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Title: M line-deficient titin causes cardiac lethality through impaired maturation of the sarcomere.
Author(s): Weinert, S.
Bergmann, N.
Luo, X.
Erdmann, B.
Gotthardt, M. (298981866)
Publication year: 2006
Document type: Article / Letter to editor
Journal: Journal of Cell Biology
ISSN: 0021-9525
Volume: vol. 173
Issue: iss. 4
Start page: p. 559
End page: p. 570
Abstract: Titin, the largest protein known to date, has been linked to sarcomere assembly and function through its elastic adaptor and signaling domains. Titin's M-line region contains a unique kinase domain that has been proposed to regulate sarcomere assembly via its substrate titin cap (T-cap). In this study, we use a titin M line-deficient mouse to show that the initial assembly of the sarcomere does not depend on titin's M-line region or the phosphorylation of T-cap by the titin kinase. Rather, titin's M-line region is required to form a continuous titin filament and to provide mechanical stability of the embryonic sarcomere. Even without titin integrating into the M band, sarcomeres show proper spacing and alignment of Z discs and M bands but fail to grow laterally and ultimately disassemble. The comparison of disassembly in the developing and mature knockout sarcomere suggests diverse functions for titin's M line in embryonic development and the adult heart that not only involve the differential expression of titin isoforms but also of titin-binding proteins.
Subject: UMCN 4.1: Microbial pathogenesis and host defense
Organization: UMCN Extern
Nuclear Medicine
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/51282

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