Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors

Transplantation of dopaminergic (DA) neurons is considered to be the most promising therapeutic strategy for replacing degenerated dopamine cells in the midbrain of Parkinson’s disease (PD), thereby restoring normal neural circuit function and slow clinical progression of the disease. Human neural s...

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Main Authors: Hongna eYang, Jing eWang, Feng eWang, Xiaodun eLiu, Heng eChen, WeiMing eDuan, Tingyu eQu
Format: Article
Language:English
Published: Frontiers Media S.A. 2016-04-01
Series:Frontiers in Neural Circuits
Subjects:
Th
PRX
Online Access:http://journal.frontiersin.org/Journal/10.3389/fncir.2016.00029/full
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spelling doaj-d13c5dcfc5f447a784d03f3ec82d53b92020-11-24T20:59:23ZengFrontiers Media S.A.Frontiers in Neural Circuits1662-51102016-04-011010.3389/fncir.2016.00029162244Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factorsHongna eYang0Hongna eYang1Jing eWang2Feng eWang3Xiaodun eLiu4Heng eChen5WeiMing eDuan6Tingyu eQu7Qilu hospital of Shandong UniversityUniversity of Illinois at ChicagoQilu hospital of Shandong UniversityUniversity of Illinois at ChicagoR &amp; D, Cell and Tissue Bank of Shandong ProvinceR &amp; D, Cell and Tissue Bank of Shandong ProvinceCapital Medical UniversityUniversity of Illinois at ChicagoTransplantation of dopaminergic (DA) neurons is considered to be the most promising therapeutic strategy for replacing degenerated dopamine cells in the midbrain of Parkinson’s disease (PD), thereby restoring normal neural circuit function and slow clinical progression of the disease. Human neural stem cells (hNSCs) derived from fetal forebrain are thought to be the important cell sources for producing DA neurons because of their multipotency for differentiation and long-term expansion property in cultures. However, low DA differentiation of the forebrain-derived hNSCs limited their therapeutic potential in PD. In the current study, we explored a combined application of Pramipexole (PRX), bone morphogenetic proteins 7 (BMP-7), and growth factors, including acidic fibroblast factor (aFGF), forskolin, and phorbol-12-myristae-13-acetate (TPA), to induce differentiation of forebrain-derived hNSCs towards DA neurons in cultures. We found that DA neuron-associated genes, including Nurr1, Neurogenin2 (Ngn2), and tyrosine hydroxylase (TH) were significantly increased after 24h of differentiation by RT-PCR analysis (p<0.01). Fluorescent examination showed that about 25% of cells became TH-positive neurons at 24h, about 5% of cells became VMAT2 (vascular monoamine transporter 2)-positive neurons, and less than 5% of cells became DAT (dopamine transporter)-positive neurons at 72h following differentiation in cultures. Importantly, these TH-, VMAT2- and DAT-expressing neurons were able to release dopamine into cultures under both of the basal and evoked conditions. Dopamine levels released by DA neurons produced using our protocol were significantly higher compared to the control groups (P<0.01), as examined by ELISA. Our results demonstrated that the combination of PRX, BMP-7, and growth factors was able to greatly promote differentiation of the forebrain-derived hNSCs into DA-releasing neurons.http://journal.frontiersin.org/Journal/10.3389/fncir.2016.00029/fullThDopamine releaseBMP-7PRXdopamiergic neuronsforebrain-derived neural stem cells
collection DOAJ
language English
format Article
sources DOAJ
author Hongna eYang
Hongna eYang
Jing eWang
Feng eWang
Xiaodun eLiu
Heng eChen
WeiMing eDuan
Tingyu eQu
spellingShingle Hongna eYang
Hongna eYang
Jing eWang
Feng eWang
Xiaodun eLiu
Heng eChen
WeiMing eDuan
Tingyu eQu
Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors
Frontiers in Neural Circuits
Th
Dopamine release
BMP-7
PRX
dopamiergic neurons
forebrain-derived neural stem cells
author_facet Hongna eYang
Hongna eYang
Jing eWang
Feng eWang
Xiaodun eLiu
Heng eChen
WeiMing eDuan
Tingyu eQu
author_sort Hongna eYang
title Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors
title_short Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors
title_full Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors
title_fullStr Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors
title_full_unstemmed Dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of BMP-7 and pramipexole with growth factors
title_sort dopaminergic neuronal differentiation from the forebrain-derived human neural stem cells induced in cultures by using a combination of bmp-7 and pramipexole with growth factors
publisher Frontiers Media S.A.
series Frontiers in Neural Circuits
issn 1662-5110
publishDate 2016-04-01
description Transplantation of dopaminergic (DA) neurons is considered to be the most promising therapeutic strategy for replacing degenerated dopamine cells in the midbrain of Parkinson’s disease (PD), thereby restoring normal neural circuit function and slow clinical progression of the disease. Human neural stem cells (hNSCs) derived from fetal forebrain are thought to be the important cell sources for producing DA neurons because of their multipotency for differentiation and long-term expansion property in cultures. However, low DA differentiation of the forebrain-derived hNSCs limited their therapeutic potential in PD. In the current study, we explored a combined application of Pramipexole (PRX), bone morphogenetic proteins 7 (BMP-7), and growth factors, including acidic fibroblast factor (aFGF), forskolin, and phorbol-12-myristae-13-acetate (TPA), to induce differentiation of forebrain-derived hNSCs towards DA neurons in cultures. We found that DA neuron-associated genes, including Nurr1, Neurogenin2 (Ngn2), and tyrosine hydroxylase (TH) were significantly increased after 24h of differentiation by RT-PCR analysis (p<0.01). Fluorescent examination showed that about 25% of cells became TH-positive neurons at 24h, about 5% of cells became VMAT2 (vascular monoamine transporter 2)-positive neurons, and less than 5% of cells became DAT (dopamine transporter)-positive neurons at 72h following differentiation in cultures. Importantly, these TH-, VMAT2- and DAT-expressing neurons were able to release dopamine into cultures under both of the basal and evoked conditions. Dopamine levels released by DA neurons produced using our protocol were significantly higher compared to the control groups (P<0.01), as examined by ELISA. Our results demonstrated that the combination of PRX, BMP-7, and growth factors was able to greatly promote differentiation of the forebrain-derived hNSCs into DA-releasing neurons.
topic Th
Dopamine release
BMP-7
PRX
dopamiergic neurons
forebrain-derived neural stem cells
url http://journal.frontiersin.org/Journal/10.3389/fncir.2016.00029/full
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