IDENTIFICATION OF THE PRIMER BINDING DOMAIN IN HUMAN-IMMUNODEFICIENCY-VIRUS REVERSE-TRANSCRIPTASE
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BASU, A
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UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103
BASU, A
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AHLUWALIA, KK
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UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103
AHLUWALIA, KK
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BASU, S
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UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103
BASU, S
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MODAK, MJ
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UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103
MODAK, MJ
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[1] UNIV MED & DENT NEW JERSEY,NEW JERSEY MED SCH,DEPT BIOCHEM & MOLEC BIOL,185 S ORANGE AVE,NEWARK,NJ 07103
We have labeled the primer binding domain of HIVI-RT with 5'-P-32-labeled (dT)15 primer using ultraviolet light energy. The specificity of the primer cross-linking to HIVI-RT was demonstrated by competition experiments. Both synthetic and natural primers, e.g., p(dA)15, p(dC)15, and tRNA(Lys), inhibit p(dT)15 binding and cross-linking to the enzyme. The observed binding and cross-linking of the primer to the enzyme were further shown to be functionally significant by the observation that tRNA(Lys) inhibits the polymerase activity on poly(rA)-(dT)15 template-primer as well as the cross-linking of p(dT)15 to the enzyme to a similar extent. At an enzyme to p(dT)15 ratio of 1:3, about 15% of the enzyme can be cross-linked to the primer. To identify the domain cross-linked to (dT)15, tryptic peptides were generated and purified by a combination of HPLC on a C-18 reverse-phase column and DEAE-Sephadex chromatography. A single peptide cross-linked to p(dT)15 was identified. This peptide corresponded to amino acid residues 288-307 in the primary sequence of HIV1 -RT as judged by amino acid composition and sequence analyses. Further, Leu(289)-Thr(290) and Leu(295)-Thr(296) of HIV1-RT appear to be the probable sites of cross-linking to the primer p(dT)15.
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
ARAYA, A
KEITH, G
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
KEITH, G
FOURNIER, M
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
FOURNIER, M
GANDAR, JC
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
GANDAR, JC
LABOUESSE, J
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
LABOUESSE, J
LITVAK, S
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
ARAYA, A
KEITH, G
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h-index: 0
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
KEITH, G
FOURNIER, M
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
FOURNIER, M
GANDAR, JC
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
GANDAR, JC
LABOUESSE, J
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CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE
LABOUESSE, J
LITVAK, S
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机构:
CNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCECNRS,INST BIOCHIM CELLULAIRE & NEUROCHIM,1 RUE CAMILLE ST SAENS,F-33000 BORDEAUX,FRANCE