Frontiers in Molecular Biosciences (Jun 2022)

Muscle Histopathological Abnormalities in a Patient With a CCT5 Mutation Predicted to Affect the Apical Domain of the Chaperonin Subunit

  • Federica Scalia,
  • Federica Scalia,
  • Rosario Barone,
  • Francesca Rappa,
  • Antonella Marino Gammazza,
  • Fabrizio Lo Celso,
  • Fabrizio Lo Celso,
  • Giosuè Lo Bosco,
  • Giosuè Lo Bosco,
  • Giampaolo Barone,
  • Vincenzo Antona,
  • Maria Vadalà,
  • Maria Vadalà,
  • Alessandra Maria Vitale,
  • Alessandra Maria Vitale,
  • Giuseppe Donato Mangano,
  • Domenico Amato,
  • Giusy Sentiero,
  • Giusy Sentiero,
  • Filippo Macaluso,
  • Kathryn H. Myburgh,
  • Everly Conway de Macario,
  • Alberto J. L. Macario,
  • Alberto J. L. Macario,
  • Mario Giuffrè,
  • Francesco Cappello,
  • Francesco Cappello

DOI
https://doi.org/10.3389/fmolb.2022.887336
Journal volume & issue
Vol. 9

Abstract

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Recognition of diseases associated with mutations of the chaperone system genes, e.g., chaperonopathies, is on the rise. Hereditary and clinical aspects are established, but the impact of the mutation on the chaperone molecule and the mechanisms underpinning the tissue abnormalities are not. Here, histological features of skeletal muscle from a patient with a severe, early onset, distal motor neuropathy, carrying a mutation on the CCT5 subunit (MUT) were examined in comparison with normal muscle (CTR). The MUT muscle was considerably modified; atrophy of fibers and disruption of the tissue architecture were prominent, with many fibers in apoptosis. CCT5 was diversely present in the sarcolemma, cytoplasm, and nuclei in MUT and in CTR and was also in the extracellular space; it colocalized with CCT1. In MUT, the signal of myosin appeared slightly increased, and actin slightly decreased as compared with CTR. Desmin was considerably delocalized in MUT, appearing with abnormal patterns and in precipitates. Alpha-B-crystallin and Hsp90 occurred at lower signals in MUT than in CTR muscle, appearing also in precipitates with desmin. The abnormal features in MUT may be the consequence of inactivity, malnutrition, denervation, and failure of protein homeostasis. The latter could be at least in part caused by malfunction of the CCT complex with the mutant CCT5 subunit. This is suggested by the results of the in silico analyses of the mutant CCT5 molecule, which revealed various abnormalities when compared with the wild-type counterpart, mostly affecting the apical domain and potentially impairing chaperoning functions. Thus, analysis of mutated CCT5 in vitro and in vivo is anticipated to provide additional insights on subunit involvement in neuromuscular disorders.

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