Your search keyword '"Andrew E. Gelman"' showing total 227 results

1. Tissue-resident CCR2+ macrophage TREM-1/3 signaling is necessary for monocyte and neutrophil recruitment to injured hearts

Author

Yuriko Terada, Wenjun Li, Junedh M. Amrute, Amit I. Bery, Charles R. Liu, Venkatrao Nunna, Christian Corbin Frye, Hao Dun, Andrew L. Koenig, Hannah P. Luehmann, Gyu Seong Heo, Macee C. Owen, Alexander N. Wein, Yongjian Liu, Jon H. Ritter, Sumanth D. Prabhu, Ruben G. Nava, Andrew E. Gelman, Marina Cella, Marco Colonna, Kory J. Lavine, and Daniel Kreisel

Subjects

CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: Triggering receptor expressed on myeloid cells 1 (TREM-1) has been shown to amplify inflammatory signals, such as Toll-like receptor signaling, after infection and sterile injury. While previous studies have demonstrated that TREM-1 activation in circulating immune cells promotes injury, the role of TREM-1 signaling in tissue-resident cells in the context of sterile inflammation remains poorly understood. Here, we used a cardiac transplantation model to dissect how Trem1/3 expression on heart-resident cells regulates sterile inflammation. TREM-1 is expressed in heart-resident C-C chemokine receptor 2 (CCR2)+ macrophages in mice and humans. TREM-1/3 signaling in tissue-resident CCR2+ macrophages promotes C-C motif chemokine ligand 3 (CCL3) production and is critical for recruiting neutrophils and CCR2+ monocytes after heart transplantation. We demonstrate prolonged allograft survival after transplantation of Trem1/3-deficient compared with wild-type hearts. We identify TREM-1/3 signaling in donor grafts as a potential future therapeutic target to blunt inflammation after myocardial ischemia-reperfusion injury.

Published

2025

2. Increased clonal hematopoiesis involving DNA damage response genes in patients undergoing lung transplantation

Author

Laneshia K. Tague, Karolyn A. Oetjen, Anirudh Mahadev, Matthew J. Walter, Hephzibah Anthony, Daniel Kreisel, Daniel C. Link, and Andrew E. Gelman

Subjects

Genetics, Transplantation, Medicine

Abstract

BACKGROUND Cellular stressors influence the development of clonal hematopoiesis (CH). We hypothesized that environmental, inflammatory, and genotoxic stresses drive the emergence of CH in lung transplant recipients. METHODS We performed a cross-sectional cohort study of 85 lung transplant recipients to characterize CH prevalence. We evaluated somatic variants using duplex error-corrected sequencing and germline variants using whole exome sequencing. We evaluated CH frequency and burden using χ2 and Poisson regression, and we evaluated associations with clinical and demographic variables and clinical outcomes using χ2, logistic regression, and Cox regression. RESULTS CH in DNA damage response (DDR) genes TP53, PPM1D, and ATM was increased in transplant recipients compared with a control group of older adults (28% versus 0%, adjusted OR [aOR], 12.9 [1.7–100.3], P = 0.0002). Age (OR, 1.13 [1.03–1.25], P = 0.014) and smoking history (OR 4.25 [1.02–17.82], P = 0.048) were associated with DDR CH. Germline variants predisposing to idiopathic pulmonary fibrosis were identified but not associated with CH. DDR CH was associated with increased cytomegalovirus viremia versus patients with no (OR, 7.23 [1.95–26.8], P = 0.018) or non-DDR CH (OR, 7.64 [1.77–32.89], P = 0.024) and mycophenolate discontinuation (aOR, 3.8 [1.3–12.9], P = 0.031). CONCLUSION CH in DDR genes is prevalent in lung transplant recipients and is associated with posttransplant outcomes including cytomegalovirus activation and mycophenolate intolerance. FUNDING NIH/NHLBI K01HL155231 (LKT), R25HL105400 (LKT), Foundation for Barnes-Jewish Hospital (LKT), Evans MDS Center at Washington University (KAO, MJW), ASH Scholar Award (KAO), NIH K12CA167540 (KAO), NIH P01AI116501 (AEG, DK), NIH R01HL094601 (AEG), and NIH P01CA101937 (DCL).

