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对 21 号染色体三拷贝同源物进行遗传剖析,为唐氏综合征模型鼠的骨骼特征提供了多样性。

Genetic dissection of triplicated chromosome 21 orthologs yields varying skeletal traits in Down syndrome model mice.

机构信息

Department of Biology, Indiana University-Purdue University Indianapolis, Indianapolis, IN 46202, USA.

The Francis Crick Institute, London NW1 1AT, UK.

出版信息

Dis Model Mech. 2023 Apr 1;16(4). doi: 10.1242/dmm.049927. Epub 2023 Apr 26.

Abstract

Down syndrome (DS) phenotypes result from triplicated genes, but the effects of three copy genes are not well known. A mouse mapping panel genetically dissecting human chromosome 21 (Hsa21) syntenic regions was used to investigate the contributions and interactions of triplicated Hsa21 orthologous genes on mouse chromosome 16 (Mmu16) on skeletal phenotypes. Skeletal structure and mechanical properties were assessed in femurs of male and female Dp9Tyb, Dp2Tyb, Dp3Tyb, Dp4Tyb, Dp5Tyb, Dp6Tyb, Ts1Rhr and Dp1Tyb;Dyrk1a+/+/- mice. Dp1Tyb mice, with the entire Hsa21 homologous region of Mmu16 triplicated, display bone deficits similar to those of humans with DS and served as a baseline for other strains in the panel. Bone phenotypes varied based on triplicated gene content, sex and bone compartment. Three copies of Dyrk1a played a sex-specific, essential role in trabecular deficits and may interact with other genes to influence cortical deficits related to DS. Triplicated genes in Dp9Tyb and Dp2Tyb mice improved some skeletal parameters. As triplicated genes can both improve and worsen bone deficits, it is important to understand the interaction between and molecular mechanisms of skeletal alterations affected by these genes.

摘要

唐氏综合征(DS)的表型是由三倍基因引起的,但三倍基因的影响尚不清楚。本研究使用一种遗传解析人类 21 号染色体(Hsa21)同源区域的小鼠图谱,来研究 16 号染色体(Mmu16)上三倍的 Hsa21 直系同源基因对骨骼表型的影响及其相互作用。通过对雄性和雌性 Dp9Tyb、Dp2Tyb、Dp3Tyb、Dp4Tyb、Dp5Tyb、Dp6Tyb、Ts1Rhr 和 Dp1Tyb;Dyrk1a+/+/- 小鼠的股骨进行评估,来检测骨骼结构和力学性能。Dp1Tyb 小鼠具有三倍的 Mmu16 同源区域,其骨骼缺陷类似于唐氏综合征患者,作为该图谱中其他品系的基线。骨骼表型因三倍基因含量、性别和骨骼区域而异。三倍的 Dyrk1a 基因在骨小梁缺陷中具有性别特异性的重要作用,可能与其他基因相互作用,影响与 DS 相关的皮质骨缺陷。Dp9Tyb 和 Dp2Tyb 小鼠中的三倍基因改善了一些骨骼参数。由于三倍基因既可以改善也可以恶化骨骼缺陷,因此了解这些基因影响的骨骼改变之间的相互作用和分子机制非常重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f563/10163323/53f103141d3f/dmm-16-049927-g1.jpg

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