A Link between the Synthesis of Nucleoporins and the Biogenesis of the Nuclear Envelope

doi:10.1083/jcb.153.4.709

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Published online 7 May 2001. doi:10.1083/jcb.153.4.709

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© The Rockefeller University Press, 0021-9525/2001/5/709/ $5.00
The Journal of Cell Biology, Volume 153, Number 4, May 14, 2001 709-724

Original Article

A Link between the Synthesis of Nucleoporins and the Biogenesis of the Nuclear Envelope

Marcello Marelli^a, C. Patrick Lusk^a, Honey Chan^a, John D. Aitchison^b, and Richard W. Wozniak^a
^a Department of Cell Biology, University of Alberta, Edmonton, Alberta T6G 2H7, Canada
^b Institute for Systems Biology, Seattle, Washington 98105

Correspondence to: Richard W. Wozniak, 5-14 Medical Sciences Bldg., Department of Cell Biology, University of Alberta, Edmonton, Alberta T6G 2H7, Canada. Tel:(780) 492-1384 Fax:(780) 492-0450 E-mail:rick.wozniak{at}ualberta.ca.

The nuclear pore complex (NPC) is a multicomponent structurecontaining a subset of proteins that bind nuclear transportfactors or karyopherins and mediate their movement across thenuclear envelope. By altering the expression of a single nucleoporingene, NUP53, we showed that the overproduction of Nup53p alterednuclear transport and had a profound effect on the structureof the nuclear membrane. Strikingly, conventional and immunoelectronmicroscopy analysis revealed that excess Nup53p entered thenucleus and associated with the nuclear membrane. Here, Nup53pinduced the formation of intranuclear, tubular membranes thatlater formed flattened, double membrane lamellae structurallysimilar to the nuclear envelope. Like the nuclear envelope,the intranuclear double membrane lamellae enclosed a definedcisterna that was interrupted by pores but, unlike the nuclearenvelope pores, they lacked NPCs. Consistent with this observation,we detected only two NPC proteins, the pore membrane proteinsPom152p and Ndc1p, in association with these membrane structures.Thus, these pores likely represent an intermediate in NPC assembly.We also demonstrated that the targeting of excess Nup53p tothe NPC and its specific association with intranuclear membraneswere dependent on the karyopherin Kap121p and the nucleoporinNup170p. At the nuclear envelope, the abilities of Nup53p toassociate with the membrane and drive membrane proliferationwere dependent on a COOH-terminal segment containing a potentialamphipathic ${alpha}$ -helix. The implications of these results with regardsto the biogenesis of the nuclear envelope are discussed.

Key Words: nuclear pore complex, nucleoporins, nuclear membrane, nucleartransport, karyopherin

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