Genetics. Published Articles Ahead of Print: November 13, 2007, Copyright © 2007
doi:10.1534/genetics.107.078717


A more recent version of this article appeared on December 1, 2007.
Originally published as Genetics Published Articles Ahead of Print on October 18, 2007.


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The Formation of the Central Element of Synaptonemal Complex May Occur By Multiple Mechanisms: The Roles of the N- and C-Terminal Domains of the Drosophila C(3)G Protein in Mediating Synapsis and Recombination

1 University of Oregon, Eugene
2 James Cook University
3 Colorado State University
4 Stowers Institute for Medical Research

* To whom correspondence should be addressed. E-mail: rsh{at}stowers-institute.org.

Submitted on July 12, 2007
Revised on August 6, 2007
Accepted on 27 September 2007


Abstract

In Drosophila melanogaster oocytes, the C(3)G protein comprises the transverse filaments (TFs) of the synaptonemal complex (SC). Like other TF proteins, such as Zip1p in yeast and SCP1 in mammals, C(3)G is comprised of a central coiled-coil-rich domain flanked by N- and C-terminal globular domains. Here, we analyze in-frame deletions within the N- and C-terminal regions of C(3)G in Drosophila oocytes. As is the case for Zip1p, a C-terminal deletion of C(3)G fails to attach to the lateral elements of the SC. Instead, this C-terminal deletion protein forms a large cylindrical polycomplex structure. EM analysis of this structure reveals a polycomplex of concentric rings alternating dark and light bands. However, unlike both yeast and mammals, all three proteins deleted for N-terminal regions completely abolished both SC and polycomplex formation. Both the N- and C-terminal deletions significantly reduce or abolish meiotic recombination similar to c(3)G null homozygotes. To explain these data, we propose that in Drosophila, the N-terminus, but not the C-terminal globular domain, of C(3)G is critical for the formation of anti-parallel pairs of C(3)G homodimers that span the central region, and thus for assembly of complete TFs, while the C-terminus is required to affix these homodimers to the lateral elements.

Key Words: meiosis, Chromosome, Synaptonemal Complex, recombination




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