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人类疾病中的DNA探针

DNA probes in human disease.

作者信息

Malcolm A D, Fallon R A, Langdale J A, Figueiredo H, Nicholls P J, Voss U B, Wickenden C, Woodhead J L

机构信息

Department of Biochemistry, Charing Cross and Westminster Medical School, London, U.K.

出版信息

Biochem Soc Symp. 1987;53:131-43.

PMID:3332764
Abstract

Nucleic acid probes are able to detect the presence of particular sequences in a sample down to the level of a few hundred molecules. They can discriminate between similar sequences to a resolution of better than one part in 10(9). They are capable of detecting inherited defects in tissues where the phenotype is not being expressed, and in cases where the biochemical aberration is not understood. They can characterize acquired diseases in somatic cells (both tumours and infectious agents). Additionally, they can be used to characterize multifactorial (either polygenic or requiring an environmental stimulus to interact with a genetic predisposition) diseases. Nucleic acid 'fingerprints' provide an unequivocal identification of the origin of cells which may be applied in criminal law, civil law, and in the follow up to bone marrow transplants. In spite of this tremendous potential, there is still a large gap between their use in research laboratories and their widespread application in pathology laboratories. There are two basic reasons for this. The first is the number of labour-intensive steps involved in the various 'blotting' techniques which greatly reduces the rate at which assays may be performed. The second is the need to use probes labelled with isotopes which are short-lived and may require stringent safety measures to be employed. Recent work both in this laboratory and elsewhere is designed to circumvent both these problems.

摘要

核酸探针能够检测样本中特定序列的存在,检测下限可达几百个分子水平。它们能够区分相似序列,分辨率优于10⁹分之一。它们能够检测表型未表达的组织中的遗传缺陷,以及生化异常尚不明确的情况。它们能够鉴定体细胞中的后天性疾病(包括肿瘤和感染因子)。此外,它们可用于鉴定多因素(多基因或需要环境刺激与遗传易感性相互作用)疾病。核酸“指纹”能明确鉴定细胞来源,可应用于刑法、民法以及骨髓移植的后续跟踪。尽管有如此巨大的潜力,但它们在研究实验室中的应用与在病理实验室中的广泛应用之间仍存在很大差距。造成这种情况有两个基本原因。第一个原因是各种“印迹”技术涉及大量劳动密集型步骤,这大大降低了检测的执行速度。第二个原因是需要使用用半衰期短的同位素标记的探针,这可能需要采取严格的安全措施。本实验室和其他地方最近的工作旨在解决这两个问题。

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