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Human immunodeficiency virus type-1 reverse transcriptase and ribonuclease h as substrates of the viral protease 下载免费PDF全文
Alfredo G. Tomasselli Jean L. Sarcich Linda J. Barrett Ilene M. Reardon W. Jeffrey Howe David B. Evans Satish K. Sharma Robert L. Heinrikson 《Protein science : a publication of the Protein Society》1993,2(12):2167-2176
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Yasuyuki Miyazaki Eric L. Garcia Steven R. King Kilali Iyalla Patrice Starck Alice Telesnitsky Michael F. Summers 《Journal of molecular biology》2010,396(1):141-633
Retroviruses selectively package two copies of their RNA genomes via mechanisms that have yet to be fully deciphered. Recent studies with small fragments of the Moloney murine leukemia virus (MoMuLV) genome suggested that selection may be mediated by an RNA switch mechanism, in which conserved UCUG elements that are sequestered by base-pairing in the monomeric RNA become exposed upon dimerization to allow binding to the cognate nucleocapsid (NC) domains of the viral Gag proteins. Here we show that a large fragment of the MoMuLV 5′ untranslated region that contains all residues necessary for efficient RNA packaging (ΨWT; residues 147-623) also exhibits a dimerization-dependent affinity for NC, with the native dimer ([ΨWT]2) binding 12 ± 2 NC molecules with high affinity (Kd = 17 ± 7 nM) and with the monomer, stabilized by substitution of dimer-promoting loop residues with hairpin-stabilizing sequences (ΨM), binding 1-2 NC molecules. Identical dimer-inhibiting mutations in MoMuLV-based vectors significantly inhibit genome packaging in vivo (∼ 100-fold decrease), whereas a large deletion of nearly 200 nucleotides just upstream of the gag start codon has minimal effects. Our findings support the proposed RNA switch mechanism and further suggest that virus assembly may be initiated by a complex comprising as few as 12 Gag molecules bound to a dimeric packaging signal. 相似文献
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