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Cell-type-specific resolution epigenetics without the need for cell sorting or single-cell biology

机译:细胞型特异性分辨率表观遗传学,无需细胞分选或单细胞生物学

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High costs and technical limitations of cell sorting and single-cell techniques currently restrict the collection of large-scale, cell-type-specific DNA methylation data. This, in turn, impedes our ability to tackle key biological questions that pertain to variation within a population, such as identification of disease-associated genes at a cell-type-specific resolution. Here, we show mathematically and empirically that cell-type-specific methylation levels of an individual can be learned from its tissue-level bulk data, conceptually emulating the case where the individual has been profiled with a single-cell resolution and then signals were aggregated in each cell population separately. Provided with this unprecedented way to perform powerful large-scale epigenetic studies with cell-type-specific resolution, we revisit previous studies with tissue-level bulk methylation and reveal novel associations with leukocyte composition in blood and with rheumatoid arthritis. For the latter, we further show consistency with validation data collected from sorted leukocyte sub-types.
机译:细胞分选和单细胞技术的高成本和技术限制目前限制了大规模,细胞型特异性DNA甲基化数据的集合。反过来,这阻碍了我们解决患有人口内变异的关键生物学问题的能力,例如以细胞类型特异性分辨率鉴定疾病相关基因。在这里,我们在数学上和经验上显示个人的细胞类型特异性甲基化水平可以从其组织级批量数据学习,概念性地模拟个体用单个小区分辨率分辨的情况,然后汇总信号在每种细胞群中分别。提供了这种前所未有的方法来进行具有细胞类型特异性分辨率的强大的大规模表观遗传研究,我们重新审视了以往的组织级甲基化的研究,并揭示了与白细胞组合物中的新型关联和类风湿性关节炎。对于后者,我们进一步显示了从从分类的白细胞子类型收集的验证数据的一致性。

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