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1. MNK-driven eIF4E phosphorylation regulates the fibrogenic transformation of mesenchymal cells and chronic lung allograft dysfunction

Author

Walker, Natalie M., Ibuki, Yuta, McLinden, A. Patrick, Misumi, Keizo, Mitchell, Dylan C., Kleer, Gabriel G., Lock, Alison M., Vittal, Ragini, Sonenberg, Nahum, Garner, Amanda L., and Lama, Vibha N.

Subjects
Fibrosis -- Diagnosis -- Care and treatment, Enzyme inhibitors -- Testing, Graft versus host reaction -- Diagnosis -- Care and treatment, Cellular signal transduction -- Health aspects
Abstract

Tissue fibrosis remains unamenable to meaningful therapeutic interventions and is the primary cause of chronic graft failure after organ transplantation. Eukaryotic translation initiation factor (eIF4E), a key translational regulator, serves as convergent target of multiple upstream profibrotic signaling pathways that contribute to mesenchymal cell (MC) activation. Here, we investigate the role of MAP kinase-interacting serine/threonine kinase-induced (MNK-induced) direct phosphorylation of eIF4E at serine 209 (Ser209) in maintaining fibrotic transformation of MCs and determine the contribution of the MNK/ eIF4E pathway to the pathogenesis of chronic lung allograft dysfunction (CLAD). MCs from patients with CLAD demonstrated constitutively higher eIF4E phosphorylation at Ser209, and eIF4E phospho-Ser209 was found to be critical in regulating key fibrogenic protein autotaxin, leading to sustained p-catenin activation and profibrotic functions of CLAD MCs. MNK1 signaling was upregulated in CLAD MCs, and genetic or pharmacologic targeting of MNK1 activity inhibited eIF4E phospho- Ser209 and profibrotic functions of CLAD MCs in vitro. Treatment with an MNK1/2 inhibitor (eFT-508) abrogated allograft fibrosis in an orthotopic murine lung-transplant model. Together these studies identify what we believe is a previously unrecognized MNK/ eIF4E/ATX/[beta]-catenin signaling pathway of fibrotic transformation of MCs and present the first evidence, to our knowledge, for the utility of MNK inhibitors in fibrosis., Introduction Lung transplantation has the worst long-term prognosis among all solid-organ transplantations, with a 10-year survival of only 20% (1). The major cause of these poor long-term outcomes is progressive [...]

Published
2024
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3. Development and validation of primary graft dysfunction predictive algorithm for lung transplant candidates

Author

Diamond, Joshua M., Anderson, Michaela R., Cantu, Edward, Clausen, Emily S., Shashaty, Michael G.S., Kalman, Laurel, Oyster, Michelle, Crespo, Maria M., Bermudez, Christian A., Benvenuto, Luke, Palmer, Scott M., Snyder, Laurie D., Hartwig, Matthew G., Wille, Keith, Hage, Chadi, McDyer, John F., Merlo, Christian A., Shah, Pali D., Orens, Jonathan B., Dhillon, Ghundeep S., Lama, Vibha N., Patel, Mrunal G., Singer, Jonathan P., Hachem, Ramsey R., Michelson, Andrew P., Hsu, Jesse, Russell Localio, A., and Christie, Jason D.

Published
2024
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5. Defibrotide Therapy for SARS-CoV-2 ARDS

Author

Frame, David, Scappaticci, Gianni B., Braun, Thomas M., Maliarik, Mary, Sisson, Thomas H., Pipe, Steven W., Lawrence, Daniel A., Richardson, Paul G., Holinstat, Michael, Hyzy, Robert C., Kaul, Daniel R., Gregg, Kevin S., Lama, Vibha N., and Yanik, Gregory A.

Published
2022
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7. Quantitative Evidence for Revising the Definition of Primary Graft Dysfunction after Lung Transplant

Author

Cantu, Edward, Diamond, Joshua M, Suzuki, Yoshikazu, Lasky, Jared, Schaufler, Christian, Lim, Brian, Shah, Rupal, Porteous, Mary, Lederer, David J, Kawut, Steven M, Palmer, Scott M, Snyder, Laurie D, Hartwig, Matthew G, Lama, Vibha N, Bhorade, Sangeeta, Bermudez, Christian, Crespo, Maria, McDyer, John, Wille, Keith, Orens, Jonathan, Shah, Pali D, Weinacker, Ann, Weill, David, Wilkes, David, Roe, David, Hage, Chadi, Ware, Lorraine B, Bellamy, Scarlett L, and Christie, Jason D

Subjects
Transplantation, Acute Respiratory Distress Syndrome, Rare Diseases, Organ Transplantation, Lung, Good Health and Well Being, Adult, Biomarkers, Cause of Death, Cohort Studies, Consensus, Female, Graft Rejection, Graft Survival, Humans, Kaplan-Meier Estimate, Logistic Models, Lung Transplantation, Male, Middle Aged, Primary Graft Dysfunction, Proportional Hazards Models, Reproducibility of Results, Retrospective Studies, Risk Assessment, Severity of Illness Index, Survival Rate, Time Factors, United States, Young Adult, Lung Transplant Outcomes Group, lung transplant, lung transplant outcomes, primary graft dysfunction, Medical and Health Sciences, Respiratory System
Abstract

RationalePrimary graft dysfunction (PGD) is a form of acute lung injury that occurs after lung transplantation. The definition of PGD was standardized in 2005. Since that time, clinical practice has evolved, and this definition is increasingly used as a primary endpoint for clinical trials; therefore, validation is warranted.ObjectivesWe sought to determine whether refinements to the 2005 consensus definition could further improve construct validity.MethodsData from the Lung Transplant Outcomes Group multicenter cohort were used to compare variations on the PGD definition, including alternate oxygenation thresholds, inclusion of additional severity groups, and effects of procedure type and mechanical ventilation. Convergent and divergent validity were compared for mortality prediction and concurrent lung injury biomarker discrimination.Measurements and main resultsA total of 1,179 subjects from 10 centers were enrolled from 2007 to 2012. Median length of follow-up was 4 years (interquartile range = 2.4-5.9). No mortality differences were noted between no PGD (grade 0) and mild PGD (grade 1). Significantly better mortality discrimination was evident for all definitions using later time points (48, 72, or 48-72 hours; P

Published
2018

10. Clinical Risk Factors and Prognostic Model for Primary Graft Dysfunction after Lung Transplantation in Patients with Pulmonary Hypertension.

