Temperature-Sensitive Random Insulin Granule Diffusion is a Prerequisite for Recruiting Granules for Release
Article first published online: 18 AUG 2004
DOI: 10.1111/j.1600-0854.2004.00216.x
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How to Cite
Ivarsson, R., Obermüller, S., Rutter, G. A., Galvanovskis, J. and Renström, E. (2004), Temperature-Sensitive Random Insulin Granule Diffusion is a Prerequisite for Recruiting Granules for Release. Traffic, 5: 750–762. doi: 10.1111/j.1600-0854.2004.00216.x
Publication History
- Issue published online: 18 AUG 2004
- Article first published online: 18 AUG 2004
- Received 17 May 2004, revised and accepted for publication 23 June 2004
- Abstract
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Keywords:
- diffusion;
- granule movement;
- insulin;
- microtubule;
- temperature sensitivity
Glucose-evoked insulin secretion exhibits a biphasic time course and is associated with accelerated intracellular granule movement. We combined live confocal imaging of EGFP-labelled insulin granules with capacitance measurements of exocytosis in clonal INS-1 cells to explore the relation between distinct random and directed modes of insulin granule movement, as well as exocytotic capacity. Reducing the temperature from 34 °C to 24 °C caused a dramatic 81% drop in the frequency of directed events, but reduced directed velocities by a mere 25%. The much stronger temperature sensitivity of the frequency of directed events (estimated energy of activation ∼ 135 kJ/mol) than that of the granule velocities (∼ 22 kJ/mol) suggests that cooling-induced suppression of insulin granule movement is attributable to factors other than reduced motor protein adenosine 5'-triphosphatase activity. Indeed, cooling suppresses random granule diffusion by ∼ 50%. In the single cell, the number of directed events depends on the extent of granule diffusion. Finally, single-cell exocytosis exhibits a biphasic pattern corresponding to that observed in vivo, and only the component reflecting 2nd phase insulin secretion is affected by cooling. We conclude that random diffusive movement is a prerequisite for directed insulin granule transport and for the recruitment of insulin granules released during 2nd phase insulin secretion.

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