DYC-1, a Protein Functionally Linked to Dystrophin inCaenorhabditis elegansIs Associated with the Dense Body, Where It Interacts with the Muscle LIM Domain Protein ZYX-1
- 1 March 2008
- journal article
- research article
- Published by American Society for Cell Biology (ASCB) in Molecular Biology of the Cell
- Vol. 19 (3) , 785-796
- https://doi.org/10.1091/mbc.e07-05-0497
Abstract
In Caenorhabditis elegans, mutations of the dystrophin homologue, dys-1, produce a peculiar behavioral phenotype (hyperactivity and a tendency to hypercontract). In a sensitized genetic background, dys-1 mutations also lead to muscle necrosis. The dyc-1 gene was previously identified in a genetic screen because its mutation leads to the same phenotype as dys-1, suggesting that the two genes are functionally linked. Here, we report the detailed characterization of the dyc-1 gene. dyc-1 encodes two isoforms, which are expressed in neurons and muscles. Isoform-specific RNAi experiments show that the absence of the muscle isoform, and not that of the neuronal isoform, is responsible for the dyc-1 mutant phenotype. In the sarcomere, the DYC-1 protein is localized at the edges of the dense body, the nematode muscle adhesion structure where actin filaments are anchored and linked to the sarcolemma. In yeast two-hybrid assays, DYC-1 interacts with ZYX-1, the homologue of the vertebrate focal adhesion LIM domain protein zyxin. ZYX-1 localizes at dense bodies and M-lines as well as in the nucleus of C. elegans striated muscles. The DYC-1 protein possesses a highly conserved 19 amino acid sequence, which is involved in the interaction with ZYX-1 and which is sufficient for addressing DYC-1 to the dense body. Altogether our findings indicate that DYC-1 may be involved in dense body function and stability. This, taken together with the functional link between the C. elegans DYC-1 and DYS-1 proteins, furthermore suggests a requirement of dystrophin function at this structure. As the dense body shares functional similarity with both the vertebrate Z-disk and the costamere, we therefore postulate that disruption of muscle cell adhesion structures might be the primary event of muscle degeneration occurring in the absence of dystrophin, in C. elegans as well as vertebrates.This publication has 50 references indexed in Scilit:
- The V0-ATPase mediates apical secretion of exosomes containing Hedgehog-related proteins in Caenorhabditis elegans The Journal of cell biology, 2006
- The SLO-1 BK Channel of Caenorhabditis elegans is Critical for Muscle Function and is Involved in Dystrophin-dependent Muscle DystrophyJournal of Molecular Biology, 2006
- CAPON expression in skeletal muscle is regulated by position, repair, NOS activity, and dystrophyExperimental Cell Research, 2005
- Molecular, genetic and physiological characterisation of dystrobrevin-like (dyb-1) mutants of Caenorhabditis elegansJournal of Molecular Biology, 2001
- Toward a functional analysis of the yeast genome through exhaustive two-hybrid screensNature Genetics, 1997
- Chapter 19 DNA TransformationPublished by Elsevier ,1995
- Green Fluorescent Protein as a Marker for Gene ExpressionScience, 1994
- Vinculin is essential for muscle function in the nematode.The Journal of cell biology, 1991
- Muscle organization in Caenorhabditis elegans: localization of proteins implicated in thin filament attachment and I-band organization.The Journal of cell biology, 1985
- Dominant mutations affecting muscle structure in Caenorhabditis elegans that map near the actin gene clusterJournal of Molecular Biology, 1984