Author

Porteous, Mary K, Lee, James C, Lederer, David J, Palmer, Scott M, Cantu, Edward, Shah, Rupal J, Bellamy, Scarlett L, Lama, Vibha N, Bhorade, Sangeeta M, Crespo, Maria M, McDyer, John F, Wille, Keith M, Localio, A Russell, Orens, Jonathan B, Shah, Pali D, Weinacker, Ann B, Arcasoy, Selim, Wilkes, David S, Ware, Lorraine B, Christie, Jason D, Kawut, Steven M, Diamond, Joshua M, and Lung Transplant Outcomes Group

Subjects
Lung Transplant Outcomes Group, Lung, Humans, Hypertension, Pulmonary, Obesity, Body Mass Index, Prognosis, Lung Transplantation, Linear Models, Logistic Models, Risk Factors, Retrospective Studies, Time Factors, Adult, Middle Aged, Tissue Donors, United States, Female, Male, Primary Graft Dysfunction, Young Adult, lung transplantation, primary graft dysfunction, pulmonary hypertension, Rare Diseases, Clinical Research, Cardiovascular, Transplantation, Organ Transplantation, Respiratory, Good Health and Well Being
Abstract

RationalePulmonary hypertension from pulmonary arterial hypertension or parenchymal lung disease is associated with an increased risk for primary graft dysfunction after lung transplantation.ObjectiveWe evaluated the clinical determinants of severe primary graft dysfunction in pulmonary hypertension and developed and validated a prognostic model.MethodsWe conducted a retrospective cohort study of patients in the multicenter Lung Transplant Outcomes Group with pulmonary hypertension at transplant listing. Severe primary graft dysfunction was defined as PaO2/FiO2 ≤200 with allograft infiltrates at 48 or 72 hours after transplantation. Donor, recipient, and operative characteristics were evaluated in a multivariable explanatory model. A prognostic model derived using donor and recipient characteristics was then validated in a separate cohort.ResultsIn the explanatory model of 826 patients with pulmonary hypertension, donor tobacco smoke exposure, higher recipient body mass index, female sex, listing mean pulmonary artery pressure, right atrial pressure and creatinine at transplant, cardiopulmonary bypass use, transfusion volume, and reperfusion fraction of inspired oxygen were associated with primary graft dysfunction. Donor obesity was associated with a lower risk for primary graft dysfunction. Using a 20% threshold for elevated risk, the prognostic model had good negative predictive value in both derivation and validation cohorts (89.1% [95% confidence interval, 85.3-92.8] and 83.3% [95% confidence interval, 78.5-88.2], respectively), but low positive predictive value.ConclusionsSeveral recipient, donor, and operative characteristics were associated with severe primary graft dysfunction in patients with pulmonary hypertension, including several risk factors not identified in the overall transplant population. A prognostic model with donor and recipient clinical risk factors alone had low positive predictive value, but high negative predictive value, to rule out high risk for primary graft dysfunction.

Published
2017

11. Models of Lung Transplant Research: a consensus statement from the National Heart, Lung, and Blood Institute workshop

Author

Lama, Vibha N, Belperio, John A, Christie, Jason D, El-Chemaly, Souheil, Fishbein, Michael C, Gelman, Andrew E, Hancock, Wayne W, Keshavjee, Shaf, Kreisel, Daniel, Laubach, Victor E, Looney, Mark R, McDyer, John F, Mohanakumar, Thalachallour, Shilling, Rebecca A, Panoskaltsis-Mortari, Angela, Wilkes, David S, Eu, Jerry P, and Nicolls, Mark R

Subjects
Lung, Rare Diseases, Acute Respiratory Distress Syndrome, Organ Transplantation, Transplantation, Respiratory, Immunology
Abstract

Lung transplantation, a cure for a number of end-stage lung diseases, continues to have the worst long-term outcomes when compared with other solid organ transplants. Preclinical modeling of the most common and serious lung transplantation complications are essential to better understand and mitigate the pathophysiological processes that lead to these complications. Various animal and in vitro models of lung transplant complications now exist and each of these models has unique strengths. However, significant issues, such as the required technical expertise as well as the robustness and clinical usefulness of these models, remain to be overcome or clarified. The National Heart, Lung, and Blood Institute (NHLBI) convened a workshop in March 2016 to review the state of preclinical science addressing the three most important complications of lung transplantation: primary graft dysfunction (PGD), acute rejection (AR), and chronic lung allograft dysfunction (CLAD). In addition, the participants of the workshop were tasked to make consensus recommendations on the best use of these complimentary models to close our knowledge gaps in PGD, AR, and CLAD. Their reviews and recommendations are summarized in this report. Furthermore, the participants outlined opportunities to collaborate and directions to accelerate research using these preclinical models.

Published
2017

12. The Lung Microbiome Predicts Mortality and Response to Azithromycin in Lung Transplant Recipients with Chronic Rejection.

Author

Combs, Michael P., Luth, Jenna E., Falkowski, Nicole R., Wheeler, David S., Walker, Natalie M., Erb-Downward, John R., Wakeam, Elliot, Sjoding, Michael W., Dunlap, Daniel G., Admon, Andrew J., Dickson, Robert P., and Lama, Vibha N.

Subjects
LUNG transplantation, LUNGS, AZITHROMYCIN, MORTALITY risk factors, OVERALL survival
Abstract

Rationale: Chronic lung allograft dysfunction (CLAD) is the leading cause of death after lung transplant, and azithromycin has variable efficacy in CLAD. The lung microbiome is a risk factor for developing CLAD, but the relationship between lung dysbiosis, pulmonary inflammation, and allograft dysfunction remains poorly understood. Whether lung microbiota predict outcomes or modify treatment response after CLAD is unknown. Objectives: To determine whether lung microbiota predict post-CLAD outcomes and clinical response to azithromycin. Methods: Retrospective cohort study using acellular BAL fluid prospectively collected from recipients of lung transplant within 90 days of CLAD onset. Lung microbiota were characterized using 16S rRNA gene sequencing and droplet digital PCR. In two additional cohorts, causal relationships of dysbiosis and inflammation were evaluated by comparing lung microbiota with CLAD-associated cytokines and measuring ex vivo P. aeruginosa growth in sterilized BAL fluid. Measurements and Main Results: Patients with higher bacterial burden had shorter post-CLAD survival, independent of CLAD phenotype, azithromycin treatment, and relevant covariates. Azithromycin treatment improved survival in patients with high bacterial burden but had negligible impact on patients with low or moderate burden. Lung bacterial burden was positively associated with CLAD-associated cytokines, and ex vivo growth of P. aeruginosa was augmented in BAL fluid from transplant recipients with CLAD. Conclusions: In recipients of lung transplants with chronic rejection, increased lung bacterial burden is an independent risk factor for mortality and predicts clinical response to azithromycin. Lung bacterial dysbiosis is associated with alveolar inflammation and may be promoted by underlying lung allograft dysfunction. [ABSTRACT FROM AUTHOR]