Published

2023

3. Avoid being trapped by your liver: ischemia-reperfusion injury in liver transplant triggers S1P-mediated NETosis

Author

Davide Scozzi and Andrew E. Gelman

Subjects

Medicine

Abstract

Liver transplantation can be a life-saving treatment for end-stage hepatic disease. Unfortunately, some recipients develop ischemia-reperfusion injury (IRI) that leads to poor short- and long-term outcomes. Recent work has shown neutrophils contribute to IRI by undergoing NETosis, a form of death characterized by DNA ejection resulting in inflammatory extracellular traps. In this issue of the JCI, Hirao and Kojima et al. report that sphingosine-1-phosphate (S1P) expression induced by liver transplant–mediated IRI triggers NETosis. They also provide evidence that neutrophil expression of the carcinoembryonic antigen–related cell adhesion molecule-1 (CC1) long isoform inhibited NETosis by controlling S1P receptor–mediated autophagic flux. These findings suggest stimulating regulatory mechanisms that suppress NETosis could be used to prevent IRI.

Published

2023

4. Reprogramming alveolar macrophage responses to TGF-β reveals CCR2+ monocyte activity that promotes bronchiolitis obliterans syndrome

Author

Zhiyi Liu, Fuyi Liao, Jihong Zhu, Dequan Zhou, Gyu Seong Heo, Hannah P. Leuhmann, Davide Scozzi, Antanisha Parks, Ramsey Hachem, Derek E. Byers, Laneshia K. Tague, Hrishikesh S. Kulkarni, Marlene Cano, Brian W. Wong, Wenjun Li, Howard J. Huang, Alexander S. Krupnick, Daniel Kreisel, Yongjian Liu, and Andrew E. Gelman

Subjects

Immunology, Inflammation, Medicine

Abstract

Bronchiolitis obliterans syndrome (BOS) is a major impediment to lung transplant survival and is generally resistant to medical therapy. Extracorporeal photophoresis (ECP) is an immunomodulatory therapy that shows promise in stabilizing BOS patients, but its mechanisms of action are unclear. In a mouse lung transplant model, we show that ECP blunts alloimmune responses and inhibits BOS through lowering airway TGF-β bioavailability without altering its expression. Surprisingly, ECP-treated leukocytes were primarily engulfed by alveolar macrophages (AMs), which were reprogrammed to become less responsive to TGF-β and reduce TGF-β bioavailability through secretion of the TGF-β antagonist decorin. In untreated recipients, high airway TGF-β activity stimulated AMs to express CCL2, leading to CCR2+ monocyte-driven BOS development. Moreover, we found TGF-β receptor 2–dependent differentiation of CCR2+ monocytes was required for the generation of monocyte-derived AMs, which in turn promoted BOS by expanding tissue-resident memory CD8+ T cells that inflicted airway injury through Blimp-1–mediated granzyme B expression. Thus, through studying the effects of ECP, we have identified an AM functional plasticity that controls a TGF-β–dependent network that couples CCR2+ monocyte recruitment and differentiation to alloimmunity and BOS.

Published

2022

5. The role of neutrophil extracellular traps in acute lung injury

Author

Davide Scozzi, Fuyi Liao, Alexander S. Krupnick, Daniel Kreisel, and Andrew E. Gelman

Subjects

NETs (neutrophil extracellular traps), ALI (acute lung injury), ARDS (acute respiratory distress syndrome), sterile inflammatory response, infections and sepsis, COVID-19, Immunologic diseases. Allergy, RC581-607

