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sivsm quasispecies adaptation to a new simian hostsivsm准物种适应新猴主人
SIVsm Quasispecies Adaptation to a New
Simian Host
1¤a 1¤b 1 2¤c 2*
Linda J. Demma , John M. Logsdon, Jr. , Thomas H. Vanderford , Mark B. Feinberg , Silvija I. Staprans
1 Department of Biology, Emory University, Atlanta, Georgia, United States of America, 2 Departments of Medicine and Microbiology and Immunology, and Emory Vaccine
Center, Emory University School of Medicine, Atlanta, Georgia, United States of America
Despite the potential for infectious agents harbored by other species to become emerging human pathogens, little is
known about why some agents establish successful cross-species transmission, while others do not. The simian
immunodeficiency viruses (SIVs), certain variants of which gave rise to the human HIV-1 and HIV-2 epidemics, have
demonstrated tremendous success in infecting new host species, both simian and human. SIVsm from sooty
mangabeys appears to have infected humans on several occasions, and was readily transmitted to nonnatural Asian
macaque species, providing animal models of AIDS. Here we describe the first in-depth analysis of the tremendous
SIVsm quasispecies sequence variation harbored by individual sooty mangabeys, and how this diverse quasispecies
adapts to two different host species—new nonnatural rhesus macaque hosts and natural sooty mangabey hosts. Viral
adaptation to rhesus macaques was associated with the immediate amplification of a phylogenetically related subset
of envelope (env) variants. These variants contained a shorter variable region 1 loop and lacked two specific
glycosylation sites, which may be selected for during acute infection. In contrast, transfer of SIVsm to its natural host
did not subject
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