In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.

In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.

BACKGROUND AND AIMS: Endoprotease activation is a key step in acute pancreatitis and early inhibition of these enzymes may protect from organ damage. In vivo models commonly used to evaluate protease inhibitors require animal sacrifice and therefore limit the assessment of dynamic processes. Here, w...

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Main Authors: Abhiruchi Agarwal, Andreas Boettcher, Rainer Kneuer, Farid Sari-Sarraf, Adriana Donovan, Julian Woelcke, Oliver Simic, Trixi Brandl, Thomas Krucker
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3569412?pdf=render
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spelling doaj-685a8db557fa415b8d07c6ac5aa241bb2020-11-25T02:42:46ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0182e5595910.1371/journal.pone.0055959In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.Abhiruchi AgarwalAndreas BoettcherRainer KneuerFarid Sari-SarrafAdriana DonovanJulian WoelckeOliver SimicTrixi BrandlThomas KruckerBACKGROUND AND AIMS: Endoprotease activation is a key step in acute pancreatitis and early inhibition of these enzymes may protect from organ damage. In vivo models commonly used to evaluate protease inhibitors require animal sacrifice and therefore limit the assessment of dynamic processes. Here, we established a non-invasive fluorescence imaging-based biomarker assay to assess real-time protease inhibition and disease progression in a preclinical model of experimental pancreatitis. METHODS: Edema development and trypsin activation were imaged in a rat caerulein-injection pancreatitis model. A fluorescent "smart" probe, selectively activated by trypsin, was synthesized by labeling with Cy5.5 of a pegylated poly-L-lysine copolymer. Following injection of the probe, trypsin activation was monitored in the presence or absence of inhibitors by in vivo and ex vivo imaging. RESULTS: We established the trypsin-selectivity of the fluorescent probe in vitro using a panel of endopeptidases and specific inhibitor. In vivo, the probe accumulated in the liver and a region attributed to the pancreas by necropsy. A dose dependent decrease of total pancreatic fluorescence signal occurred upon administration of known trypsin inhibitors. The fluorescence-based method was a better predictor of trypsin inhibition than pancreatic to body weight ratio. CONCLUSIONS: We established a fluorescence imaging assay to access trypsin inhibition in real-time in vivo. This method is more sensitive and dynamic than classic tissue sample readouts and could be applied to preclinically optimize trypsin inhibitors towards intrapancreatic target inhibition.http://europepmc.org/articles/PMC3569412?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Abhiruchi Agarwal
Andreas Boettcher
Rainer Kneuer
Farid Sari-Sarraf
Adriana Donovan
Julian Woelcke
Oliver Simic
Trixi Brandl
Thomas Krucker
spellingShingle Abhiruchi Agarwal
Andreas Boettcher
Rainer Kneuer
Farid Sari-Sarraf
Adriana Donovan
Julian Woelcke
Oliver Simic
Trixi Brandl
Thomas Krucker
In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
PLoS ONE
author_facet Abhiruchi Agarwal
Andreas Boettcher
Rainer Kneuer
Farid Sari-Sarraf
Adriana Donovan
Julian Woelcke
Oliver Simic
Trixi Brandl
Thomas Krucker
author_sort Abhiruchi Agarwal
title In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
title_short In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
title_full In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
title_fullStr In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
title_full_unstemmed In vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
title_sort in vivo imaging with fluorescent smart probes to assess treatment strategies for acute pancreatitis.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description BACKGROUND AND AIMS: Endoprotease activation is a key step in acute pancreatitis and early inhibition of these enzymes may protect from organ damage. In vivo models commonly used to evaluate protease inhibitors require animal sacrifice and therefore limit the assessment of dynamic processes. Here, we established a non-invasive fluorescence imaging-based biomarker assay to assess real-time protease inhibition and disease progression in a preclinical model of experimental pancreatitis. METHODS: Edema development and trypsin activation were imaged in a rat caerulein-injection pancreatitis model. A fluorescent "smart" probe, selectively activated by trypsin, was synthesized by labeling with Cy5.5 of a pegylated poly-L-lysine copolymer. Following injection of the probe, trypsin activation was monitored in the presence or absence of inhibitors by in vivo and ex vivo imaging. RESULTS: We established the trypsin-selectivity of the fluorescent probe in vitro using a panel of endopeptidases and specific inhibitor. In vivo, the probe accumulated in the liver and a region attributed to the pancreas by necropsy. A dose dependent decrease of total pancreatic fluorescence signal occurred upon administration of known trypsin inhibitors. The fluorescence-based method was a better predictor of trypsin inhibition than pancreatic to body weight ratio. CONCLUSIONS: We established a fluorescence imaging assay to access trypsin inhibition in real-time in vivo. This method is more sensitive and dynamic than classic tissue sample readouts and could be applied to preclinically optimize trypsin inhibitors towards intrapancreatic target inhibition.
url http://europepmc.org/articles/PMC3569412?pdf=render
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