Abstract

Acute lung injury (ALI) is a heterogeneous inflammatory condition associated with high morbidity and mortality. Neutrophils play a key role in the development of different forms of ALI, and the release of neutrophil extracellular traps (NETs) is emerging as a common pathogenic mechanism. NETs are essential in controlling pathogens, and their defective release or increased degradation leads to a higher risk of infection. However, NETs also contain several pro-inflammatory and cytotoxic molecules than can exacerbate thromboinflammation and lung tissue injury. To reduce NET-mediated lung damage and inflammation, DNase is frequently used in preclinical models of ALI due to its capability of digesting NET DNA scaffold. Moreover, recent advances in neutrophil biology led to the development of selective NET inhibitors, which also appear to reduce ALI in experimental models. Here we provide an overview of the role of NETs in different forms of ALI discussing existing gaps in our knowledge and novel therapeutic approaches to modulate their impact on lung injury.

Published

2022

6. Targeting fatty acid β-oxidation impairs monocyte differentiation and prolongs heart allograft survival

Author

Yuehui Zhu, Hao Dun, Li Ye, Yuriko Terada, Leah P. Shriver, Gary J. Patti, Daniel Kreisel, Andrew E. Gelman, and Brian W. Wong

Subjects

Metabolism, Transplantation, Medicine

Abstract

Monocytes play an important role in the regulation of alloimmune responses after heart transplantation (HTx). Recent studies have highlighted the importance of immunometabolism in the differentiation and function of myeloid cells. While the importance of glucose metabolism in monocyte differentiation and function has been reported, a role for fatty acid β-oxidation (FAO) has not been explored. Heterotopic HTx was performed using hearts from BALB/c donor mice implanted into C57BL/6 recipient mice and treated with etomoxir (eto), an irreversible inhibitor of carnitine palmitoyltransferase 1 (Cpt1), a rate-limiting step of FAO, or vehicle control. FAO inhibition prolonged HTx survival, reduced early T cell infiltration/activation, and reduced DC and macrophage infiltration to heart allografts of eto-treated recipients. ELISPOT demonstrated that splenocytes from eto-treated HTx recipients were less reactive to activated donor antigen-presenting cells. FAO inhibition reduced monocyte-to-DC and monocyte-to-macrophage differentiation in vitro and in vivo. FAO inhibition did not alter the survival of heart allografts when transplanted into Ccr2-deficient recipients, suggesting that the effects of FAO inhibition were dependent on monocyte mobilization. Finally, we confirmed the importance of FAO on monocyte differentiation in vivo using conditional deletion of Cpt1a. Our findings demonstrate that targeting FAO attenuates alloimmunity after HTx, in part through impairing monocyte differentiation.

Published

2022

7. Circulating mitochondrial DNA is an early indicator of severe illness and mortality from COVID-19

Author

Davide Scozzi, Marlene Cano, Lina Ma, Dequan Zhou, Ji Hong Zhu, Jane A. O’Halloran, Charles Goss, Adriana M. Rauseo, Zhiyi Liu, Sanjaya K. Sahu, Valentina Peritore, Monica Rocco, Alberto Ricci, Rachele Amodeo, Laura Aimati, Mohsen Ibrahim, Ramsey Hachem, Daniel Kreisel, Philip A. Mudd, Hrishikesh S. Kulkarni, and Andrew E. Gelman

Subjects

COVID-19, Immunology, Medicine

Abstract

Background Mitochondrial DNA (MT-DNA) are intrinsically inflammatory nucleic acids released by damaged solid organs. Whether circulating cell-free MT-DNA quantitation could be used to predict the risk of poor COVID-19 outcomes remains undetermined.Methods We measured circulating MT-DNA levels in prospectively collected, cell-free plasma samples from 97 subjects with COVID-19 at hospital presentation. Our primary outcome was mortality. Intensive care unit (ICU) admission, intubation, vasopressor, and renal replacement therapy requirements were secondary outcomes. Multivariate regression analysis determined whether MT-DNA levels were independent of other reported COVID-19 risk factors. Receiver operating characteristic and area under the curve assessments were used to compare MT-DNA levels with established and emerging inflammatory markers of COVID-19.Results Circulating MT-DNA levels were highly elevated in patients who eventually died or required ICU admission, intubation, vasopressor use, or renal replacement therapy. Multivariate regression revealed that high circulating MT-DNA was an independent risk factor for these outcomes after adjusting for age, sex, and comorbidities. We also found that circulating MT-DNA levels had a similar or superior area under the curve when compared against clinically established measures of inflammation and emerging markers currently of interest as investigational targets for COVID-19 therapy.Conclusion These results show that high circulating MT-DNA levels are a potential early indicator for poor COVID-19 outcomes.Funding Washington University Institute of Clinical Translational Sciences COVID-19 Research Program and Washington University Institute of Clinical Translational Sciences (ICTS) NIH grant UL1TR002345.

