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Cellular retinoic acid-binding proteins are essential for hindbrain patterning and signal robustness in zebrafish

机译:细胞视黄酸结合蛋白对于斑马鱼的后脑模式和信号稳健性至关重要

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摘要

The vitamin A derivative retinoic acid (RA) is a morphogen that patterns the anterior-posterior axis of the vertebrate hindbrain. Cellular retinoic acid-binding proteins (Crabps) transport RA within cells to both its nuclear receptors (RARs) and degrading enzymes (Cyp26s). However, mice lacking Crabps are viable, suggesting that Crabp functions are redundant with those of other fatty acid-binding proteins. Here we show that Crabps in zebrafish are essential for posterior patterning of the hindbrain and that they provide a key feedback mechanism that makes signaling robust as they are able to compensate for changes in RA production. Of the four zebrafish Crabps, Crabp2a is uniquely RA inducible and depletion or overexpression of Crabp2a makes embryos hypersensitive to exogenous RA. Computational models confirm that Crabp2a improves robustness within a narrow concentration range that optimizes a ‘robustness index’, integrating spatial information along the RA morphogen gradient. Exploration of signaling parameters in our models suggests that the ability of Crabp2a to transport RA to Cyp26 enzymes for degradation is a major factor in promoting robustness. These results demonstrate a previously unrecognized requirement for Crabps in RA signaling and hindbrain development, as well as a novel mechanism for stabilizing morphogen gradients despite genetic or environmental fluctuations in morphogen availability.
机译:维生素A衍生物视黄酸(RA)是一种能使脊椎动物后脑的前后轴模式化的形态发生子。细胞视黄酸结合蛋白(Crabps)在细胞内将RA转运至其核受体(RAR)和降解酶(Cyp26s)。但是,缺少Crabps的小鼠是可行的,这表明Crabp功能与其他脂肪酸结合蛋白的功能是多余的。在这里,我们证明了斑马鱼的Crabps对于后脑的后部模式至关重要,并且它们提供了一种关键的反馈机制,该机制使信号强大,因为它们能够补偿RA产生的变化。在四种斑马鱼的Crabps中,Crapb2a独特地是RA诱导的,Crabp2a的耗竭或过度表达使胚胎对外源RA过敏。计算模型证实,Crabp2a可在狭窄的浓度范围内提高鲁棒性,从而优化“鲁棒性指数”,并沿RA形态发生子梯度整合空间信息。对我们模型中信号参数的探索表明,Crabp2a将RA转运至Cyp26酶进行降解的能力是促进鲁棒性的主要因素。这些结果表明,RA信号传导和后脑发育中对Crabps的需求以前未被认识,并且尽管形态发生素的遗传或环境存在波动,但该稳定形态形成素梯度的新机制仍然存在。

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