Temporal induction of the homeodomain transcription factor Nkx2-1 is sufficient to respecify foregut and hindgut endoderm to a pulmonary fate in Xenopus laevis.

microPublication biology Pub Date : 2025-05-07 eCollection Date: 2025-01-01 DOI:10.17912/micropub.biology.001610

Brian A Hyatt, Erin Lundberg, Rachael Eye, Scott A Rankin, Aaron M Zorn

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Abstract

The ability of transcription factors (TFs) to regulate cell fate decisions is paramount in developmental, homeostatic, and pathogenic contexts. The homeodomain TF NKX2-1 is an essential and evolutionarily conserved master regulator of pulmonary fate in vertebrates. In this study, we tested the spatial-temporal ability of Xenopus and Human NKX2-1 to respecify foregut and hindgut endoderm in developing Xenopus laevis embryos into a pulmonary fate, as indicated by expression of pulmonary surfactant genes sftpc and sftpb . Interestingly, we find that both Human and Xenopus NKX2-1 can induce the ectopic expression of pulmonary surfactant genes in foregut and hindgut endoderm over a wide range of developmental times, as well as suppress the expression of midgut and hindgut specific genes. These results suggest a single pulmonary TF can reprogram developing endoderm and specify pulmonary fate. In addition, our work provides a comparative platform for future studies investigating how mutations in Human NKX2-1 may affect its transcriptional activity.

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在非洲爪蟾中，同源结构域转录因子Nkx2-1的时间诱导足以重新指定前肠和后肠内胚层的肺命运。

转录因子（TFs）调节细胞命运决定的能力在发育、体内平衡和致病环境中是至关重要的。同域TF NKX2-1是脊椎动物肺命运的重要且进化保守的主调控因子。在本研究中，我们通过肺表面活性物质基因sftpc和sftpb的表达，测试了爪蟾和人类NKX2-1在爪蟾胚胎发育成肺命运过程中重新指定前肠和后肠内胚层的时空能力。有趣的是，我们发现人类和非洲爪蟾NKX2-1均可诱导前肠和后肠内胚层肺表面活性物质基因的异位表达，并抑制中肠和后肠特异性基因的表达。这些结果表明，单个肺TF可以重编程发育中的内胚层并指定肺的命运。此外，我们的工作为未来研究人类NKX2-1突变如何影响其转录活性提供了一个比较平台。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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microPublication biology

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3 weeks