Li Xiao-Jun, Morgan Charles, Nadar-Ponniah Prathamesh T, Kolanus Waldemar, Doetzlhofer Angelika
bioRxiv. 2023 Jan 13:2023.01.12.523802. doi: 10.1101/2023.01.12.523802.
Cochlear hair cell loss is a leading cause of deafness in humans. Neighboring supporting cells have some capacity to regenerate hair cells. However, their regenerative potential sharply declines as supporting cells undergo maturation (postnatal day 5 in mice). We recently reported that reactivation of the RNA-binding protein LIN28B restores the hair cell-regenerative potential of P5 cochlear supporting cells. Here, we identify the LIN28B target as a novel and equally potent enhancer of supporting cell plasticity. TRIM71 is a critical regulator of stem cell behavior and cell reprogramming, however, its role in cell regeneration is poorly understood. Employing an organoid-based assay, we show that TRIM71 reactivation increases the mitotic and hair cell-forming potential of P5 cochlear supporting cells by facilitating their de-differentiation into progenitor-like cells. Our mechanistic work indicates that TRIM71’s RNA-binding activity is essential for such ability, and our transcriptomic analysis identifies gene modules that are linked to TRIM71 and LIN28B-mediated supporting cell reprogramming. Furthermore, our study uncovers that the TRIM71-LIN28B target is essential for supporting cell self-renewal and hair cell formation.
耳蜗毛细胞丢失是人类耳聋的主要原因。相邻的支持细胞具有一定的毛细胞再生能力。然而,随着支持细胞成熟(小鼠出生后第5天),它们的再生潜力急剧下降。我们最近报道,RNA结合蛋白LIN28B的重新激活可恢复P5耳蜗支持细胞的毛细胞再生潜力。在此,我们确定LIN28B的靶标是支持细胞可塑性的一种新型且同样有效的增强子。TRIM71是干细胞行为和细胞重编程的关键调节因子,然而,其在细胞再生中的作用尚不清楚。利用基于类器官的检测方法,我们发现TRIM71的重新激活通过促进P5耳蜗支持细胞去分化为祖细胞样细胞,增加了其有丝分裂和毛细胞形成潜力。我们的机制研究表明,TRIM71的RNA结合活性对于这种能力至关重要,我们的转录组分析确定了与TRIM71和LIN28B介导的支持细胞重编程相关的基因模块。此外,我们的研究发现TRIM71-LIN28B靶标对于支持细胞自我更新和毛细胞形成至关重要。
