Filamin C accumulation is a strong but nonspecific immunohistochemical marker of core formation in muscle.

6533b824fe1ef96bd1280011

RESEARCH PRODUCT

Filamin C accumulation is a strong but nonspecific immunohistochemical marker of core formation in muscle.

Hans-hilmar Goebel Jens Reimann Alan H. Beggs F Takada Carsten G. Bönnemann Carsten G. Bönnemann Mathias Gautel Louis M. Kunkel B Vollmers P.f.m. Van Der Ven Folker Hanefeld Rolf Schröder Dieter O. Fürst Irene Warlo Jochen Herms T. G. Thompson

subject

Pathology medicine.medical_specialty animal structures Biopsy Filamins macromolecular substances Biology Filamin 03 medical and health sciences 0302 clinical medicine Contractile Proteins Muscular Diseases Reference Values medicine Myotilin Humans Protein Isoforms Cytoskeleton Myopathy Microscopy Immunoelectron Muscle Skeletal 030304 developmental biology 0303 health sciences Sarcolemma Microfilament Proteins medicine.disease Immunohistochemistry Cell biology body regions Neurology Desmin Neurology (clinical)medicine.symptom Myofibril Carrier Proteins 030217 neurology & neurosurgery Central core disease Biomarkers

description

Filamin C is the muscle isoform of a group of large actin-crosslinking proteins. On the one hand, filamin C is associated with the Z-disk of the myofibrillar apparatus and binds to myotilin; on the other hand, it interacts with the sarcoglycan complex at the sarcolemma. Filamin C may be involved in reorganizing the cytoskeleton in response to signalling events and in muscle it may, in addition, fulfill structural functions at the Z-disk. An examination of biopsies from patients with multi-minicore myopathy, central core myopathy and neurogenic target fibers with core-like target formations (TF) revealed strong reactivity of all the cores and target formations with two different anti-filamin C antibodies. In all three conditions, the immunoreactivity in the cores for filamin C was considerably stronger than that for desmin. Only for alphaB-crystallin were comparable levels of immunoreactivity detected. There was no difference in intensity for filamin C between the three pathological conditions. Thus, filamin C along with alphaB-crystallin is a strong and robust, but nonspecific marker of core formation. The reason why filamin C accumulates in cores is unclear at present, but we postulate that it may be critically involved in the chain of events eventually leading to myofibrillar degeneration.

year	journal	country	edition	language
2002-12-14	Journal of the neurological sciences

10.1016/s0022-510x(02)00341-6 https://pubmed.ncbi.nlm.nih.gov/12480088