Literature DB >> 16728723

Structural characterization and expression studies of Dby and its homologs in the mouse.

Queenie P Vong1, Yunmin Li, Yun-Fai Chris Lau, Martin Dym, Owen M Rennert, Wai-Yee Chan.   

Abstract

In spite of recent evidence showing the importance of DBY (DEAD-box RNA helicase Y) in spermatogenesis in human, the biologic role of its homolog Dby (also known as Ddx3y) in the mouse is less clear. The present study aims at characterizing the molecular structure of Dby and comparing its expression with its X- and autosome-linked homologs in embryonic gonads and developing germ cells in mice. Molecular cloning by rapid amplification of 3'-cDNA ends showed that the Dby gene in the mouse gives rise to 2 transcripts that differ only in the length of the 3'-untranslated region as a consequence of the use of alternative polyadenylation signals. Measurement by quantitative real-time polymerase chain reaction showed that both transcripts were ubiquitously expressed and were present in male germ cells and Sertoli cells. They were more abundant in type A spermatogonia compared with pachytene spermatocytes and round spermatids. Expression of Dby in the embryonic gonad increased from day 10.5 and reached a peak at day 17.5. The expression level of Dby decreased after birth and remained low in adult male gonads. Although the level of expression of Dby was much lower than its X chromosome homolog, Ddx3 (also known as Ddx3x) in all samples examined, the pattern of expression of the 2 genes was comparable. In contrast, their autosomal homolog, D1Pas1(also known as PL10), was predominantly expressed in pachytene spermatocytes and round spermatids. This result is in accord with meiotic sex chromosome inactivation in that Dby and Ddx are replaced in pachytene spermatocytes by their autosomal retroposon. These observations indicate that unlike DBY in humans, the role of Dby in spermatogenesis is less obvious in the mouse and its biologic activity may be replaced by that of Ddx3 and D1Pas1.

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Year:  2006        PMID: 16728723     DOI: 10.2164/jandrol.106.000471

Source DB:  PubMed          Journal:  J Androl        ISSN: 0196-3635


  13 in total

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2.  Induction of sperm impairments in mice as a sensitive biomarker of arsenic toxicity.

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3.  The role of Dby mRNA in early development of male mouse zygotes.

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Journal:  Asian J Androl       Date:  2010-06-14       Impact factor: 3.285

4.  The molecular evolution of PL10 homologs.

Authors:  Ti-Cheng Chang; Wan-Sheng Liu
Journal:  BMC Evol Biol       Date:  2010-05-03       Impact factor: 3.260

5.  Global survey of protein expression during gonadal sex determination in mice.

Authors:  Katherine Ewen; Mark Baker; Dagmar Wilhelm; R John Aitken; Peter Koopman
Journal:  Mol Cell Proteomics       Date:  2009-07-17       Impact factor: 5.911

6.  Developmental staging of male murine embryonic gonad by SAGE analysis.

Authors:  Tin-Lap Lee; Yunmin Li; Diana Alba; Queenie P Vong; Shao-Ming Wu; Vanessa Baxendale; Owen M Rennert; Yun-Fai Chris Lau; Wai-Yee Chan
Journal:  J Genet Genomics       Date:  2009-04       Impact factor: 4.275

7.  Complex transcriptional control of the AZFa gene DDX3Y in human testis.

Authors:  M-A Rauschendorf; J Zimmer; R Hanstein; C Dickemann; P H Vogt
Journal:  Int J Androl       Date:  2011-02

8.  Comparative Evolution of Duplicated Ddx3 Genes in Teleosts: Insights from Japanese Flounder, Paralichthys olivaceus.

Authors:  Zhongkai Wang; Wei Liu; Huayu Song; Huizhen Wang; Jinxiang Liu; Haitao Zhao; Xinxin Du; Quanqi Zhang
Journal:  G3 (Bethesda)       Date:  2015-06-24       Impact factor: 3.154

9.  DDX3X regulates cell survival and cell cycle during mouse early embryonic development.

Authors:  Qian Li; Pan Zhang; Chao Zhang; Ying Wang; Ru Wan; Ye Yang; Xuejiang Guo; Ran Huo; Min Lin; Zuomin Zhou; Jiahao Sha
Journal:  J Biomed Res       Date:  2014-03-03

Review 10.  DDX3, a potential target for cancer treatment.

Authors:  Guus Martinus Bol; Min Xie; Venu Raman
Journal:  Mol Cancer       Date:  2015-11-05       Impact factor: 27.401

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