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首页> 外文期刊>Developmental genetics >Screening mosaic F1 females for mutations affecting zebrafish heartinduction and patterning
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Screening mosaic F1 females for mutations affecting zebrafish heartinduction and patterning

机译:筛选镶嵌F1雌性以寻找影响斑马鱼心脏诱导和模式的突变

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摘要

The genetic pathways underlying the induction and anterior-posterior patterning of the heart are poorly understood. The recent emergence of the zebrafish model system now allows a classical genetic approach to such challenging problems in vertebrate development. Two large-scale screens for mutations affecting zebrafish embryonic development have recently been completed; among the hundreds of mutations identified were several that affect specific aspects of cardiac morphogenesis, differentiation, and function. However, very few mutations affecting induction and/or anterior-posterior patterning of the heart were identified. We hypothesize that a directed approach utilizing molecular markers to examine these particular steps of heart development will uncover additional such mutations. To test this hypothesis, we are conducting two parallel screens for mutations that affect either the induction or the anterior-posterior patterning of the zebrafish heart. As an indicator of cardiac induction, we examine expression of nkx2.5, the earliest known marker of precardiac mesoderm; to assess anterior-posterior patterning, we distinguish ventricle from atrium with antibodies that recognize different myosin heavy chain isoforms. in order to expedite the examination of a large number of mutations, we are screening the haploid progeny of mosaic Fl females, in these ongoing screens, we have identified four mutations that effect nkx2.5 expression as well as 21 that disrupt either ventricular or atrial development and thus far have recovered several of these mutations, demonstrating the value of our approach. Future analysis of thee and other cardiac mutations will provide further insight into the processes of induction and anterior-posterior patterning of the heart.
机译:心脏的诱导和前后模式的遗传途径知之甚少。斑马鱼模型系统的最新出现现在为解决脊椎动物发育中的此类难题提供了经典的遗传方法。最近完成了两个大型的影响斑马鱼胚胎发育突变的筛选。在确定的数百种突变中,有几种会影响心脏形态发生,分化和功能的特定方面。但是,几乎没有发现影响心脏诱导和/或前后模式的突变。我们假设使用分子标记物检查心脏发育的这些特定步骤的直接方法将发现其他此类突变。为了检验该假设,我们正在对影响斑马鱼心脏诱导或前后模式的突变进行两个平行筛选。作为心脏诱导的指标,我们研究了心前中胚层最早的已知标志物nkx2.5的表达。为了评估前后模式,我们使用识别不同肌球蛋白重链同工型的抗体将心室与心房区分开。为了加快对大量突变的检查,我们正在筛选镶嵌Fl雌性的单倍体后代,在这些正在进行的筛选中,我们确定了影响nkx2.5表达的四个突变以及破坏心室或心房的21个突变。的发展,到目前为止已经恢复了其中的一些突变,证明了我们方法的价值。您和其他心脏突变的未来分析将提供对心脏诱导和前后模式的过程的进一步了解。

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