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Journal of Clinical Microbiology
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Virology

Dried-Plasma Transport Using a Novel Matrix and Collection System for Human Immunodeficiency Virus and Hepatitis C Virus Virologic Testing

R. M. Lloyd Jr., D. A. Burns, J. T. Huong, R. L. Mathis, M. A. Winters, M. Tanner, A. De La Rosa, B. Yen-Lieberman, W. Armstrong, A. Taege, D. R. McClernon, J. L. Wetshtein, Brian M. Friedrich, Monique R. Ferguson, William O'Brien, P. M. Feorino, M. Holodniy
R. M. Lloyd Jr.
1Research Think Tank, Inc., Buford, Georgia
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D. A. Burns
1Research Think Tank, Inc., Buford, Georgia
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J. T. Huong
1Research Think Tank, Inc., Buford, Georgia
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R. L. Mathis
1Research Think Tank, Inc., Buford, Georgia
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M. A. Winters
2VA Palo Alto Healthcare System, Palo Alto, California
3Division of Infectious Diseases and Geographic Medicine, Stanford University, Palo Alto, California
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M. Tanner
4Family HealthCare of Atlanta, Atlanta, Georgia
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A. De La Rosa
5Pharmasset, Inc., Princeton, New Jersey
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B. Yen-Lieberman
6Cleveland Clinic Foundation, Cleveland, Ohio
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W. Armstrong
6Cleveland Clinic Foundation, Cleveland, Ohio
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A. Taege
6Cleveland Clinic Foundation, Cleveland, Ohio
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D. R. McClernon
7McClernon LLC, Cary, North Carolina
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J. L. Wetshtein
1Research Think Tank, Inc., Buford, Georgia
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Brian M. Friedrich
8University of Texas Medical Branch, Galveston, Texas
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Monique R. Ferguson
8University of Texas Medical Branch, Galveston, Texas
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William O'Brien
9Zirus, Inc., Buford, Georgia
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P. M. Feorino
1Research Think Tank, Inc., Buford, Georgia
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M. Holodniy
2VA Palo Alto Healthcare System, Palo Alto, California
3Division of Infectious Diseases and Geographic Medicine, Stanford University, Palo Alto, California
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  • For correspondence: Holodniy@stanford.edu
DOI: 10.1128/JCM.02354-08
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ABSTRACT

A novel method for the collection and transportation of dried-blood-plasma samples, SampleTanker (ST), was developed and compared to standard shipping protocols for frozen-plasma specimens containing human immunodeficiency virus type 1 (HIV-1) and/or hepatitis C virus (HCV). Matched frozen and dried 1-ml EDTA-containing plasma samples were collected and analyzed by several molecular-based virologic assays. After addition of 1.175 ml of reconstitution buffer, 1.035 ml of dried plasma was recovered. Mean intra-assay variances were 0.05, 0.05, and 0.06 log10 copies/ml for the Versant, Amplicor, and NucliSens QT HIV-1 load assays, respectively (P, not significant). However, mean HIV-1 viral load was consistently reduced in dried samples by 0.32 to 0.51 log10 copies/ml, depending on assay type (P < 0.05). Infectious HIV-1 was not recovered from dried ST plasma. There was no significant difference in HIV-1 viral load results obtained using ST after 8 weeks of storage at ambient temperature. Compared to frozen plasma, HIV-1 genotypic results were >99% concordant at the nucleotide and amino acid levels, as well as for resistance-associated mutations. We further demonstrated successful detection of multiple analytes, including HIV-1 viral load, HIV-1 antiretroviral resistance genotype, and HCV genotype, from a single ST unit. Dried plasma collected with ST yielded comparable results to frozen samples for multiple-analyte clinical testing. As such, ST could be a useful alternative for virologic tests and clinical trials worldwide by significantly diminishing transportation cost and the sample volume restrictions associated with dried-blood-spot technology.

  • Copyright © 2009 American Society for Microbiology
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Dried-Plasma Transport Using a Novel Matrix and Collection System for Human Immunodeficiency Virus and Hepatitis C Virus Virologic Testing
R. M. Lloyd Jr., D. A. Burns, J. T. Huong, R. L. Mathis, M. A. Winters, M. Tanner, A. De La Rosa, B. Yen-Lieberman, W. Armstrong, A. Taege, D. R. McClernon, J. L. Wetshtein, Brian M. Friedrich, Monique R. Ferguson, William O'Brien, P. M. Feorino, M. Holodniy
Journal of Clinical Microbiology Apr 2009, 47 (5) 1491-1496; DOI: 10.1128/JCM.02354-08

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Dried-Plasma Transport Using a Novel Matrix and Collection System for Human Immunodeficiency Virus and Hepatitis C Virus Virologic Testing
R. M. Lloyd Jr., D. A. Burns, J. T. Huong, R. L. Mathis, M. A. Winters, M. Tanner, A. De La Rosa, B. Yen-Lieberman, W. Armstrong, A. Taege, D. R. McClernon, J. L. Wetshtein, Brian M. Friedrich, Monique R. Ferguson, William O'Brien, P. M. Feorino, M. Holodniy
Journal of Clinical Microbiology Apr 2009, 47 (5) 1491-1496; DOI: 10.1128/JCM.02354-08
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KEYWORDS

Desiccation
HIV
HIV Infections
Hepacivirus
hepatitis C
plasma
Specimen Handling

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