Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism

Rationale: Poor β cell proliferation is one of the detrimental factors hindering islet cell replacement therapy for patients with diabetes. Smad3 is an important transcriptional factor of TGF-β signaling and has been shown to promote diabetes by inhibiting β cell proliferation. Therefore, we hypothe...

Descripción completa

Detalles Bibliográficos
Autores principales: Wang, Hong-Lian, Wei, Biao, He, Hui-Jun, Huang, Xiao-Ru, Sheng, Jing-Yi, Chen, Xiao-Cui, Wang, Li, Tan, Rui-Zhi, Li, Jian-Chun, Liu, Jian, Yang, Si-Jin, Ma, Ronald CW, Lan, Hui-Yao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2022
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8690916/
https://www.ncbi.nlm.nih.gov/pubmed/34987651
http://dx.doi.org/10.7150/thno.67034
_version_ 1784618702984970240
author Wang, Hong-Lian
Wei, Biao
He, Hui-Jun
Huang, Xiao-Ru
Sheng, Jing-Yi
Chen, Xiao-Cui
Wang, Li
Tan, Rui-Zhi
Li, Jian-Chun
Liu, Jian
Yang, Si-Jin
Ma, Ronald CW
Lan, Hui-Yao
author_facet Wang, Hong-Lian
Wei, Biao
He, Hui-Jun
Huang, Xiao-Ru
Sheng, Jing-Yi
Chen, Xiao-Cui
Wang, Li
Tan, Rui-Zhi
Li, Jian-Chun
Liu, Jian
Yang, Si-Jin
Ma, Ronald CW
Lan, Hui-Yao
author_sort Wang, Hong-Lian
collection PubMed
description Rationale: Poor β cell proliferation is one of the detrimental factors hindering islet cell replacement therapy for patients with diabetes. Smad3 is an important transcriptional factor of TGF-β signaling and has been shown to promote diabetes by inhibiting β cell proliferation. Therefore, we hypothesize that Smad3-deficient islets may be a novel cell replacement therapy for diabetes. Methods: We examined this hypothesis in streptozocin-induced type-1 diabetic mice and type-2 diabetic db/db mice by transplanting Smad3 knockout (KO) and wild type (WT) islets under the renal capsule, respectively. The effects of Smad3KO versus WT islet replacement therapy on diabetes and diabetic kidney injury were examined. In addition, RNA-seq was applied to identify the downstream target gene underlying Smad3-regulated β cell proliferation in Smad3KO-db/db versus Smad3WT-db/db mouse islets. Results: Compared to Smad3WT islet therapy, treatment with Smad3KO islets produced a much better therapeutic effect on both type-1 and type-2 diabetes by significantly lowering serum levels of blood glucose and HbA1c and protected against diabetic kidney injuries by preventing an increase in serum creatinine and the development of proteinuria, mesangial matrix expansion, and fibrosis. These were associated with a significant increase in grafted β cell proliferation and blood insulin levels, resulting in improved glucose intolerance. Mechanistically, RNA-seq revealed that compared with Smad3WT-db/db mouse islets, deletion of Smad3 from db/db mouse islets markedly upregulated E2F3, a pivotal regulator of cell cycle G1/S entry. Further studies found that Smad3 could bind to the promoter of E2F3, and thus inhibit β cell proliferation via an E2F3-dependent mechanism as silencing E2F3 abrogated the proliferative effect on Smad3KO β cells. Conclusion: Smad3-deficient islet replacement therapy can significantly improve both type-1 and type-2 diabetes and protect against diabetic kidney injury, which is mediated by a novel mechanism of E2F3-dependent β cell proliferation.
format Online
Article
Text
id pubmed-8690916
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-86909162022-01-04 Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism Wang, Hong-Lian Wei, Biao He, Hui-Jun Huang, Xiao-Ru Sheng, Jing-Yi Chen, Xiao-Cui Wang, Li Tan, Rui-Zhi Li, Jian-Chun Liu, Jian Yang, Si-Jin Ma, Ronald CW Lan, Hui-Yao Theranostics Research Paper Rationale: Poor β cell proliferation is one of the detrimental factors hindering islet cell replacement therapy for patients with diabetes. Smad3 is an important transcriptional factor of TGF-β signaling and has been shown to promote diabetes by inhibiting β cell proliferation. Therefore, we hypothesize that Smad3-deficient islets may be a novel cell replacement therapy for diabetes. Methods: We examined this hypothesis in streptozocin-induced type-1 diabetic mice and type-2 diabetic db/db mice by transplanting Smad3 knockout (KO) and wild type (WT) islets under the renal capsule, respectively. The effects of Smad3KO versus WT islet replacement therapy on diabetes and diabetic kidney injury were examined. In addition, RNA-seq was applied to identify the downstream target gene underlying Smad3-regulated β cell proliferation in Smad3KO-db/db versus Smad3WT-db/db mouse islets. Results: Compared to Smad3WT islet therapy, treatment with Smad3KO islets produced a much better therapeutic effect on both type-1 and type-2 diabetes by significantly lowering serum levels of blood glucose and HbA1c and protected against diabetic kidney injuries by preventing an increase in serum creatinine and the development of proteinuria, mesangial matrix expansion, and fibrosis. These were associated with a significant increase in grafted β cell proliferation and blood insulin levels, resulting in improved glucose intolerance. Mechanistically, RNA-seq revealed that compared with Smad3WT-db/db mouse islets, deletion of Smad3 from db/db mouse islets markedly upregulated E2F3, a pivotal regulator of cell cycle G1/S entry. Further studies found that Smad3 could bind to the promoter of E2F3, and thus inhibit β cell proliferation via an E2F3-dependent mechanism as silencing E2F3 abrogated the proliferative effect on Smad3KO β cells. Conclusion: Smad3-deficient islet replacement therapy can significantly improve both type-1 and type-2 diabetes and protect against diabetic kidney injury, which is mediated by a novel mechanism of E2F3-dependent β cell proliferation. Ivyspring International Publisher 2022-01-01 /pmc/articles/PMC8690916/ /pubmed/34987651 http://dx.doi.org/10.7150/thno.67034 Text en © The author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Wang, Hong-Lian
Wei, Biao
He, Hui-Jun
Huang, Xiao-Ru
Sheng, Jing-Yi
Chen, Xiao-Cui
Wang, Li
Tan, Rui-Zhi
Li, Jian-Chun
Liu, Jian
Yang, Si-Jin
Ma, Ronald CW
Lan, Hui-Yao
Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism
title Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism
title_full Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism
title_fullStr Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism
title_full_unstemmed Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism
title_short Smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the E2F3-dependent mechanism
title_sort smad3 deficiency improves islet-based therapy for diabetes and diabetic kidney injury by promoting β cell proliferation via the e2f3-dependent mechanism
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8690916/
https://www.ncbi.nlm.nih.gov/pubmed/34987651
http://dx.doi.org/10.7150/thno.67034
work_keys_str_mv AT wanghonglian smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT weibiao smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT hehuijun smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT huangxiaoru smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT shengjingyi smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT chenxiaocui smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT wangli smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT tanruizhi smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT lijianchun smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT liujian smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT yangsijin smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT maronaldcw smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism
AT lanhuiyao smad3deficiencyimprovesisletbasedtherapyfordiabetesanddiabetickidneyinjurybypromotingbcellproliferationviathee2f3dependentmechanism

Ejemplares similares