Published
2024
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14. Multicenter evaluation of parametric response mapping as an indicator of bronchiolitis obliterans syndrome after hematopoietic stem cell transplantation

Author

Cheng, Guang-Shing, Selwa, Katherine E., Hatt, Charles, Ram, Sundaresh, Fortuna, Aleksa B., Guerriero, Margaret, Himelhoch, Ben, McAree, Daniel, Hoffman, Timothy C., Brisson, Joseph, Nazareno, Ryan, Bloye, Kiernan, Johnson, Timothy D., Remberger, Mats, Mattsson, Jonas, Vummidi, Dharshan, Kazerooni, Ella E., Lama, Vibha N., Galban, Stefanie, Boeckh, Michael, Yanik, Gregory A., and Galban, Craig J.

Published
2020
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15. The relationship between plasma lipid peroxidation products and primary graft dysfunction after lung transplantation is modified by donor smoking and reperfusion hyperoxia

Author

Diamond, Joshua M, Porteous, Mary K, Roberts, L Jackson, Wickersham, Nancy, Rushefski, Melanie, Kawut, Steven M, Shah, Rupal J, Cantu, Edward, Lederer, David J, Chatterjee, Shampa, Lama, Vibha N, Bhorade, Sangeeta, Crespo, Maria, McDyer, John, Wille, Keith, Orens, Jonathan, Weinacker, Ann, Arcasoy, Selim, Shah, Pali D, Wilkes, David S, Hage, Chadi, Palmer, Scott M, Snyder, Laurie, Calfee, Carolyn S, Ware, Lorraine B, Christie, Jason D, and Group, for the Lung Transplant Outcomes

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Lung, Tobacco Smoke and Health, Tobacco, Organ Transplantation, Clinical Research, Transplantation, Respiratory, Adult, Biomarkers, Female, Follow-Up Studies, Humans, Hyperoxia, Lipid Peroxidation, Lung Transplantation, Male, Postoperative Complications, Primary Graft Dysfunction, Reperfusion Injury, Retrospective Studies, Smoking, Time Factors, Tissue Donors, lung transplantation, lipid peroxidation, primary graft dysfunction, F2-isoprostane, isofuran, ischemia reperfusion, Lung Transplant Outcomes Group, Cardiorespiratory Medicine and Haematology, Surgery, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundDonor smoking history and higher fraction of inspired oxygen (FIO2) at reperfusion are associated with primary graft dysfunction (PGD) after lung transplantation. We hypothesized that oxidative injury biomarkers would be elevated in PGD, with higher levels associated with donor exposure to cigarette smoke and recipient hyperoxia at reperfusion.MethodsWe performed a nested case-control study of 72 lung transplant recipients from the Lung Transplant Outcomes Group cohort. Using mass spectroscopy, F2-isoprostanes and isofurans were measured in plasma collected after transplantation. Cases were defined in 2 ways: grade 3 PGD present at day 2 or day 3 after reperfusion (severe PGD) or any grade 3 PGD (any PGD).ResultsThere were 31 severe PGD cases with 41 controls and 35 any PGD cases with 37 controls. Plasma F2-isoprostane levels were higher in severe PGD cases compared with controls (28.6 pg/ml vs 19.8 pg/ml, p = 0.03). Plasma F2-isoprostane levels were higher in severe PGD cases compared with controls (29.6 pg/ml vs 19.0 pg/ml, p = 0.03) among patients reperfused with FIO2 >40%. Among recipients of lungs from donors with smoke exposure, plasma F2-isoprostane (38.2 pg/ml vs 22.5 pg/ml, p = 0.046) and isofuran (66.9 pg/ml vs 34.6 pg/ml, p = 0.046) levels were higher in severe PGD compared with control subjects.ConclusionsPlasma levels of lipid peroxidation products are higher in patients with severe PGD, in recipients of lungs from donors with smoke exposure, and in recipients exposed to higher Fio2 at reperfusion. Oxidative injury is an important mechanism of PGD and may be magnified by donor exposure to cigarette smoke and hyperoxia at reperfusion.

Published
2016

16. Development and validation of primary graft dysfunction predictive algorithm for lung transplant candidates

Author

Diamond, Joshua M., primary, Anderson, Michaela R., additional, Cantu, Edward, additional, Clausen, Emily S., additional, Shashaty, Michael G.S., additional, Kalman, Laurel, additional, Oyster, Michelle, additional, Crespo, Maria M., additional, Bermudez, Christian A., additional, Benvenuto, Luke, additional, Palmer, Scott M., additional, Snyder, Laurie D., additional, Hartwig, Matthew G., additional, Wille, Keith, additional, Hage, Chadi, additional, McDyer, John F., additional, Merlo, Christian A., additional, Shah, Pali D., additional, Orens, Jonathan B., additional, Dhillon, Ghundeep S., additional, Lama, Vibha N., additional, Patel, Mrunal G., additional, Singer, Jonathan P., additional, Hachem, Ramsey R., additional, Michelson, Andrew P., additional, Hsu, Jesse, additional, Russell Localio, A., additional, and Christie, Jason D., additional

Published
2023
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17. Genetic Variation in the Prostaglandin E2 Pathway Is Associated with Primary Graft Dysfunction

Author

Diamond, Joshua M, Akimova, Tatiana, Kazi, Altaf, Shah, Rupal J, Cantu, Edward, Feng, Rui, Levine, Matthew H, Kawut, Steven M, Meyer, Nuala J, Lee, James C, Hancock, Wayne W, Aplenc, Richard, Ware, Lorraine B, Palmer, Scott M, Bhorade, Sangeeta, Lama, Vibha N, Weinacker, Ann, Orens, Jonathan, Wille, Keith, Crespo, Maria, Lederer, David J, Arcasoy, Selim, Demissie, Ejigayehu, Christie, Jason D, and Group, for the Lung Transplant Outcomes

