Difference: RodriguezCai07 (1 vs. 9)

Revision 929 Jun 2007 - Main.DavidCowburn

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Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, and Geacintov, N.E. 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 35 1555–1568 nyu.gif mskc.gif

The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and 5'-...CGG*C... sequence contexts in otherwise identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50- ... CGG*C... case, the 50-flanking G!C base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- ...CG*GC... context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- ...CGG*C.... Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 829 Jun 2007 - Main.DavidCowburn

 
META TOPICPARENT name="TmpPrints"
Changed:
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Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 35 1555–1568 nyu.gif mskc.gif
>
>
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, and Geacintov, N.E. 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 35 1555–1568 nyu.gif mskc.gif
  The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and 5'-...CGG*C... sequence contexts in otherwise identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50- ... CGG*C... case, the 50-flanking G!C base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- ...CG*GC... context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- ...CGG*C.... Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 712 Apr 2007 - Main.JasperShahn

 
META TOPICPARENT name="TmpPrints"
Changed:
<
<
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif
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>
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 35 1555–1568 nyu.gif mskc.gif
  The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and 5'-...CGG*C... sequence contexts in otherwise identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50- ... CGG*C... case, the 50-flanking G!C base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- ...CG*GC... context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- ...CGG*C.... Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 602 Mar 2007 - Main.JasperShahn

 
META TOPICPARENT name="TmpPrints"
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif
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<		 The environmental carcinogen benzo[a]pyrene (BP)
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>		 The environmental carcinogen benzo[a]pyrene (BP)
 is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and
Changed:
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<		5'-...CGG*C...qus sequence contexts in otherwise
>
>		5'-...CGG*C... sequence contexts in otherwise
 identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for
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<		placement of the BP. In the 50-  CGG*C case, the 50-flanking GC base pair is severely untwisted,
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>		placement of the BP. In the 50- ... CGG*C... case, the 50-flanking G!C base pair is severely untwisted,
 concomitant with a bend deduced from electrophoretic
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<		mobility. In the 50- CG*GC context,
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>		mobility. In the 50- ...CG*GC... context,
 there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the
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<		lesion in both cases, but more for 50- CGG*C.
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>		lesion in both cases, but more for 50- ...CGG*C....
 Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation
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<		hotspot phenomenon.
>
>		hotspot phenomenon.

Revision 528 Feb 2007 - Main.DavidCowburn

 
META TOPICPARENT name="TmpPrints"
Changed:
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<
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif
>
>
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif
  The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and 5'-...CGG*C...qus sequence contexts in otherwise identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50-  CGG*C case, the 50-flanking GC base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- CG*GC context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- CGG*C. Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 428 Feb 2007 - Main.DavidCowburn

 
META TOPICPARENT name="TmpPrints"
Changed:
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<		Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif
>
>
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif
  The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and 5'-...CGG*C...qus sequence contexts in otherwise identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50-  CGG*C case, the 50-flanking GC base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- CG*GC context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- CGG*C. Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 322 Feb 2007 - Main.DavidCowburn

 
META TOPICPARENT name="TmpPrints"
Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif

The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 5'- ...GG... dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 5'- ...CG*GC... and

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<		5'-...CGG*C...quence contexts in otherwise
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>		5'-...CGG*C...qus sequence contexts in otherwise
 identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50-  CGG*C case, the 50-flanking GC base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- CG*GC context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- CGG*C. Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 222 Feb 2007 - Main.DavidCowburn

 
META TOPICPARENT name="TmpPrints"
Deleted:
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 Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif

The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts

Changed:
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<		are frequently found in 50- GG dinucleotide
>
>		are frequently found in 5'- ...GG... dinucleotide
 sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences
Changed:
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<		in G* adduct conformations in 50- CG*GC and 50-  CGG*C sequence contexts in otherwise
>
>		in G* adduct conformations in 5'- ...CG*GC... and 5'-...CGG*C...quence contexts in otherwise
 identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50-  CGG*C case, the 50-flanking GC base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- CG*GC context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- CGG*C. Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

Revision 122 Feb 2007 - Main.DavidCowburn

 
META TOPICPARENT name="TmpPrints"

Rodriguez FA, Cai Y, Lin C, Tang Y, Kolbanovskiy A, Amin S, Patel DJ, Broyde S, ... 'Exocyclic amino groups of flanking guanines govern sequence-dependent adduct conformations and local structural distortions for minor groove-aligned benzo[a]pyrenyl-guanine lesions in a GG mutation hotspot context.' Nucleic Acids Res 2007 in press nyu.gif mskc.gif

The environmental carcinogen benzo[a]pyrene (BP) is metabolized to reactive diol epoxides that bind to cellular DNA by predominantly forming N2-guanine adducts (G*). Mutation hotspots for these adducts are frequently found in 50- GG dinucleotide sequences, but their origins are poorly understood. Here we used high resolution NMR and molecular dynamics simulations to investigate differences in G* adduct conformations in 50- CG*GC and 50-  CGG*C sequence contexts in otherwise identical 12-mer duplexes. The BP rings are positioned 50 along the modified strand in the minor groove in both cases. However, subtle orientational differences cause strong distinctions in structural distortions of the DNA duplexes, because the exocyclic amino groups of flanking guanines on both strands compete for space with the BP rings in the minor groove, acting as guideposts for placement of the BP. In the 50-  CGG*C case, the 50-flanking GC base pair is severely untwisted, concomitant with a bend deduced from electrophoretic mobility. In the 50- CG*GC context, there is no untwisting, but there is significant destabilization of the 50-flanking Watson–Crick base pair. The minor groove width opens near the lesion in both cases, but more for 50- CGG*C. Differential sequence-dependent removal rates of this lesion result and may contribute to the mutation hotspot phenomenon.

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