Functional importance of polymerization and localization of calsequestrin in C. elegans

Author:

Cho J. H.1,Ko K. M.1,Singaruvelu Gunasekaran1,Lee Wonhae1,Kang Gil Bu1,Rho Seong-Hwan1,Park Byung-Jae1,Yu Jae-Ran2,Kagawa Hiroaki3,Eom S. H.1,Kim D. H.1,Ahnn Joohong1

Affiliation:

1. Department of Life Science, Gwangju Institute of Science and Technology, Gwangju, 500-712, Korea

2. Department of Parasitology, College of Medicine, Kon-Kuk University, Chungju, 380-710, Korea

3. Department of Biology, Faculty of Science, Okayama University, Okayama, 700-8530, Japan

Abstract

Dual roles of calsequestrin (CSQ-1) being the Ca2+ donor and Ca2+ acceptor make it an excellent Ca2+-buffering protein within the sarcoplasmic reticulum (SR). We have isolated and characterized a calsequestrin (csq-1)-null mutant in Caenorhabditis elegans. To our surprise, this mutant csq-1(jh109) showed no gross defects in muscle development or function but, however, is highly sensitive to perturbation of Ca2+ homeostasis. By taking advantage of the viable null mutant, we investigated the domains of CSQ-1 that are important for polymerization and cellular localization, and required for its correct buffering functions. In transgenic animals rescued with various CSQ-1 constructs, the in vivo patterns of polymerization and localization of several mutated calsequestrins were observed to correlate with the structure-function relationship. Our results suggest that polymerization of CSQ-1 is essential but not sufficient for correct cellular localization and function of CSQ-1. In addition, direct interaction between CSQ-1 and the ryanodine receptor (RyR) was found for the first time, suggesting that the cellular localization of CSQ-1 in C. elegans is indeed modulated by RyR through a physical interaction.

Publisher

The Company of Biologists

Subject

Cell Biology

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