Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.

Intrahepatic transplantation of donor islets of Langerhans is a promising therapy for patients with type 1 diabetes. It is of critical importance to accurately monitor islet quality before transplantation, which is currently done by standard histological methods that are performed off-line and requi...

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Main Authors: Janneke Hilderink, Cees Otto, Cees Slump, Aufried Lenferink, Marten Engelse, Clemens van Blitterswijk, Eelco de Koning, Marcel Karperien, Aart van Apeldoorn
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3805587?pdf=render
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spelling doaj-84bca18cf40341b79e66b84d978b26db2020-11-25T00:59:37ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01810e7814810.1371/journal.pone.0078148Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.Janneke HilderinkCees OttoCees SlumpAufried LenferinkMarten EngelseClemens van BlitterswijkEelco de KoningMarcel KarperienAart van ApeldoornIntrahepatic transplantation of donor islets of Langerhans is a promising therapy for patients with type 1 diabetes. It is of critical importance to accurately monitor islet quality before transplantation, which is currently done by standard histological methods that are performed off-line and require extensive sample preparation. As an alternative, we propose Raman spectroscopy which is a non-destructive and label-free technique that allows continuous real-time monitoring of the tissue to study biological changes as they occur. By performing Raman spectroscopic measurements on purified insulin and glucagon, we showed that the 520 cm(-1) band assigned to disulfide bridges in insulin, and the 1552 cm(-1) band assigned to tryptophan in glucagon are mutually exclusive and could therefore be used as indirect markers for the label-free distinction between both hormones. High-resolution hyperspectral Raman imaging for these bands showed the distribution of disulfide bridges and tryptophan at sub-micrometer scale, which correlated with the location of insulin and glucagon as revealed by conventional immunohistochemistry. As a measure for this correlation, quantitative analysis was performed comparing the Raman images with the fluorescence images, resulting in Dice coefficients (ranging between 0 and 1) of 0.36 for insulin and 0.19 for glucagon. Although the use of separate microscope systems with different spatial resolution and the use of indirect Raman markers cause some image mismatch, our findings indicate that Raman bands for disulfide bridges and tryptophan can be used as distinctive markers for the label-free detection of insulin and glucagon in human islets of Langerhans.http://europepmc.org/articles/PMC3805587?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Janneke Hilderink
Cees Otto
Cees Slump
Aufried Lenferink
Marten Engelse
Clemens van Blitterswijk
Eelco de Koning
Marcel Karperien
Aart van Apeldoorn
spellingShingle Janneke Hilderink
Cees Otto
Cees Slump
Aufried Lenferink
Marten Engelse
Clemens van Blitterswijk
Eelco de Koning
Marcel Karperien
Aart van Apeldoorn
Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.
PLoS ONE
author_facet Janneke Hilderink
Cees Otto
Cees Slump
Aufried Lenferink
Marten Engelse
Clemens van Blitterswijk
Eelco de Koning
Marcel Karperien
Aart van Apeldoorn
author_sort Janneke Hilderink
title Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.
title_short Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.
title_full Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.
title_fullStr Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.
title_full_unstemmed Label-free detection of insulin and glucagon within human islets of Langerhans using Raman spectroscopy.
title_sort label-free detection of insulin and glucagon within human islets of langerhans using raman spectroscopy.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Intrahepatic transplantation of donor islets of Langerhans is a promising therapy for patients with type 1 diabetes. It is of critical importance to accurately monitor islet quality before transplantation, which is currently done by standard histological methods that are performed off-line and require extensive sample preparation. As an alternative, we propose Raman spectroscopy which is a non-destructive and label-free technique that allows continuous real-time monitoring of the tissue to study biological changes as they occur. By performing Raman spectroscopic measurements on purified insulin and glucagon, we showed that the 520 cm(-1) band assigned to disulfide bridges in insulin, and the 1552 cm(-1) band assigned to tryptophan in glucagon are mutually exclusive and could therefore be used as indirect markers for the label-free distinction between both hormones. High-resolution hyperspectral Raman imaging for these bands showed the distribution of disulfide bridges and tryptophan at sub-micrometer scale, which correlated with the location of insulin and glucagon as revealed by conventional immunohistochemistry. As a measure for this correlation, quantitative analysis was performed comparing the Raman images with the fluorescence images, resulting in Dice coefficients (ranging between 0 and 1) of 0.36 for insulin and 0.19 for glucagon. Although the use of separate microscope systems with different spatial resolution and the use of indirect Raman markers cause some image mismatch, our findings indicate that Raman bands for disulfide bridges and tryptophan can be used as distinctive markers for the label-free detection of insulin and glucagon in human islets of Langerhans.
url http://europepmc.org/articles/PMC3805587?pdf=render
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