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小鼠Yq上的缺失导致精子细胞中多个X和Y连锁转录本的上调。

Deletions on mouse Yq lead to upregulation of multiple X- and Y-linked transcripts in spermatids.

作者信息

Ellis Peter J I, Clemente Emily J, Ball Penny, Touré Aminata, Ferguson Lydia, Turner James M A, Loveland Kate L, Affara Nabeel A, Burgoyne Paul S

机构信息

Department of Pathology, Mammalian Molecular Genetics Group, University of Cambridge, Tennis Court Road, Cambridge CB2 1QP, UK.

出版信息

Hum Mol Genet. 2005 Sep 15;14(18):2705-15. doi: 10.1093/hmg/ddi304. Epub 2005 Aug 8.

Abstract

Deletions on the mouse Y-chromosome long arm (MSYq) lead to teratozoospermia and in severe cases to infertility. We find that the downstream transcriptional changes in the testis resulting from the loss of MSYq-encoded transcripts involve upregulation of multiple X- and Y-linked spermatid-expressed genes, but not related autosomal genes. Therefore, this indicates that in normal males, there is a specific repression of X and Y (gonosomal) transcription in post-meiotic cells, which depends on MSYq-encoded transcripts. Together with the known sex ratio skew in favour of females in the offspring of fertile MSYqdel males, this strongly suggests the existence of an intragenomic conflict between X- and Y-linked genes. Two potential antagonists in this conflict are the X-linked multicopy gene Xmr and its multicopy MSYq-linked relative Sly, which are upregulated and downregulated, respectively, in the testes of MSYqdel males. Xmr is also expressed during meiotic sex chromosome inactivation (MSCI), indicating a link between the MSCI and the MSYq-dependent gonosomal repression in spermatids. We therefore propose that this repression and MSCI itself are evolutionary adaptations to maintain a normal sex ratio in the face of X/Y antagonism.

摘要

小鼠Y染色体长臂(MSYq)的缺失会导致畸形精子症,严重时会导致不育。我们发现,由于MSYq编码转录本的缺失,睾丸中的下游转录变化涉及多个X和Y连锁的精子细胞表达基因的上调,但不涉及相关常染色体基因。因此,这表明在正常雄性中,减数分裂后细胞中存在对X和Y(性染色体)转录的特异性抑制,这取决于MSYq编码的转录本。再加上已知在可育的MSYqdel雄性后代中性别比例偏向雌性,这强烈表明X和Y连锁基因之间存在基因组内冲突。这种冲突中的两个潜在拮抗剂是X连锁的多拷贝基因Xmr及其多拷贝的MSYq连锁相关基因Sly,它们在MSYqdel雄性的睾丸中分别上调和下调。Xmr在减数分裂性染色体失活(MSCI)期间也有表达,这表明MSCI与精子细胞中MSYq依赖的性染色体抑制之间存在联系。因此,我们提出这种抑制和MSCI本身是面对X/Y拮抗时维持正常性别比例的进化适应。

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