widespread reductions in FA across the brain compared to controls (p < 0.001). A significant correlation between 11C-(R)-PK11195 binding and FA was shown (p = 0.002), driven by the NPC patient group. Conclusions: Our findings suggest that neuroinflammation—particularly in white matter—may underpin some structural and degenerative changes in patients with NPC.

Published
2020

49. OCD symptoms in succinic semialdehyde dehydrogenase (SSADH) deficiency: a case report

Author

Phakey, S, Rego, T, Gaillard, F, Panetta, J, Evans, A, De Jong, G, Walterfang, M, Phakey, S, Rego, T, Gaillard, F, Panetta, J, Evans, A, De Jong, G, and Walterfang, M

Abstract

BACKGROUND: Succinic semialdehyde dehydrogenase (SSADH) deficiency is a rare neurometabolic disorder resulting in a heterogeneous clinical phenotype. Adolescent and adult patients with SSADH deficiency may present with OCD symptoms. There is minimal literature regarding the pathological basis of OCD symptoms and their management amongst SSADH deficiency patients. CASE PRESENTATION: A 26-year-old woman with SSADH deficiency experienced obsessional slowness and hesitancy in her activities of daily living, with motor rituals and stereotypies of her hands and face. Neuroimaging revealed T2 hyperintensities of the globi pallidi bilaterally. Commencement of the serotonergic escitalopram moderately improved her OCD symptoms. The addition of the dopaminergic pramipexole hydrochloride yielded further improvement, following unsuccessful trial of other adjuncts: risperidone, methylphenidate and mirtazapine. CONCLUSIONS: Pallidal pathology may explain the manifestation of OCD symptoms amongst individuals with SSADH deficiency. Serotonergic and concomitant dopaminergic therapy may be a viable treatment regimen for SSADH deficiency patients presenting with OCD symptoms.

Published
2020

Catalog

Books, media, physical & digital resources
See catalog results