Subjects
Rare Diseases, Biotechnology, Lung, Genetics, Prevention, Clinical Research, Human Genome, Transplantation, Organ Transplantation, 2.1 Biological and endogenous factors, Aetiology, Biomarkers, Computational Biology, Dinoprostone, Female, Genetic Association Studies, Genetic Markers, Genotype, Genotyping Techniques, Humans, Intramolecular Oxidoreductases, Lung Transplantation, Male, Middle Aged, Polymorphism, Single Nucleotide, Primary Graft Dysfunction, Prospective Studies, Prostaglandin-E Synthases, Receptors, Prostaglandin E, EP4 Subtype, T-Lymphocytes, Regulatory, Lung Transplant Outcomes Group, Medical and Health Sciences, Respiratory System
Abstract

RationaleBiologic pathways with significant genetic conservation across human populations have been implicated in the pathogenesis of primary graft dysfunction (PGD). The evaluation of the role of recipient genetic variation in PGD has thus far been limited to single, candidate gene analyses.ObjectivesWe sought to identify genetic variants in lung transplant recipients that are responsible for increased risk of PGD using a two-phase large-scale genotyping approach.MethodsPhase 1 was a large-scale candidate gene association study of the multicenter, prospective Lung Transplant Outcomes Group cohort. Phase 2 included functional evaluation of selected variants and a bioinformatics screening of variants identified in phase 1.Measurements and main resultsAfter genetic data quality control, 680 lung transplant recipients were included in the analysis. In phase 1, a total of 17 variants were significantly associated with PGD, four of which were in the prostaglandin E2 family of genes. Among these were a coding variant in the gene encoding prostaglandin E2 synthase (PTGES2; P = 9.3 × 10(-5)) resulting in an arginine to histidine substitution at amino acid position 298, and three variants in a block containing the 5' promoter and first intron of the PTGER4 gene (encoding prostaglandin E2 receptor subtype 4; all P < 5 × 10(-5)). Functional evaluation in regulatory T cells identified that rs4434423A in the PTGER4 gene was associated with differential suppressive function of regulatory T cells.ConclusionsFurther research aimed at replication and additional functional insight into the role played by genetic variation in prostaglandin E2 synthetic and signaling pathways in PGD is warranted.

Published
2014

18. Genetic deficiency of the transcription factor NFAT1 confers protection against fibrogenic responses independent of immune influx

Author

Vittal, Ragini, primary, Walker, Natalie M., additional, McLinden, A. Patrick Patrick, additional, Braeuer, Russell R., additional, Ke, Fang, additional, Fattahi, Fatemeh, additional, Combs, Michael P., additional, Misumi, Keizo, additional, Aoki, Yoshiro, additional, Wheeler, David S., additional, Wilke, Carol A., additional, Huang, Steven K., additional, Moore, Bethany B., additional, Cao, Pengxiu, additional, and Lama, Vibha N., additional

Published
2023
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19. CT-based Machine Learning for Donor Lung Screening Prior to Transplantation

Author

Ram, Sundaresh, primary, Verleden, Stijn E, additional, Kumar, Madhav, additional, Bell, Alexander J., additional, Pal, Ravi, additional, Ordies, Sofie, additional, Vanstapel, Arno, additional, Dubbeldam, Adriana, additional, Vos, Robin, additional, Galban, Stefanie, additional, Ceulemans, Laurens J., additional, Frick, Anna E., additional, Van Raemdonck, Dirk E., additional, Verschakelen, Johny, additional, Vanaudenaerde, Bart M., additional, Verleden, Geert M., additional, Lama, Vibha N, additional, Neyrinck, Arne P., additional, and Galban, Craig J., additional

Published
2023
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20. Latent Class Analysis Identifies Distinct Phenotypes of Primary Graft Dysfunction After Lung Transplantation

Author

Shah, Rupal J, Diamond, Joshua M, Cantu, Edward, Lee, James C, Lederer, David J, Lama, Vibha N, Orens, Jonathan, Weinacker, Ann, Wilkes, David S, Bhorade, Sangeeta, Wille, Keith M, Ware, Lorraine B, Palmer, Scott M, Crespo, Maria, Localio, A Russell, Demissie, Ejigayehu, Kawut, Steven M, Bellamy, Scarlett L, and Christie, Jason D

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Acute Respiratory Distress Syndrome, Transplantation, Organ Transplantation, Lung, Rare Diseases, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Respiratory, Adult, Female, Humans, Lung Transplantation, Male, Middle Aged, Phenotype, Primary Graft Dysfunction, Prospective Studies, Risk Assessment, Risk Factors, Severity of Illness Index, Clinical Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundThere is significant heterogeneity within the primary graft dysfunction (PGD) syndrome. We aimed to identify distinct grade 3 PGD phenotypes based on severity of lung dysfunction and patterns of resolution.MethodsSubjects from the Lung Transplant Outcomes Group (LTOG) cohort study with grade 3 PGD within 72 h after transplantation were included. Latent class analysis (LCA) was used to statistically identify classes based on changes in PGD International Society for Heart & Lung Transplantation grade over time. Construct validity of the classes was assessed by testing for divergence of recipient, donor, and operative characteristics between classes. Predictive validity was assessed using time to death.ResultsOf 1,255 subjects, 361 had grade 3 PGD within the first 72 h after transplantation. LCA identified three distinct phenotypes: (1) severe persistent dysfunction (class 1), (2) complete resolution of dysfunction within 72 h (class 2), and (3) attenuation, without complete resolution within 72 h (class 3). Increased use of cardiopulmonary bypass, greater RBC transfusion, and higher mean pulmonary artery pressure were associated with persistent PGD (class 1). Subjects in class 1 also had the greatest risk of death (hazard ratio, 2.39; 95% CI, 1.57-3.63; P < .001).ConclusionsThere are distinct phenotypes of resolution of dysfunction within the severe PGD syndrome. Subjects with early resolution may represent a different mechanism of lung pathology, such as resolving pulmonary edema, whereas those with persistent PGD may represent a more severe phenotype. Future studies aimed at PGD mechanism or treatment may focus on phenotypes based on resolution of graft dysfunction.

