Pathogen inactivation of <i>Leishmania donovani infantum</i> in plasma and platelet concentrates using riboflavin and ultraviolet light

Cardo, Lisa J.; Rentas, Francisco J.; Ketchum, Lloyd H.; Salata, Jeanne; Harman, Ronald; Melvin, William T.; Weina, Peter J.; Mendez, J.; Reddy, Heather L.; Goodrich, Raymond P.

doi:10.1111/j.1423-0410.2005.00736.x

Cited by 93 publications

(94 citation statements)

References 26 publications

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“…Multicenter trials by Cardo et al have shown the riboflavin method to be effective for killing Leishmania and other emerging plasma and platelet pathogens (5-7 log reduction). 6,7 Numerous studies have also confirmed this method to be effective for white blood cell inactivation. Clinical trials have proved the safety of Mirasol ® PRT system-treated blood components and lack of neoantigen formation.…”

Section: Introductionmentioning

confidence: 92%

Quality control of riboflavin-treated platelet concentrates using Mirasol® PRT system: Polish experience

Lachert¹,

Kubis²,

Antoniewicz‐Papis³

et al. 2018

Adv Clin Exp Med

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Section: Introductionmentioning

confidence: 92%

Quality control of riboflavin-treated platelet concentrates using Mirasol® PRT system: Polish experience

Lachert¹,

Kubis²,

Antoniewicz‐Papis³

et al. 2018

Adv Clin Exp Med

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“…Using riboflavin as a photosensitizer, in combination with UV light, has been shown to reduce the infectivity of a broad range of pathogenic blood-borne contaminants, including bacteria 3,4,8,10,[19][20][21] .The use of riboflavin and UV light for pathogen reduction is non-toxic and non-mutagenic, and riboflavin and UV light-treated components have been shown to be safe for transfusion recipients as well as for those handling blood products 18 . Briefly, riboflavin molecules can associate with the nucleic acids (DNA and RNA) of bacteria, parasites, viruses and any nucleated cell (e.g.…”

Section: Introductionmentioning

confidence: 99%

Treatment of Platelet Products with Riboflavin and UV Light: Effectiveness Against High Titer Bacterial Contamination

Keil

Hovenga

Gilmour

et al. 2015

JoVE

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Contamination of platelet units by bacteria has long been acknowledged as a significant transfusion risk due to their post-donation storage conditions. Products are routinely stored at 22 °C on an agitating shaker, a condition that can promote bacterial growth. Although the total number of bacteria believed to be introduced into a platelet product is extremely low, these bacteria can multiply to a very high titer prior to transfusion, potentially resulting in serious adverse events. The aim of this study was to evaluate a riboflavin based pathogen reduction process against a panel of bacteria that have been identified as common contaminants of platelet products. This panel included the following organisms: S. epidermidis, S. aureus, S. mitis, S. pyogenes, S. marcescens, Y. enterocolitica, B. neotomae, B. cereus, E. coli, P. aeruginosa and K. pneumoniae. Each platelet unit was inoculated with a high bacterial load and samples were removed both before and after treatment. A colony forming assay, using an end point dilution scheme, was used to determine the pre-treatment and post-treatment bacterial titers. Log reduction was calculated by subtracting the post-treatment titer from the pre-treatment titer. The following log reductions were observed: S. epidermidis 4.7 log (99.998%), S. aureus 4.8 log (99.998%), S. mitis 3.7 log (99.98%), S. pyogenes 2.6 log (99.7%), S. marcescens 4.0 log (99.99%), Y. enterocolitica 3.3 log (99.95%), B. neotomae 5.4 log (99.9996%), B. cereus 2.6 log (99.7%), E. coli ≥5.4 log (99.9996%), P. aeruginosa 4.7 log (99.998%) and K. pneumoniae 2.8 log (99.8%). The results from this study suggest the process could help to lower the risk of severe adverse transfusion events associated with bacterial contamination.

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“…Recently, using in vitro experiments several methods designed to inactivate Leishmania in blood products have been tested. These include the use of riboflavin (as a photosensitizer) and ultraviolet light [105], and the photochemical treatment by amotosalen plus ultraviolet light in platelet concentrates [106,107] as well as by thiopyrylium in RBC suspensions [108].…”

Section: Preventionmentioning

confidence: 99%

“…As a result of these photochemical processes, pathogens in blood products are rendered unable to replicate due to nucleic acid modification. This technology exploits the absence of nucleic acids in all the blood components (including plasma and platelet concentrates), which are beneficial to transfusion, and that instead is present in the parasite [105,109].…”

Section: Preventionmentioning

confidence: 99%

Transfusion transmitted leishmaniasis. What to do with blood donors from endemic areas?

Mansueto

Seidita

Vitale

2014

Travel Medicine and Infectious Disease

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Summary Leishmaniasis clinical spectrum ranges from cryptic infection to fatal visceral leishmaniasis. Cryptic infection can be found in blood donors from areas endemic for leishmaniasis all over the world. Although leishmaniasis is a classic vector-borne disease, cases of transfusion transmitted leishmaniasis have been reported especially in nonendemic areas. Most of these cases regarded infants or children. This paper reviews the literature on this specific feature and the impact of leishmaniasis on transfusion medicine. Relevant literature was found through PubMed. The reference lists of selected articles identified further sources. Conclusions: Blood donations by emigrants or travelers from endemic areas require special attention. Routine diagnostic methods should be implemented in blood banks to exclude donors that are positive for Leishmania, and individuals who suffered from visceral leishmaniasis should be prohibited from donating blood. The use of leukodepletion filters at the time of collection should be recommended in at-risk areas especially for high-risk recipients. ª

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Pathogen inactivation of Leishmania donovani infantum in plasma and platelet concentrates using riboflavin and ultraviolet light

Cited by 93 publications

References 26 publications

Quality control of riboflavin-treated platelet concentrates using Mirasol® PRT system: Polish experience

Quality control of riboflavin-treated platelet concentrates using Mirasol® PRT system: Polish experience

Treatment of Platelet Products with Riboflavin and UV Light: Effectiveness Against High Titer Bacterial Contamination

Transfusion transmitted leishmaniasis. What to do with blood donors from endemic areas?

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