These results suggest that DH012mu escapes the neutralizing antibodies
in chimpanzee serum at the expense of exposing the
V3 region. This
envelope change is not due to four consecutive
passages of DH012 in MT4
cells during the development of the neutralization-resistant
(data not shown). The
V3 region of gp120 was shown to be a key
). Despite the
apparent change in accessibility of the
change its chemokine
receptor usage (data not shown). Both DH012
and DH012mu can use either
CCR5 or CXCR4 to enter the cells. The
has been determined. Three
mutations were observed in the V1/V2,
bridging sheet, and V3 regions of
DH012mu. Although all three
data).
Baculovirus-expressed DH012 gp120 appears to be able to induce at least
two types of neutralizing antibodies. One of the neutralization
activity is not involved in the linear V3 epitope. The
neutralizing
virus are very potent and strain specific. Broadening of this
neutralization profile. This neutralizing antibody response might
be
induced with recombinant baculovirus gp120. However, the recombinant
wild-type DH012 virus. It is likely that the native structure
activity. Alternatively, it is possible that the
neutralization
sera.
Neutralization of HIV-1 primary isolates with anti-V3 antisera has been
demonstrated in a simian/human immunodeficiency virus
). The ability of V3-immune sera to neutralize the
virus
infection. On the contrary, the data presented here indicate that
varied among
HIV-1 primary isolates. Accessibility and sequence
This work was supported by NIH grant AI40856 (C.-H.C.).
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