Published
2013

21. Clinical Risk Factors for Primary Graft Dysfunction after Lung Transplantation

Author

Diamond, Joshua M, Lee, James C, Kawut, Steven M, Shah, Rupal J, Localio, A Russell, Bellamy, Scarlett L, Lederer, David J, Cantu, Edward, Kohl, Benjamin A, Lama, Vibha N, Bhorade, Sangeeta M, Crespo, Maria, Demissie, Ejigayehu, Sonett, Joshua, Wille, Keith, Orens, Jonathan, Shah, Ashish S, Weinacker, Ann, Arcasoy, Selim, Shah, Pali D, Wilkes, David S, Ware, Lorraine B, Palmer, Scott M, Christie, Jason D, and Group, for the Lung Transplant Outcomes

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Organ Transplantation, Clinical Trials and Supportive Activities, Prevention, Cardiovascular, Clinical Research, Lung, Transplantation, Respiratory, Good Health and Well Being, Adolescent, Adult, Aged, Aged, 80 and over, Female, Humans, Logistic Models, Lung Transplantation, Male, Middle Aged, Multivariate Analysis, Primary Graft Dysfunction, Prospective Studies, Risk Factors, United States, Lung Transplant Outcomes Group, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationalePrimary graft dysfunction (PGD) is the main cause of early morbidity and mortality after lung transplantation. Previous studies have yielded conflicting results for PGD risk factors.ObjectivesWe sought to identify donor, recipient, and perioperative risk factors for PGD.MethodsWe performed a 10-center prospective cohort study enrolled between March 2002 and December 2010 (the Lung Transplant Outcomes Group). The primary outcome was International Society for Heart and Lung Transplantation grade 3 PGD at 48 or 72 hours post-transplant. The association of potential risk factors with PGD was analyzed using multivariable conditional logistic regression.Measurements and main resultsA total of 1,255 patients from 10 centers were enrolled; 211 subjects (16.8%) developed grade 3 PGD. In multivariable models, independent risk factors for PGD were any history of donor smoking (odds ratio [OR], 1.8; 95% confidence interval [CI], 1.2-2.6; P = 0.002); FiO2 during allograft reperfusion (OR, 1.1 per 10% increase in FiO2; 95% CI, 1.0-1.2; P = 0.01); single lung transplant (OR, 2; 95% CI, 1.2-3.3; P = 0.008); use of cardiopulmonary bypass (OR, 3.4; 95% CI, 2.2-5.3; P < 0.001); overweight (OR, 1.8; 95% CI, 1.2-2.7; P = 0.01) and obese (OR, 2.3; 95% CI, 1.3-3.9; P = 0.004) recipient body mass index; preoperative sarcoidosis (OR, 2.5; 95% CI, 1.1-5.6; P = 0.03) or pulmonary arterial hypertension (OR, 3.5; 95% CI, 1.6-7.7; P = 0.002); and mean pulmonary artery pressure (OR, 1.3 per 10 mm Hg increase; 95% CI, 1.1-1.5; P < 0.001). PGD was significantly associated with 90-day (relative risk, 4.8; absolute risk increase, 18%; P < 0.001) and 1-year (relative risk, 3; absolute risk increase, 23%; P < 0.001) mortality.ConclusionsWe identified grade 3 PGD risk factors, several of which are potentially modifiable and should be prioritized for future research aimed at preventative strategies. Clinical trial registered with www.clinicaltrials.gov (NCT 00552357).

Published
2013

22. Variation in PTX3 Is Associated with Primary Graft Dysfunction after Lung Transplantation

Author

Diamond, Joshua M, Meyer, Nuala J, Feng, Rui, Rushefski, Melanie, Lederer, David J, Kawut, Steven M, Lee, James C, Cantu, Edward, Shah, Rupal J, Lama, Vibha N, Bhorade, Sangeeta, Crespo, Maria, Demissie, Ejigayehu, Sonett, Joshua, Wille, Keith, Orens, Jonathan, Weinacker, Ann, Weill, David, Arcasoy, Selim, Shah, Pali D, Belperio, John A, Wilkes, David, Ware, Lorraine B, Palmer, Scott M, Christie, Jason D, and Group, for the Lung Transplant Outcomes

Subjects
Lung, Clinical Trials and Supportive Activities, Rare Diseases, Organ Transplantation, Genetics, Clinical Research, Transplantation, Aetiology, 2.1 Biological and endogenous factors, Respiratory, C-Reactive Protein, Cohort Studies, Confidence Intervals, Female, Follow-Up Studies, Genetic Association Studies, Genotype, Graft Rejection, Graft Survival, Haplotypes, Humans, Idiopathic Pulmonary Fibrosis, Incidence, Logistic Models, Lung Transplantation, Male, Middle Aged, Odds Ratio, Polymorphism, Single Nucleotide, Primary Graft Dysfunction, Pulmonary Disease, Chronic Obstructive, Retrospective Studies, Risk Assessment, Serum Amyloid P-Component, Severity of Illness Index, Statistics, Nonparametric, Time Factors, primary graft dysfunction, single-nucleotide polymorphism, long pentraxin 3, lung transplantation, Lung Transplant Outcomes Group, Medical and Health Sciences, Respiratory System
Abstract

RationaleElevated long pentraxin-3 (PTX3) levels are associated with the development of primary graft dysfunction (PGD) after lung transplantation. Abnormalities in innate immunity, mediated by PTX3 release, may play a role in PGD pathogenesis.ObjectivesOur goal was to test whether variants in the gene encoding PTX3 are risk factors for PGD.MethodsWe performed a candidate gene association study in recipients from the multicenter, prospective Lung Transplant Outcomes Group cohort enrolled between July 2002 and July 2009. The primary outcome was International Society for Heart and Lung Transplantation grade 3 PGD within 72 hours of transplantation. Targeted genotyping of 10 haplotype-tagging PTX3 single-nucleotide polymorphisms (SNPs) was performed in lung transplant recipients. The association between PGD and each SNP was evaluated by logistic regression, adjusting for pretransplantation lung disease, cardiopulmonary bypass use, and population stratification. The association between SNPs and plasma PTX3 levels was tested across genotypes in a subset of recipients with idiopathic pulmonary fibrosis.Measurements and main resultsSix hundred fifty-four lung transplant recipients were included. The incidence of PGD was 29%. Two linked 5' region variants, rs2120243 and rs2305619, were associated with PGD (odds ratio, 1.5; 95% confidence interval, 1.1 to 1.9; P = 0.006 and odds ratio, 1.4; 95% confidence interval, 1.1 to 1.9; P = 0.007, respectively). The minor allele of rs2305619 was significantly associated with higher plasma PTX3 levels measured pretransplantation (P = 0.014) and at 24 hours (P = 0.047) after transplantation in patients with idiopathic pulmonary fibrosis.ConclusionsGenetic variants of PTX3 are associated with PGD after lung transplantation, and are associated with increased PTX3 plasma levels.

