Multiphoton imaging of the effect of monosaccharide diffusion and formation of fluorescent advanced end products in porcine aorta

Prolonged exposure of tissues to elevated blood sugar levels lead to the formation of advanced glycation end products (AGEs), thus contributing to diabetic complications. Since the vascular system is in immediate contact with blood, diabetic effects on aorta is a major health concern. However, the r...

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Veröffentlicht in:Journal of biophotonics 2021-07, Vol.14 (7), p.e202000439-n/a
Hauptverfasser: Lin, Chih‐Ju, Lee, Sheng‐Lin, Kang, Jeon‐Woong, So, Peter T.C., Dong, Chen‐Yuan
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container_issue 7
container_start_page e202000439
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creator Lin, Chih‐Ju
Lee, Sheng‐Lin
Kang, Jeon‐Woong
So, Peter T.C.
Dong, Chen‐Yuan
description Prolonged exposure of tissues to elevated blood sugar levels lead to the formation of advanced glycation end products (AGEs), thus contributing to diabetic complications. Since the vascular system is in immediate contact with blood, diabetic effects on aorta is a major health concern. However, the relative effect of the diffusion of sugar molecular through the vascular wall and the rate of AGE formation is not known. In this study, we aim to address this issue by incubating excised porcine aorta in D‐glucose, D‐galactose, and D‐fructose solutions for different periods. The tissue specimens were then excised for multiphoton imaging of autofluorescence intensity profiles across the aorta wall. We found that for Days 4 to 48 incubation, autofluorescence is constant along the radial direction of the aorta sections, suggesting that monosaccharide diffusion is rapid in comparison to the rate of formation of fluorescent AGEs (fAGEs). Moreover, we found that in porcine aorta, the rate of fAGE formation of D‐fructose and D‐glucose are factors 2.08 and 1.14 that of D‐galactose. Our results suggest that for prolonged exposure of the cardiovascular system to elevated monosaccharides 4 days or longer, damage to the aorta is uniform throughout the tissues. In this manuscript, we used porcine aorta and monosaccharide solutions to simulate the diffusion of sugar molecules from blood into the artery wall and advanced glycated end products. Fluorescent advanced glycation end products would be obtained via multiphoton microscopy. In daily sugars, fructose caused the most fluorescent advanced glycated end products. Glucose was measured daily by diabetes patients, it caused the less glycation.
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Since the vascular system is in immediate contact with blood, diabetic effects on aorta is a major health concern. However, the relative effect of the diffusion of sugar molecular through the vascular wall and the rate of AGE formation is not known. In this study, we aim to address this issue by incubating excised porcine aorta in D‐glucose, D‐galactose, and D‐fructose solutions for different periods. The tissue specimens were then excised for multiphoton imaging of autofluorescence intensity profiles across the aorta wall. We found that for Days 4 to 48 incubation, autofluorescence is constant along the radial direction of the aorta sections, suggesting that monosaccharide diffusion is rapid in comparison to the rate of formation of fluorescent AGEs (fAGEs). Moreover, we found that in porcine aorta, the rate of fAGE formation of D‐fructose and D‐glucose are factors 2.08 and 1.14 that of D‐galactose. Our results suggest that for prolonged exposure of the cardiovascular system to elevated monosaccharides 4 days or longer, damage to the aorta is uniform throughout the tissues. In this manuscript, we used porcine aorta and monosaccharide solutions to simulate the diffusion of sugar molecules from blood into the artery wall and advanced glycated end products. Fluorescent advanced glycation end products would be obtained via multiphoton microscopy. In daily sugars, fructose caused the most fluorescent advanced glycated end products. Glucose was measured daily by diabetes patients, it caused the less glycation.</description><identifier>ISSN: 1864-063X</identifier><identifier>EISSN: 1864-0648</identifier><identifier>DOI: 10.1002/jbio.202000439</identifier><identifier>PMID: 33611855</identifier><language>eng</language><publisher>Weinheim: WILEY‐VCH Verlag GmbH &amp; Co. 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subjects advanced glycation end products
Advanced glycosylation end products
Aorta
autofluorescence
Blood
Cardiovascular system
Complications
Coronary vessels
Diabetes
Diabetes mellitus
Diffusion
Diffusion effects
Diffusion rate
Exposure
Fluorescence
Fructose
Galactose
Glucose
Glycosylation
Hyperglycemia
Monosaccharides
multiphoton imaging
Tissues
Vascular system
title Multiphoton imaging of the effect of monosaccharide diffusion and formation of fluorescent advanced end products in porcine aorta
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