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      Identification of long-lived proteins reveals exceptional stability of essential cellular structures.

      Cell
      Animals, Brain, cytology, metabolism, Cell Aging, Neuroglia, Neurons, Nuclear Pore, Nuclear Pore Complex Proteins, Protein Biosynthesis, Proteome, Rats

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          Abstract

          Intracellular proteins with long lifespans have recently been linked to age-dependent defects, ranging from decreased fertility to the functional decline of neurons. Why long-lived proteins exist in metabolically active cellular environments and how they are maintained over time remains poorly understood. Here, we provide a system-wide identification of proteins with exceptional lifespans in the rat brain. These proteins are inefficiently replenished despite being translated robustly throughout adulthood. Using nucleoporins as a paradigm for long-term protein persistence, we found that nuclear pore complexes (NPCs) are maintained over a cell's life through slow but finite exchange of even its most stable subcomplexes. This maintenance is limited, however, as some nucleoporin levels decrease during aging, providing a rationale for the previously observed age-dependent deterioration of NPC function. Our identification of a long-lived proteome reveals cellular components that are at increased risk for damage accumulation, linking long-term protein persistence to the cellular aging process. PAPERCLIP: Copyright © 2013 Elsevier Inc. All rights reserved.

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          Author and article information

          Journal
          23993091
          3788602
          10.1016/j.cell.2013.07.037

          Chemistry
          Animals,Brain,cytology,metabolism,Cell Aging,Neuroglia,Neurons,Nuclear Pore,Nuclear Pore Complex Proteins,Protein Biosynthesis,Proteome,Rats

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