首页> 美国卫生研究院文献>PLoS Genetics >The hedgehog Pathway Gene shifted Functions together with the hmgcr-Dependent Isoprenoid Biosynthetic Pathway to Orchestrate Germ Cell Migration
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The hedgehog Pathway Gene shifted Functions together with the hmgcr-Dependent Isoprenoid Biosynthetic Pathway to Orchestrate Germ Cell Migration

机译:刺猬通路基因转移功能以及依赖hmgcr的类异戊二烯生物合成通路来协调生殖细胞迁移

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摘要

The Drosophila embryonic gonad is assembled from two distinct cell types, the Primordial Germ Cells (PGCs) and the Somatic Gonadal Precursor cells (SGPs). The PGCs form at the posterior of blastoderm stage embryos and are subsequently carried inside the embryo during gastrulation. To reach the SGPs, the PGCs must traverse the midgut wall and then migrate through the mesoderm. A combination of local repulsive cues and attractive signals emanating from the SGPs guide migration. We have investigated the role of the hedgehog (hh) pathway gene shifted (shf) in directing PGC migration. shf encodes a secreted protein that facilitates the long distance transmission of Hh through the proteoglycan matrix after it is released from basolateral membranes of Hh expressing cells in the wing imaginal disc. shf is expressed in the gonadal mesoderm, and loss- and gain-of-function experiments demonstrate that it is required for PGC migration. Previous studies have established that the hmgcr-dependent isoprenoid biosynthetic pathway plays a pivotal role in generating the PGC attractant both by the SGPs and by other tissues when hmgcr is ectopically expressed. We show that production of this PGC attractant depends upon shf as well as a second hh pathway gene gγ1. Further linking the PGC attractant to Hh, we present evidence indicating that ectopic expression of hmgcr in the nervous system promotes the release/transmission of the Hh ligand from these cells into and through the underlying mesodermal cell layer, where Hh can contact migrating PGCs. Finally, potentiation of Hh by hmgcr appears to depend upon cholesterol modification.
机译:果蝇胚胎性腺由两种不同的细胞类型组成,即原始生殖细胞(PGC)和体细胞性腺前体细胞(SGP)。 PGC在胚盘期胚胎的后部形成,随后在胃形成期间携带在胚胎内部。为了到达SGP,PGC必须穿过中肠壁,然后通过中胚层迁移。 SGP发出的局部排斥信号和吸引人的信号共同引导迁移。我们研究了刺猬(hh)途径基因转移(shf)在指导PGC迁移中的作用。 shf编码一种分泌的蛋白质,该蛋白质从机翼假体盘中表达Hh的细胞的基底外侧膜释放后,促进Hh通过蛋白聚糖基质的长距离传输。 shf在性腺中胚层中表达,功能丧失和功能获得实验证明它是PGC迁移所必需的。先前的研究已经确定,当异位表达hmgcr时,hmgcr依赖性类异戊二烯生物合成途径在SGP和其他组织产生PGC引诱剂中起关键作用。我们表明,这种PGC引诱剂的生产取决于shf以及第二个hh通路基因gγ1。进一步将PGC引诱剂与Hh联系起来,我们提供的证据表明hmgcr在神经系统中的异位表达促进了Hh配体从这些细胞进入/通过下面的中胚层细胞层的释放/传递,Hh可以与迁移的PGCs接触。最后,hmgcr对Hh的增强作用似乎取决于胆固醇的修饰。

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