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Membrane-initiated actions of thyroid hormones on the male reproductive system.

机译:膜引发甲状腺激素对雄性生殖系统的作用。

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摘要

The presence of specific nuclear receptors to thyroid hormones, described in prepubertal Sertoli cells, implies the existence of an early and critical influence of these hormones on testis development. Although the mechanism of action thyroid hormones has been classically established as a genomic action regulating testis development, our research group has demonstrated that these hormones exert several effects in Sertoli cells lacking nuclear receptor activation. These findings led to the identification of non-classical thyroid hormone binding elements in the plasma membrane of testicular cells. Through binding to these sites, thyroid hormones could exert nongenomic effects, including those on ion fluxes at the plasma membrane, on signal transduction via kinase pathways, on amino acid accumulation, on modulation of extracellular nucleotide levels and on vimentin cytoskeleton. The evidence of the participation of different K(+), Ca(2+) and Cl(-) channels in the mechanism of action of thyroid hormones, characterizes the plasma membrane as an important microenvironment able to coordinate strategic signal transduction pathways in rat testis. The physiological responses of the Sertoli cells to hormones are dependent on continuous cross-talking of different signal transduction pathways. Apparently, the choice of the signaling pathways to be activated after the interaction of the hormone with cell surface binding sites is directly related to the physiological action to be accomplished. Yet, the enormous complexity of the nongenomic actions of thyroid hormones implies that different specific binding sites located on the plasma membrane or in the cytosol are believed to initiate specific cell responses.
机译:在Prepubertal sertoli细胞中描述的特定核受体对甲状腺激素的存在意味着这些激素对睾丸发育的早期和危重影响。虽然作用甲状腺激素的机制已被典型地确定作为调节睾丸发育的基因组作用,但我们的研究组已经证明,这些激素在缺乏核受体激活的Sertoli细胞中发挥了若干效果。这些发现导致睾丸细胞的质膜中的非古典甲状腺激素结合元素。通过与这些位点的结合,甲状腺激素可以施加Nongenomic效应,包括在质膜上的离子通量,通过激酶途径对氨基酸积聚的信号转导,对细胞外核苷酸水平和在平衡细胞骨架上的氨基酸积累。不同K(+),Ca(2+)和Cl( - )通道参与的证据表征甲状腺激素的作用机制,使质膜为一种重要的微环境,能够协调大鼠睾丸的战略信号转导途径。 Sertoli细胞对激素的生理反应依赖于不同信号转导途径的连续交叉谈话。显然,在激素与细胞表面结合位点的相互作用后待激活的信号通路的选择与要完成的生理作用直接相关。然而,甲状腺激素的Nongenomic作用的巨大复杂性意味着位于血浆膜或细胞溶溶胶上的不同特异性结合位点被认为引发特异性细胞反应。

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