Functional reservoir microcapsules generated via microfluidic fabrication for long-term cardiovascular therapeutics

Ngoc-Duy Dinh; Marek Kukumberg; Anh-Tuan Nguyen; Hamed Keramati; Song Guo; Dinh-Tuan Phan; Nurdiyana B. Ja'Afar; Erik Birgersson; Hwa Liang Leo; Ruby Yun-Ju Huang; Theodoros Kofidis; Abdul Jalil Rufaihah; Chia-Hung Chen

doi:10.1039/d0lc00296h

Functional reservoir microcapsules generated via microfluidic fabrication for long-term cardiovascular therapeutics

Ngoc-Duy Dinh
, Marek Kukumberg
, Anh-Tuan Nguyen
, Hamed Keramati
, Song Guo
, Dinh-Tuan Phan
, Nurdiyana B. Ja'Afar
, Erik Birgersson
, Hwa Liang Leo
, Ruby Yun-Ju Huang
, Theodoros Kofidis
, Abdul Jalil Rufaihah
, Chia-Hung Chen^*

^*Corresponding author for this work

Department of Biomedical Engineering

Research output: Journal Publications and Reviews › RGC 21 - Publication in refereed journal › peer-review

38 Citations (Scopus)

Abstract

Cardiovascular disease is a chronic disease that leads to impaired cardiac function and requires long-term management to control its progression. Despite the importance of hydrogels for therapeutic applications, a contradiction between the size of a hydrogel and the amount of loaded drug has been encountered when using conventional fabrication methods. In this study, biocompatible reservoir microcapsules (diameter ∼100 μm) with a large liquid core and polymeric shell were fabricated via a one-step phase separation of poly(ethylene glycol)diacrylate (PEGDA) and dextran within pre-gel droplets through microfluidics. By controlling the process of phase separation, high drug-loading efficiency (∼80%) for long-term release (30 days) of vascular endothelial growth factor (VEGF) and platelet-derived growth factor (PDGF) was achieved. Drug molecules were dispersed within the liquid core at a concentration above saturation solubility for sustained delivery via regulation of the shells. Effective therapeutic enhancement of human umbilical vein endothelial cell (HUVEC) and umbilical artery smooth muscle cell (SMC) proliferation and tube formation in vitro promoted rapid cell proliferation and increased the number of migrated cells by ∼1.7 times. Moreover, in vivo blood vessel regeneration for cardiovascular control induced by sustained dual-drug (VEGF and PDGF) delivery to the rat heart was achieved, showing the effectiveness of long-term protein delivery in improving cardiac function and significantly reducing ventricular wall thickness and fibrosis of the infarct region. The ratio of heart tissue scarring was reduced to 11.2% after microcapsule treatment compared with 21.4% after saline treatment in the rat model. By using these reservoir microcapsules, similar sustained delivery of proteins, mRNAs and biologic drugs could be developed for the treatment of a range of long-term chronic diseases and regenerative medicine.

Original language	English
Pages (from-to)	2756-2764
Journal	Lab on a Chip
Volume	20
Issue number	15
Online published	26 Jun 2020
DOIs	https://doi.org/10.1039/d0lc00296h
Publication status	Published - 7 Aug 2020

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Research Keywords

ENDOTHELIAL GROWTH-FACTOR
AQUEOUS 2-PHASE SYSTEMS
SIMULTANEOUS ENCAPSULATION
MOLECULAR-MECHANISMS
DELIVERY
VEGF
ANGIOGENESIS
HYDROGELS
CARRIERS

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10.1039/d0lc00296h

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Dinh, N.-D., Kukumberg, M., Nguyen, A.-T., Keramati, H., Guo, S., Phan, D.-T., Ja'Afar, N. B., Birgersson, E., Leo, H. L., Huang, R. Y.-J., Kofidis, T., Rufaihah, A. J., & Chen, C.-H. (2020). Functional reservoir microcapsules generated via microfluidic fabrication for long-term cardiovascular therapeutics. Lab on a Chip, 20(15), 2756-2764. https://doi.org/10.1039/d0lc00296h

