Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.

Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.

Gap junctions (GJs) are the principal membrane structures that conduct electrical impulses between cardiac myocytes while interstitial collagen (IC) can physically separate adjacent myocytes and limit cell-cell communication. Emerging evidence suggests that both GJ and interstitial structural remode...

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Main Authors: Jiajie Yan, Justin K Thomson, Xiaomin Wu, Weiwei Zhao, Andrew E Pollard, Xun Ai
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4126721?pdf=render
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spelling doaj-776cf4e9485a4e8d948a4998107166092020-11-25T01:52:49ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0198e10435710.1371/journal.pone.0104357Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.Jiajie YanJustin K ThomsonXiaomin WuWeiwei ZhaoAndrew E PollardXun AiGap junctions (GJs) are the principal membrane structures that conduct electrical impulses between cardiac myocytes while interstitial collagen (IC) can physically separate adjacent myocytes and limit cell-cell communication. Emerging evidence suggests that both GJ and interstitial structural remodeling are linked to cardiac arrhythmia development. However, automated quantitative identification of GJ distribution and IC deposition from microscopic histological images has proven to be challenging. Such quantification is required to improve the understanding of functional consequences of GJ and structural remodeling in cardiac electrophysiology studies.Separate approaches were employed for GJ and IC identification in images from histologically stained tissue sections obtained from rabbit and human atria. For GJ identification, we recognized N-Cadherin (N-Cad) as part of the gap junction connexin 43 (Cx43) molecular complex. Because N-Cad anchors Cx43 on intercalated discs (ID) to form functional GJ channels on cell membranes, we computationally dilated N-Cad pixels to create N-Cad units that covered all ID-associated Cx43 pixels on Cx43/N-Cad double immunostained confocal images. This approach allowed segmentation between ID-associated and non-ID-associated Cx43. Additionally, use of N-Cad as a unique internal reference with Z-stack layer-by-layer confocal images potentially limits sample processing related artifacts in Cx43 quantification. For IC quantification, color map thresholding of Masson's Trichrome blue stained sections allowed straightforward and automated segmentation of collagen from non-collagen pixels. Our results strongly demonstrate that the two novel image-processing approaches can minimize potential overestimation or underestimation of gap junction and structural remodeling in healthy and pathological hearts. The results of using the two novel methods will significantly improve our understanding of the molecular and structural remodeling associated functional changes in cardiac arrhythmia development in aged and diseased hearts.http://europepmc.org/articles/PMC4126721?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jiajie Yan
Justin K Thomson
Xiaomin Wu
Weiwei Zhao
Andrew E Pollard
Xun Ai
spellingShingle Jiajie Yan
Justin K Thomson
Xiaomin Wu
Weiwei Zhao
Andrew E Pollard
Xun Ai
Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
PLoS ONE
author_facet Jiajie Yan
Justin K Thomson
Xiaomin Wu
Weiwei Zhao
Andrew E Pollard
Xun Ai
author_sort Jiajie Yan
title Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
title_short Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
title_full Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
title_fullStr Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
title_full_unstemmed Novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
title_sort novel methods of automated quantification of gap junction distribution and interstitial collagen quantity from animal and human atrial tissue sections.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Gap junctions (GJs) are the principal membrane structures that conduct electrical impulses between cardiac myocytes while interstitial collagen (IC) can physically separate adjacent myocytes and limit cell-cell communication. Emerging evidence suggests that both GJ and interstitial structural remodeling are linked to cardiac arrhythmia development. However, automated quantitative identification of GJ distribution and IC deposition from microscopic histological images has proven to be challenging. Such quantification is required to improve the understanding of functional consequences of GJ and structural remodeling in cardiac electrophysiology studies.Separate approaches were employed for GJ and IC identification in images from histologically stained tissue sections obtained from rabbit and human atria. For GJ identification, we recognized N-Cadherin (N-Cad) as part of the gap junction connexin 43 (Cx43) molecular complex. Because N-Cad anchors Cx43 on intercalated discs (ID) to form functional GJ channels on cell membranes, we computationally dilated N-Cad pixels to create N-Cad units that covered all ID-associated Cx43 pixels on Cx43/N-Cad double immunostained confocal images. This approach allowed segmentation between ID-associated and non-ID-associated Cx43. Additionally, use of N-Cad as a unique internal reference with Z-stack layer-by-layer confocal images potentially limits sample processing related artifacts in Cx43 quantification. For IC quantification, color map thresholding of Masson's Trichrome blue stained sections allowed straightforward and automated segmentation of collagen from non-collagen pixels. Our results strongly demonstrate that the two novel image-processing approaches can minimize potential overestimation or underestimation of gap junction and structural remodeling in healthy and pathological hearts. The results of using the two novel methods will significantly improve our understanding of the molecular and structural remodeling associated functional changes in cardiac arrhythmia development in aged and diseased hearts.
url http://europepmc.org/articles/PMC4126721?pdf=render
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AT justinkthomson novelmethodsofautomatedquantificationofgapjunctiondistributionandinterstitialcollagenquantityfromanimalandhumanatrialtissuesections
AT xiaominwu novelmethodsofautomatedquantificationofgapjunctiondistributionandinterstitialcollagenquantityfromanimalandhumanatrialtissuesections
AT weiweizhao novelmethodsofautomatedquantificationofgapjunctiondistributionandinterstitialcollagenquantityfromanimalandhumanatrialtissuesections
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