Published
2012

23. A panel of lung injury biomarkers enhances the definition of primary graft dysfunction (PGD) after lung transplantation

Author

Shah, Rupal J, Bellamy, Scarlett L, Localio, A Russell, Wickersham, Nancy, Diamond, Joshua M, Weinacker, Ann, Lama, Vibha N, Bhorade, Sangeeta, Belperio, John A, Crespo, Maria, Demissie, Ejigayehu, Kawut, Steven M, Wille, Keith M, Lederer, David J, Lee, James C, Palmer, Scott M, Orens, Jonathan, Reynolds, John, Shah, Ashish, Wilkes, David S, Ware, Lorraine B, and Christie, Jason D

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Acute Respiratory Distress Syndrome, Rare Diseases, Lung, Transplantation, Organ Transplantation, Good Health and Well Being, Adult, Biomarkers, Female, Humans, Lung Injury, Lung Transplantation, Male, Middle Aged, Primary Graft Dysfunction, Prospective Studies, primary graft dysfunction, lung transplantation, biomarkers, acute lung injury, Cardiorespiratory Medicine and Haematology, Surgery, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundWe aimed to identify combinations of biomarkers to enhance the definition of primary graft dysfunction (PGD) for translational research.MethodsBiomarkers reflecting lung epithelial injury (soluble receptor for advance glycation end products [sRAGE] and surfactant protein-D [SP-D]), coagulation cascade (plasminogen activator inhibitor-1 [PAI-1] and protein C), and cell adhesion (intracellular adhesion molecule-1 [ICAM-1]) were measured in the plasma of 315 individuals derived from the Lung Transplant Outcomes Group cohort at 6 and 24 hours after transplantation. We assessed biomarker utility in 2 ways: first, we tested the discrimination of grade 3 PGD within 72 hours; second, we tested the predictive utility of plasma biomarkers for 90-day mortality.ResultsPGD developed in 86 of 315 individuals (27%). Twenty-patients (8%) died within 90 days of transplantation, of which 16 (70%) had PGD. Biomarkers measured at 24 hours had greater discrimination than at 6 hours. Individually, sRAGE (area under the curve [AUC], 0.71) and PAI-1 (AUC, 0.73) had the best discrimination of PGD. The combinations of sRAGE with PAI-1 (AUC, 0.75), PAI-1 with ICAM-1 (AUC, 0.75), and PAI-1 with SP-D (AUC, 0.76) had the best discrimination. Combinations of greater than 2 biomarkers did not significantly enhance discrimination of PGD. ICAM-1 with PAI-1 (AUC, 0.72) and ICAM-1 with sRAGE (AUC, 0.72) had the best prediction for 90-day mortality. The addition of ICAM-1, PAI-1, or sRAGE to the concurrent clinical PGD grade significantly improved the prediction of 90-day mortality (p < 0.001 each).ConclusionsMeasurement of the combination of a marker of impaired fibrinolysis with an epithelial injury or cell adhesion marker had the best discrimination for PGD and prediction for early death and may provide an alternative outcome useful in future research.

Published
2012

26. Transcription factor FOXF1 identifies compartmentally distinct mesenchymal cells with a role in lung allograft fibrogenesis

Author

Braeuer, Russell R., Walker, Natalie M., Misumi, Keizo, Mazzoni-Putman, Serina, Aoki, Yoshiro, Liao, Ruohan, Vittal, Ragini, Kleer, Gabriel G., Wheeler, David S., Sexton, Jonathan Z., Farver, Carol F., Welch, Joshua D., and Lama, Vibha N.

Subjects
Lungs -- Transplantation, Fibrosis -- Risk factors -- Genetic aspects -- Development and progression, Stem cells -- Genetic aspects -- Physiological aspects -- Health aspects, Health care industry
Abstract

In this study, we demonstrate that forkhead box F1 (FOXF1), a mesenchymal transcriptional factor essential for lung development, was retained in a topographically distinct mesenchymal stromal cell population along the bronchovascular space in an adult lung and identify this distinct subset of collagen-expressing cells as key players in lung allograft remodeling and fibrosis. Using Foxf1-tdTomato BAC (Foxfi-tdTomato) and Foxf1-tdTomato Col1a1-GFP mice, we show that [Lin.sup.-][Foxf1.sup.+] cells encompassed the stem cell antigen [1.sup.+][CD34.sup.+] ([Sca1.sup.+][CD34.sup.+]) subset of collagen 1-expressing mesenchymal cells (MCs) with a capacity to generate CFU and lung epithelial organoids. Histologically, FOXF1- expressing MCs formed a 3D network along the conducting airways; FOXF1 was noted to be conspicuously absent in MCs in the alveolar compartment. Bulk and single-cell RNA-Seq confirmed distinct transcriptional signatures of [Foxf1.sup.-] and [Foxf1.sup.-] MCs, with Foxf1-expressing cells delineated by their high expression of the transcription factor glioma-associated oncogene 1 (Gli1) and low expression of integrin [alpha]8 (Itga), versus other collagen-expressing MCs. [FOXF1.sup.+][Gli1.sup.+] MCs showed proximity to Sonic hedgehog-expressing (Shh-expressing) bronchial epithelium, and mesenchymal expression of Foxf1 and Gli1 was found to be dependent on paracrine Shh signaling in epithelial organoids. Using a murine lung transplant model, we show dysregulation of epithelial-mesenchymal SHH/GLI1/ FOXF1 crosstalk and expansion of this specific peribronchial MC population in chronically rejecting fibrotic lung allografts., Introduction It is increasingly recognized that characterization of mesenchymal cell (MC) populations within distinct anatomic locations is key to understanding local homeostatic and regenerative processes as well as delineating unique [...]

Published
2021
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27. Genetic deficiency of the transcription factor NFAT1 confers protection against fibrogenic responses independent of immune influx.

Author

Vittal, Ragini, Walker, Natalie M., McLinden, A. Patrick, Braeuer, Russell R., Fang Ke, Fattahi, Fatemeh, Combs, Michael P., Keizo Misumi, Yoshiro Aoki, Wheeler, David S., Wilke, Carol A., Huang, Steven K., Moore, Bethany B., Pengxiu Cao, and Lama, Vibha N.

