The Spectrum of Neurological and White Matter Changes and Premutation Status Categories of Older Male Carriers of the FMR1 Alleles Are Linked to Genetic (CGG and FMR1 mRNA) and Cellular Stress (AMPK) Markers

Loesch, Danuta Z.; Trost, Nicholas; Bui, Minh; Hammersley, Eleanor; Lay, Sui T.; Annesley, Sarah J.; Sanislav, Oana; Allan, Claire Y.; Tassone, Flora; Chen, Zhi Ping; Ngoei, Kevin R.W.; Kemp, Bruce E.; Francis, David; Fisher, Paul R.; Storey, Elsdon

doi:10.3389/fgene.2018.00531

Cited by 10 publications

(46 citation statements)

References 64 publications

(81 reference statements)

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“…Notably, when taken together with our previous study (19), the current findings imply a continuity in the clinical and white matter changes extending from non-affected older male carriers, to non-syndromic forms separate from FXTAS, and eventually to the full manifestation of FXTAS. Moreover, the finding of significant correlations between the wmhs in infratentorial regions and the motor and cognitive scores in the total sample of PM carriers suggests that the underlying primary pathology might be initially confined to this region.…”

Section: Discussionsupporting

confidence: 83%

“…This suggests that white matter alterations may serve as sensitive markers of incipient decline to FXTAS, or to asyndromic neurological manifestations not meeting the diagnostic criteria for FXTAS. This aspect was discussed in our earlier publication (19), where we reported an example of the presence of the MCP sign in some non-FXTAS PM carriers, consistent with similar observations in five such individuals most recently reported by Famula et al (20).…”

Section: Introductionsupporting

confidence: 93%

“…We have shown that whms within the infratentorial region is associated with impairments across the categories of clinical status for all the three motor rating scores, and a range of neuropsychological cognitive measures. This is supportive of the notion that the scope of the spectrum of premutation-related clinical and brain changes, especially those in infratentorial regions specifically affected in FXTAS, appear to extend beyond the classical syndromic forms of FXTAS, and across the categories of non-affected and non-syndromic carriers, comprising asymptomatic, asyndromic and FXTAS groups (19). In addition, in the FXTAS group we have demonstrated a highly significant relationship between supratentorial (periventricular) lesions and parkinsonism, and between both periventricular and supratentorial deep white matter lesions and the ICARS ataxia score.…”

Section: Discussionsupporting

confidence: 72%

“…However, this approach clearly served the purpose of our study, which aimed to establish whether white matter lesions in supratentorial, as well as infratentorial regions, contribute to motor and cognitive changes characteristic of the spectrum of premutation involvement. The validity of the wmh scores applied in this study was further attested by demonstration of the highly significant associations of all the wmhs scores used here with the levels of “toxic” FMR1 mRNA in a previous study (19). Finally, our study design did not include examination of the gray matter changes that have been reported by others in FXTAS (13, 14, 39, 40).…”

Section: Discussionmentioning

confidence: 66%

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Total and Regional White Matter Lesions Are Correlated With Motor and Cognitive Impairments in Carriers of the FMR1 Premutation

et al. 2019

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This study explores the relationships between hemispheric and cerebellar white matter lesions and motor and cognitive impairments in male carriers of Fragile-X Mental Retardation 1 ( FMR1 ) premutation alleles, and in a subgroup of these carriers affected with Fragile X-Associated Tremor/Ataxia syndrome (FXTAS). Regional and total white matter hyperintensities ( wmhs ) on MRI, assessed using semiquantitative scores, were correlated with three motor rating scales (ICARS, UPDRS, Tremor), and neuropsychological measures of non-verbal reasoning, working memory and processing speed, in a sample of 30 male premutation carriers aged 39–81 years, and separately in a subsample of 17 of these carriers affected with FXTAS. There were significant relationships between wmhs in the infratentorial region and all three motor scales, as well as several cognitive measures—Prorated IQ, Matrix Reasoning, Similarities, and the Symbol Digit Modalities Test (SDMT), in the total sample of carriers, as well as in the FXTAS group separately. This shows that whms within the infratentorial region correlates across the categories of clinical status with a range of motor and cognitive impairments. In the FXTAS group, there was a highly significant relationship between supratentorial (periventricular) lesions and parkinsonism, and between both periventricular and supratentorial deep white matter and ICARS ataxia score. These findings further support the relevance of white matter changes in different brain regions to the motor and cognitive deficits across the spectrum of premutation involvement. Future longitudinal studies using larger sample sizes will be necessary to examine the factors that lead to conversion to a greater extent of neurological involvement as seen in the progression across the FXTAS spectrum.

