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Group:MUZIC:Obscurin

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(''' Obscurin ''')
(''' Obscurin ''')
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== '''Protein structure''' ==
== '''Protein structure''' ==
Obscurin is a ~800kDa protein expressed in skeletal and cardiac muscle. Its modular structure resembles the architecture of titin, indeed the NH2-terminal half of the protein consists of 49 Ig-like domains (with the characteristic β-sandwich shape) and 2 Fn3 domains, each one with a length of 88-92 amino acids residues and no linker sequences between subsequent domains (except between Ob2-Ob3 and Ob24-Ob25). Two clusters of these Ig domains show 70-90% homology at the protein level; these are Ob36-42 and Ob9-18. As in other sarcomeric proteins, the Ig domains present a highly stable structural scaffold that is necessary for mechanical stability as well as versatile surface that fits well with the role of binding site for other proteins <ref>PMID: 19466753</ref>. The COOH-terminus shows a less ordered architecture with a non-modular 417 amino acid sequence with several consensus phosphorylation motifs for ERK-kinase (SPXR) <ref>PMID: 11448995</ref>. A PH domain is located upstream of the last tandem Ig domains Ob56-57, preceding the DH/RhoGEF domain. After the Ob51 Ig domain a non-modular structure includes an IQ domain, so called for the conserved Ile-Gln that is part of a well-characterized binding motif for calmodulin or calmodulin-like protein like myosin light chains. In the isoform obscurin B, an additional COOH-terminal part includes two more Ser/Thr Kinase domains, 2 Ig like domains and an Fn3 domain <ref>PMID: 16625312</ref>. This isoform does not include the extremely COOH-terminal non-modular structure that characterizes the isoform A and contains the Ank1.5 binding site.
Obscurin is a ~800kDa protein expressed in skeletal and cardiac muscle. Its modular structure resembles the architecture of titin, indeed the NH2-terminal half of the protein consists of 49 Ig-like domains (with the characteristic β-sandwich shape) and 2 Fn3 domains, each one with a length of 88-92 amino acids residues and no linker sequences between subsequent domains (except between Ob2-Ob3 and Ob24-Ob25). Two clusters of these Ig domains show 70-90% homology at the protein level; these are Ob36-42 and Ob9-18. As in other sarcomeric proteins, the Ig domains present a highly stable structural scaffold that is necessary for mechanical stability as well as versatile surface that fits well with the role of binding site for other proteins <ref>PMID: 19466753</ref>. The COOH-terminus shows a less ordered architecture with a non-modular 417 amino acid sequence with several consensus phosphorylation motifs for ERK-kinase (SPXR) <ref>PMID: 11448995</ref>. A PH domain is located upstream of the last tandem Ig domains Ob56-57, preceding the DH/RhoGEF domain. After the Ob51 Ig domain a non-modular structure includes an IQ domain, so called for the conserved Ile-Gln that is part of a well-characterized binding motif for calmodulin or calmodulin-like protein like myosin light chains. In the isoform obscurin B, an additional COOH-terminal part includes two more Ser/Thr Kinase domains, 2 Ig like domains and an Fn3 domain <ref>PMID: 16625312</ref>. This isoform does not include the extremely COOH-terminal non-modular structure that characterizes the isoform A and contains the Ank1.5 binding site.
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==== '''PDB entries for solved obscurin domain structures''' ====
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==== '''PDB entries''' ====
[[1v1c]] - Solution structure os SH3 domain of obscurin, residues 5601-5668
[[1v1c]] - Solution structure os SH3 domain of obscurin, residues 5601-5668

Revision as of 17:19, 23 November 2012

Obscurin

Crystal Structure of the titin Ig-like domain Complex between the titin M10 (blue) - Obscurin like 1 (Red) (PDB entry: 2wp3 )

Drag the structure with the mouse to rotate

Andrea Ghisleni 17:09, 23 November 2012 (IST)

Proteopedia Page Contributors and Editors (what is this?)

Nikos Pinotsis, Andrea Ghisleni

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