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title = "Functional reservoir microcapsules generated via microfluidic fabrication for long-term cardiovascular therapeutics",

abstract = "Cardiovascular disease is a chronic disease that leads to impaired cardiac function and requires long-term management to control its progression. Despite the importance of hydrogels for therapeutic applications, a contradiction between the size of a hydrogel and the amount of loaded drug has been encountered when using conventional fabrication methods. In this study, biocompatible reservoir microcapsules (diameter ∼100 μm) with a large liquid core and polymeric shell were fabricated via a one-step phase separation of poly(ethylene glycol)diacrylate (PEGDA) and dextran within pre-gel droplets through microfluidics. By controlling the process of phase separation, high drug-loading efficiency (∼80\%) for long-term release (30 days) of vascular endothelial growth factor (VEGF) and platelet-derived growth factor (PDGF) was achieved. Drug molecules were dispersed within the liquid core at a concentration above saturation solubility for sustained delivery via regulation of the shells. Effective therapeutic enhancement of human umbilical vein endothelial cell (HUVEC) and umbilical artery smooth muscle cell (SMC) proliferation and tube formation in vitro promoted rapid cell proliferation and increased the number of migrated cells by ∼1.7 times. Moreover, in vivo blood vessel regeneration for cardiovascular control induced by sustained dual-drug (VEGF and PDGF) delivery to the rat heart was achieved, showing the effectiveness of long-term protein delivery in improving cardiac function and significantly reducing ventricular wall thickness and fibrosis of the infarct region. The ratio of heart tissue scarring was reduced to 11.2\% after microcapsule treatment compared with 21.4\% after saline treatment in the rat model. By using these reservoir microcapsules, similar sustained delivery of proteins, mRNAs and biologic drugs could be developed for the treatment of a range of long-term chronic diseases and regenerative medicine.",

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author = "Ngoc-Duy Dinh and Marek Kukumberg and Anh-Tuan Nguyen and Hamed Keramati and Song Guo and Dinh-Tuan Phan and Ja'Afar, \{Nurdiyana B.\} and Erik Birgersson and Leo, \{Hwa Liang\} and Huang, \{Ruby Yun-Ju\} and Theodoros Kofidis and Rufaihah, \{Abdul Jalil\} and Chia-Hung Chen",

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doi = "10.1039/d0lc00296h",

language = "English",

volume = "20",

pages = "2756--2764",

journal = "Lab on a Chip",

issn = "1473-0197",

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TY - JOUR

T1 - Functional reservoir microcapsules generated via microfluidic fabrication for long-term cardiovascular therapeutics

AU - Dinh, Ngoc-Duy

AU - Kukumberg, Marek

AU - Nguyen, Anh-Tuan

AU - Keramati, Hamed

AU - Guo, Song

AU - Phan, Dinh-Tuan

AU - Ja'Afar, Nurdiyana B.

AU - Birgersson, Erik

AU - Leo, Hwa Liang

AU - Huang, Ruby Yun-Ju

AU - Kofidis, Theodoros

AU - Rufaihah, Abdul Jalil

AU - Chen, Chia-Hung

PY - 2020/8/7

Y1 - 2020/8/7

N2 - Cardiovascular disease is a chronic disease that leads to impaired cardiac function and requires long-term management to control its progression. Despite the importance of hydrogels for therapeutic applications, a contradiction between the size of a hydrogel and the amount of loaded drug has been encountered when using conventional fabrication methods. In this study, biocompatible reservoir microcapsules (diameter ∼100 μm) with a large liquid core and polymeric shell were fabricated via a one-step phase separation of poly(ethylene glycol)diacrylate (PEGDA) and dextran within pre-gel droplets through microfluidics. By controlling the process of phase separation, high drug-loading efficiency (∼80%) for long-term release (30 days) of vascular endothelial growth factor (VEGF) and platelet-derived growth factor (PDGF) was achieved. Drug molecules were dispersed within the liquid core at a concentration above saturation solubility for sustained delivery via regulation of the shells. Effective therapeutic enhancement of human umbilical vein endothelial cell (HUVEC) and umbilical artery smooth muscle cell (SMC) proliferation and tube formation in vitro promoted rapid cell proliferation and increased the number of migrated cells by ∼1.7 times. Moreover, in vivo blood vessel regeneration for cardiovascular control induced by sustained dual-drug (VEGF and PDGF) delivery to the rat heart was achieved, showing the effectiveness of long-term protein delivery in improving cardiac function and significantly reducing ventricular wall thickness and fibrosis of the infarct region. The ratio of heart tissue scarring was reduced to 11.2% after microcapsule treatment compared with 21.4% after saline treatment in the rat model. By using these reservoir microcapsules, similar sustained delivery of proteins, mRNAs and biologic drugs could be developed for the treatment of a range of long-term chronic diseases and regenerative medicine.

