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表观遗传学与自身免疫。

Epigenetics and autoimmunity.

机构信息

Experimental HTS, Drug Discovery, H. Lee Moffitt Cancer Center & Research Institute, Tampa, Florida, USA.

出版信息

J Autoimmun. 2010 May;34(3):J207-19. doi: 10.1016/j.jaut.2009.12.006. Epub 2010 Jan 6.

DOI:10.1016/j.jaut.2009.12.006
PMID:20053532
Abstract

Advances in genetics, such as sequencing of the human genome, have contributed to identification of susceptible genetic patterns in autoimmune diseases (AID). However, genetics is only one aspect of the diseases that does not reflect the influence of environment, sex or aging. Epigenetics, the control of gene packaging and expression independent of alterations in the DNA sequence, is providing new directions linking genetics and environmental factors. Recent findings have contributed to our understanding of how epigenetic modifications could influence AID development, showing differences between AID patients and healthy controls but also showing how one disease differs from another. With regards to epigenetic abnormalities, DNA methylation and histone modifications could be affected leading to large spatial and temporal changes in gene regulation. Other epigenetic processes, such as the influence of the ionic milieu around chromatin and DNA supercoiling stresses may be suspected also. The newly described role of microRNAs in control of gene expression is important by promoting or suppressing autoreactivity in AID. As a consequence control of cellular processes is affected becoming conducive, for example, to the development of autoreactive lymphocytes in systemic lupus erythematosus, synoviocyte proliferation in rheumatoid arthritis, or neural demyelination in multiple sclerosis. Application of epigenetics to AID is in its infancy and requires new hypotheses, techniques, tools, and collaborations between basic epigenetic researchers and autoimmune researchers in order to improve our comprehension of AID. From this will arise new therapeutics, means for early intervention, and perhaps prevention.

摘要

遗传学的进步,如人类基因组测序,有助于鉴定自身免疫性疾病(AID)中易感的遗传模式。然而,遗传只是疾病的一个方面,它不能反映环境、性别或衰老的影响。表观遗传学是指独立于 DNA 序列改变控制基因包装和表达的机制,它为将遗传学和环境因素联系起来提供了新的方向。最近的发现有助于我们理解表观遗传修饰如何影响 AID 的发展,显示了 AID 患者和健康对照组之间的差异,但也显示了一种疾病与另一种疾病的不同之处。关于表观遗传异常,DNA 甲基化和组蛋白修饰可能受到影响,导致基因调控的大空间和时间变化。其他表观遗传过程,如染色质周围离子环境的影响和 DNA 超螺旋张力的影响,也可能受到怀疑。新发现的 microRNAs 在控制基因表达中的作用很重要,它可以促进或抑制 AID 中的自身反应。因此,细胞过程的控制受到影响,例如,系统性红斑狼疮中自身反应性淋巴细胞的发育、类风湿关节炎中滑膜细胞的增殖或多发性硬化症中的神经脱髓鞘。表观遗传学在 AID 中的应用还处于起步阶段,需要新的假设、技术、工具,并需要基础表观遗传学研究人员和自身免疫研究人员之间的合作,以提高我们对 AID 的理解。由此将产生新的治疗方法、早期干预的手段,也许还能预防疾病。

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