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Section: Discussionsupporting

confidence: 83%

Section: Introductionsupporting

confidence: 93%

Section: Discussionsupporting

confidence: 72%

Section: Discussionmentioning

confidence: 66%

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Total and Regional White Matter Lesions Are Correlated With Motor and Cognitive Impairments in Carriers of the FMR1 Premutation

et al. 2019

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“…Our data on progression of the premutation-associated changes from sub-symptomatic to clinical forms, especially in females, may have an important impact on future research, as well as on clinical approaches, because it introduces the concept of continuity. Combined with earlier evidence for the existence of subclinical neural or metabolic changes in both male and female carriers over a broad age range (Tassone et al, 2012 ; Wang et al, 2012 , 2013 , 2017 ; Battistella et al, 2013 ; Shelton et al, 2016 ; Loesch et al, 2017 , 2018 ; Hocking et al, 2019 ; O'Keeffe et al, 2019 ), these data have shown that the focus of such research should be on trajectories rather than on the final outcome of the premutation-associated process. The most recent study, based on a wide range of metabolic and proteomic biomarkers, showed a decline of mitochondrial activities in pre-symptomatic female PM carriers, leading the authors to the conclusion that the development of neurodegeneration or other clinical symptoms in older carriers could be linked to a lifetime accumulation of cellular damage, aggravated by the aging process (Napoli et al, 2020 ).…”

Section: Discussionmentioning

confidence: 62%

Differential Progression of Motor Dysfunction Between Male and Female Fragile X Premutation Carriers Reveals Novel Aspects of Sex-Specific Neural Involvement

Loesch

Tassone

Atkinson

et al. 2021

Front. Mol. Biosci.

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Expansions of the CGG repeat in the non-coding segment of the FMR1 X-linked gene are associated with a variety of phenotypic changes. Large expansions (>200 repeats), which cause a severe neurodevelopmental disorder, the fragile x syndrome (FXS), are transmitted from the mothers carrying smaller, unstable expansions ranging from 55 to 200 repeats, termed the fragile X premutation. Female carriers of this premutation may themselves experience a wide range of clinical problems throughout their lifespan, the most severe being the late onset neurodegenerative condition called “Fragile X-Associated Tremor Ataxia Syndrome” (FXTAS), occurring between 8 and 16% of these carriers. Male premutation carriers, although they do not transmit expanded alleles to their daughters, have a much higher risk (40–50%) of developing FXTAS. Although this disorder is more prevalent and severe in male than female carriers, specific sex differences in clinical manifestations and progress of the FXTAS spectrum have been poorly documented. Here we compare the pattern and rate of progression (per year) in three motor scales including tremor/ataxia (ICARS), tremor (Clinical Tremor Rating scale, CRST), and parkinsonism (UPDRS), and in several cognitive and psychiatric tests scores, between 13 female and 9 male carriers initially having at least one of the motor scores ≥10. Moreover, we document the differences in each of the clinical and cognitive measures between the cross-sectional samples of 21 female and 24 male premutation carriers of comparable ages with FXTAS spectrum disorder (FSD), that is, who manifest one or more features of FXTAS. The results of progression assessment showed that it was more than twice the rate in male than in female carriers for the ICARS-both gait ataxia and kinetic tremor domains and twice as high in males on the CRST scale. In contrast, sex difference was negligible for the rate of progress in UPDRS, and all the cognitive measures. The overall psychiatric pathology score (SCL-90), as well as Anxiety and Obsessive/Compulsive domain scores, showed a significant increase only in the female sample. The pattern of sex differences for progression in motor scores was consistent with the results of comparison between larger, cross-sectional samples of male and female carriers affected with the FSD. These results were in concert with sex-specific distribution of MRI T2 white matter hyperintensities: all males, but no females, showed the middle cerebellar peduncle white matter hyperintensities (MCP sign), although the distribution and severity of these hyperintensities in the other brain regions were not dissimilar between the two sexes. In conclusion, the magnitude and specific pattern of sex differences in manifestations and progression of clinically recorded changes in motor performance and MRI lesion distribution support, on clinical grounds, the possibility of certain sex-limited factor(s) which, beyond the predictable effect of the second, normal FMR1 alleles in female premutation carriers, may have neuroprotective effects, specifically concerning the cerebellar circuitry.

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Enlarged perivascular spaces and their association with motor, cognition, MRI markers and cerebrovascular risk factors in male fragile X premutation carriers

Elias-Mas,

Wang,

Rodríguez-Revenga

et al. 2024

Journal of the Neurological Sciences

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The Spectrum of Neurological and White Matter Changes and Premutation Status Categories of Older Male Carriers of the FMR1 Alleles Are Linked to Genetic (CGG and FMR1 mRNA) and Cellular Stress (AMPK) Markers

Cited by 10 publications

References 64 publications

Total and Regional White Matter Lesions Are Correlated With Motor and Cognitive Impairments in Carriers of the FMR1 Premutation

Total and Regional White Matter Lesions Are Correlated With Motor and Cognitive Impairments in Carriers of the FMR1 Premutation

Differential Progression of Motor Dysfunction Between Male and Female Fragile X Premutation Carriers Reveals Novel Aspects of Sex-Specific Neural Involvement

Enlarged perivascular spaces and their association with motor, cognition, MRI markers and cerebrovascular risk factors in male fragile X premutation carriers

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