AB - Cardiovascular disease is a chronic disease that leads to impaired cardiac function and requires long-term management to control its progression. Despite the importance of hydrogels for therapeutic applications, a contradiction between the size of a hydrogel and the amount of loaded drug has been encountered when using conventional fabrication methods. In this study, biocompatible reservoir microcapsules (diameter ∼100 μm) with a large liquid core and polymeric shell were fabricated via a one-step phase separation of poly(ethylene glycol)diacrylate (PEGDA) and dextran within pre-gel droplets through microfluidics. By controlling the process of phase separation, high drug-loading efficiency (∼80%) for long-term release (30 days) of vascular endothelial growth factor (VEGF) and platelet-derived growth factor (PDGF) was achieved. Drug molecules were dispersed within the liquid core at a concentration above saturation solubility for sustained delivery via regulation of the shells. Effective therapeutic enhancement of human umbilical vein endothelial cell (HUVEC) and umbilical artery smooth muscle cell (SMC) proliferation and tube formation in vitro promoted rapid cell proliferation and increased the number of migrated cells by ∼1.7 times. Moreover, in vivo blood vessel regeneration for cardiovascular control induced by sustained dual-drug (VEGF and PDGF) delivery to the rat heart was achieved, showing the effectiveness of long-term protein delivery in improving cardiac function and significantly reducing ventricular wall thickness and fibrosis of the infarct region. The ratio of heart tissue scarring was reduced to 11.2% after microcapsule treatment compared with 21.4% after saline treatment in the rat model. By using these reservoir microcapsules, similar sustained delivery of proteins, mRNAs and biologic drugs could be developed for the treatment of a range of long-term chronic diseases and regenerative medicine.

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KW - AQUEOUS 2-PHASE SYSTEMS

KW - SIMULTANEOUS ENCAPSULATION

KW - MOLECULAR-MECHANISMS

KW - DELIVERY

KW - VEGF

KW - ANGIOGENESIS

KW - HYDROGELS

KW - CARRIERS

KW - ENDOTHELIAL GROWTH-FACTOR

KW - AQUEOUS 2-PHASE SYSTEMS

KW - SIMULTANEOUS ENCAPSULATION

KW - MOLECULAR-MECHANISMS

KW - DELIVERY

KW - VEGF

KW - ANGIOGENESIS

KW - HYDROGELS

KW - CARRIERS

KW - ENDOTHELIAL GROWTH-FACTOR

KW - AQUEOUS 2-PHASE SYSTEMS

KW - SIMULTANEOUS ENCAPSULATION

KW - MOLECULAR-MECHANISMS

KW - DELIVERY

KW - VEGF

KW - ANGIOGENESIS

KW - HYDROGELS

KW - CARRIERS

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U2 - 10.1039/d0lc00296h

DO - 10.1039/d0lc00296h

M3 - RGC 21 - Publication in refereed journal

C2 - 32609786

SN - 1473-0197

VL - 20

SP - 2756

EP - 2764

JO - Lab on a Chip

JF - Lab on a Chip

IS - 15

ER -

Functional reservoir microcapsules generated via microfluidic fabrication for long-term cardiovascular therapeutics

Abstract

UN SDGs

Research Keywords

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