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通过DNA微阵列上的共调控表达鉴定T淋巴细胞激活基因

T lymphocyte activation gene identification by coregulated expression on DNA microarrays.

作者信息

Mao Mao, Biery Matt C, Kobayashi Sumire V, Ward Terry, Schimmack Greg, Burchard Julja, Schelter Janell M, Dai Hongyue, He Yudong D, Linsley Peter S

机构信息

Rosetta Inpharmatics LLC, Merck Research Laboratories, 401 Terry Avenue N, Seattle, WA 98109, USA.

出版信息

Genomics. 2004 Jun;83(6):989-99. doi: 10.1016/j.ygeno.2003.12.019.

Abstract

High-capacity methods for assessing gene function have become increasingly important because of the increasing number of newly identified genes emerging from large-scale genome sequencing and cDNA cloning efforts. We investigated the use of DNA microarrays to identify uncharacterized genes specifically involved in human T cell activation. Activation of human peripheral blood T lymphocytes induced significant changes in hundreds of transcripts, but most of these were not unique to T cell activation. Variation of experimental parameters and analysis techniques allowed better enrichment for gene expression changes unique to T cell activation. Best results were achieved by identification of genes that were most highly coregulated with the T-cell-specific transcript interleukin 2 (IL2) in a "compendium" of experiments involving both T cells and other cell types. Among the genes most highly coregulated with IL2 were many genes known to function during T cell activation, together with ESTs of unknown function. Four of these ESTs were extended to novel full-length clones encoding T-cell-regulated proteins with predicted functions in GTP metabolism, cell organization, and signal transduction.

摘要

由于大规模基因组测序和cDNA克隆工作中不断涌现出越来越多新鉴定的基因,用于评估基因功能的高容量方法变得越来越重要。我们研究了使用DNA微阵列来鉴定特异性参与人类T细胞活化的未表征基因。人类外周血T淋巴细胞的活化诱导了数百种转录本的显著变化,但其中大多数并非T细胞活化所特有的。实验参数和分析技术的变化使得能够更好地富集T细胞活化所特有的基因表达变化。在涉及T细胞和其他细胞类型的实验“汇编”中,通过鉴定与T细胞特异性转录本白细胞介素2(IL2)共调控程度最高的基因,获得了最佳结果。与IL2共调控程度最高的基因中,有许多已知在T细胞活化过程中发挥作用的基因,以及功能未知的EST。其中四个EST被扩展为新的全长克隆,编码在GTP代谢、细胞组织和信号转导中具有预测功能的T细胞调节蛋白。

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