Anti-Ku + myositis: an acquired inflammatory protein-aggregate myopathy.
Marie-Therese HolzerAkinori UruhaAndreas RoosAndreas HentschelAnne SchänzerJoachim WeisKristl G ClaeysBenedikt SchoserFederica MontagneseHans-Hilmar GoebelMelanie HuberSarah Léonard-LouisIna KötterNathalie StreichenbergerLaure GallayOlivier BenvenisteUdo SchneiderCorinna PreusseMartin KruscheWerner StenzelPublished in: Acta neuropathologica (2024)
Myositis with anti-Ku-autoantibodies is a rare inflammatory myopathy associated with various connective tissue diseases. Histopathological studies have identified inflammatory and necrotizing aspects, but a precise morphological analysis and pathomechanistic disease model are lacking. We therefore aimed to carry out an in-depth morpho-molecular analysis to uncover possible pathomechanisms. Muscle biopsy specimens from 26 patients with anti-Ku-antibodies and unequivocal myositis were analyzed by immunohistochemistry, immunofluorescence, transcriptomics, and proteomics and compared to biopsy specimens of non-disease controls, immune-mediated necrotizing myopathy (IMNM), and inclusion body myositis (IBM). Clinical findings and laboratory parameters were evaluated retrospectively and correlated with morphological and molecular features. Patients were mainly female (92%) with a median age of 56.5 years. Isolated myositis and overlap with systemic sclerosis were reported in 31%, respectively. Isolated myositis presented with higher creatine kinase levels and cardiac involvement (83%), whereas systemic sclerosis-overlap patients often had interstitial lung disease (57%). Histopathology showed a wide spectrum from mild to pronounced myositis with diffuse sarcolemmal MHC-class I (100%) and -II (69%) immunoreactivity, myofiber necrosis (88%), endomysial inflammation (85%), thickened capillaries (84%), and vacuoles (60%). Conspicuous sarcoplasmic protein aggregates were p62, BAG3, myotilin, or immunoproteasomal beta5i-positive. Proteomic and transcriptomic analysis identified prominent up-regulation of autophagy, proteasome, and hnRNP-related cell stress. To conclude, Ku + myositis is morphologically characterized by myofiber necrosis, MHC-class I and II positivity, variable endomysial inflammation, and distinct protein aggregation varying from IBM and IMNM, and it can be placed in the spectrum of scleromyositis and overlap myositis. It features characteristic sarcoplasmic protein aggregation on an acquired basis being functionally associated with altered chaperone, proteasome, and autophagy function indicating that Ku + myositis exhibit aspects of an acquired inflammatory protein-aggregate myopathy.
Keyphrases
- interstitial lung disease
- systemic sclerosis
- oxidative stress
- rheumatoid arthritis
- idiopathic pulmonary fibrosis
- end stage renal disease
- protein protein
- late onset
- myasthenia gravis
- ejection fraction
- chronic kidney disease
- newly diagnosed
- peritoneal dialysis
- amino acid
- endoplasmic reticulum stress
- stem cells
- single cell
- small molecule
- systemic lupus erythematosus
- signaling pathway
- mass spectrometry
- muscular dystrophy
- mesenchymal stem cells
- atrial fibrillation
- patient reported outcomes
- protein kinase