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New molecular research technologies in the study of muscle disease.

机译:研究肌肉疾病的新分子研究技术。

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SUMMARY: PURPOSE OF REVIEW To describe the current technologies and progress in DNA polymorphism association studies, mRNA expression profiling (microarrays), and proteomics with respect to muscle disease, and the increasing impact of public-access databases of genome-wide information.RECENT FINDINGS mRNA expression profiling is becoming the most mature of the highly parallel molecular technologies, with microarrays now able to query the large majority of all genes using 1 million oligonucleotide probes built on 1.2-cm2 glass substrates. Applications of microarrays to normal muscle physiology and muscle disease are discussed. Single nucleotide polymorphism association studies promise to determine the predisposition of individuals to acquired muscle disease, including sarcopenia and atrophy, although such studies are in their infancy. Proteomics technologies do not enjoy the sensitivity and specificity of hybridization, and must instead rely on mass spectrometers. Mass spectrometry technology is advancing rapidly, although the sensitivity and throughput is far behind that of mRNA expression profiling.SUMMARY As the gene mutations responsible for many types of muscular dystrophy and myopathy have been discovered, protein and gene testing has been integrated into the standard patient diagnostic workup. Future developments will include simpler and less expensive molecular diagnostics, advances in the understanding of downstream consequences of these defects, and the genetic predispositions underlying acquired muscle disease.
机译:摘要:综述的目的描述与肌肉疾病有关的DNA多态性关联研究,mRNA表达谱(微阵列)和蛋白质组学的最新技术和进展,以及全基因组信息公共访问数据库的日益增长的影响。 mRNA表达谱分析已成为高度并行分子技术中最成熟的技术,微阵列现在可以使用在1.2平方厘米玻璃基板上构建的100万个寡核苷酸探针来查询绝大多数基因。讨论了微阵列在正常肌肉生理和肌肉疾病中的应用。单核苷酸多态性关联研究有望确定个体易患获得性肌肉疾病(包括肌肉减少症和萎缩)的倾向,尽管此类研究尚处于婴儿期。蛋白质组学技术不具有杂交的敏感性和特异性,而必须依靠质谱仪。质谱技术正在迅速发展,尽管其灵敏度和通量远远落后于mRNA表达谱。概述由于发现了导致多种类型的肌营养不良和肌病的基因突变,蛋白质和基因检测已被纳入标准患者诊断性检查。未来的发展将包括更简单,更便宜的分子诊断,对这些缺陷的下游后果的理解的进步以及后天性肌肉疾病的遗传易感性。

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