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A functional role for transfer RNA-derived microRNAs in human B cells.

机译:在人类B细胞中转移RNA衍生的microRNA的功能作用。

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摘要

Sequencing studies performed in recent decades have revealed that the cells of most eukaryotic organisms express a diverse repertoire of small RNAs. Genetic and biochemical investigation of these molecules has demonstrated that many small RNAs, most notably the microRNA subclass, possess the capacity to influence the expression of other genes, adding substantial complexity to our understanding of genetic regulatory networks. In the years since their initial discovery, microRNAs have been implicated in nearly every aspect of metazoan biology, including medically relevant processes such as the development of mammalian immune cells and the oncogenic transformation of such cells into leukemias and lymphomas. Even in these well-studied systems, however, the function of only a small fraction of microRNAs is understood, and novel RNAs may yet remain undiscovered. Thus, in order to better define the microRNA landscape of both normal mature B cells and their oncogenic counterparts, we undertook sequencing of their small RNA transcriptomes. In addition to microRNAs, these studies unexpectedly identified a class of RNA fragments whose sequences matched to transfer RNA, but whose size distribution resembled that of microRNAs. Deep sequencing of small RNAs from a panel of normal mature B cells and B cell lymphomas reveals that these cell types express thousands of unique transfer RNA-derived fragments, with highly distinct expression profiles in each biological subtype. We hypothesized that these fragments might be derived from direct processing of tRNA but nonetheless function as microRNA, and sought to experimentally characterize one representative sequence of this class, cloned from human mature B cells and designated CU1276. The resulting data demonstrate that CU1276 does indeed possesses the functional characteristics of a microRNA, including a DICER1-dependent biogenesis, physical association with Argonaute proteins, and the ability to repress mRNA transcripts in a sequence-specific manner. Specifically, CU1276 represses endogenous expression of RPA1, a gene with critical functions in many aspects of DNA dynamics, including replication and repair. CU1276 is abundantly expressed in normal mature B cells but strongly downregulated in B cell-derived lymphomas, while its target, RPA1 , is overexpressed in lymphomas. Furthermore, enforced expression of CU1276 in a lymphoma cell line results in an RPA1-dependent impairment of both proliferation and DNA damage repair. These results suggest that relief from CU1276-mediated repression of RPA1 may confer a selective advantage to lymphoma cells, and they shed light on a possible regulatory role for transfer RNA-derived microRNA in the in the maturation of normal B cells. Taken together with published data, these results suggest that in a broad spectrum of organisms and tissues, transfer RNAs act as a previously unrecognized substrate for the biogenesis of microRNA, with substantial implications for the future study of small RNA-mediated gene regulation.
机译:近几十年来进行的测序研究表明,大多数真核生物的细胞表达各种小RNA。对这些分子的遗传和生化研究表明,许多小RNA,最显着的是microRNA亚类,具有影响其他基因表达的能力,为我们对遗传调控网络的理解增加了相当大的复杂性。自从最初发现以来,多年来,microRNA已涉及后生动物生物学的几乎每个方面,包括医学上相关的过程,例如哺乳动物免疫细胞的发育以及此类细胞向白血病和淋巴瘤的致癌转化。但是,即使在这些经过充分研究的系统中,也仅能理解一小部分microRNA的功能,而新颖的RNA可能仍未被发现。因此,为了更好地定义正常成熟B细胞及其致癌对应物的microRNA格局,我们对其小RNA转录组进行了测序。除了微RNA,这些研究出乎意料地鉴定出一类RNA片段,其序列与转移RNA匹配,但其大小分布类似于微RNA。从一组正常的成熟B细胞和B细胞淋巴瘤中对小RNA进行深度测序后发现,这些细胞类型表达成千上万个独特的,源自转移RNA的片段,每个生物亚型中的表达谱高度不同。我们假设这些片段可能源自tRNA的直接加工,但仍起microRNA的作用,并试图通过实验表征从人类成熟B细胞克隆并命名为CU1276的该类代表性序列。所得数据表明CU1276确实具有microRNA的功能特征,包括DICER1依赖的生物发生,与Argonaute蛋白质的物理缔合以及以序列特异性方式抑制mRNA转录本的能力。具体而言,CU1276抑制RPA1的内源表达,该基因在DNA动力学的许多方面(包括复制和修复)都具有关键功能。 CU1276在正常成熟的B细胞中大量表达,但在B细胞衍生的淋巴瘤中强烈下调,而其靶标RPA1在淋巴瘤中过表达。此外,CU1276在淋巴瘤细胞系中的强制表达导致RPA1依赖性的增殖和DNA损伤修复受损。这些结果表明,缓解CU1276介导的RPA1抑制可能赋予淋巴瘤细胞选择性优势,并且它们阐明了在正常B细胞​​成熟中转移RNA衍生的microRNA的可能调控作用。连同已发表的数据,这些结果表明,在广泛的生物体和组织中,转移RNA充当了microRNA生物发生的先前未被认识的底物,对小RNA介导的基因调控的未来研究具有重大意义。

著录项

  • 作者

    Maute, Roy.;

  • 作者单位

    Columbia University.;

  • 授予单位 Columbia University.;
  • 学科 Biology Molecular.;Chemistry Biochemistry.
  • 学位 Ph.D.
  • 年度 2013
  • 页码 141 p.
  • 总页数 141
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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