Association of <i>NOTCH2NLC</i> Repeat Expansions With Parkinson Disease

Ma, Dongrui; Tan, Yi Jayne; Ng, Adeline Su Lyn; Ong, Helen; Sim, Weiying; Lim, Weng Khong; Teo, Jing Xian; Ng, Ebonne Yulin; Lim, Ee-Chien; Lim, Ee-Wei; Chan, Ling‐Ling; Tan, Louis C.S.; Zhao, Yongxiang; Tan, Eng‐King

doi:10.1001/jamaneurol.2020.3023

Cited by 74 publications

(80 citation statements)

References 11 publications

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“…2.B.C). A growing number of diseases caused by non-coding repeat expansions are often associate with parkinsonism, including fragile X-associated tremor/ataxia syndrome (FXTAS) and neuronal intranuclear inclusion disease [26,27]. Midbrain atrophy-related parkinsonism was reported in patients with FXTAS although its association with this disease remains elusive [28][29][30].…”

Section: Discussionmentioning

confidence: 99%

Midbrain Atrophy Related to Parkinsonism in a Non-Coding Repeat Expansion Disorder: Five Cases of Spinocerebellar Ataxia Type 31 With Nigrostriatal Dopaminergic Dysfunction

Norioka;¹,

Sugaya

Murayama

et al. 2021

Preprint

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BackgroundSpinocerebellar ataxia type 31 (SCA31) is caused by non-coding pentanucleotide repeat expansions in the BEAN1 gene. Clinically, SCA31 is characterized by late-adult onset, pure cerebellar ataxia. To explore the association between parkinsonism and SCA31, five patients with SCA31 with concomitant nigrostriatal dopaminergic dysfunction (NSDD) development, including three cases of L-DOPA responsive parkinsonism, were characterized. MethodsTo assess regional brain atrophy, cross-sectional and longitudinal imaging analyses were retrospectively performed using Magnetic resonance imaging (MRI) planimetry. The midbrain-to-pons (M/P) area ratio and cerebellar area were measured on midsagittal T1-weighted MRI in five patients with NSDD (NSDD(+)), 14 patients with SCA31 without NSDD (NSDD(-)), 32 patients with Parkinson’s disease (PD), and 15 patients with progressive supranuclear palsy. Longitudinal changes in the M/P area ratio were assessed by serial MRI of NSDD(+) (n = 5) and NSDD(-) (n = 9). ResultsThe clinical characteristics relevant to parkinsonism in NSDD(+) were indistinguishable from those of PD except for the prominence of bradykinesia/akinesia (5/5) and the absence of dysautonomia (5/5). However, a clear reduction in the midbrain area and the M/P area ratio was observed in NSDD(+) (p <0.05) while there was no significant difference in disease duration or in the pons area among NSDD(+), NSDD(-), and PD. A faster rate of decline in the midbrain area and the M/P area ratio was evident in NSDD(+) (p <0.05).ConclusionThe unique features of midbrain atrophy related to NSDD in our patients suggest that SCA31 belongs to the group of non-coding repeat expansion disorders causing parkinsonism.

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Section: Discussionmentioning

confidence: 99%

Midbrain Atrophy Related to Parkinsonism in a Non-Coding Repeat Expansion Disorder: Five Cases of Spinocerebellar Ataxia Type 31 With Nigrostriatal Dopaminergic Dysfunction

Norioka;¹,

Sugaya

Murayama

et al. 2021

Preprint

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“…3.B.C). A growing number of diseases caused by non-coding repeat expansions are often associate with parkinsonism, including fragile X-associated tremor/ataxia syndrome (FXTAS) and neuronal intranuclear inclusion disease [33,34]. Midbrain atrophy-related parkinsonism was reported in patients with FXTAS although its association with this disease remains elusive [35][36][37].…”

Section: Discussionmentioning

confidence: 99%

Midbrain atrophy related to parkinsonism in a non-coding repeat expansion disorder: five cases of spinocerebellar ataxia type 31 with nigrostriatal dopaminergic dysfunction

