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Leveraging cell‐specific differentially methylated regions to identify leukocyte infiltration in adipose tissue

机译:利用细胞特异性差异甲基化区域以鉴定脂肪组织中的白细胞浸润

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Abstract Obesity is understood to be an inflammatory condition characterized in part by changes in resident immune cell populations in adipose tissue. However, much of this knowledge has been obtained through experimental animal models. Epigenetic mechanisms, such as DNA methylation may be useful tools for characterizing the changes in immune cell populations in human subjects. In this study, we introduce a simple and intuitive method for assessing cellular infiltration by blood into other heterogeneous, admixed tissues such as adipose tissue, and apply this approach in a large human cohort study. Associations between higher leukocyte infiltration, measured by evaluating a distance measure between the methylation signatures of leukocytes and adipose tissue, and increasing body mass index (BMI) or android fat mass (AFM) were identified and validated in independent replication samples for CD4 (p BMI ?=?0.009, p AFM ?=?0.020), monocytes (p BMI ?=?0.001, p AFM ?=?4.3?×?10 ?4 ), and dendritic cells (p BMI ?=?0.571, p AFM ?=?0.012). Patterns of depletion with increasing adiposity were observed for plasma B (p BMI ?=?0.430, p AFM ?=?0.004) and immature B (p BMI ?=?0.022, p AFM ?=?0.042) cells. CD4, dendritic, monocytes, immature B, and plasma B cells may be important agents in the inflammatory process. Finally, the method used to assess leukocyte infiltration in this study is straightforwardly extended to other cell types and tissues in which infiltration might be of interest.
机译:摘要肥胖应理解为一种炎症病症,其特征在于脂肪组织中常驻免疫细胞群的变化。然而,通过实验动物模型获得了大部分知识。表观遗传机制,例如DNA甲基化可能是用于表征人受试者免疫细胞群的变化的有用工具。在这项研究中,我们介绍了一种简单而直观的方法,用于评估血液中的细胞浸润到其他异质,混合组织如脂肪组织,并在大型人的队列研究中应用这种方法。通过评估白细胞和脂肪组织的甲基化签名之间的距离测量来测量的较高白细胞浸润之间的关联,并在CD4的独立复制样品中鉴定并验证体重指数(BMI)或Android脂肪质量(Android脂肪质量(AFM)(P BMI ?=?0.009,p afm?=?0.020),单核细胞(p bmi?= 0.001,p afm?=α.4.3?×10?4)和树突细胞(p bmi?=?0.571,p afm? =?0.012)。对等离子体B观察到随着肥胖的耗水模式(P BMIα= 0.430,P AFM?0.004)和未成熟的B(P BMI?= 0.022,P AFM?= 0.042)细胞。 CD4,树突状,单核细胞,未成熟B和血浆B细胞可能是炎症过程中的重要药剂。最后,用于评估该研究中的白细胞浸润的方法直接扩展到其他细胞类型和组织,其中渗透可能是感兴趣的。

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