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PDBsum entry 2m8l
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Viral protein
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PDB id
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2m8l
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References listed in PDB file
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Key reference
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Title
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Structure and dynamics of full-Length HIV-1 capsid protein in solution.
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Authors
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L.Deshmukh,
C.D.Schwieters,
A.Grishaev,
R.Ghirlando,
J.L.Baber,
G.M.Clore.
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Ref.
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J Am Chem Soc, 2013,
135,
16133-16147.
[DOI no: ]
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PubMed id
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Abstract
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The HIV-1 capsid protein plays a crucial role in viral infectivity, assembling
into a cone that encloses the viral RNA. In the mature virion, the N-terminal
domain of the capsid protein forms hexameric and pentameric rings, while
C-terminal domain homodimers connect adjacent N-terminal domain rings to one
another. Structures of disulfide-linked hexamer and pentamer assemblies, as well
as structures of the isolated domains, have been solved previously. The dimer
configuration in C-terminal domain constructs differs in solution (residues
144-231) and crystal (residues 146-231) structures by ∼30°, and it has been
postulated that the former connects the hexamers while the latter links
pentamers to hexamers. Here we study the structure and dynamics of full-length
capsid protein in solution, comprising a mixture of monomeric and dimeric forms
in dynamic equilibrium, using ensemble simulated annealing driven by
experimental NMR residual dipolar couplings and X-ray scattering data. The
complexity of the system necessitated the development of a novel computational
framework that should be generally applicable to many other challenging systems
that currently escape structural characterization by standard application of
mainstream techniques of structural biology. We show that the orientation of the
C-terminal domains in dimeric full-length capsid and isolated C-terminal domain
constructs is the same in solution, and we obtain a quantitative description of
the conformational space sampled by the N-terminal domain relative to the
C-terminal domain on the nano- to millisecond time scale. The positional
distribution of the N-terminal domain relative to the C-terminal domain is large
and modulated by the oligomerization state of the C-terminal domain. We also
show that a model of the hexamer/pentamer assembly can be readily generated with
a single configuration of the C-terminal domain dimer, and that capsid assembly
likely proceeds via conformational selection of sparsely populated
configurations of the N-terminal domain within the capsid protein dimer.
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