Nucleic acid testing: the US approach

doi:10.1017/CBO9780511545245.019

15 - Nucleic acid testing: the US approach

from Section 2 - Selection and testing

Published online by Cambridge University Press: 12 January 2010

Susan L. Stramer

Edited by

John A. J. Barbara ,

Fiona A. M. Regan and

Marcela Contreras

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Susan L. Stramer: Affiliation:
Executive Scientific Officer, American Red Cross, Gaithersburg, MD, USA
John A. J. Barbara: Affiliation:
University of the West of England, Bristol
Fiona A. M. Regan: Affiliation:
HNSBT and Hammersmith Hospitals NHS Trust, London
Marcela Contreras: Affiliation:
University of the West of England, Bristol

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Summary

The central goal of blood centres is to provide a safe, adequate and effective blood supply. Towards that end, the focus on infectious disease testing has resulted in a high level of blood component safety. Today, in the developed world, the risk of transfusion-transmission of a major agent has been dramatically reduced by the introduction of next generation tests for antibodies and antigens, and with the introduction of nucleic acid testing (NAT). In the USA, with the introduction of NAT, the residual risk of HIV-1 and HCV has been reduced to approximately 1:2,000,000 donations screened (Dodd and Stramer, 2000). The yield of HIV-1 infected donors detected by NAT has been reported at 1:3.1 million and that for HCV (relative to third-generation antibody screening) at 1:270,000 (Stramer et al., 2004). The low frequency of these findings reinforces the safety of the blood supply today. In addition, the specificity of HIV-1 and HCV NAT relative to providing a false-positive result to a blood donor has been exceedingly high, with lower false-positive rates than any of the serological tests used in blood donor screening (e.g. 1:40,000 for NAT for the American Red Cross, ARC).

In addition to recipient safety, another aspect of the blood donation testing process is that it serves a public health function in identifying those individuals who are infected by a disease agent, particularly at the time shortly following exposure.

Type: Chapter
Information: Transfusion Microbiology , pp. 203 - 208

DOI: https://doi.org/10.1017/CBO9780511545245.019 [Opens in a new window]

Publisher: Cambridge University Press

Print publication year: 2008

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References

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