NDLI: Adenovirus-mediated hypoxia-inducible factor 1α double-mutant promotes differentiation of bone marrow stem cells to cardiomyocytes

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Adenovirus-mediated hypoxia-inducible factor 1α double-mutant promotes differentiation of bone marrow stem cells to cardiomyocytes

Content Provider	Semantic Scholar
Author	Wang, Yesong Feng, Chong Xue, Jiaojie Sun, Aijiao Wu, Juekan
Copyright Year	2009
Abstract	The hypoxia-inducible factor 1α (HIF-1α) regulates transcriptional genes involved in cell proliferation, survival, and differentiation. Under normoxia, HIF-1α has a short half-life (t½ ≈ 5 min) and low transcriptional activity. An HIF-1α mutant, produced by substitution of alanine (Ala) for proline (Pro) at position 564 and asparagine (Asp) at position 803, can prevent HIF-1α hydroxylation and results in a highly active form of HIF-1α (HIF-1α-Ala564-Ala803). We hypothesized that adenovirus (Ad)-mediated transfer of the active form of HIF-1α (pAd-HIF-1α-Ala564-Ala803) could effectively occur in bone marrow stem cells (MSCs) and promote MSC differentiation under normoxia. PCR-based site-specific mutagenesis was used to construct the Ad vector expressing HIF-1α-Ala564-Ala803. RT-PCR and immunostaining were used to study whether pAd-HIF-1α-Ala564-Ala803 affected MSC differentiation to cardiomyocyte (CMC). pAd-HIF-1α-Ala564-Ala803 exhibited higher transcriptional activity and stable HIF-1α protein expression. Under normoxia, an MSC–CMC co-culture treated with pAd-HIF1a-Ala564-Ala803 augmented TGF-β1, Smad4, NKx2.5, and GATA4 expression. Higher expression of cTnT and α-actinin was observed by immunostaining in MSCs, compared with the control and contrast groups. Adenovirus-mediated hypoxia-inducible factor 1α double-mutant, pAd-HIF-1α-Ala564-Ala803, can stably express HIF-1α and promote its downstream genes and MSC differentiation to CMC in the MSC–CMC co-culture system under normoxia.
Starting Page	413
Ending Page	420
Page Count	8
File Format	PDF HTM / HTML
DOI	10.1007/s12576-009-0050-x
PubMed reference number	19603255
Journal	Medline
Volume Number	59
Alternate Webpage(s)	https://jps.biomedcentral.com/track/pdf/10.1007/s12576-009-0050-x
Alternate Webpage(s)	https://doi.org/10.1007/s12576-009-0050-x
Journal	The Journal of Physiological Sciences
Language	English
Access Restriction	Open
Content Type	Text
Resource Type	Article

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