Revealing myopathy spectrum: integrating transcriptional and clinical features of human skeletal muscles with varying health conditions

Author:

Zhong HuahuaORCID,Sian VeronicaORCID,Johari MridulORCID,Katayama ShintaroORCID,Oghabian Ali,Jonson Per HaraldORCID,Hackman Peter,Savarese Marco,Udd Bjarne

Abstract

AbstractMyopathy refers to a large group of heterogeneous, rare muscle diseases. Bulk RNA-sequencing has been utilized for the diagnosis and research of these diseases for many years. However, the existing valuable sequencing data often lack integration and clinical interpretation. In this study, we integrated bulk RNA-sequencing data from 1221 human skeletal muscles (292 with myopathies, 929 controls) from both databases and our local samples. By applying a method similar to single-cell analysis, we revealed a general spectrum of muscle diseases, ranging from healthy to mild disease, moderate muscle wasting, and severe muscle disease. This spectrum was further partly validated in three specific myopathies (97 muscles) through clinical features including trinucleotide repeat expansion, magnetic resonance imaging fat fraction, pathology, and clinical severity scores. This spectrum helped us identify 234 genuinely healthy muscles as unprecedented controls, providing a new perspective for deciphering the hallmark genes and pathways among different myopathies. The newly identified featured genes of general myopathy, inclusion body myositis, and titinopathy were highly expressed in our local muscles, as validated by quantitative polymerase chain reaction.

Funder

Samfundet Folkhälsan

Academy of Finland

Jane ja Aatos Erkon Säätiö

Magnus Ehrnroothin Säätiö

AFM-Téléthon

China Scholarship Council

Publisher

Springer Science and Business Media LLC

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