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hoxa-9和hoxb-9中的靶向突变揭示了协同相互作用。

Targeted mutations in hoxa-9 and hoxb-9 reveal synergistic interactions.

作者信息

Chen F, Capecchi M R

机构信息

Department of Human Genetics, Howard Hughes Medical Institute, University of Utah School of Medicine, Salt Lake City 84112, USA.

出版信息

Dev Biol. 1997 Jan 15;181(2):186-96. doi: 10.1006/dbio.1996.8440.

Abstract

Mice were generated with a targeted disruption of the homeobox-containing gene hoxb-9. Mice homozygous for this mutation show defects in the development of the first and second ribs. In most cases the first and second ribs are fused near the point at which the first and second pairs of ribs normally attach to the sternum. Abnormalities of the sternum accompany the rib fusions. These include abnormal attachment of the ribs to the sternum, a reduction in the number of intercostal segments of the sternum, and abnormal growth of the intercostal segments. Over half of the homozygous mutants, as well as some heterozygotes, also have an eighth rib attached to the sternum. These results show that hoxb-9 plays a significant role in the specification of thoracic skeletal elements. To reveal potential interactions between the paralogous Hox genes hoxa-9 and hoxb-9, mice heterozygous for both mutations were intercrossed. Mice homozygous for both mutations show more severe phenotypes than predicted by the addition of the individual mutant phenotypes. Both the penetrance and the expressivity of the rib and sternal defects are increased, suggesting synergistic interactions between these genes. In particular, the sternum defects are greatly exacerbated. Interestingly, the defects in hoxb-9 and hoxa-9/ hoxb-9 mutant mice are concentrated along the axial column at points of transition between vertebral types.

摘要

通过靶向破坏含同源框基因hoxb - 9培育出小鼠。该突变的纯合子小鼠在第一和第二肋骨的发育上表现出缺陷。在大多数情况下,第一和第二肋骨在第一和第二对肋骨正常附着于胸骨的位置附近融合。胸骨异常伴随肋骨融合出现。这些异常包括肋骨与胸骨的异常附着、胸骨肋间节段数量减少以及肋间节段的异常生长。超过一半的纯合突变体以及一些杂合子还存在第八根肋骨附着于胸骨的情况。这些结果表明hoxb - 9在胸段骨骼元件的特化过程中发挥着重要作用。为了揭示同源Hox基因hoxa - 9和hoxb - 9之间的潜在相互作用,将两种突变的杂合子小鼠进行杂交。两种突变均为纯合子的小鼠表现出比单个突变体表型相加所预测的更严重的表型。肋骨和胸骨缺陷的外显率和表现度均增加,表明这些基因之间存在协同相互作用。特别是,胸骨缺陷大大加剧。有趣的是,hoxb - 9和hoxa - 9/hoxb - 9突变小鼠的缺陷集中在脊柱类型转变点的沿轴柱处。

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