首页> 外文期刊>Fish Physiology and Biochemistry >The C-terminal kinesin motor KIFC1 may participate in nuclear reshaping and flagellum formation during spermiogenesis of Larimichthys crocea
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The C-terminal kinesin motor KIFC1 may participate in nuclear reshaping and flagellum formation during spermiogenesis of Larimichthys crocea

机译:C型末端Kinesin Motor Kifc1可以在Larimichthys Crocea的精子发生期间参与核簧皮和鞭毛形成

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Spermatogenesis is a highly ordered process in the differentiation of male germ cells. Nuclear morphogenesis is one of the most fundamental cellular transformations to take place during spermatogenesis. These striking transformations from spermatogonia to spermatozoa are a result of phase-specific adaption of the cytoskeleton and its association with molecular motor proteins. KIFC1 is a C-terminal kinesin motor protein that plays an essential role in acrosome formation and nuclear reshaping during spermiogenesis in mammals. To explore its functions during the same process in Larimichthys crocea, we cloned and characterized the cDNA of a mammalian KIFC1 homolog (termed lc-KIFC1) from the total RNA of the testis. The 2481 bp complete lc-KIFC1 cDNA contained a 53 bp 5' untranslated region, a 535 bp 3' untranslated region, and a 1893 bp open reading frame that encoded a special protein of 630 amino acids. The predicted lc-KIFC1 protein possesses a divergent tail region, stalk region, and conserved carboxyl motor region. Protein alignment demonstrated that lc-KIFC1 had 73.2, 49.8, 49.3, 54.6, 56.5, 53.1, and 52.1% identity with its homologs in Danio rerio, Eriocheir sinensis, Octopus tankahkeei, Gallus gallus, Xenopus laevis, Mus musculus, and Homo sapiens, respectively. Tissue expression analysis revealed that lc-kifc1 mRNA was mainly expressed in the testis. The trend of lc-kifc1 mRNA expression at different growth stages of the testis showed that the expression increased first and then decreased, in the stage IV of testis, its expression quantity achieved the highest level. In situ hybridization and immunofluorescence results showed that KIFC1 was localized around the nucleus in early spermatids. As spermatid development progressed, the signals increased substantially. These signals peaked and were concentrated at one end of the nucleus when the spermatids began to undergo dramatic changes. In the mature sperm, the signal for KIFC1 gradually became weak and was mainly localized in the tail. In summary, evaluation of the expression pattern for lc-KIFC1 at specific stages of spermiogenesis has shed light on the potential functions of this motor protein in major cytological transformations. In addition, this study may provide a model for researching the molecular mechanisms involved in spermatogenesis in other teleost species, which will lead to a better understanding of the teleost fertilization process.
机译:精子发生是雄性生殖细胞分化中的高度有序的过程。核形态发生是在精子发生期间发生的最基本的细胞转化之一。这些从精子转化到精子上的转化是细胞骨架的相相适应和其与分子运动蛋白的关系。 KIFC1是一种C末端Kinesin Motor蛋白,其在哺乳动物中的精子发生过程中起着基本作用和核重塑。为了探讨其在Larimichthys Crocea同一过程中的功能,我们克隆并表征了哺乳动物KIFC1同源物(称为LC-KIFC1)的cDNA,从睾丸的总RNA中探讨。 2481bp完全Lc-kifc1 cDNA含有53bp 5'未翻译区域,535bp 3'未翻译区域,1893bp开放读数框架,其编码了630个氨基酸的特殊蛋白质。预测的LC-KIFC1蛋白具有发散的尾部区域,茎区域和保守的羧基电机区。蛋白质对准表明,LC-KIFC1具有73.2,49.8,49.3,54.6,56.5,53.1和52.1%在Danio Rerio,Eriocheir Sinensis,八达通坦克,血小板,Xenopus Laevis,Mus Musculus和Homo Sapiens和Homo Sapiens和Homo Sapiens和Homo Sapiens和Homo Sapiens和Homo Sapiens和Homo Sapiens和Homo Sapiens的同源物中的73.2,49.8,49.3,54.6,56.5,53.1和52.1%的同一性。分别。组织表达分析显示LC-KIFC1 mRNA主要在睾丸中表达。睾丸不同生长阶段的LC-KIFC1 mRNA表达的趋势表明,在睾丸阶段IV中,表达首先增加,然后在睾丸阶段达到最高水平。原位杂交和免疫荧光结果表明,KIFC1在早期精子中围绕细胞核定位。随着精菌的发展进展,信号大大增加。当精子开始发生巨大变化时,这些信号达到峰值并且在核的一端浓缩。在成熟精子中,KIFC1的信号逐渐变得薄弱,主要是尾部的局部化。总之,在精子发生特定阶段的LC-KIFC1的表达模式的评价已经对该机动蛋白的主要细胞学转化的潜在功能进行了脱光。此外,该研究可以提供研究在其他紧邻物种中的精子发生的分子机制的模型,这将导致更好地了解Textost受精过程。

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