Subjects
TRANSCRIPTION factors, IDIOPATHIC pulmonary fibrosis, URIDINE, PULMONARY fibrosis, BONE marrow cells, TISSUE remodeling
Abstract

Idiopathic pulmonary fibrosis (IPF) is marked by unremitting matrix deposition and architectural distortion. Multiple profibrotic pathways contribute to the persistent activation of mesenchymal cells (MCs) in fibrosis, highlighting the need to identify and target common signaling pathways. The transcription factor nuclear factor of activated T cells 1 (NFAT1) lies downstream of second messenger calcium signaling and has been recently shown to regulate key profibrotic mediator autotaxin (ATX) in lung MCs. Herein, we investigate the role of NFAT1 in regulating fibroproliferative responses during the development of lung fibrosis. Nfat1−/−-deficient mice subjected to bleomycin injury demonstrated improved survival and protection from lung fibrosis and collagen deposition as compared with bleomycin-injured wild-type (WT) mice. Chimera mice, generated by reconstituting bone marrow cells from WT or Nfat1−/− mice into irradiated WT mice (WT→WT and Nfat1−/−→WT), demonstrated no difference in bleomycin-induced fibrosis, suggesting immune influx-independent fibro protection in Nfat1−/− mice. Examination of lung tissue and flow sorted lineageneg/platelet-derived growth factor receptor alpha (PDGFRα)pos MCs demonstrated decreased MC numbers, proliferation [↓ cyclin D1 and 5-ethynyl-2′-deoxyuridine (EdU) incorporation], myofibroblast differentiation [↓ α-smooth muscle actin (α-SMA)], and survival (↓ Birc5) in Nfat1−/− mice. Nfat1 deficiency abrogated ATX expression in response to bleomycin in vivo and MCs derived from Nfat1−/− mice demonstrated decreased ATX expression and migration in vitro. Human IPF MCs demonstrated constitutive NFAT1 activation, and regulation of ATX in these cells by NFAT1 was confirmed using pharmacological and genetic inhibition. Our findings identify NFAT1 as a critical mediator of profibrotic processes, contributing to dysregulated lung remodeling and suggest its targeting in MCs as a potential therapeutic strategy in IPF. NEW & NOTEWORTHY Idiopathic pulmonary fibrosis (IPF) is a fatal disease with hallmarks of fibroblastic foci and exuberant matrix deposition, unknown etiology, and ineffective therapies. Several profibrotic/proinflammatory pathways are implicated in accelerating tissue remodeling toward a honeycombed end-stage disease. NFAT1 is a transcriptional factor activated in IPF tissues. Nfat1-deficient mice subjected to chronic injury are protected against fibrosis independent of immune influxes, with suppression of profibrotic mesenchymal phenotypes including proliferation, differentiation, resistance to apoptosis, and autotaxin-related migration. [ABSTRACT FROM AUTHOR]

Published
2024
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29. Autocrine lysophosphatidic acid signaling activates [beta]-catenin and promotes lung allograft fibrosis

Author

Cao, Pengxiu, Aoki, Yoshiro, Badri, Linda, Walker, Natalie M., Manning, Casey M., Lagstein, Amir, Fearon, Eric R., and Lama, Vibha N.

Subjects
Tumor suppressor genes -- Health aspects, Lung diseases -- Genetic aspects -- Development and progression -- Care and treatment, Cellular signal transduction -- Genetic aspects -- Health aspects, Fibrosis -- Genetic aspects -- Development and progression -- Care and treatment, Health care industry
Abstract

Tissue fibrosis is the primary cause of long-term graft failure after organ transplantation. In lung allografts, progressive terminal airway fibrosis leads to an irreversible decline in lung function termed bronchiolitis obliterans syndrome (BOS). Here, we have identified an autocrine pathway linking nuclear factor of activated T cells 2 (NFAT1), autotaxin (ATX), lysophosphatidic acid (LPA), and [beta]-catenin that contributes to progression of fibrosis in lung allografts. Mesenchymal cells (MCs) derived from fibrotic lung allografts (BOS MCs) demonstrated constitutive nuclear [beta]-catenin expression that was dependent on autocrine ATX secretion and LPA signaling. We found that NFAT1 upstream of ATX regulated expression of ATX as well as [beta]-catenin. Silencing NFAT1 in BOS MCs suppressed ATX expression, and sustained overexpression of NFAT1 increased ATX expression and activity in non-fibrotic MCs. LPA signaling induced NFAT1 nuclear translocation, suggesting that autocrine LPA synthesis promotes NFAT1 transcriptional activation and ATX secretion in a positive feedback loop. In an in vivo mouse orthotopic lung transplant model of BOS, antagonism of the LPA receptor (LPA1) or ATX inhibition decreased allograft fibrosis and was associated with lower active [beta]-catenin and dephosphorylated NFAT1 expression. Lung allografts from [beta]-catenin reporter mice demonstrated reduced [beta]-catenin transcriptional activation in the presence of LPA1 antagonist, confirming an in vivo role for LPA signaling in [beta]-catenin activation., Introduction Fibrogenesis in the transplanted organ is the predominant cause of allograft failure and death across all solid organs. By 5 years after transplantation, 50% of lung transplant recipients develop [...]

Published
2017
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31. The mitigating effect of exogenous carbon monoxide on chronic allograft rejection and fibrosis post-lung transplantation

Author

Aoki, Yoshiro, primary, Walker, Natalie M., additional, Misumi, Keizo, additional, Mimura, Takeshi, additional, Vittal, Ragini, additional, McLinden, Aidan P., additional, Fitzgerald, Linda, additional, Combs, Michael P., additional, Lyu, Dennis, additional, Osterholzer, John J., additional, Pinsky, David J., additional, and Lama, Vibha N., additional

Published
2022
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35. Quantitative CT Correlates with Local Inflammation in Lung of Patients with Subtypes of Chronic Lung Allograft Dysfunction

Author

Ram, Sundaresh, primary, Verleden, Stijn E., additional, Bell, Alexander J., additional, Hoff, Benjamin A., additional, Labaki, Wassim W., additional, Murray, Susan, additional, Vanaudenaerde, Bart M., additional, Vos, Robin, additional, Verleden, Geert M., additional, Kazerooni, Ella A., additional, Galbán, Stefanie, additional, Hatt, Charles R., additional, Han, Meilan K., additional, Lama, Vibha N., additional, and Galbán, Craig J., additional

Published
2022
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43. Risk of primary graft dysfunction following lung transplantation in selected adults with connective tissue disease-associated interstitial lung disease

Author

Natalini, Jake G., primary, Diamond, Joshua M., additional, Porteous, Mary K., additional, Lederer, David J., additional, Wille, Keith M., additional, Weinacker, Ann B., additional, Orens, Jonathan B., additional, Shah, Pali D., additional, Lama, Vibha N., additional, McDyer, John F., additional, Snyder, Laurie D., additional, Hage, Chadi A., additional, Singer, Jonathan P., additional, Ware, Lorraine B., additional, Cantu, Edward, additional, Oyster, Michelle, additional, Kalman, Laurel, additional, Christie, Jason D., additional, Kawut, Steven M., additional, and Bernstein, Elana J., additional

Published
2021
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44. Early growth response gene-1 promotes airway allograft rejection

Author

Harada, Hiroaki, Lama, Vibha N., Badri, Linda N., Ohtsuka, Takashi, Petrovic-Djergovic, Danica, Liao, Hui, Yoshikawa, Yasushi, Iwanaga, Koichiro, Lau, Chris L., and Pinsky, David J.

