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Hoxa-1 3'视黄酸反应元件(3'RARE)的体内功能分析

In vivo functional analysis of the Hoxa-1 3' retinoic acid response element (3'RARE).

作者信息

Dupé V, Davenne M, Brocard J, Dollé P, Mark M, Dierich A, Chambon P, Rijli F M

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, CNRS/INSERM/ULP, Collège de France, Illkirch, CU de Strasbourg, France.

出版信息

Development. 1997 Jan;124(2):399-410. doi: 10.1242/dev.124.2.399.

Abstract

Retinoids are essential for normal development and both deficiency and excess of retinoic acid (RA) are teratogenic. Retinoic acid response elements (RAREs) have been identified in Hox gene promoters suggesting that endogenous retinoids may be involved in the direct control of Hox gene patterning functions. In order to test this hypothesis, we have mutated the Hoxa-1 3'RARE using the Cre-loxP targeting strategy, and studied its functional role during mouse development. We find that this enhancer plays an important role in the early establishment of the Hoxa-1 anterior expression boundary in the neural plate. This early disturbance in Hoxa-1 activation results in rhombomere and cranial nerve abnormalities reminiscent of those obtained in the Hoxa-1 total knockout, although their severity and penetrance are lower, thus providing strong evidence for direct control of Hox gene function by retinoids during normal development. Interestingly, we also find that the Hoxa-1 expression response to RA treatment is not entirely controlled by the RARE, suggesting the existence of other retinoid-induced factors mediating the Hoxa-1 response to RA and/or the presence of additional RAREs. Interestingly, although the RARE is not required for the spatiotemporal control of colinear expression of the Hoxa genes, it is absolutely required for correct Hoxa-2 expression in rhombomere 5.

摘要

维甲酸对于正常发育至关重要,维甲酸(RA)缺乏和过量均具有致畸性。在Hox基因启动子中已鉴定出维甲酸反应元件(RAREs),这表明内源性维甲酸可能参与Hox基因模式形成功能的直接调控。为了验证这一假设,我们使用Cre-loxP靶向策略对Hoxa-1 3'RARE进行了突变,并研究了其在小鼠发育过程中的功能作用。我们发现该增强子在神经板中Hoxa-1前部表达边界的早期建立中起重要作用。Hoxa-1激活的这种早期干扰导致节段和颅神经异常,这让人联想到在Hoxa-1完全敲除小鼠中观察到的异常,尽管其严重程度和发生率较低,从而为正常发育过程中维甲酸对Hox基因功能的直接调控提供了有力证据。有趣的是,我们还发现Hoxa-1对RA处理的表达反应并不完全受RARE控制,这表明存在其他维甲酸诱导因子介导Hoxa-1对RA的反应和/或存在额外的RAREs。有趣的是,尽管RARE对于Hoxa基因共线性表达的时空控制并非必需,但它对于菱形节5中Hoxa-2的正确表达绝对是必需的。

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