Aberrant cell cycle reentry in human and experimental inclusion body myositis and polymyositis.

[inclusion body myositis]

Inclusion body myositis (IBM ), a degenerative and inflammatory disorder of skeletal muscle , and Alzheimer 's disease share protein derangements and attrition of postmitotic cells . Overexpression of cyclins and proliferating cell nuclear antigen (PCNA ) and evidence for DNA replication is reported in Alzheimer 's disease brain , possibly contributing to neuronal death . It is unknown whether aberrant cell cycle reentry also occurs in IBM . We examined cell cycle markers in IBM compared with normal control , polymyositis (PM ) and non-inflammatory dystrophy sample sets . Next , we tested for evidence of reentry and DNA synthesis in C 2 C 12 myotubes induced to express β-amyloid (Aβ 42 ). We observed increased levels of Ki-67 , PCNA and cyclins E /D 1 in IBM compared with normals and non-inflammatory conditions . Interestingly , PM samples displayed similar increases . Satellite cell markers did not correlate with Ki-67 -affected myofiber nuclei . DNA synthesis and cell cycle markers were induced in A β-bearing myotubes . Cell cycle marker and cyclin protein expressions were also induced in an experimental allergic myositis -like model of PM in mice . Levels of p 21 (Cip 1 /WAF 1 ), a cyclin-dependent kinase inhibitor , were decreased in affected myotubes . However , overexpression of p 21 did not rescue cells from Aβ-induced toxicity . This is the first report of cell cycle reentry in human myositis . The absence of rescue and evidence for reentry in separate models of myodegeneration and inflammation suggest that new DNA synthesis may be a reactive response to either or both stressors .