| Literature DB >> 25770104 |
Genevieve S Griffiths1, Jinger Doe2, Mayumi Jijiwa3, Pam Van Ry2, Vivian Cruz2, Michelle de la Vega3, Joe W Ramos3, Dean J Burkin2, Michelle L Matter4.
Abstract
Muscle differentiation requires a complex signaling cascade that leads to the production of multinucleated myofibers. Genes regulating the intrinsic mitochondrial apoptotic pathway also function in controlling cell differentiation. How such signaling pathways are regulated during differentiation is not fully understood. Bit-1 (also known as PTRH2) mutations in humans cause infantile-onset multisystem disease with muscle weakness. We demonstrate here that Bit-1 controls skeletal myogenesis through a caspase-mediated signaling pathway. Bit-1-null mice exhibit a myopathy with hypotrophic myofibers. Bit-1-null myoblasts prematurely express muscle-specific proteins. Similarly, knockdown of Bit-1 expression in C2C12 myoblasts promotes early differentiation, whereas overexpression delays differentiation. In wild-type mice, Bit-1 levels increase during differentiation. Bit-1-null myoblasts exhibited increased levels of caspase 9 and caspase 3 without increased apoptosis. Bit-1 re-expression partially rescued differentiation. In Bit-1-null muscle, Bcl-2 levels are reduced, suggesting that Bcl-2-mediated inhibition of caspase 9 and caspase 3 is decreased. Bcl-2 re-expression rescued Bit-1-mediated early differentiation in Bit-1-null myoblasts and C2C12 cells with knockdown of Bit-1 expression. These results support an unanticipated yet essential role for Bit-1 in controlling myogenesis through regulation of Bcl-2.Entities:
Keywords: Bit‐1; Caspase 3; Differentiation; Myogenesis
Mesh:
Substances:
Year: 2015 PMID: 25770104 PMCID: PMC4446732 DOI: 10.1242/jcs.158964
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285