Novel diabetic mouse models as tools for investigating diabetic retinopathy.

Novel diabetic mouse models as tools for investigating diabetic retinopathy.

Mouse models possessing green fluorescent protein (GFP) and/or human aldose reductase (hAR) in vascular tissues have been established and crossed with naturally diabetic Akita mice to produce new diabetic mouse models.Colonies of transgenic C57BL mice expressing GFP (SMAA-GFP), hAR (SMAA-hAR) or bot...

Full description

Bibliographic Details
Main Authors: Peter F Kador, Peng Zhang, Jun Makita, Zifeng Zhang, Changmei Guo, James Randazzo, Hiroyoshi Kawada, Neena Haider, Karen Blessing
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3520987?pdf=render
id doaj-f78f137389ec4472a66891a5e4d1d28d
record_format Article
spelling doaj-f78f137389ec4472a66891a5e4d1d28d2020-11-25T02:32:57ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01712e4942210.1371/journal.pone.0049422Novel diabetic mouse models as tools for investigating diabetic retinopathy.Peter F KadorPeng ZhangJun MakitaZifeng ZhangChangmei GuoJames RandazzoHiroyoshi KawadaNeena HaiderKaren BlessingMouse models possessing green fluorescent protein (GFP) and/or human aldose reductase (hAR) in vascular tissues have been established and crossed with naturally diabetic Akita mice to produce new diabetic mouse models.Colonies of transgenic C57BL mice expressing GFP (SMAA-GFP), hAR (SMAA-hAR) or both (SMAA-GFP-hAR) in vascular tissues expressing smooth muscle actin were established and crossbred with C57BL/6-Ins2(Akita)/J (AK) mice to produce naturally diabetic offspring AK-SMAA-GFP and AK-SMAA-GFP-hAR. Aldose reductase inhibitor AL1576 (ARI) was administered in chow. Retinal and lenticular sorbitol levels were determined by HPLC. Retinal functions were evaluated by electroretinography (ERGs). Growth factor and signaling changes were determined by Western Blots using commercially available antibodies. Retinal vasculatures were isolated from the neural retina by enzymatic digestion. Flat mounts were stained with PAS-hematoxylin and analyzed.Akita transgenics developed DM by 8 weeks of age with blood glucose levels higher in males than females. Sorbitol levels were higher in neural retinas of AK-SMAA-GFP-hAR compared to AK-SMAA-GFP mice. AK-SMAA-GFP-hAR mice also had higher VEGF levels and reduced ERG scotopic b-wave function, both of which were normalized by AL1576. AK-SMAA-GFP-hAR mice showed induction of the retinal growth factors bFGF, IGF-1, and TGFβ, as well as signaling changes in P-Akt, P-SAPK/JNK and P-44/42 MAPK that were also reduced by ARI treatment. Quantitative analysis of flat mounts in 18 week AK-SMAA-GFP-hAR mice revealed increased loss of nuclei/capillary length and a significant increase in the percentage of acellular capillaries present which was not seen in AK-SMAA-GFP-hAR treated with ARI.These new mouse models of early onset diabetes may be valuable tools for assessing both the role of hyperglycemia and AR in the development of retinal lesions associated with diabetic retinopathy.http://europepmc.org/articles/PMC3520987?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Peter F Kador
Peng Zhang
Jun Makita
Zifeng Zhang
Changmei Guo
James Randazzo
Hiroyoshi Kawada
Neena Haider
Karen Blessing
spellingShingle Peter F Kador
Peng Zhang
Jun Makita
Zifeng Zhang
Changmei Guo
James Randazzo
Hiroyoshi Kawada
Neena Haider
Karen Blessing
Novel diabetic mouse models as tools for investigating diabetic retinopathy.
PLoS ONE
author_facet Peter F Kador
Peng Zhang
Jun Makita
Zifeng Zhang
Changmei Guo
James Randazzo
Hiroyoshi Kawada
Neena Haider
Karen Blessing
author_sort Peter F Kador
title Novel diabetic mouse models as tools for investigating diabetic retinopathy.
title_short Novel diabetic mouse models as tools for investigating diabetic retinopathy.
title_full Novel diabetic mouse models as tools for investigating diabetic retinopathy.
title_fullStr Novel diabetic mouse models as tools for investigating diabetic retinopathy.
title_full_unstemmed Novel diabetic mouse models as tools for investigating diabetic retinopathy.
title_sort novel diabetic mouse models as tools for investigating diabetic retinopathy.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Mouse models possessing green fluorescent protein (GFP) and/or human aldose reductase (hAR) in vascular tissues have been established and crossed with naturally diabetic Akita mice to produce new diabetic mouse models.Colonies of transgenic C57BL mice expressing GFP (SMAA-GFP), hAR (SMAA-hAR) or both (SMAA-GFP-hAR) in vascular tissues expressing smooth muscle actin were established and crossbred with C57BL/6-Ins2(Akita)/J (AK) mice to produce naturally diabetic offspring AK-SMAA-GFP and AK-SMAA-GFP-hAR. Aldose reductase inhibitor AL1576 (ARI) was administered in chow. Retinal and lenticular sorbitol levels were determined by HPLC. Retinal functions were evaluated by electroretinography (ERGs). Growth factor and signaling changes were determined by Western Blots using commercially available antibodies. Retinal vasculatures were isolated from the neural retina by enzymatic digestion. Flat mounts were stained with PAS-hematoxylin and analyzed.Akita transgenics developed DM by 8 weeks of age with blood glucose levels higher in males than females. Sorbitol levels were higher in neural retinas of AK-SMAA-GFP-hAR compared to AK-SMAA-GFP mice. AK-SMAA-GFP-hAR mice also had higher VEGF levels and reduced ERG scotopic b-wave function, both of which were normalized by AL1576. AK-SMAA-GFP-hAR mice showed induction of the retinal growth factors bFGF, IGF-1, and TGFβ, as well as signaling changes in P-Akt, P-SAPK/JNK and P-44/42 MAPK that were also reduced by ARI treatment. Quantitative analysis of flat mounts in 18 week AK-SMAA-GFP-hAR mice revealed increased loss of nuclei/capillary length and a significant increase in the percentage of acellular capillaries present which was not seen in AK-SMAA-GFP-hAR treated with ARI.These new mouse models of early onset diabetes may be valuable tools for assessing both the role of hyperglycemia and AR in the development of retinal lesions associated with diabetic retinopathy.
url http://europepmc.org/articles/PMC3520987?pdf=render
work_keys_str_mv AT peterfkador noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT pengzhang noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT junmakita noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT zifengzhang noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT changmeiguo noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT jamesrandazzo noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT hiroyoshikawada noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT neenahaider noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
AT karenblessing noveldiabeticmousemodelsastoolsforinvestigatingdiabeticretinopathy
_version_ 1724816576806387712

Similar Items