Subjects
Airway (Medicine) -- Research, Airway (Medicine) -- Physiological aspects, Graft rejection -- Research, Lungs -- Transplantation, Lungs -- Research, Biological sciences
Abstract

Chronic airway rejection, characterized by lymphocytic bronchitis, epithelial cell damage, and ohliterative bronchiolitis (OB), limits long-term survival after lung transplantation. The transcription factor early growth response gene-1 (Egr-1) induces diverse inflammatory mediators, some involved in OB pathogenesis. An orthotopic mouse tracheal transplant model was used to determine whether Egr-1 promotes development of airway allograft rejection. Significantly higher Egr-1 mRNA levels were seen in allografts (3.2-fold increase vs. isografts, P = 0.012). Allografts revealed thickening of epithelial and subepithelial airway layers (51 [+ or -] 4% luminal encroachment for allografts vs. 20 [+ or -] 3% for isografts, P < 0.0001) marked by significant lymphocytic infiltration. Absence of the Egr-1 gene in donor (but not recipient) tissue resulted in significant reduction in luminal narrowing (34 [+ or -] 4%, P = 0.0001) with corresponding diminution of T cell infiltration. Egr-1 null allografts exhibited a striking reduction in inducible nitric oxide synthase (iNOS) expression. Effector cytokines previously implicated in OB pathogenesis with known Egr- 1 promoter motifs (IL- 1[beta] and JE/monocyte chemoattractant protein-1) were reduced in Egr-1 null allografts. These data suggest a paradigm wherein local induction of Egr-1 in tracheal allografts drives expression of inflammatory mediators responsible for lymphocyte recruitment and tissue destruction characteristic of airway rejection. transplantation; inflammation; lymphocytic bronchiolitis; obliterative bronchiolitis doi:10.1152/ajplung.00285.2006

Published
2007

45. Evidence for tissue-resident mesenchymal stem cells in human adult lung from studies of transplanted allografts

Author

Lama, Vibha N., Smith, Lisa, Badri, Linda, Flint, Andrew, Andrei, Adin-Cristian, Murray, Susan, Wang, Zhuo, Liao, Hui, Toews, Galen B., Krebsbach, Paul H., Peters-Golden, Marc, Pinsky, David J., Martinez, Fernando J., and Thannickal, Victor J.

Abstract

The origin and turnover of connective tissue cells in adult human organs, including the lung, are not well understood. Here, studies of cells derived from human lung allografts demonstrate the [...]

Published
2007

46. Multicenter evaluation of parametric response mapping as an indicator of bronchiolitis obliterans syndrome after hematopoietic stem cell transplantation

Author

Cheng, Guang‐Shing, Selwa, Katherine E., Hatt, Charles, Ram, Sundaresh, Fortuna, Aleksa B., Guerriero, Margaret, Himelhoch, Ben, McAree, Daniel, Hoffman, Timothy C., Brisson, Joseph, Nazareno, Ryan, Bloye, Kiernan, Johnson, Timothy D., Remberger, Mats, Mattsson, Jonas, Vummidi, Dharshan, Kazerooni, Ella E., Lama, Vibha N., Galban, Stefanie, Boeckh, Michael, Yanik, Gregory A., Galban, Craig J., Cheng, Guang‐Shing, Selwa, Katherine E., Hatt, Charles, Ram, Sundaresh, Fortuna, Aleksa B., Guerriero, Margaret, Himelhoch, Ben, McAree, Daniel, Hoffman, Timothy C., Brisson, Joseph, Nazareno, Ryan, Bloye, Kiernan, Johnson, Timothy D., Remberger, Mats, Mattsson, Jonas, Vummidi, Dharshan, Kazerooni, Ella E., Lama, Vibha N., Galban, Stefanie, Boeckh, Michael, Yanik, Gregory A., and Galban, Craig J.

Abstract

Parametric response mapping (PRM) is a novel computed tomography (CT) technology that has shown potential for assessment of bronchiolitis obliterans syndrome (BOS) after hematopoietic stem cell transplantation (HCT). The primary aim of this study was to evaluate whether variations in image acquisition under real-world conditions affect the PRM measurements of clinically diagnosed BOS. CT scans were obtained retrospectively from 72 HCT recipients with BOS and graft-versus-host disease from Fred Hutchinson Cancer Research Center, Karolinska Institute, and the University of Michigan. Whole lung volumetric scans were performed at inspiration and expiration using site-specific acquisition and reconstruction protocols. PRM and pulmonary function measurements were assessed. Patients with moderately severe BOS at diagnosis (median forced expiratory volume at 1 second [FEV1] 53.5% predicted) had similar characteristics between sites. Variations in site-specific CT acquisition protocols had a negligible effect on the PRM-derived small airways disease (SAD), that is, BOS measurements. PRM-derived SAD was found to correlate with FEV1% predicted and FEV1/ forced vital capacity (R = −0.236, P = .046; and R = −0.689, P < .0001, respectively), which suggests that elevated levels in the PRM measurements are primarily affected by BOS airflow obstruction and not CT scan acquisition parameters. Based on these results, PRM may be applied broadly for post-HCT diagnosis and monitoring of BOS.

Published
2020
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47. Humoral immune responses mediate the development of a restrictive phenotype of chronic lung allograft dysfunction

Author

Misumi, Keizo, primary, Wheeler, David S., additional, Aoki, Yoshiro, additional, Combs, Michael P., additional, Braeuer, Russell R., additional, Higashikubo, Ryuji, additional, Li, Wenjun, additional, Kreisel, Daniel, additional, Vittal, Ragini, additional, Myers, Jeffrey, additional, Lagstein, Amir, additional, Walker, Natalie M., additional, Farver, Carol F., additional, and Lama, Vibha N., additional

Published
2020
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