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HPF1 completes the PARP active site for DNA damage-induced ADP-ribosylation 期刊论文
NATURE, 2020, 579 (7800) : 598-+
作者:  Yao, Peng;  Wu, Huaqiang;  Gao, Bin;  Tang, Jianshi;  Zhang, Qingtian;  Zhang, Wenqiang;  Yang, J. Joshua;  Qian, He
收藏  |  浏览/下载:23/0  |  提交时间:2020/07/03

Assembly of a catalytic centre formed by HPF1 bound to PARP1 or PARP2 is essential for protein ADP-ribosylation after DNA damage in human cells.


The anti-cancer drug target poly(ADP-ribose) polymerase 1 (PARP1) and its close homologue, PARP2, are early responders to DNA damage in human cells(1,2). After binding to genomic lesions, these enzymes use NAD(+) to modify numerous proteins with mono- and poly(ADP-ribose) signals that are important for the subsequent decompaction of chromatin and the recruitment of repair factors(3,4). These post-translational modifications are predominantly serine-linked and require the accessory factor HPF1, which is specific for the DNA damage response and switches the amino acid specificity of PARP1 and PARP2 from aspartate or glutamate to serine residues(5-10). Here we report a co-structure of HPF1 bound to the catalytic domain of PARP2 that, in combination with NMR and biochemical data, reveals a composite active site formed by residues from HPF1 and PARP1 or PARP2 . The assembly of this catalytic centre is essential for the addition of ADP-ribose moieties after DNA damage in human cells. In response to DNA damage and occupancy of the NAD(+)-binding site, the interaction of HPF1 with PARP1 or PARP2 is enhanced by allosteric networks that operate within the PARP proteins, providing an additional level of regulation in the induction of the DNA damage response. As HPF1 forms a joint active site with PARP1 or PARP2, our data implicate HPF1 as an important determinant of the response to clinical PARP inhibitors.


  
Application of the 3-PG model to predict growth of Larix olgensis plantations in northeastern China 期刊论文
FOREST ECOLOGY AND MANAGEMENT, 2017, 406
作者:  Xie, Yalin;  Wang, Haiyan;  Lei, Xiangdong
收藏  |  浏览/下载:12/0  |  提交时间:2019/04/09
Forest growth model  Process-based models  3-PG  Larix olgensis  Site factors  
Radiochemically-Supported Microbial Communities: A Potential Mechanism for Biocolloid Production of Importance to Actinide Transport 科技报告
来源:US Department of Energy (DOE). 出版年: 2014
作者:  Moser, Duane P;  Hamilton-Brehm, Scott D;  Fisher, Jenny C;  Bruckner, James C;  Kruger, Brittany;  Sackett, Joshua;  Russell, Charles E;  Onstott, Tullis C;  Czerwinski, Ken
收藏  |  浏览/下载:42/0  |  提交时间:2019/04/05
Due to the legacy of Cold War nuclear weapons testing  the Nevada National Security Site (NNSS  formerly known as the Nevada Test Site (NTS)) contains millions of Curies of radioactive contamination. Presented here is a summary of the results of the first comprehensive study of subsurface microbial communities of radioactive and nonradioactive aquifers at this site. To achieve the objectives of this project  cooperative actions between the Desert Research Institute (DRI)  the Nevada Field Office of the National Nuclear Security Administration (NNSA)  the Underground Test Area Activity (UGTA)  and contractors such as Navarro-Interra (NI)  were required. Ultimately  fluids from 17 boreholes and two water-filled tunnels were sampled (sometimes on multiple occasions and from multiple depths) from the NNSS  the adjacent Nevada Test and Training Range (NTTR)  and a reference hole in the Amargosa Valley near Death Valley. The sites sampled ranged from highly-radioactive nuclear device test cavities to uncontaminated perched and regional aquifers. Specific areas sampled included recharge  intermediate  and discharge zones of a 100  000-km2 internally-draining province  known as the Death Valley Regional Flow System (DVRFS)  which encompasses the entirety of the NNSS/NTTR and surrounding areas. Specific geological features sampled included: West Pahute and Ranier Mesas (recharge zone)  Yucca and Frenchman Flats (transitional zone)  and the Western edge of the Amargosa Valley near Death Valley (discharge zone). The original overarching question underlying the proposal supporting this work was stated as: Can radiochemically-produced substrates support indigenous microbial communities and subsequently stimulate biocolloid formation that can affect radionuclides in NNSS subsurface nuclear test/detonation sites? Radioactive and non-radioactive groundwater samples were thus characterized for physical parameters  aqueous geochemistry  and microbial communities using both DNA- and cultivation-based tools in an effort to understand the drivers of microbial community structure (including radioactivity) and microbial interactions with select radionuclides and other factors across the range of habitats surveyed.