نتایج جستجو برای: ires

تعداد نتایج: 1709  

2017
Nehal Thakor M. Duane Smith Luc Roberts Mame Daro Faye Harshil Patel Hans-Joachim Wieden Jamie H. D. Cate Martin Holcik

IRES-mediated translation of key cell fate regulating genes has been implicated in tumorigenesis. Concerted action of canonical eukaryotic initiation factors and IRES transacting factors (ITAFs) was shown to regulate cellular IRES mediated translation; however, the precise molecular mechanism of ribosome recruitment to cellular IRESes remains unclear. Here we show that the X-linked inhibitor of...

Journal: :Proceedings of the National Academy of Sciences of the United States of America 2002
Yuri L Dorokhov Maxim V Skulachev Peter A Ivanov Svetlana D Zvereva Lydia G Tjulkina Andres Merits Yuri Y Gleba Thomas Hohn Joseph G Atabekov

The internal ribosome entry sites (IRES), IRES(CP,148)(CR) and IRES(MP,75)(CR), precede the coat protein (CP) and movement protein (MP) genes of crucifer-infecting tobamovirus (crTMV), respectively. In the present work, we analyzed the activity of these elements in transgenic plants and other organisms. Comparison of the relative activities of the crTMV IRES elements and the IRES from an animal...

2016
Shiu-Wan Chan

We have previously shown that physio/pathological levels of hydrogen peroxide (H2O2) stimulate translation from the hepatitis C virus (HCV) internal ribosome entry site (IRES) element in tissue-cultured cells. Here, using in vitro translation, we further show that H2O2 upregulates HCV IRES-dependent mRNA translation and correlates with an increase in intracellular oxidant level. Using Western b...

2013
Jun-Jie Hong Tzong-Yuan Wu Tsair-Yuan Chang Chung-Yung Chen

The internal ribosomal entry site (IRES) functions as cap-independent translation initiation sites in eukaryotic cells. IRES elements have been applied as useful tools for bi-cistronic expression vectors. Current RNA structure prediction programs are unable to predict precisely the potential IRES element. We have designed a viral IRES prediction system (VIPS) to perform the IRES secondary struc...

Journal: :Journal of molecular biology 1999
J S Kieft K Zhou R Jubin M G Murray J Y Lau J A Doudna

Hepatitis C virus (HCV) contains an internal ribosome entry site (IRES) located in the 5' untranslated region of the genomic RNA that drives cap-independent initiation of translation of the viral message. The approximate secondary structure and minimum functional length of the HCV IRES are known, and extensive mutagenesis has established that nearly all secondary structural domains are critical...

2015
Maria Licursi Ricardo A. Carmona-Martinez Seyd Razavi Kensuke Hirasawa

Internal ribosome entry site (IRES)-mediated translation is an essential replication step for certain viruses. As IRES-mediated translation is regulated differently from cap-dependent translation under various cellular conditions, we sought to investigate whether temperature influences efficiency of viral IRES-mediated translation initiation by using bicistronic reporter constructs containing a...

2016
Craig H. Kerr Zi Wang Ma Christopher J. Jang Sunnie R. Thompson Eric Jan

The dicistrovirus Cricket Paralysis virus contains a unique dicistronic RNA genome arrangement, encoding two main open reading frames that are driven by distinct internal ribosome entry sites (IRES). The intergenic region (IGR) IRES adopts an unusual structure that directly recruits the ribosome and drives translation of viral structural proteins in a factor-independent manner. While structural...

2011
Upasana Ray Saumitra Das

HCV NS3 protein plays a central role in viral polyprotein processing and RNA replication. We demonstrate that the NS3 protease (NS3(pro)) domain alone can specifically bind to HCV-IRES RNA, predominantly in the SLIV region. The cleavage activity of the NS3 protease domain is reduced upon HCV-RNA binding. More importantly, NS3(pro) binding to the SLIV hinders the interaction of La protein, a cel...

Journal: :Journal of virology 2000
R Jubin N E Vantuno J S Kieft M G Murray J A Doudna J Y Lau B M Baroudy

The hepatitis C virus (HCV) internal ribosome entry site (IRES) is a highly structured RNA element that directs cap-independent translation of the viral polyprotein. Morpholino antisense oligonucleotides directed towards stem loop IIId drastically reduced HCV IRES activity. Mutagenesis studies of this region showed that the GGG triplet (nucleotides 266 through 268) of the hexanucleotide apical ...

Journal: :BMC Biotechnology 2006
Patrick Martin Olivier Albagli Marie Christine Poggi Kim E Boulukos Philippe Pognonec

BACKGROUND Internal Ribosome Entry Site (IRES)-based bicistronic vectors are important tools in today's cell biology. Among applications, the expression of two proteins under the control of a unique promoter permits the monitoring of expression of a protein whose biological function is being investigated through the observation of an easily detectable tracer, such as Green Fluorescent Protein (...

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