Norioka

Sugaya

Murayama

et al. 2021

Preprint

View full text Add to dashboard Cite

Background Spinocerebellar ataxia type 31 (SCA31) is caused by non-coding pentanucleotide repeat expansions in the BEAN1 gene. Clinically, SCA31 is characterized by late-adult onset, pure cerebellar ataxia. To explore the association between parkinsonism and SCA31, five patients with SCA31 with concomitant nigrostriatal dopaminergic dysfunction (NSDD) development, including three cases of L-DOPA responsive parkinsonism, were characterized. Methods To assess regional brain atrophy, cross-sectional and longitudinal imaging analyses were retrospectively performed using magnetic resonance imaging (MRI) planimetry. The midbrain-to-pons (M/P) area ratio and cerebellar area were measured on midsagittal T1-weighted MRI in five patients with SCA31 with concomitant NSDD (NSDD(+)), 14 patients with SCA31 without NSDD (NSDD(-)), 32 patients with Parkinson’s disease (PD), and 15 patients with progressive supranuclear palsy (PSP). Longitudinal changes in the M/P area ratio were assessed by serial MRI of NSDD(+) (n = 5) and NSDD(-) (n = 9). Results The clinical characteristics assessed in the five patients with NSDD were as follows: the mean age at NSDD onset (72.0 ± 10.8 years), prominence of bradykinesia/akinesia (5/5), rigidity (4/5), tremor (2/5), dysautonomia (0/5), vertical gaze limitation (1/5), and abnormalities on 123I-ioflupane dopamine transporter scintigraphy (3/3) and 3-Tesla neuromelanin MRI (4/4). A clear reduction in the midbrain area and the M/P area ratio was observed in the NSDD(+) group (p < 0.05) while there was no significant difference in disease duration or in the pons area among the NSDD(+), NSDD(-), and PD groups. There was also a significant difference in the midbrain and pons area between NSDD(+) and PSP (p < 0.05). Thus, mild but significant midbrain atrophy was observed in NSDD(+). A faster rate of decline in the midbrain area and the M/P area ratio was evident in NSDD(+) (p < 0.05). Conclusion The clinical characteristics of five patients with SCA31 with concomitant NSDD, together with the topographical pattern of atrophy, were inconsistent with those of PD, PSP, or multiple system atrophy, suggesting that SCA31 may manifest NSDD in association with the pathomechanisms underlying SCA31.

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“…3b, c). A growing number of diseases caused by non-coding repeat expansions are often associated with parkinsonism, including fragile X-associated tremor/ataxia syndrome (FXTAS) and neuronal intranuclear inclusion disease [33,34]. Midbrain atrophy-related parkinsonism was reported in patients with FXTAS although its association with this disease remains elusive [35][36][37].…”

Section: Discussionmentioning

confidence: 99%

Midbrain atrophy related to parkinsonism in a non-coding repeat expansion disorder: five cases of spinocerebellar ataxia type 31 with nigrostriatal dopaminergic dysfunction

et al. 2021

View full text Add to dashboard Cite

Background Spinocerebellar ataxia type 31 (SCA31) is caused by non-coding pentanucleotide repeat expansions in the BEAN1 gene. Clinically, SCA31 is characterized by late adult-onset, pure cerebellar ataxia. To explore the association between parkinsonism and SCA31, five patients with SCA31 with concomitant nigrostriatal dopaminergic dysfunction (NSDD) development, including three cases of L-DOPA responsive parkinsonism, were analyzed. Methods To assess regional brain atrophy, cross-sectional and longitudinal imaging analyses were retrospectively performed using magnetic resonance imaging (MRI) planimetry. The midbrain-to-pons (M/P) area ratio and cerebellar area were measured on midsagittal T1-weighted MRI in five patients with SCA31 with concomitant NSDD (NSDD(+)), 14 patients with SCA31 without NSDD (NSDD(−)), 32 patients with Parkinson’s disease (PD), and 15 patients with progressive supranuclear palsy (PSP). Longitudinal changes in the M/P area ratio were assessed by serial MRI of NSDD(+) (n = 5) and NSDD(−) (n = 9). Results The clinical characteristics assessed in the five patients with NSDD were as follows: the mean age at NSDD onset (72.0 ± 10.8 years), prominence of bradykinesia/akinesia (5/5), rigidity (4/5), tremor (2/5), dysautonomia (0/5), vertical gaze limitation (1/5), and abnormalities on 123I-ioflupane dopamine transporter scintigraphy (3/3) and 3-Tesla neuromelanin MRI (4/4). A clear reduction in the midbrain area and the M/P area ratio was observed in the NSDD(+) group (p < 0.05) while there was no significant difference in disease duration or in the pons area among the NSDD(+), NSDD(−), and PD groups. There was also a significant difference in the midbrain and pons area between NSDD(+) and PSP (p < 0.05). Thus, mild but significant midbrain atrophy was observed in NSDD(+). A faster rate of decline in the midbrain area and the M/P area ratio was evident in NSDD(+) (p < 0.05). Conclusion The clinical characteristics of the five patients with SCA31 with concomitant NSDD, together with the topographical pattern of atrophy, were inconsistent with PD, PSP, and multiple system atrophy, suggesting that SCA31 may manifest NSDD in association with the pathomechanisms underlying SCA31.

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Association of NOTCH2NLC Repeat Expansions With Parkinson Disease

Cited by 74 publications

References 11 publications

Midbrain Atrophy Related to Parkinsonism in a Non-Coding Repeat Expansion Disorder: Five Cases of Spinocerebellar Ataxia Type 31 With Nigrostriatal Dopaminergic Dysfunction

Midbrain Atrophy Related to Parkinsonism in a Non-Coding Repeat Expansion Disorder: Five Cases of Spinocerebellar Ataxia Type 31 With Nigrostriatal Dopaminergic Dysfunction

Midbrain atrophy related to parkinsonism in a non-coding repeat expansion disorder: five cases of spinocerebellar ataxia type 31 with nigrostriatal dopaminergic dysfunction

Midbrain atrophy related to parkinsonism in a non-coding repeat expansion disorder: five cases of spinocerebellar ataxia type 31 with nigrostriatal dopaminergic dysfunction

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