Transfusion‐associated graft‐versus‐host disease reexamined: potential for improved prevention using a universally applied intervention

Kleinman, Steven; Stassinopoulos, Adonis

doi:10.1111/trf.14930

Cited by 33 publications

(26 citation statements)

References 96 publications

(266 reference statements)

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“…While this review focused on the inactivation of viruses and parasites, the amotosalen/UVA PRT has proven efficacy to prevent transfusion‐associated graft‐versus‐host disease and bacterial TTIs, the most significant infectious risk in transfusion today . PRT is now considered an alternative to bacterial screening, irradiation, and CMV testing .…”

Section: Discussionmentioning

confidence: 99%

Inactivation of a broad spectrum of viruses and parasites by photochemical treatment of plasma and platelets using amotosalen and ultraviolet A light

et al. 2020

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BACKGROUND The INTERCEPT Blood System pathogen reduction technology (PRT), which uses amotosalen and ultraviolet A light treatment (amotosalen/UV‐PRT), inactivates pathogens in plasma and platelet components (PCs). This review summarizes data describing the inactivation efficacy of amotosalen/UVA‐PRT for a broad spectrum of viruses and parasites. METHODS Twenty‐five enveloped viruses, six nonenveloped viruses (NEVs), and four parasites species were evaluated for sensitivity to amotosalen/UVA‐PRT. Pathogens were spiked into plasma and PC at high titers. Samples were collected before and after PRT and assessed for infectivity with cell cultures or animal models. Log reduction factors (LRFs) were defined as the difference in infectious titers before and after amotosalen/UV‐PRT. RESULTS LRFs of ≥4.0 log were reported for 19 pathogens in plasma (range, ≥4.0 to ≥7.6), 28 pathogens in PC in platelet additive solution (PC‐PAS; ≥4.1‐≥7.8), and 14 pathogens in PC in 100% plasma (PC‐100%; (≥4.3‐>8.4). Twenty‐five enveloped viruses and two NEVs were sensitive to amotosalen/UV‐PRT; LRF ranged from >2.9 to ≥7.6 in plasma, 2.4 or greater to greater than 6.9 in PC‐PAS and >3.5 to >6.5 in PC‐100%. Infectious titers for four parasites were reduced by >4.0 log in all PC and plasma (≥4.9 to >8.4). CONCLUSION Amotosalen/UVA‐PRT demonstrated effective infectious titer reduction for a broad spectrum of viruses and parasites. This confirms the capacity of this system to reduce the risk of viral and parasitic transfusion‐transmitted infections by plasma and PCs in various geographies.

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Section: Discussionmentioning

confidence: 99%

Inactivation of a broad spectrum of viruses and parasites by photochemical treatment of plasma and platelets using amotosalen and ultraviolet A light

et al. 2020

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“…Our studies indicate that the first round of filtration results in a 5 log reduction, and the following round is indicative of a further 3 log reduction. In contrast, gamma irradiation showed that the inactivation level of T cells resulted in a range of 3-6 log reduction [7]. Pathogen inactivation methods provided better rate of inactivation, being 6.2 log for amotosalen/UVA [39], 5.9 log for amustaline/GSH [7] or 4.7-6.5 for riboflavin/UV [20,40].…”

Section: Plos Onementioning

confidence: 93%

“…Removal of these cells before transfusion has been proposed to reduce the incidence of TA-GvHD, but reports of TA-GvHD after transfusion of leukoreduced blood components can be found in the literature [2][3][4]. Despite these reports being from many years ago, leukoreduction by filtration is generally not accepted as a method to sufficiently to prevent TA-GvHD [5,6] Irradiation disables T cells' mitotic capabilities and is currently the de facto golden standard method for full prevention of TA-GvHD, despite some incidences of TA-GvHD being reported after irradiation [7].…”

Section: Introductionmentioning

confidence: 99%

“…An investigation on whether a method is suitable to fully prevent whether it can fully prevent TA-GvHD is not possible; even the current method of gamma-ray irradiation has not been subject to any randomized clinical trial on this matter [7]. We relied on investigating the level of leukocytes left after two rounds of filtration, and compared that with data on the level of mononuclear cells required to show proliferation in vitro, or GvHD symtomes in vivo.…”

Section: Introductionmentioning

confidence: 99%

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Double-filtered leukoreduction as a method for risk reduction of transfusion-associated graft-versus-host disease

et al. 2020

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Background Transfusion-associated graft-versus-host disease (TA-GvHD) is caused by leukocytes, specifically T cells within a transfused blood product. Currently, the prevention of transfusionassociated graft-versus-host disease is performed by irradiation of blood products. With a sufficient reduction of leukocytes, the risk for TA-GvHD can be decreased. With consistent advances in current state-of-the-art blood filters, we herein propose that double filtration can sufficiently reduce leukocytes to reduce the risk for TA-GvHD. Materials Thirty RBC concentrates were filtered with leukocyte filters, followed by storage at 1-6 o C for 72 hours, and then a second filtration was performed. Residual leukocytes in the doublefiltered RBC units (n = 30) were assessed with flow cytometric methods, and an additional assay with isolated peripheral blood mononuclear cells (PBMCs) (n = 6) was done by both flow cytometric methods and an automated hematology analyzer. Quality of the RBCs after filtration was evaluated by hematological and biochemical tests. In vitro T cell expansion was performed using anti-CD3/CD28-coated Dynabeads or anti-CD3 (OKT3). In vivo experiment for GvHD was performed by using NOD.Cg-Prkdc scid Il2rg tm1Wjl /SzJ (NSG) mice. Results Double-filtered blood products showed residual leukocyte levels below detection limits, which calculated to be below 1200-2500 cells per blood unit. In vitro expansion rate of T cells showed that 6x10 3 and 1x10 3 cell-seeded specimens showed 60.8±10.6 fold and 10.2 ±9.7-fold expansion, respectively. Cell expansion was not sufficiently observed in wells

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“…Transfusion of nonleukoreduced blood products does carry risks including the rare but lethal complication of transfusionassociated graft versus host disease. 66,67 A 2015 review by Kopolovic et al found 348 all-time reported cases of graftversus-host disease. Conversely, there were over 200,000 trauma fatalities in 2017 in the United States alone, 68 and trauma patients receiving a blood transfusion have an odds ratio of mortality of 3.35 compared with those who do not receive a transfusion.…”

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confidence: 99%

The Evolution of Blood Transfusion in the Trauma Patient: Whole Blood Has Come Full Circle

Black

Pierce

Kerby

et al. 2019

Semin Thromb Hemost

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Whole blood transfusion in the United States dates back to the Civil War, and it was widely used in all major conflicts since World War I. To understand our current civilian transfusion practices and to anticipate future changes in trauma resuscitation, it is important to understand the series of decisions that led trauma surgeons away from whole blood resuscitation and toward component therapy. In this review, we examine the historical basis for blood transfusion in trauma and examine the recent literature and future directions pertaining to blood product resuscitation in hemorrhaging patients.

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Transfusion‐associated graft‐versus‐host disease reexamined: potential for improved prevention using a universally applied intervention

Cited by 33 publications

References 96 publications

Inactivation of a broad spectrum of viruses and parasites by photochemical treatment of plasma and platelets using amotosalen and ultraviolet A light

Inactivation of a broad spectrum of viruses and parasites by photochemical treatment of plasma and platelets using amotosalen and ultraviolet A light

Double-filtered leukoreduction as a method for risk reduction of transfusion-associated graft-versus-host disease

The Evolution of Blood Transfusion in the Trauma Patient: Whole Blood Has Come Full Circle

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