Abstract

The effect of glucose concentration in medium on the functional maturation of developing B cells was studied in pancreatic monolayer cultures of the neonatal rat. After a 3-day treatment with 10 microM iodoacetic acid in TCM 199 medium containing 5.5 mM glucose to selectively delete fibroblasts, the monolayer cultures were kept in the medium with either 5.5 mM glucose or 16.7 mM glucose for up to a total of 12 days. They were then perifused several times so that the phasic insulin secretion could be examined. On day 0, untreated B cells showed a monophasic insulin secretion in response to a 16.7 mM single dose of glucose, whereas in the presence of 200 nM 12-o-tetradecanoyl phorbol-13-acetate, 10 microM forskolin, 1 mM 3-isobutyl-1-methylxanthine or 40 microM lysophosphatidylcholine, the same dose of glucose stimulated insulin secretion in a biphasic fashion. Further, 20 mg/dl sodium salicylate, 100 microM tetracaine or 100 microM p-bromophenacylbromide used concurrently with 16.7 mM glucose also induced a biphasic insulin secretion, but their ability to stimulate insulin secretion was less than that of the other drugs mentioned above. Also, B cells on day 3 that had been exposed to iodoacetic acid responded to glucose in a similar manner to that of B cells on day 0, and the response to 10 mM of either leucine or 2-ketoisocaproate was monophasic. By contrast, B cells that had been kept in 5.5 mM glucose on day 7 responded in a biphasic fashion, not only to 16.7 mM glucose but also to 10 mM of either leucine or 2-ketoisocaproate. The biphasic pattern evoked by glucose was still preserved in magnitude on day 15, whereas the response to leucine and 2-ketoisocaproate decreased to one-third that of B cells on day 7. On the other hand, when the concentration of 16.7 mM glucose was present in the medium, B cells on day 7 showed a biphasic pattern of insulin secretion in response to 16.7 mM glucose, although the magnitude of the response was quantitatively less than that of B cells in a physiological concentration of glucose. And again the response to 10 mM of either leucine or 2-ketoisocaproate appeared monophasic. On day 15, an increased response to secretagogues with a biphasic pattern of insulin secretion was observed.(ABSTRACT TRUNCATED AT 400 WORDS)

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