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- [6] DESIGN, ACTIVITY, AND 2.8 A CRYSTAL-STRUCTURE OF A C2 SYMMETRICAL INHIBITOR COMPLEXED TO HIV-1 PROTEASE[J]. SCIENCE, 1990, 249 (4968) : 527 - 533ERICKSON, JNEIDHART, DJVANDRIE, JKEMPF, DJWANG, XCNORBECK, DWPLATTNER, JJRITTENHOUSE, JWTURON, MWIDEBURG, NKOHLBRENNER, WESIMMER, RHELFRICH, RPAUL, DAKNIGGE, M
- [7] HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 POL GENE-MUTATIONS WHICH CAUSE DECREASED SUSCEPTIBILITY TO 2',3'-DIDEOXYCYTIDINE[J]. ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1992, 36 (01) : 153 - 157FITZGIBBON, JEHOWELL, RMHABERZETTL, CASPERBER, SJGOCKE, DJDUBIN, DT
- [8] PCR AMPLIFICATION OF HIV-1 PROTEINASE SEQUENCES DIRECTLY FROM LAB ISOLATES ALLOWS DETERMINATION OF 5 CONSERVED DOMAINS[J]. VIROLOGY, 1992, 190 (01) : 1 - 10FONTENOT, GJOHNSTON, KCOHEN, JCGALLAHER, WRROBINSON, JLUFTIG, RB
- [9] DIFFERENT REQUIREMENTS FOR PRODUCTIVE INTERACTION BETWEEN THE ACTIVE-SITE OF HIV-1 PROTEINASE AND SUBSTRATES CONTAINING -HYDROPHOBIC-ASTERISK HYDROPHOBIC- OR -AROMATIC-ASTERISK PRO- CLEAVAGE SITES[J]. BIOCHEMISTRY, 1992, 31 (22) : 5193 - 5200GRIFFITHS, JTPHYLIP, LHKONVALINKA, JSTROP, PGUSTCHINA, AWLODAWER, ADAVENPORT, RJBRIGGS, RDUNN, BMKAY, J
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