AI Article Synopsis

  • * A study at the Mayo Clinic identified 31 individuals with pathogenic mutations, finding that myopathy was nearly universal among VCP-MSP patients, and various strength patterns and muscle biopsy results were observed.
  • * VCP-MSP was the most prevalent disorder in the study, with unique features like rimmed vacuolar myopathy and cardiac dysfunction observed primarily in these patients.

Article Abstract

Objectives: Mutations in VCP, HNRNPA2B1, HNRNPA1, and SQSTM1, encoding RNA-binding proteins or proteins in quality-control pathways, cause multisystem proteinopathies (MSP). They share pathological findings of protein aggregation and clinical combinations of inclusion body myopathy (IBM), neurodegeneration [motor neuron disorder (MND)/frontotemporal dementia (FTD)], and Paget disease of bone (PDB). Subsequently, additional genes were linked to similar but not full clinical-pathological spectrum (MSP-like disorders). We aimed to define the phenotypic-genotypic spectrum of MSP and MSP-like disorders at our institution, including long-term follow-up features.

Methods: We searched the Mayo Clinic database (January 2010-June 2022) to identify patients with mutations in MSP and MSP-like disorders causative genes. Medical records were reviewed.

Results: Thirty-one individuals (27 families) had pathogenic mutations in: VCP (n = 17), SQSTM1 + TIA1 (n = 5), TIA1 (n = 5), MATR3, HNRNPA1, HSPB8, and TFG (n = 1, each). Myopathy occurred in all but 2 VCP-MSP patients with disease onset at age 52 (median). Weakness pattern was limb-girdle in 12/15 VCP-MSP and HSPB8 patient, and distal-predominant in other MSP and MSP-like disorders. Twenty/24 muscle biopsies showed rimmed vacuolar myopathy. MND and FTD occurred in 5 (4 VCP, 1 TFG) and 4 (3 VCP, 1 SQSTM1 + TIA1) patients, respectively. PDB manifested in 4 VCP-MSP. Diastolic dysfunction occurred in 2 VCP-MSP. After 11.5 years (median) from symptom onset, 15 patients ambulated without gait-aids; loss of ambulation (n = 5) and death (n = 3) were recorded only in VCP-MSP.

Interpretation: VCP-MSP was the most common disorder; rimmed vacuolar myopathy was the most frequent manifestation; distal-predominant weakness occurred frequently in non-VCP-MSP; and cardiac involvement was observed only in VCP-MSP.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10109322PMC
http://dx.doi.org/10.1002/acn3.51751DOI Listing

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Article Synopsis
  • * A study at the Mayo Clinic identified 31 individuals with pathogenic mutations, finding that myopathy was nearly universal among VCP-MSP patients, and various strength patterns and muscle biopsy results were observed.
  • * VCP-MSP was the most prevalent disorder in the study, with unique features like rimmed vacuolar myopathy and cardiac dysfunction observed primarily in these patients.
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