Published

2021

8. Galuminox: Preclinical validation of a novel PET tracer for non-invasive imaging of oxidative stress in vivo

Author

Jothilingam Sivapackiam, Fuyi Liao, Dequan Zhou, Kooresh I. Shoghi, Robert J. Gropler, Andrew E. Gelman, and Vijay Sharma

Subjects

Galuminox, Acute lung injury, Oxidative stress, PET imaging, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Overproduction of reactive oxygen species (ROS) is a well-established indicator of ongoing tissue inflammation. However, there is a scarcity of molecular imaging probes capable of providing noninvasive sensitive detection of ROS for allowing longitudinal studies of disease pathology and/or monitoring therapeutic efficacy of ROS scavengers. Herein, we report synthesis and chemical characterization of a novel metalloprobe, Galuminox, a moderately fluorescent agent that detects superoxide and hydrogen peroxide generation. Using live-cell fluorescence imaging analysis, Galuminox demonstrates ability to detect superoxide and monitor effects of ROS-attenuating agents, such as Carvedilol, Dexrazoxane, and mitoTempo in lung epithelial A549 cells. Furthermore, LPS stimulation of A549 cells that either express the mitochondria targeted fluorescent protein Keima or are stained with MitoSOX, a mitochondria-specific superoxide probe, indicates preferential co-localization of Galuminox with mitochondria producing elevated amounts of superoxide. Dynamic PET/CT scans 45 min post tail-vein administration of 68Ga-Galuminox show 4-fold higher uptake and stable retention in lungs of LPS treated mice compared to their saline-only treated counterparts. Post preclinical PET imaging, quantitative biodistribution studies also correlate with 4-fold higher retention of the radiotracer in lungs of LPS treated mice compared with their saline-only treated control counterparts. Consistent with these observations, lung cells isolated from LPS-treated mice demonstrated elevated ROS production deploying CellROX, the ROS probe. Finally, Galuminox uptake correlates with histological and physiological evidence of acute lung injury as evident by polynuclear infiltration, thickening of the alveolar epithelial membranes and increased bronchioalveolar lavage protein content. Taken collectively, these data indicate that 68Ga-Galuminox tracer uptake is a measure of ROS activity in acutely injured lungs and suggests its potential utility in monitoring oxidative stress in other diseases.

Published

2020

9. Local complement activation is associated with primary graft dysfunction after lung transplantation

Author

Hrishikesh S. Kulkarni, Kristy Ramphal, Lina Ma, Melanie Brown, Michelle Oyster, Kaitlyn N. Speckhart, Tsuyoshi Takahashi, Derek E. Byers, Mary K. Porteous, Laurel Kalman, Ramsey R. Hachem, Melanie Rushefski, Ja’Nia McPhatter, Marlene Cano, Daniel Kreisel, Masina Scavuzzo, Brigitte Mittler, Edward Cantu III, Katrine Pilely, Peter Garred, Jason D. Christie, John P. Atkinson, Andrew E. Gelman, and Joshua M. Diamond

