Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes

Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes

Therapeutic modalities targeting vascular endothelial growth factor (VEGF) have been used to treat neovascularization and macular edema. However, anti-VEGF treatment alone may cause up-regulation of connective tissue growth factor (CTGF) in the retina, increasing the risk of fibrosis and tractional...

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Main Authors: Bojie Hu, Yan Zhang, Qing Zeng, Qian Han, Lijuan Zhang, Mian Liu, Xiaorong Li
Format: Article
Language:English
Published: MDPI AG 2014-01-01
Series:International Journal of Molecular Sciences
Subjects:
vascular endothelial growth factor
connective tissue growth factor
diabetic retinopathy
ranibizumab
shRNA
Online Access:http://www.mdpi.com/1422-0067/15/1/1606
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spelling doaj-63dde54eb7d64017ab024a925b2c8f642020-11-24T21:25:19ZengMDPI AGInternational Journal of Molecular Sciences1422-00672014-01-011511606162410.3390/ijms15011606ijms15011606Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of DiabetesBojie Hu0Yan Zhang1Qing Zeng2Qian Han3Lijuan Zhang4Mian Liu5Xiaorong Li6Tianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTianjin Medical University Eye Hospital/Eye Institute, Fukang Rd. 251#, Nankai Dist., Tianjin 300384, ChinaTherapeutic modalities targeting vascular endothelial growth factor (VEGF) have been used to treat neovascularization and macular edema. However, anti-VEGF treatment alone may cause up-regulation of connective tissue growth factor (CTGF) in the retina, increasing the risk of fibrosis and tractional retinal detachment. Therefore, in this study, we employ a novel dual-target intervention that involves intravitreal injection of the VEGF inhibitor ranibizumab and a transfection reagent-treated non-viral vector carrying anti-CTGF short hairpin RNA (shRNA) driven by human RNA polymerase III promoter U6. The effects of the dual-target intervention on the expression of VEGF and CTGF and on microvessel ultrastructure were examined in retina of streptozocin-induced diabetic rats. CTGF was significantly up-regulated at week 8 after diabetic induction, whereas VEGF was not up-regulated until week 10. The high expression of both genes was maintained at week 12. Transmission electron microscopy also revealed progressive exacerbation of microvessel ultrastructure during the same period. In addition, ranibizumab significantly lowered VEGF but elevated CTGF mRNA, whereas CTGF shRNA significantly reduced the mRNA levels of both CTGF and VEGF in diabetic retinas. Importantly, dual-target intervention normalized the transcript levels of both target genes and ameliorated retinal microvessel ultrastructural damage better than either single-target intervention. These results suggest the advantages of dual-target over single-target interventions in diabetic retina and reveal a novel therapeutic modality for diabetic retinopathy.http://www.mdpi.com/1422-0067/15/1/1606vascular endothelial growth factorconnective tissue growth factordiabetic retinopathyranibizumabshRNA
collection DOAJ
language English
format Article
sources DOAJ
author Bojie Hu
Yan Zhang
Qing Zeng
Qian Han
Lijuan Zhang
Mian Liu
Xiaorong Li
spellingShingle Bojie Hu
Yan Zhang
Qing Zeng
Qian Han
Lijuan Zhang
Mian Liu
Xiaorong Li
Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes
International Journal of Molecular Sciences
vascular endothelial growth factor
connective tissue growth factor
diabetic retinopathy
ranibizumab
shRNA
author_facet Bojie Hu
Yan Zhang
Qing Zeng
Qian Han
Lijuan Zhang
Mian Liu
Xiaorong Li
author_sort Bojie Hu
title Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes
title_short Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes
title_full Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes
title_fullStr Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes
title_full_unstemmed Intravitreal Injection of Ranibizumab and CTGF shRNA Improves Retinal Gene Expression and Microvessel Ultrastructure in a Rodent Model of Diabetes
title_sort intravitreal injection of ranibizumab and ctgf shrna improves retinal gene expression and microvessel ultrastructure in a rodent model of diabetes
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2014-01-01
description Therapeutic modalities targeting vascular endothelial growth factor (VEGF) have been used to treat neovascularization and macular edema. However, anti-VEGF treatment alone may cause up-regulation of connective tissue growth factor (CTGF) in the retina, increasing the risk of fibrosis and tractional retinal detachment. Therefore, in this study, we employ a novel dual-target intervention that involves intravitreal injection of the VEGF inhibitor ranibizumab and a transfection reagent-treated non-viral vector carrying anti-CTGF short hairpin RNA (shRNA) driven by human RNA polymerase III promoter U6. The effects of the dual-target intervention on the expression of VEGF and CTGF and on microvessel ultrastructure were examined in retina of streptozocin-induced diabetic rats. CTGF was significantly up-regulated at week 8 after diabetic induction, whereas VEGF was not up-regulated until week 10. The high expression of both genes was maintained at week 12. Transmission electron microscopy also revealed progressive exacerbation of microvessel ultrastructure during the same period. In addition, ranibizumab significantly lowered VEGF but elevated CTGF mRNA, whereas CTGF shRNA significantly reduced the mRNA levels of both CTGF and VEGF in diabetic retinas. Importantly, dual-target intervention normalized the transcript levels of both target genes and ameliorated retinal microvessel ultrastructural damage better than either single-target intervention. These results suggest the advantages of dual-target over single-target interventions in diabetic retina and reveal a novel therapeutic modality for diabetic retinopathy.
topic vascular endothelial growth factor
connective tissue growth factor
diabetic retinopathy
ranibizumab
shRNA
url http://www.mdpi.com/1422-0067/15/1/1606
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AT yanzhang intravitrealinjectionofranibizumabandctgfshrnaimprovesretinalgeneexpressionandmicrovesselultrastructureinarodentmodelofdiabetes
AT qingzeng intravitrealinjectionofranibizumabandctgfshrnaimprovesretinalgeneexpressionandmicrovesselultrastructureinarodentmodelofdiabetes
AT qianhan intravitrealinjectionofranibizumabandctgfshrnaimprovesretinalgeneexpressionandmicrovesselultrastructureinarodentmodelofdiabetes
AT lijuanzhang intravitrealinjectionofranibizumabandctgfshrnaimprovesretinalgeneexpressionandmicrovesselultrastructureinarodentmodelofdiabetes
AT mianliu intravitrealinjectionofranibizumabandctgfshrnaimprovesretinalgeneexpressionandmicrovesselultrastructureinarodentmodelofdiabetes
AT xiaorongli intravitrealinjectionofranibizumabandctgfshrnaimprovesretinalgeneexpressionandmicrovesselultrastructureinarodentmodelofdiabetes
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