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      Insulin, not C-peptide (proinsulin), is present in crinophagic bodies of the pancreatic B-cell

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      The Journal of Cell Biology
      The Rockefeller University Press

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          Abstract

          We have obtained evidence by autoradiography and immunocytochemistry that mature secretory granules of the pancreatic B-cell gain access to a lysosomal compartment (multigranular or crinophagic bodies) where the secretory granule content is degraded. Whereas the mature secretory granule content shows both insulin and C-peptide (proinsulin) immunoreactivities, in crinophagic bodies only insulin, but not C- peptide, immunoreactivity was detectable. The absence of C-peptide (proinsulin) immunoreactivity in multigranular bodies, i.e., in early morphological stages of lysosomal digestion, was compatible with the ready access and breakdown of C-peptide and/or proinsulin by lysosomal degrading enzymes, while the insulin crystallized in secretory granule cores remained relatively protected. However, in the final stage of lysosomal digestion, i.e., in residual bodies where the secretory granule core material is no longer present, insulin immunoreactivity became undetectable. Lysosomal digestion thus appears to be a normal pathway for insulin degradation in the pancreatic B-cell.

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          Author and article information

          Journal
          J Cell Biol
          The Journal of Cell Biology
          The Rockefeller University Press
          0021-9525
          1540-8140
          1 January 1984
          : 98
          : 1
          : 222-228
          Article
          84162278
          10.1083/jcb.98.1.222
          2112993
          6368567
          1b4be80e-a263-431a-8322-7889fa13f8a7
          History
          Categories
          Articles

          Cell biology
          Cell biology

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