The genetics of motor neuron disease in New Zealand

Miran Mrkela; Miriam Rodrigues; Serey Naidoo; Jules B. L. Devaux; Siobhan E. Kirk; Chitra Vinnakota; Christina M. Buchanan; Dympna Mulroy; Harry Fraser; Jessie C. Jacobsen; Hannah Wyatt; Kylie Drake; Elsa Parker; Howard Potter; Lyndal Henden; Emily P. McCann; Kelly L. Williams; Anjali K. Henders; Richard H. Roxburgh; Emma L. Scotter

doi:10.1016/j.jns.2025.123472

The genetics of motor neuron disease in New Zealand

Miran Mrkela, Miriam Rodrigues, Serey Naidoo, Jules B. L. Devaux, Siobhan E. Kirk, Chitra Vinnakota, Christina M. Buchanan, Dympna Mulroy, Harry Fraser, Jessie C. Jacobsen, Hannah Wyatt, Kylie Drake, Elsa Parker, Howard Potter, Lyndal Henden, Emily P. McCann, Kelly L. Williams, Anjali K. Henders, Richard H. Roxburgh, Emma L. Scotter

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

Abstract

Motor neuron disease (MND) is a group of adult-onset neurodegenerative diseases characterised by progressive motor neuron degeneration, of which amyotrophic lateral sclerosis (ALS) is the most common. MND is clinically heterogeneous with complex etiology, caused by or associated with over 40 different genes and multiple environmental risk factors. New Zealand has one of the highest global incidence and mortality rates of MND, however the reasons are unknown.We sought to identify the frequencies of genetic variants in known MND-linked genes among people with MND in New Zealand. We enrolled 184 participants: 149 with a clinical diagnosis of MND (128 sporadic, 21 familial) and 35 clinically unaffected but at-risk individuals. Participants' DNA was screened for genetic variation in 46 MND-associated genes using Sanger sequencing, Illumina SNP microarray, repeat-primed PCR for C9orf72, and an Invitae gene panel.Clinical phenotypes mirrored European trends: males and spinal-onset cases had earlier disease onset. Thirty-three participants (17.9?%) carried known pathogenic variants: 24 had C9orf72 repeat expansions, and 9 had pathogenic SOD1 variants (p.(Ile114Thr) and p.(Glu101Gly)). All New Zealand SOD1 p.(Ile114Thr) cases (n?=?4) were distantly related to each other and to over 30 Australian cases with the same variant. Variants of interest were found in 14 participants with the splicing variants DCTN1:c.279?+?1G?>?C and ATP13A2:c.2412G?>?A, p.(Lys804=) subject to further study. Notably, 48.4?% of pathogenic variants were in pre-symptomatic, unaffected individuals with family history, highlighting the importance of offering cascade testing and symptom surveillance for families, particularly as gene-specific treatments emerge.

Original language	English
Article number	123472
Pages (from-to)	1-13
Number of pages	13
Journal	Journal of the Neurological Sciences
Volume	474
DOIs	https://doi.org/10.1016/j.jns.2025.123472
Publication status	Accepted/In press - 23 Mar 2025

Bibliographical note

Copyright the Author(s) 2025. Version archived for private and non-commercial use with the permission of the author/s and according to publisher conditions. For further rights please contact the publisher.

Keywords

Amyotrophic lateral sclerosis
Genetic screening
Genetics
Motor neuron disease
New Zealand
Pre-symptomatic

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10.1016/j.jns.2025.123472Licence: CC BY

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Mrkela, M., Rodrigues, M., Naidoo, S., Devaux, J. B. L., Kirk, S. E., Vinnakota, C., Buchanan, C. M., Mulroy, D., Fraser, H., Jacobsen, J. C., Wyatt, H., Drake, K., Parker, E., Potter, H., Henden, L., McCann, E. P., Williams, K. L., Henders, A. K., Roxburgh, R. H., & Scotter, E. L. (Accepted/In press). The genetics of motor neuron disease in New Zealand. Journal of the Neurological Sciences, 474, 1-13. Article 123472. https://doi.org/10.1016/j.jns.2025.123472

