Batchelder Cynthia A, Lee C Chang I, Matsell Douglas G, Yoder Mervin C, Tarantal Alice F
Center of Excellence in Translational Human Stem Cell Research, University of California, Davis, CA, USA.
Differentiation. 2009 Jul;78(1):45-56. doi: 10.1016/j.diff.2009.05.001. Epub 2009 Jun 4.
The development of the metanephric kidney was studied immunohistochemically across gestation in monkeys to identify markers of cell specification, and to aid in developing experimental paradigms for renal precursor differentiation from human embryonic stem cells (hESC). PAX2, an important kidney developmental marker, was expressed at the tips of the ureteric bud, in the surrounding condensing mesenchyme, and in the renal vesicle. Vimentin, a mesenchymal and renal marker, was strongly expressed in the metanephric blastema then found to be limited to the glomerulus and interstitial cells of the medulla and cortex. A model of gene expression based on human and nonhuman primate renal ontogeny was developed and incorporated into studies of hESC differentiation. Spontaneous hESC differentiation revealed markers of metanephric mesenchyme (OSR1, PAX2, SIX2, WT1) that increased over time, followed by upregulation of kidney precursor markers (EYA1, LIM1, CD24). Directed hESC differentiation was also evaluated with the addition of retinoic acid, Activin-A, and BMP-4 or BMP-7, and using different culture substrate conditions. Of the culture substrates studied, gelatin most closely recapitulated the anticipated directed developmental pattern of renal gene expression. No differences were found when BMP-4 and BMP-7 were compared with baseline conditions. PAX2 and Vimentin immunoreactivity in differentiating hESC was also similar to the renal precursor patterns reported for human fetal kidneys and findings described in rhesus monkeys. The results of these studies are as follows: (1) provide additional data to support that rhesus monkey kidney development parallels that of humans, and (2) provide a useful model for hESC directed differentiation towards renal precursors.
通过免疫组织化学方法,对猴子整个妊娠期的后肾发育进行了研究,以确定细胞特化的标志物,并辅助开发从人胚胎干细胞(hESC)分化出肾前体细胞的实验范式。PAX2是一种重要的肾脏发育标志物,在输尿管芽的尖端、周围凝聚的间充质以及肾小泡中表达。波形蛋白是一种间充质和肾脏标志物,在后肾胚基中强烈表达,随后局限于髓质和皮质的肾小球及间质细胞。基于人类和非人类灵长类动物肾脏个体发育的基因表达模型得以建立,并纳入hESC分化研究中。hESC的自发分化显示出后肾间充质的标志物(OSR1、PAX2、SIX2、WT1)随时间增加,随后肾前体细胞标志物(EYA1、LIM1、CD24)上调。还通过添加视黄酸、激活素-A以及骨形态发生蛋白-4(BMP-4)或骨形态发生蛋白-7(BMP-7)并使用不同的培养底物条件,对hESC的定向分化进行了评估。在所研究的培养底物中,明胶最能重现预期的肾脏基因表达定向发育模式。将BMP-4和BMP-7与基线条件进行比较时未发现差异。分化中的hESC中PAX2和波形蛋白的免疫反应性也类似于人类胎儿肾脏报道的肾前体细胞模式以及恒河猴中描述的结果。这些研究的结果如下:(1)提供了额外的数据支持恒河猴肾脏发育与人类相似,以及(2)为hESC定向分化为肾前体细胞提供了一个有用的模型。