The Perioperative Lung Transplant Virome: Torque Teno Viruses Are Elevated in Donor Lungs and Show Divergent Dynamics in Primary Graft Dysfunction

Abbas, Arwa; Diamond, Joshua M.; Chehoud, Christel; Chang, B.; Kotzin, Jonathan J.; Young, J. C.; Imai, Ize; Haas, Andrew R.; Cantu, Edward; Lederer, David J.; Meyer, Keith C.; Milewski, Rita K.; Olthoff, Kim M.; Shaked, Abraham; Christie, Jason D.; Bushman, Frederic D.; Collman, Ronald G.

doi:10.1111/ajt.14076

Cited by 99 publications

(96 citation statements)

References 75 publications

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“…Linkeramplified shotgun library (LASL) was applied for virus sequencing from marine water samples [8]. The anchored random PCR approach, as used in our study, has been frequently used and described in detail in previous studies [16,[36][37][38][39][40][41][42].…”

Section: Introductionmentioning

confidence: 99%

Optimization and validation of sample preparation for metagenomic sequencing of viruses in clinical samples

et al. 2017

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BackgroundSequence-specific PCR is the most common approach for virus identification in diagnostic laboratories. However, as specific PCR only detects pre-defined targets, novel virus strains or viruses not included in routine test panels will be missed. Recently, advances in high-throughput sequencing allow for virus-sequence-independent identification of entire virus populations in clinical samples, yet standardized protocols are needed to allow broad application in clinical diagnostics. Here, we describe a comprehensive sample preparation protocol for high-throughput metagenomic virus sequencing using random amplification of total nucleic acids from clinical samples.ResultsIn order to optimize metagenomic sequencing for application in virus diagnostics, we tested different enrichment and amplification procedures on plasma samples spiked with RNA and DNA viruses. A protocol including filtration, nuclease digestion, and random amplification of RNA and DNA in separate reactions provided the best results, allowing reliable recovery of viral genomes and a good correlation of the relative number of sequencing reads with the virus input. We further validated our method by sequencing a multiplexed viral pathogen reagent containing a range of human viruses from different virus families. Our method proved successful in detecting the majority of the included viruses with high read numbers and compared well to other protocols in the field validated against the same reference reagent. Our sequencing protocol does work not only with plasma but also with other clinical samples such as urine and throat swabs.ConclusionsThe workflow for virus metagenomic sequencing that we established proved successful in detecting a variety of viruses in different clinical samples. Our protocol supplements existing virus-specific detection strategies providing opportunities to identify atypical and novel viruses commonly not accounted for in routine diagnostic panels.Electronic supplementary materialThe online version of this article (doi:10.1186/s40168-017-0317-z) contains supplementary material, which is available to authorized users.

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Section: Introductionmentioning

confidence: 99%

Optimization and validation of sample preparation for metagenomic sequencing of viruses in clinical samples

et al. 2017

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“…15 Patients who developed PGD after lung transplantation underwent a smaller increase in anellovirus levels from before to after transplant, as compared to non-PGD controls (P = .0026). 27 In another study of lung transplant recipients, alphatorquevirus levels assessed prior to the diagnosis of CLAD were significantly lower in patients who subsequently developed CLAD (P = .020). 17 While no association between alphatorqueviruses and CLAD (defined in the current analysis as either BO or BOS) was established in the current study, the different results may be due to differences in the cohorts or in the timing of the samples tested.…”

Section: Discussionmentioning

confidence: 93%

“…Low blood anellovirus loads were reported in heart transplant recipients with moderate‐to‐severe graft rejection, as compared to non‐rejecting patients ( P = .011) . Patients who developed PGD after lung transplantation underwent a smaller increase in anellovirus levels from before to after transplant, as compared to non‐PGD controls ( P = .0026) . In another study of lung transplant recipients, alphatorquevirus levels assessed prior to the diagnosis of CLAD were significantly lower in patients who subsequently developed CLAD ( P = .020) .…”

Section: Discussionmentioning

confidence: 98%

Anellovirus loads are associated with outcomes in pediatric lung transplantation

Blatter

Sweet

Conrad

et al. 2017

Pediatric Transplantation

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Anelloviruses are DNA viruses ubiquitously present in human blood. Due to their elevated levels in immunosuppressed patients, anellovirus levels have been proposed as a marker of immune status. We hypothesized that low anellovirus levels, reflecting relative immunocompetence, would be associated with adverse outcomes in pediatric lung transplantation. We assayed blood samples from 57 patients in a multicenter study for alpha- and betatorquevirus, two anellovirus genera. The primary short-term outcome of interest was acute rejection, and longer-term outcomes were analyzed individually and as "composite" (death, chronic rejection, or retransplant within 2 years). Patients with low alphatorquevirus levels at 2 weeks post-transplantation were more likely to develop acute rejection within 3 months after transplant (P = .013). Low betatorquevirus levels at 6 weeks and 6 months after transplant were associated with death (P = .047) and the composite outcome (P = .017), respectively. There was an association between low anellovirus levels and adverse outcomes in pediatric lung transplantation. Alphatorquevirus levels were associated with short-term outcomes (ie, acute rejection), while betatorquevirus levels were associated with longer-term outcomes (ie, death, or composite outcome within 2 years). These observations suggest that anelloviruses may serve as useful biomarkers of immune status and predictors of adverse outcomes.

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“…The prevalence of each microbe in each respiratory sample was described using 2 criteria: abundance relative to other microbes in the same sample, wherein we normalized sequencing reads per million total sequencing reads (rpm), and (2) abundance relative to the same microbe in other samples in the cohort, wherein we normalized sequencing reads as the number of standard deviations above or below the mean log 10 -transformed rpm for the total cohort (Z-score). Given the anticipated wide array of respiratory bacteria and the paucity of knowledge regarding the significance of low-level viruses and fungi, we aimed to maximize specificity for bacterial pathogens and to maximize sensitivity for viral and fungal pathogens [15,23,24]. Therefore, we defined microbial outliers as those with Z-score ≥2 and ≥10 rpm (bacteria) or ≥1 rpm (viruses/fungi).…”

Section: Resultsmentioning

confidence: 99%

Pulmonary Metagenomic Sequencing Suggests Missed Infections in Immunocompromised Children

Zinter

Dvorak

Mayday

et al. 2018

Clinical Infectious Diseases

123

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An optimized mNGS assay for pulmonary microbes demonstrates significant inoculation of the lower airways of immunocompromised children with diverse bacteria, fungi, and viruses. Potential pathogens can be identified based on absolute and relative abundance. Ongoing investigation is needed to determine the pathogenic significance of outlier microbes in the lungs of immunocompromised children with pulmonary disease.

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The Perioperative Lung Transplant Virome: Torque Teno Viruses Are Elevated in Donor Lungs and Show Divergent Dynamics in Primary Graft Dysfunction

Cited by 99 publications

References 75 publications

Optimization and validation of sample preparation for metagenomic sequencing of viruses in clinical samples

Optimization and validation of sample preparation for metagenomic sequencing of viruses in clinical samples

Anellovirus loads are associated with outcomes in pediatric lung transplantation

Pulmonary Metagenomic Sequencing Suggests Missed Infections in Immunocompromised Children

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