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title = "The genetics of motor neuron disease in New Zealand",

abstract = "Motor neuron disease (MND) is a group of adult-onset neurodegenerative diseases characterised by progressive motor neuron degeneration, of which amyotrophic lateral sclerosis (ALS) is the most common. MND is clinically heterogeneous with complex etiology, caused by or associated with over 40 different genes and multiple environmental risk factors. New Zealand has one of the highest global incidence and mortality rates of MND, however the reasons are unknown.We sought to identify the frequencies of genetic variants in known MND-linked genes among people with MND in New Zealand. We enrolled 184 participants: 149 with a clinical diagnosis of MND (128 sporadic, 21 familial) and 35 clinically unaffected but at-risk individuals. Participants' DNA was screened for genetic variation in 46 MND-associated genes using Sanger sequencing, Illumina SNP microarray, repeat-primed PCR for C9orf72, and an Invitae gene panel.Clinical phenotypes mirrored European trends: males and spinal-onset cases had earlier disease onset. Thirty-three participants (17.9?%) carried known pathogenic variants: 24 had C9orf72 repeat expansions, and 9 had pathogenic SOD1 variants (p.(Ile114Thr) and p.(Glu101Gly)). All New Zealand SOD1 p.(Ile114Thr) cases (n?=?4) were distantly related to each other and to over 30 Australian cases with the same variant. Variants of interest were found in 14 participants with the splicing variants DCTN1:c.279?+?1G?>?C and ATP13A2:c.2412G?>?A, p.(Lys804=) subject to further study. Notably, 48.4?% of pathogenic variants were in pre-symptomatic, unaffected individuals with family history, highlighting the importance of offering cascade testing and symptom surveillance for families, particularly as gene-specific treatments emerge.",

keywords = "Amyotrophic lateral sclerosis, Genetic screening, Genetics, Motor neuron disease, New Zealand, Pre-symptomatic",

author = "Miran Mrkela and Miriam Rodrigues and Serey Naidoo and Devaux, {Jules B. L.} and Kirk, {Siobhan E.} and Chitra Vinnakota and Buchanan, {Christina M.} and Dympna Mulroy and Harry Fraser and Jacobsen, {Jessie C.} and Hannah Wyatt and Kylie Drake and Elsa Parker and Howard Potter and Lyndal Henden and McCann, {Emily P.} and Williams, {Kelly L.} and Henders, {Anjali K.} and Roxburgh, {Richard H.} and Scotter, {Emma L.}",

note = "Copyright the Author(s) 2025. Version archived for private and non-commercial use with the permission of the author/s and according to publisher conditions. For further rights please contact the publisher.",

year = "2025",

month = mar,

day = "23",

doi = "10.1016/j.jns.2025.123472",

language = "English",

volume = "474",

pages = "1--13",

journal = "Journal of the Neurological Sciences",

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Mrkela, M, Rodrigues, M, Naidoo, S, Devaux, JBL, Kirk, SE, Vinnakota, C, Buchanan, CM, Mulroy, D, Fraser, H, Jacobsen, JC, Wyatt, H, Drake, K, Parker, E, Potter, H, Henden, L, McCann, EP, Williams, KL, Henders, AK, Roxburgh, RH & Scotter, EL 2025, 'The genetics of motor neuron disease in New Zealand', Journal of the Neurological Sciences, vol. 474, 123472, pp. 1-13. https://doi.org/10.1016/j.jns.2025.123472

TY - JOUR

T1 - The genetics of motor neuron disease in New Zealand

AU - Mrkela, Miran

AU - Rodrigues, Miriam

AU - Naidoo, Serey

AU - Devaux, Jules B. L.

AU - Kirk, Siobhan E.

AU - Vinnakota, Chitra

AU - Buchanan, Christina M.

AU - Mulroy, Dympna

AU - Fraser, Harry

AU - Jacobsen, Jessie C.

AU - Wyatt, Hannah

AU - Drake, Kylie

AU - Parker, Elsa

AU - Potter, Howard

AU - Henden, Lyndal

AU - McCann, Emily P.

AU - Williams, Kelly L.

AU - Henders, Anjali K.

AU - Roxburgh, Richard H.

AU - Scotter, Emma L.

