首页> 美国卫生研究院文献>G3: GenesGenomesGenetics >Molecular Insight into the Association Between Cartilage Regeneration and Ear Wound Healing in Genetic Mouse Models: Targeting New Genes in Regeneration
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Molecular Insight into the Association Between Cartilage Regeneration and Ear Wound Healing in Genetic Mouse Models: Targeting New Genes in Regeneration

机译:在遗传小鼠模型中软骨再生与耳朵伤口愈合之间关联的分子洞察:针对再生中的新基因

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摘要

Tissue regeneration is a complex trait with few genetic models available. Mouse strains LG/J and MRL are exceptional healers. Using recombinant inbred strains from a large (LG/J, healer) and small (SM/J, nonhealer) intercross, we have previously shown a positive genetic correlation between ear wound healing, knee cartilage regeneration, and protection from osteoarthritis. We hypothesize that a common set of genes operates in tissue healing and articular cartilage regeneration. Taking advantage of archived histological sections from recombinant inbred strains, we analyzed expression of candidate genes through branched-chain DNA technology directly from tissue lysates. We determined broad-sense heritability of candidates, Pearson correlation of candidates with healing phenotypes, and Ward minimum variance cluster analysis for strains. A bioinformatic assessment of allelic polymorphisms within and near candidate genes was also performed. The expression of several candidates was significantly heritable among strains. Although several genes correlated with both ear wound healing and cartilage healing at a marginal level, the expression of four genes representing DNA repair (Xrcc2, Pcna) and Wnt signaling (Axin2, Wnt16) pathways was significantly positively correlated with both phenotypes. Cluster analysis accurately classified healers and nonhealers for seven out of eight strains based on gene expression. Specific sequence differences between LG/J and SM/J were identified as potential causal polymorphisms. Our study suggests a common genetic basis between tissue healing and osteoarthritis susceptibility. Mapping genetic variations causing differences in diverse healing responses in multiple tissues may reveal generic healing processes in pursuit of new therapeutic targets designed to induce or enhance regeneration and, potentially, protection from osteoarthritis.
机译:组织再生是一个复杂的特征,几乎没有可用的遗传模型。小鼠品系LG / J和MRL是出色的治疗者。使用来自大型(LG / J,治愈者)和小型(SM / J,非治愈者)杂交的重组近交菌株,我们先前已经显示出耳部伤口愈合,膝关节软骨再生和对骨关节炎的保护之间存在正向遗传相关性。我们假设一组常见的基因在组织愈合和关节软骨再生中起作用。利用重组自交系中存档的组织学切片,我们直接通过组织裂解液通过支链DNA技术分析了候选基因的表达。我们确定了候选人的广义遗传力,具有治愈表型的候选人的Pearson相关性以及菌株的Ward最小方差聚类分析。还对候选基因内部和附近的等位基因多态性进行了生物信息学评估。几种候选物的表达在菌株之间显着遗传。尽管一些基因在一定程度上与耳伤口愈合和软骨愈合相关,但是代表DNA修复(Xrcc2,Pcna)和Wnt信号传导(Axin2,Wnt16)途径的四个基因的表达与这两种表型均显着正相关。聚类分析可根据基因表达对八种菌株中的七种准确地分类为治疗者和非治疗者。 LG / J和SM / J之间的特定序列差异被确定为潜在的因果多态性。我们的研究表明组织愈合和骨关节炎易感性之间的共同遗传基础。定位导致多个组织中不同愈合反应差异的遗传变异,可以揭示寻求新的治疗靶标的通用愈合过程,这些靶标旨在诱导或增强再生并可能预防骨关节炎。

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