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 The ubiquitin-proteasome proteolytic pathway: destruction for the sake of  construction Glickman MH; Ciechanover APhysiol Rev  2002[Apr]; 82 (2): 373-428Between the 1960s and 1980s, most life scientists focused their attention on  studies of nucleic acids and the translation of the coded information. Protein  degradation was a neglected area, considered to be a nonspecific, dead-end  process. Although it was known that proteins do turn over, the large extent and  high specificity of the process, whereby distinct proteins have half-lives that  range from a few minutes to several days, was not appreciated. The discovery of  the lysosome by Christian de Duve did not significantly change this view, because  it became clear that this organelle is involved mostly in the degradation of  extracellular proteins, and their proteases cannot be substrate specific. The  discovery of the complex cascade of the ubiquitin pathway revolutionized the  field. It is clear now that degradation of cellular proteins is a highly complex,  temporally controlled, and tightly regulated process that plays major roles in a  variety of basic pathways during cell life and death as well as in health and  disease. With the multitude of substrates targeted and the myriad processes  involved, it is not surprising that aberrations in the pathway are implicated in  the pathogenesis of many diseases, certain malignancies, and neurodegeneration  among them. Degradation of a protein via the ubiquitin/proteasome pathway  involves two successive steps: 1) conjugation of multiple ubiquitin moieties to  the substrate and 2) degradation of the tagged protein by the downstream 26S  proteasome complex. Despite intensive research, the unknown still exceeds what we  currently know on intracellular protein degradation, and major key questions have  remained unsolved. Among these are the modes of specific and timed recognition  for the degradation of the many substrates and the mechanisms that underlie  aberrations in the system that lead to pathogenesis of diseases.|Animals[MESH]|Cysteine Endopeptidases/*metabolism[MESH]|Humans[MESH]|Multienzyme Complexes/*metabolism[MESH]|Proteasome Endopeptidase Complex[MESH]|Proteins/metabolism[MESH]|Ubiquitin/*metabolism[MESH]
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