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2010年05月24日

【期刊论文】Regulation of Geminin Functions by Cell Cycle-Dependent Nuclear-Cytoplasmic Shuttling▽

罗凌飞, Lingfei Luo, * Yvonne Uerlings, Nicole Happel, Naisana S. Asli, Hendrik Knoetgen, and Michael Kessel

MOLECULAR AND CELLULAR BIOLOGY, July 2007, p. 4737-4744,-0001,():

-1年11月30日

摘要

The geminin protein functions both as a DNA rereplication inhibitor through association with Cdt1 and as a repressor of Hox gene transcription through the polycomb pathway. Here, we report that the functions of avian geminin are coordinated with and regulated by cell cycle-dependent nuclear-cytoplasmic shuttling. In S phase, geminin enters nuclei and inhibits both loading of the minichromosome maintenance (MCM) complex onto chromatin and Hox gene transcription. At the end of mitosis, geminin is exported from nuclei by the exportin protein Crm1 and is unavailable in the nucleus during the next G1 phase, thus ensuring proper chromatin loading of the MCM complex and Hox gene transcription. This mechanism for regulating the functions of geminin adds to distinct mechanisms, such as protein degradation and ubiquitination, applied in other vertebrates.

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2011年07月12日

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2010年05月24日

【期刊论文】TIPT2 and geminin interact with basal transcription factors to synergize in transcriptional regulation

罗凌飞, Mara E Pitulescu, Martin Teichmann, Lingfei Luo and Michael Kessel*

BMC Biochemistry 2009, 10: 16,-0001,():

-1年11月30日

摘要

Background: The re-replication inhibitor Geminin binds to several transcription factors including homeodomain proteins, and to members of the polycomb and the SWI/SNF complexes. Results: Here we describe the TATA-binding protein-like factor-interacting protein (TIPT) isoform 2, as a strong binding partner of Geminin. TIPT2 is widely expressed in mouse embryonic and adult tissues, residing both in cyto- and nucleoplasma, and enriched in the nucleolus. Like Geminin, also TIPT2 interacts with several polycomb factors, with the general transcription factor TBP (TATA box binding protein), and with the related protein TBPL1 (TRF2). TIPT2 synergizes with geminin and TBP in the activation of TATA box-containing promoters, and with TBPL1 and geminin in the activation of the TATA-less NF1 promoter. Geminin and TIPT2 were detected in the chromatin near TBP/TBPL1 binding sites. Conclusion: Together, our study introduces a novel transcriptional regulator and its function in cooperation with chromatin associated factors and the basal transcription machinery.

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2010年05月24日

【期刊论文】Geminin Coordinates Cell Cycle and Developmental Control

罗凌飞, Lingfei Luo, Michael Kessel*

Cell Cycle 3:6, 711-714; June 2004,-0001,():

-1年11月30日

摘要

Growth and differentiation are two major themes in embryonic development. Numerous cell divisions have to be regulated on the path from a unicellular embryo, the zygote, to the multicellular structures of a mature being. Numerous functions, specializations and cellular identities have to be generated, in order to form a complex and mature animal. Numerous mechanisms have to control the correct assignment and acquisition of cellular fates, as well as the right timing and allocation of cells. Therefore, a strict coordination has to occur between embryonic patterning and the cell cycle. From this point of view, dual roles or mutual interactions of typical proliferation and developmental control genes are likely. Recently, new light was shed on these issues by identifying the nuclear protein Geminin as a molecular coordinator between the cell cycle and axial patterning. We summarize the role of Geminin in cell cycle, in the embryonic patterning controlled by Hox genes, providing insights into cell cycle regulators in embryonic development, and conversely, typical developmental control genes in cell cycle regulation.

Geminin,, Hox,, Polycomb,, Cdt1,, cell cycle,, embryonic patterning,, coordination

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2011年07月12日

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  • 罗凌飞 邀请

    西南大学,四川

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