Please use this identifier to cite or link to this item: https://doi.org/10.1038/s41598-020-80326-w
Title: Hypoxia-induced amniotic fluid stem cell secretome augments cardiomyocyte proliferation and enhances cardioprotective effects under hypoxic-ischemic conditions
Authors: Kukumberg, Marek 
Phermthai, Tatsanee
Wichitwiengrat, Suparat
Wang, Xiaoyuan 
Arjunan, Subramanian
Chong, Suet Yen 
Fong, Chui-Yee 
Wang, Jiong-Wei 
Rufaihah, Abdul Jalil 
Mattar, Citra Nurfarah Zaini 
Keywords: Science & Technology
Multidisciplinary Sciences
Science & Technology - Other Topics
Issue Date: 8-Jan-2021
Publisher: NATURE RESEARCH
Citation: Kukumberg, Marek, Phermthai, Tatsanee, Wichitwiengrat, Suparat, Wang, Xiaoyuan, Arjunan, Subramanian, Chong, Suet Yen, Fong, Chui-Yee, Wang, Jiong-Wei, Rufaihah, Abdul Jalil, Mattar, Citra Nurfarah Zaini (2021-01-08). Hypoxia-induced amniotic fluid stem cell secretome augments cardiomyocyte proliferation and enhances cardioprotective effects under hypoxic-ischemic conditions. SCIENTIFIC REPORTS 11 (1). ScholarBank@NUS Repository. https://doi.org/10.1038/s41598-020-80326-w
Abstract: Secretome derived from human amniotic fluid stem cells (AFSC-S) is rich in soluble bioactive factors (SBF) and offers untapped therapeutic potential for regenerative medicine while avoiding putative cell-related complications. Characterization and optimal generation of AFSC-S remains challenging. We hypothesized that modulation of oxygen conditions during AFSC-S generation enriches SBF and confers enhanced regenerative and cardioprotective effects on cardiovascular cells. We collected secretome at 6-hourly intervals up to 30 h following incubation of AFSC in normoxic (21%O2, nAFSC-S) and hypoxic (1%O2, hAFSC-S) conditions. Proliferation of human adult cardiomyocytes (hCM) and umbilical cord endothelial cells (HUVEC) incubated with nAFSC-S or hAFSC-S were examined following culture in normoxia or hypoxia. Lower AFSC counts and richer protein content in AFSC-S were observed in hypoxia. Characterization of AFSC-S by multiplex immunoassay showed higher concentrations of pro-angiogenic and anti-inflammatory SBF. hCM demonstrated highest proliferation with 30h-hAFSC-S in hypoxic culture. The cardioprotective potential of concentrated 30h-hAFSC-S treatment was demonstrated in a myocardial ischemia–reperfusion injury mouse model by infarct size and cell apoptosis reduction and cell proliferation increase when compared to saline treatment controls. Thus, we project that hypoxic-generated AFSC-S, with higher pro-angiogenic and anti-inflammatory SBF, can be harnessed and refined for tailored regenerative applications in ischemic cardiovascular disease.
Source Title: SCIENTIFIC REPORTS
URI: https://scholarbank.nus.edu.sg/handle/10635/207077
ISSN: 20452322
DOI: 10.1038/s41598-020-80326-w
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