Characterization of δ-sarcoglycan, a novel component of the oligomeric sarcoglycan complex involved in limb-girdle muscular dystrophy

Daniel Jung; Franck Duclos; Barbara Apostol; Volker Straub; Jane C. Lee; Valérie Allamand; David P. Venzke; Yoshihide Sunada; Carolyn R. Moomaw; Cynthia J. Leveille; Clive A. Slaughter; Thomas O. Crawford; John D. McPherson; Kevin P. Campbell

doi:10.1074/jbc.271.50.32321

Characterization of δ-sarcoglycan, a novel component of the oligomeric sarcoglycan complex involved in limb-girdle muscular dystrophy

Daniel Jung, Franck Duclos, Barbara Apostol, Volker Straub, Jane C. Lee, Valérie Allamand, David P. Venzke, Yoshihide Sunada, Carolyn R. Moomaw, Cynthia J. Leveille, Clive A. Slaughter, Thomas O. Crawford, John D. McPherson, Kevin P. Campbell

School of Medicine

Research output: Contribution to journal › Article › peer-review

80 Scopus citations

Abstract

The sarcoglycan complex is known to be involved in limb-girdle muscular dystrophy (LGMD) and is composed of at least three proteins: α-, β-, and γ-sarcoglycan. δ-Sarcoglycan has now been identified as a second 35-kDa sarcolemmal transmembrane glycoprotein that shares high homology with γ- sarcoglycan and is expressed mainly in skeletal and cardiac muscle. Biochemical analysis has demonstrated that γ- and δ-sarcoglycan are separate entities within the sarcoglycan complex and that all four sarcoglycans exist in the complex on a stoichiometrically equal basis. Immunohistochemical analysis of skeletal muscle biopsies from patients with LGMD2C, LGMD2D, and LGMD2E demonstrated a reduction of the entire sarcoglycan complex in these muscular dystrophies. Furthermore, we have mapped the human δ-sarcoglycan gene to chromosome 5q33-q34 in a region overlapping the recently linked autosomal recessive LGMD2F locus.

Original language	English (US)
Pages (from-to)	32321-32329
Number of pages	9
Journal	Journal of Biological Chemistry
Volume	271
Issue number	50
DOIs	https://doi.org/10.1074/jbc.271.50.32321
State	Published - 1996

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Cell Biology

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Jung, D., Duclos, F., Apostol, B., Straub, V., Lee, J. C., Allamand, V., Venzke, D. P., Sunada, Y., Moomaw, C. R., Leveille, C. J., Slaughter, C. A., Crawford, T. O., McPherson, J. D., & Campbell, K. P. (1996). Characterization of δ-sarcoglycan, a novel component of the oligomeric sarcoglycan complex involved in limb-girdle muscular dystrophy. Journal of Biological Chemistry, 271(50), 32321-32329. https://doi.org/10.1074/jbc.271.50.32321

Jung, D, Duclos, F, Apostol, B, Straub, V, Lee, JC, Allamand, V, Venzke, DP, Sunada, Y, Moomaw, CR, Leveille, CJ, Slaughter, CA, Crawford, TO, McPherson, JD & Campbell, KP 1996, 'Characterization of δ-sarcoglycan, a novel component of the oligomeric sarcoglycan complex involved in limb-girdle muscular dystrophy', Journal of Biological Chemistry, vol. 271, no. 50, pp. 32321-32329. https://doi.org/10.1074/jbc.271.50.32321

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title = "Characterization of δ-sarcoglycan, a novel component of the oligomeric sarcoglycan complex involved in limb-girdle muscular dystrophy",

abstract = "The sarcoglycan complex is known to be involved in limb-girdle muscular dystrophy (LGMD) and is composed of at least three proteins: α-, β-, and γ-sarcoglycan. δ-Sarcoglycan has now been identified as a second 35-kDa sarcolemmal transmembrane glycoprotein that shares high homology with γ- sarcoglycan and is expressed mainly in skeletal and cardiac muscle. Biochemical analysis has demonstrated that γ- and δ-sarcoglycan are separate entities within the sarcoglycan complex and that all four sarcoglycans exist in the complex on a stoichiometrically equal basis. Immunohistochemical analysis of skeletal muscle biopsies from patients with LGMD2C, LGMD2D, and LGMD2E demonstrated a reduction of the entire sarcoglycan complex in these muscular dystrophies. Furthermore, we have mapped the human δ-sarcoglycan gene to chromosome 5q33-q34 in a region overlapping the recently linked autosomal recessive LGMD2F locus.",

author = "Daniel Jung and Franck Duclos and Barbara Apostol and Volker Straub and Lee, {Jane C.} and Val{\'e}rie Allamand and Venzke, {David P.} and Yoshihide Sunada and Moomaw, {Carolyn R.} and Leveille, {Cynthia J.} and Slaughter, {Clive A.} and Crawford, {Thomas O.} and McPherson, {John D.} and Campbell, {Kevin P.}",

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doi = "10.1074/jbc.271.50.32321",

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AU - Straub, Volker

AU - Lee, Jane C.

AU - Allamand, Valérie

AU - Venzke, David P.

AU - Sunada, Yoshihide

AU - Moomaw, Carolyn R.

AU - Leveille, Cynthia J.

AU - Slaughter, Clive A.

AU - Crawford, Thomas O.

AU - McPherson, John D.

AU - Campbell, Kevin P.

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N2 - The sarcoglycan complex is known to be involved in limb-girdle muscular dystrophy (LGMD) and is composed of at least three proteins: α-, β-, and γ-sarcoglycan. δ-Sarcoglycan has now been identified as a second 35-kDa sarcolemmal transmembrane glycoprotein that shares high homology with γ- sarcoglycan and is expressed mainly in skeletal and cardiac muscle. Biochemical analysis has demonstrated that γ- and δ-sarcoglycan are separate entities within the sarcoglycan complex and that all four sarcoglycans exist in the complex on a stoichiometrically equal basis. Immunohistochemical analysis of skeletal muscle biopsies from patients with LGMD2C, LGMD2D, and LGMD2E demonstrated a reduction of the entire sarcoglycan complex in these muscular dystrophies. Furthermore, we have mapped the human δ-sarcoglycan gene to chromosome 5q33-q34 in a region overlapping the recently linked autosomal recessive LGMD2F locus.

AB - The sarcoglycan complex is known to be involved in limb-girdle muscular dystrophy (LGMD) and is composed of at least three proteins: α-, β-, and γ-sarcoglycan. δ-Sarcoglycan has now been identified as a second 35-kDa sarcolemmal transmembrane glycoprotein that shares high homology with γ- sarcoglycan and is expressed mainly in skeletal and cardiac muscle. Biochemical analysis has demonstrated that γ- and δ-sarcoglycan are separate entities within the sarcoglycan complex and that all four sarcoglycans exist in the complex on a stoichiometrically equal basis. Immunohistochemical analysis of skeletal muscle biopsies from patients with LGMD2C, LGMD2D, and LGMD2E demonstrated a reduction of the entire sarcoglycan complex in these muscular dystrophies. Furthermore, we have mapped the human δ-sarcoglycan gene to chromosome 5q33-q34 in a region overlapping the recently linked autosomal recessive LGMD2F locus.

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Characterization of δ-sarcoglycan, a novel component of the oligomeric sarcoglycan complex involved in limb-girdle muscular dystrophy

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