TY - JOUR
T1 - Quantitative Muscle MRI and Clinical Findings in Women With Pathogenic Dystrophin Gene Variants
AU - Fornander, Freja
AU - Solheim, Tuva Åsatun
AU - Eisum, Anne-Sofie Vibæk
AU - Poulsen, Nanna Scharff
AU - Andersen, Annarita Ghosh
AU - Dahlqvist, Julia Rebecka
AU - Dunø, Morten
AU - Vissing, John
N1 - Copyright © 2021 Fornander, Solheim, Eisum, Poulsen, Andersen, Dahlqvist, Dunø and Vissing.
PY - 2021/9/3
Y1 - 2021/9/3
N2 - Objective: To explore fat replacement, muscle strength, and clinical features in women heterozygous for a pathogenic DMD variant, we prospectively examined 53 women, assuming that some of these women-despite of the recessive X-linked inheritance-manifested clinical symptoms. Methods: We performed a cross-sectional observational study using MRI and stationary dynamometry of lower extremities, extracted blood muscle biomarkers, and investigated subjective complaints. Results were compared with 19 healthy women. Results: DMD variant carriers were weaker and had higher fat fractions than controls in all investigated muscle groups (p < 0.02). Fat fractions were 18% in carriers vs. 11% in controls in thighs (p = 0.008), and 15 vs. 11% in calf muscles (p = 0.032). Seventy-two percent had fat fractions deviating from controls by two standard deviations (SDs) in one or more of the 16 investigated muscle groups. On strength testing, 40% of the carriers had results deviating from control muscle strength by two SDs in one or more dynamometry assessments. Forty-three carriers (81%) had either reduced muscle strength (<2 SDs from control mean) and/or elevated muscle fat fraction (>2 SDs from control mean). Thirty of these had subjective symptoms. Blood creatine kinase and myoglobin were elevated in 57% of the carriers. Conclusion: Using quantitative methods, this study shows that both clinically symptomatic and asymptomatic women with pathogenic DMD variants show a high prevalence of muscle affection. Longitudinal studies in female carriers of pathogenic DMD variants are needed to follow the evolution of these changes.
AB - Objective: To explore fat replacement, muscle strength, and clinical features in women heterozygous for a pathogenic DMD variant, we prospectively examined 53 women, assuming that some of these women-despite of the recessive X-linked inheritance-manifested clinical symptoms. Methods: We performed a cross-sectional observational study using MRI and stationary dynamometry of lower extremities, extracted blood muscle biomarkers, and investigated subjective complaints. Results were compared with 19 healthy women. Results: DMD variant carriers were weaker and had higher fat fractions than controls in all investigated muscle groups (p < 0.02). Fat fractions were 18% in carriers vs. 11% in controls in thighs (p = 0.008), and 15 vs. 11% in calf muscles (p = 0.032). Seventy-two percent had fat fractions deviating from controls by two standard deviations (SDs) in one or more of the 16 investigated muscle groups. On strength testing, 40% of the carriers had results deviating from control muscle strength by two SDs in one or more dynamometry assessments. Forty-three carriers (81%) had either reduced muscle strength (<2 SDs from control mean) and/or elevated muscle fat fraction (>2 SDs from control mean). Thirty of these had subjective symptoms. Blood creatine kinase and myoglobin were elevated in 57% of the carriers. Conclusion: Using quantitative methods, this study shows that both clinically symptomatic and asymptomatic women with pathogenic DMD variants show a high prevalence of muscle affection. Longitudinal studies in female carriers of pathogenic DMD variants are needed to follow the evolution of these changes.
KW - Dixon MRI
KW - dynamometry
KW - dystrophinopathy
KW - female carriers
KW - muscle fat infiltration
KW - muscle strength
UR - http://www.scopus.com/inward/record.url?scp=85115173148&partnerID=8YFLogxK
U2 - 10.3389/fneur.2021.707837
DO - 10.3389/fneur.2021.707837
M3 - Journal article
C2 - 34539555
SN - 1664-2295
VL - 12
SP - 707837
JO - Frontiers in Neurology
JF - Frontiers in Neurology
M1 - 707837
ER -