AI Article Synopsis

  • The study focused on how GP-2, a glycoprotein in pancreatic zymogen granules, is transported and reaches the cell surface.
  • It was found that GP-2 starts incorporating into the granules about 60 minutes after synthesis and appears on the cell surface within the same timeframe.
  • The research indicates that GP-2 has a high turnover rate on the plasma membrane and can bypass the usual pathway through mature zymogen granules, while the initial transport is unaffected by the N-glycosylation inhibitor tunicamycin.

Article Abstract

The intracellular transport and destination of the major glycoprotein associated with zymogen granule membranes in the pancreas (GP-2) was established. In suspensions of isolated acinar cells from rat pancreas, pulse-chase experiments were performed. The incorporation of the first newly synthesized GP-2 molecules into zymogen granule membranes occurred at about 60 min after beginning of the pulse. We demonstrated by using two different methods that newly made GP-2 reaches the cell surface within the same time span. After 6-8 h chase considerable more newly synthesized GP-2 has reached the cell surface than would be expected on account of secreted newly synthesized zymogens. These observations strongly suggest that at least part of the GP-2 molecules bypass the mature zymogen granule compartment on their way to the plasma membrane. GP-2 is the only protein that appears in discernable quantity in the plasma membrane during 1-4 h after a pulse label. Nevertheless GP-2 comprises only a small percentage of externally 125I-iodinated plasma membrane proteins. We conclude that GP-2 has a high turnover rate at the plasma membrane level. Treatment of the acinar cells with the N-glycosylation inhibitor tunicamycin does not block the intracellular transport of GP-2.

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Source
http://dx.doi.org/10.1111/j.1432-1033.1984.tb08446.xDOI Listing

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