Multiplexed PLGA scaffolds with nitric oxide-releasing zinc oxide and melatonin-modulated extracellular vesicles for severe chronic kidney disease

Author:

Han* Dong Keun1ORCID,Rhim Won-Kyu1,Woo Jiwon1,Kim Jun Yong1ORCID,Lee Eun Hye2,Cha Seung-Gyu1,Kim Da-Seul1,Baek Seung-Woon1,Park Chun Gwon3,Kim Bum Soo2,Kwon Tae Gyun2

Affiliation:

1. CHA University

2. Kyungpook National University

3. Sungkyunkwan University

Abstract

Abstract With prevalence of chronic kidney disease (CKD) in worldwide, the strategies to recover renal function via tissue regeneration could provide alternatives to kidney replacement therapies. However, due to relatively low reproducibility of renal basal cells and limited bioactivities of implanted biomaterials along with the high probability of substance-inducible inflammation and immunogenicity, kidney tissue regeneration could be challenging. To exclude various side effects from cell transplantations, in this study, we have designed cell-free hybrid PMEZ scaffolds incorporating essential bioactive components, such as ricinoleic acid grafted Mg(OH)2 (M), extracellular matrix (E), and alpha lipoic acid-conjugated ZnO (Z) based on biodegradable porous PLGA (P) platform. Consecutively, for functional improvements, melatonin-modulated extracellular vesicles (mEVs), derived from the human umbilical cord MSCs in chemically defined media without serum impurities, were also attached onto PMEZ scaffolds to construct the multiplexed PMEZ/mEV scaffold. The continuous nitric oxide-releasing property of modified ZnO and remarkably upregulated regenerative functionalities of mEVs showed significantly enhanced kidney regenerative activities. Based on these, the structural and functional restoration has been practically achieved in 5/6 nephrectomy mouse models that mimicked severe human CKD. Our innovative implantations aim at kidney tissue recovery with functional restoration and could be a promising therapeutic alternative for CKD treatment.

Publisher

Research Square Platform LLC

Reference71 articles.

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