Analysis of HIV-1 replication block due to substitutions at F61 residue of reverse transcriptase reveals additional defects involving the RNase H function - Test2 - elhamkhani - TriplyDB

Analysis of HIV-1 replication block due to substitutions at F61 residue of reverse transcriptase reveals additional defects involving the RNase H function

Analysis of HIV-1 replication block due to substitutions at F61 residue of reverse transcriptase reveals additional defects involving the RNase H function

http://www.wikidata.org/entity/Q34658171

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RNase H activity: structure, specificity, and function in reverse transcription Ribonuclease H: properties, substrate specificity and roles in retroviral reverse transcription Substitution of alanine for tyrosine-64 in the fingers subdomain of M-MuLV reverse transcriptase impairs strand displacement synthesis and blocks viral replication in vivo.Mutations M184V and Y115F in HIV-1 reverse transcriptase discriminate against "nucleotide-competing reverse transcriptase inhibitors".Preferred sequences within a defined cleavage window specify DNA 3' end-directed cleavages by retroviral RNases H Mutation rates and intrinsic fidelity of retroviral reverse transcriptases.HIV-1 Reverse Transcriptase Polymerase and RNase H (Ribonuclease H) Active Sites Work Simultaneously and Independently.LEDGF/p75 Deficiency Increases Deletions at the HIV-1 cDNA Ends.Thermostable HIV-1 group O reverse transcriptase variants with the same fidelity as murine leukaemia virus reverse transcriptase.Discovery of a semi-synthesized cyclolignan as a potent HIV-1 non-nucleoside reverse transcriptase inhibitor.

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P2860

Analysis of HIV-1 replication block due to substitutions at F61 residue of reverse transcriptase reveals additional defects involving the RNase H function

http://www.wikidata.org/entity/Q34658171

description

2006 nî lūn-bûn

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2006 թուականի Մայիսին հրատարակուած գիտական յօդուած

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2006 թվականի մայիսին հրատարակված գիտական հոդված

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2006年の論文

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2006年論文

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2006年論文

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2006年論文

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2006年論文

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2006年論文

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2006年论文

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name

Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Analysis of HIV-1 replication ...... involving the RNase H function

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Dibyakanti Mandal

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Stuart F J Le Grice

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P2860

Structure of a covalently trapped catalytic complex of HIV-1 reverse transcriptase: implications for drug resistance

HIV-1 nucleocapsid protein and replication protein A influence the strand displacement DNA synthesis of lentiviral reverse transcriptase

A second origin of DNA plus-strand synthesis is required for optimal human immunodeficiency virus replication

Detection of replication-competent and pseudotyped human immunodeficiency virus with a sensitive cell line on the basis of activation of an integrated beta-galactosidase gene

Structural alterations in the DNA ahead of the primer terminus during displacement synthesis by reverse transcriptases.

Effect of polypurine tract (PPT) mutations on human immunodeficiency virus type 1 replication: a virus with a completely randomized PPT retains low infectivity.

Replication of phenotypically mixed human immunodeficiency virus type 1 virions containing catalytically active and catalytically inactive reverse transcriptase.

Linker insertion mutagenesis of the human immunodeficiency virus reverse transcriptase expressed in bacteria: definition of the minimal polymerase domain.

Role of the non-homologous DNA end joining pathway in the early steps of retroviral infection.

Specific cleavages by RNase H facilitate initiation of plus-strand RNA synthesis by Moloney murine leukemia virus.

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10.1093/NAR/GKL360

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10

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34

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Vinayaka R. Prasad

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