4.6 Article

High Specific Infectivity of Plasma Virus from the Pre-Ramp-Up and Ramp-Up Stages of Acute Simian Immunodeficiency Virus Infection

Journal

JOURNAL OF VIROLOGY
Volume 83, Issue 7, Pages 3288-3297

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/JVI.02423-08

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Funding

  1. National Center for Research Resources [U51R R00169]
  2. National Institute of Allergy and Infectious Diseases [P01 AI066314]
  3. James B. Pendleton Charitable Trust
  4. National Cancer Institute, National Institutes of Health [NO1-CO-124000, HHSN266200400088C]

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To define the ratio of simian immunodeficiency virus (SIV) RNA molecules to infectious virions in plasma, a ramp-up-stage plasma pool was made from the earliest viral RNA (vRNA)-positive plasma samples (collected approximately 7 days after inoculation) from seven macaques, and a set-point-stage plasma pool was made from plasma samples collected 10 to 16 weeks after peak viremia from seven macaques; vRNA levels in these plasma pools were determined, and serial 10-fold dilutions containing 1 to 1,500 vRNA copies/ml were made. Intravenous (i.v.) inoculation of a 1-ml aliquot of diluted ramp-up-stage plasma containing 20 vRNA copies infected 2 of 2 rhesus macaques, while for the set-point-stage plasma, i.v. inoculation with 1,500 vRNA copies was needed to transmit infection. Further, when the heat-inactivated set-point-stage plasma pool was mixed with ramp-up-stage virions, infection of inoculated macaques was blocked. Notably, 2 of 2 animals inoculated with 85 ml of a pre-ramp-up plasma pool containing < 3 SIV RNA copies/ml developed SIV infections characterized by high levels of viral replication, demonstrating that vRNA-negative plasma collected from macaques in the pre-ramp-up stage is infectious. Furthermore, there is a high ratio of infectious virions to total virions in ramp-up-stage plasma (between 1: 1 and 1: 10) and a lower ratio in set-point-stage plasma (between 1: 75 and 1: 750). Heat-inactivated chronic-stage plasma can neutralize the highly infectious ramp-up-stage virions. These findings have implications for the understanding of the natural history of SIV and human immunodeficiency virus infection and transmission.

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