A hub-and-spoke nuclear lamina architecture in trypanosomes

Author:

Padilla-Mejia Norma E.1,Koreny Ludek1,Holden Jennifer1,Vancová Marie2,Lukeš Julius2,Zoltner Martin13,Field Mark C.12ORCID

Affiliation:

1. School of Life Sciences, University of Dundee, Dundee DD1 5EH, UK

2. Institute of Parasitology, Biology Centre and Faculty of Sciences, University of South Bohemia, 37005 České Budějovice, Czech Republic

3. Department of Parasitology, Faculty of Science, Charles University in Prague, BIOCEV 252 50, Vestec, Czech Republic

Abstract

ABSTRACT The nuclear lamina supports many functions, including maintaining nuclear structure and gene expression control, and correct spatio-temporal assembly is vital to meet these activities. Recently, multiple lamina systems have been described that, despite independent evolutionary origins, share analogous functions. In trypanosomatids the two known lamina proteins, NUP-1 and NUP-2, have molecular masses of 450 and 170 kDa, respectively, which demands a distinct architecture from the ∼60 kDa lamin-based system of metazoa and other lineages. To uncover organizational principles for the trypanosome lamina we generated NUP-1 deletion mutants to identify domains and their arrangements responsible for oligomerization. We found that both the N- and C-termini act as interaction hubs, and that perturbation of these interactions impacts additional components of the lamina and nuclear envelope. Furthermore, the assembly of NUP-1 terminal domains suggests intrinsic organizational capacity. Remarkably, there is little impact on silencing of telomeric variant surface glycoprotein genes. We suggest that both terminal domains of NUP-1 have roles in assembling the trypanosome lamina and propose a novel architecture based on a hub-and-spoke configuration.

Funder

Medical Research Council

Wellcome Trust

Ministry of Education, Youth and Science

Publisher

The Company of Biologists

Subject

Cell Biology

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