open reading frame sequence
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2021 ◽  
Author(s):  
Jing Feng ◽  
Wenbo Chen ◽  
Xin Dong ◽  
Jun Wang ◽  
Xiangfei Mei ◽  
...  

Abstract The significant function of circRNAs in cancer was recognized in recent work, so a well-organized resource is required for characterizing the interactions between circRNAs and other functional molecules (such as microRNA and RNA-binding protein) in cancer. We previously developed cancer-specific circRNA database (CSCD), a comprehensive database for cancer-specific circRNAs, which is widely used in circRNA research. Here, we updated CSCD to CSCD2 (http://geneyun.net/CSCD2 or http://gb.whu.edu.cn/CSCD2), which includes significantly more cancer-specific circRNAs identified from a large number of human cancer and normal tissues/cell lines. CSCD2 contains >1000 samples (825 tissues and 288 cell lines) and identifies a large number of circRNAs: 1 013 461 cancer-specific circRNAs, 1 533 704 circRNAs from only normal samples and 354 422 circRNAs from both cancer and normal samples. In addition, CSCD2 predicts potential miRNA–circRNA and RBP–circRNA interactions using binding motifs from >200 RBPs and 2000 microRNAs. Furthermore, the potential full-length and open reading frame sequence of these circRNAs were also predicted. Collectively, CSCD2 provides a significantly enhanced resource for exploring the function and regulation of circRNAs in cancer.


2019 ◽  
Vol 8 (42) ◽  
Author(s):  
Martin Schou Pedersen ◽  
Sarah Mollerup ◽  
Lone Gilmor Nielsen ◽  
Håvard Jenssen ◽  
Jens Bukh ◽  
...  

The surveillance and correct subtyping of hepatitis C virus strains require available and up-to-date publicly available reference genomes. Here, we present the complete open reading frame sequence of a hepatitis C virus genotype 6 strain of an unknown subtype that was discovered during routine subtyping of patients in the clinic.


2006 ◽  
Vol 78 (4) ◽  
pp. 517-522 ◽  
Author(s):  
Ying Qi ◽  
Zhi-Qin Mao ◽  
Qiang Ruan ◽  
Rong He ◽  
Yan-Ping Ma ◽  
...  

2002 ◽  
Vol 83 (7) ◽  
pp. 1721-1728 ◽  
Author(s):  
Helene Norder ◽  
Lotte Bjerregaard ◽  
Lars O. Magnius

Phylogenetic analysis within the VP1 region now enables molecular typing of enteroviruses consistent with neutralization results. Three untypable isolates, 2776/82, 57/99 and 22/00, from Korea, North India and Bangladesh, respectively, showed within this region 98·0–99·0% amino acid identities. These were less than 77% to the previous enterovirus prototypes, but 91·5–92·5% to CA55-1988, the recently identified enterovirus 73 (EV73) prototype from California. All three strains were, however, most similar to CA64-4454, an EV73 prime strain, to which they shared 96·5–98·5% identity. Seven compared EV73 strains formed two clusters in the VP1 dendrogram, one cluster with strains from South and East Asia and CA64-4454, and the other with strains from Oman and California including the prototype. When sequencing the complete open reading frame of 2776/82, its non-structural region was found to be divergent from all human enterovirus B (HEV-B) strains, including CA55-1988, indicating that one or other strain was recombinant. Boot scanning of the genomes showed a recombination point within the P2 region. Therefore, part of this was sequenced for 57/99 and 22/00 and was found similar to 2776/82, while CA55-1988 was similar to coxsackievirus B3, demonstrating that CA55-1988 was the recombinant. Since all strains of EV73 isolated so far outside California originate from Asia, where it has a broad geographical distribution, it seems that EV73 may have been introduced to California from Asia. Further analysis of EV73 strains will reveal if the recombination occurred in the USA or in Asia and will help to elucidate the origin of this virus.


10.1038/85913 ◽  
2001 ◽  
Vol 27 (3) ◽  
pp. 332-336 ◽  
Author(s):  
Jérôme Reboul ◽  
Philippe Vaglio ◽  
Nia Tzellas ◽  
Nicolas Thierry-Mieg ◽  
Troy Moore ◽  
...  

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