Literature DB >> 14692966

Evaluation of HTLV-I removal by filtration of blood cell components in a routine setting.

Raymond Césaire1, Brigitte Kérob-Bauchet, Olivier Bourdonné, Hélène Maier, Karim Ould Amar, Philippe Halbout, Axelle Dehée, Nathalie Désiré, Fabienne Dantin, Odile Béra, Agnès Lézin.   

Abstract

BACKGROUND: WBC depletion by filtration may prevent the transmission of HTLV-I, which requires cell-to-cell contact. The removal of HTLV-I-infected cells in routinely filtered blood cell components was measured. STUDY DESIGN AND METHODS: The study was conducted in Martinique where systematic screening for HTLV-I and -II and universal leukoreduction are mandatory. HTLV-I was quantified by use of real-time PCR in 8 RBC units and 4 PLT concentrates before and after filtration. HTLV-I proviral load in PBMNCs was determined in five of the eight HTLV-I-infected blood donors.
RESULTS: The amount of MNC-associated HTLV-I DNA in RBC units before filtration was 21 x 10(6)+/- 29 x 10(6) copies (mean +/- SD). HTLV-I was detected in 4 of 8 RBC units after filtration, with a number of copies in the MNC fraction ranging from 20 to 140, following a 4.9 to 5.8 log reduction. Flow cytometry analysis performed in 2 of the filtered RBC units containing detectable HTLV-I showed suboptimal and out-of-range leukoreduction (0.56 x 10(6) and 1.22 x 10(6) residual WBCs). HTLV was not detected in filtered RBCs from the blood donor with the highest percentage of HTLV-I-infected PBMCs (9%).
CONCLUSION: This study confirms that HTLV-I-infected cells can be detected in filtered blood cell components and shows that optimal leukoreduction is critical for HTLV-I removal.

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Year:  2004        PMID: 14692966     DOI: 10.1111/j.0041-1132.2004.00629.x

Source DB:  PubMed          Journal:  Transfusion        ISSN: 0041-1132            Impact factor:   3.157


  2 in total

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2.  Human T-lymphotropic virus in Irish blood donors: Impact on future testing strategy.

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Journal:  Transfusion       Date:  2022-07-13       Impact factor: 3.337

  2 in total

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