N1 - Copyright the Author(s) 2025. Version archived for private and non-commercial use with the permission of the author/s and according to publisher conditions. For further rights please contact the publisher.

PY - 2025/3/23

Y1 - 2025/3/23

N2 - Motor neuron disease (MND) is a group of adult-onset neurodegenerative diseases characterised by progressive motor neuron degeneration, of which amyotrophic lateral sclerosis (ALS) is the most common. MND is clinically heterogeneous with complex etiology, caused by or associated with over 40 different genes and multiple environmental risk factors. New Zealand has one of the highest global incidence and mortality rates of MND, however the reasons are unknown.We sought to identify the frequencies of genetic variants in known MND-linked genes among people with MND in New Zealand. We enrolled 184 participants: 149 with a clinical diagnosis of MND (128 sporadic, 21 familial) and 35 clinically unaffected but at-risk individuals. Participants' DNA was screened for genetic variation in 46 MND-associated genes using Sanger sequencing, Illumina SNP microarray, repeat-primed PCR for C9orf72, and an Invitae gene panel.Clinical phenotypes mirrored European trends: males and spinal-onset cases had earlier disease onset. Thirty-three participants (17.9?%) carried known pathogenic variants: 24 had C9orf72 repeat expansions, and 9 had pathogenic SOD1 variants (p.(Ile114Thr) and p.(Glu101Gly)). All New Zealand SOD1 p.(Ile114Thr) cases (n?=?4) were distantly related to each other and to over 30 Australian cases with the same variant. Variants of interest were found in 14 participants with the splicing variants DCTN1:c.279?+?1G?>?C and ATP13A2:c.2412G?>?A, p.(Lys804=) subject to further study. Notably, 48.4?% of pathogenic variants were in pre-symptomatic, unaffected individuals with family history, highlighting the importance of offering cascade testing and symptom surveillance for families, particularly as gene-specific treatments emerge.

AB - Motor neuron disease (MND) is a group of adult-onset neurodegenerative diseases characterised by progressive motor neuron degeneration, of which amyotrophic lateral sclerosis (ALS) is the most common. MND is clinically heterogeneous with complex etiology, caused by or associated with over 40 different genes and multiple environmental risk factors. New Zealand has one of the highest global incidence and mortality rates of MND, however the reasons are unknown.We sought to identify the frequencies of genetic variants in known MND-linked genes among people with MND in New Zealand. We enrolled 184 participants: 149 with a clinical diagnosis of MND (128 sporadic, 21 familial) and 35 clinically unaffected but at-risk individuals. Participants' DNA was screened for genetic variation in 46 MND-associated genes using Sanger sequencing, Illumina SNP microarray, repeat-primed PCR for C9orf72, and an Invitae gene panel.Clinical phenotypes mirrored European trends: males and spinal-onset cases had earlier disease onset. Thirty-three participants (17.9?%) carried known pathogenic variants: 24 had C9orf72 repeat expansions, and 9 had pathogenic SOD1 variants (p.(Ile114Thr) and p.(Glu101Gly)). All New Zealand SOD1 p.(Ile114Thr) cases (n?=?4) were distantly related to each other and to over 30 Australian cases with the same variant. Variants of interest were found in 14 participants with the splicing variants DCTN1:c.279?+?1G?>?C and ATP13A2:c.2412G?>?A, p.(Lys804=) subject to further study. Notably, 48.4?% of pathogenic variants were in pre-symptomatic, unaffected individuals with family history, highlighting the importance of offering cascade testing and symptom surveillance for families, particularly as gene-specific treatments emerge.

KW - Amyotrophic lateral sclerosis

KW - Genetic screening

KW - Genetics

KW - Motor neuron disease

KW - New Zealand

KW - Pre-symptomatic

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U2 - 10.1016/j.jns.2025.123472

DO - 10.1016/j.jns.2025.123472

M3 - Article

C2 - 40424855

SN - 0022-510X

VL - 474

SP - 1

EP - 13

JO - Journal of the Neurological Sciences

JF - Journal of the Neurological Sciences

M1 - 123472

ER -

The genetics of motor neuron disease in New Zealand

Abstract

Bibliographical note

Keywords

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