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Sox2-CreER mice are useful for fate mapping of mature but not neonatal cochlear supporting cells in hair cell regeneration studies

机译:Sox2-CreER小鼠可用于毛细胞再生研究中成熟的而非新生儿的人工耳蜗支持细胞的命运定位

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摘要

Studies of hair cell regeneration in the postnatal cochlea rely on fate mapping of supporting cells. Here we characterized a Sox2-CreER knock-in mouse line with two independent reporter mouse strains at neonatal and mature ages. Regardless of induction age, reporter expression was robust, with CreER activity being readily detectable in >85% of supporting cells within the organ of Corti. When induced at postnatal day (P) 28, Sox2-CreER activity was exclusive to supporting cells demonstrating its utility for fate mapping studies beyond this age. However, when induced at P1, Sox2-CreER activity was also detected in >50% of cochlear hair cells, suggesting that Sox2-CreER may not be useful to fate map a supporting cell origin of regenerated hair cells if induced at neonatal ages. Given that this model is currently in use by several investigators for fate mapping purposes, and may be adopted by others in the future, our finding that current protocols are effective for restricting CreER activity to supporting cells at mature but not neonatal ages is both significant and timely.
机译:产后耳蜗中毛细胞再生的研究依赖于支持细胞的命运定位。在这里我们表征了Sox2-CreER敲入小鼠品系,具有两个独立的新生鼠和成年鼠。无论诱导年龄如何,报告基因的表达都非常强健,在Corti器官中的> 85%的支持细胞中都容易检测到CreER活性。当在出生后第28天被诱导时,Sox2-CreER活性是支持细胞所独有的,这证明了其在该年龄以后的命运作图研究中的效用。但是,当在P1诱导时,在超过50%的耳蜗毛细胞中也检测到了Sox2-CreER活性,这表明Sox2-CreER如果在新生年龄被诱导,可能对确定新生毛细胞的支持细胞来源可能无效。鉴于该模型目前已被几位研究者用于命运作图目的,并且将来可能会被其他人采用,因此我们发现,当前的协议有效地限制了CreER活性以支持成熟而不是新生儿的细胞,这一发现意义重大,而且及时。

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