
The nuclear pore complex (NPC) serves as the sole bidirectional gateway of macromolecules in and out of the nucleus. Owing to its size and complexity (∼1,000 protein subunits, ∼110 MDa in humans), the NPC has remained one of the foremost challenges for structure determination. Structural studies have now provided atomic-resolution crystal structures of most nucleoporins. The acquisition of these structures, combined with biochemical reconstitution experiments, cross-linking mass spectrometry, and cryo–electron tomography, has facilitated the determination of the near-atomic overall architecture of the symmetric core of the human, fungal, and algal NPCs. Here, we discuss the insights gained from these new advances and outstanding issues regarding NPC structure and function. The powerful combination of bottom-up and top-down approaches toward determining the structure of the NPC offers a paradigm for uncovering the architectures of other complex biological machines to near-atomic resolution.
mRNA export, Cell Nucleus, Models, Molecular, nucleocytoplasmic transport, 570, electron microscopy, Protein Conformation, Cryoelectron Microscopy, Active Transport, Cell Nucleus, 610, Eukaryota, Crystallography, X-Ray, Nuclear Pore Complex Proteins, Protein Subunits, nuclear pore complex, Nuclear Pore, Animals, Humans, RNA, Messenger, integrative structural biology, X-ray crystallography
mRNA export, Cell Nucleus, Models, Molecular, nucleocytoplasmic transport, 570, electron microscopy, Protein Conformation, Cryoelectron Microscopy, Active Transport, Cell Nucleus, 610, Eukaryota, Crystallography, X-Ray, Nuclear Pore Complex Proteins, Protein Subunits, nuclear pore complex, Nuclear Pore, Animals, Humans, RNA, Messenger, integrative structural biology, X-ray crystallography
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