Subjects

Pulmonology, Medicine

Abstract

BACKGROUND The complement system plays a key role in host defense but is activated by ischemia/reperfusion injury (IRI). Primary graft dysfunction (PGD) is a form of acute lung injury occurring predominantly due to IRI, which worsens survival after lung transplantation (LTx). Local complement activation is associated with acute lung injury, but whether it is more reflective of allograft injury compared with systemic activation remains unclear. We proposed that local complement activation would help identify those who develop PGD after LTx. We also aimed to identify which complement activation pathways are associated with PGD.METHODS We performed a multicenter cohort study at the University of Pennsylvania and Washington University School of Medicine. Bronchoalveolar lavage (BAL) and plasma specimens were obtained from recipients within 24 hours after LTx. PGD was scored based on the consensus definition. Complement activation products and components of each arm of the complement cascade were measured using ELISA.RESULTS In both cohorts, sC4d and sC5b-9 levels were increased in BAL of subjects with PGD compared with those without PGD. Subjects with PGD also had higher C1q, C2, C4, and C4b, compared with subjects without PGD, suggesting classical and lectin pathway involvement. Ba levels were higher in subjects with PGD, suggesting alternative pathway activation. Among lectin pathway–specific components, MBL and FCN-3 had a moderate-to-strong correlation with the terminal complement complex in the BAL but not in the plasma.CONCLUSION Complement activation fragments are detected in the BAL within 24 hours after LTx. Components of all 3 pathways are locally increased in subjects with PGD. Our findings create a precedent for investigating complement-targeted therapeutics to mitigate PGD.FUNDING This research was supported by the NIH, American Lung Association, Children’s Discovery Institute, Robert Wood Johnson Foundation, Cystic Fibrosis Foundation, Barnes-Jewish Hospital Foundation, Danish Heart Foundation, Danish Research Foundation of Independent Research, Svend Andersen Research Foundation, and Novo Nordisk Research Foundation.

Published

2020

10. CD36 Deficiency Impairs the Small Intestinal Barrier and Induces Subclinical Inflammation in MiceSummary

Author

Vincenza Cifarelli, Stoyan Ivanov, Yan Xie, Ni-Huiping Son, Brian T. Saunders, Terri A. Pietka, Trevor M. Shew, Jun Yoshino, Sinju Sundaresan, Nicholas O. Davidson, Ira J. Goldberg, Andrew E. Gelman, Bernd H. Zinselmeyer, Gwendalyn J. Randolph, and Nada A. Abumrad

Subjects

Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: CD36 has immunometabolic actions and is abundant in the small intestine on epithelial, endothelial, and immune cells. We examined the role of CD36 in gut homeostasis by using mice null for CD36 (CD36KO) and with CD36 deletion specific to enterocytes (Ent-CD36KO) or endothelial cells (EC-CD36KO). Methods: Intestinal morphology was evaluated by using immunohistochemistry and electron microscopy. Intestinal inflammation was determined from neutrophil infiltration and expression of cytokines, toll-like receptors, and cyclooxygenase-2. Barrier integrity was assessed from circulating lipopolysaccharide and dextran administered intragastrically. Epithelial permeability to luminal dextran was visualized by using two-photon microscopy. Results: The small intestines of CD36KO mice fed a chow diet showed several abnormalities including extracellular matrix accumulation with increased expression of extracellular matrix proteins, evidence of neutrophil infiltration, inflammation, and compromised barrier function. Electron microscopy showed shortened desmosomes with decreased desmocollin 2 expression. Systemically, leukocytosis and neutrophilia were present together with 80% reduction of anti-inflammatory Ly6Clow monocytes. Bone marrow transplants supported the primary contribution of non-hematopoietic cells to the inflammatory phenotype. Specific deletion of endothelial but not of enterocyte CD36 reproduced many of the gut phenotypes of germline CD36KO mice including fibronectin deposition, increased interleukin 6, neutrophil infiltration, desmosome shortening, and impaired epithelial barrier function. Conclusions: CD36 loss results in chronic neutrophil infiltration of the gut, impairs barrier integrity, and systemically causes subclinical inflammation. Endothelial cell CD36 deletion reproduces the major intestinal phenotypes. The findings suggest an important role of the endothelium in etiology of gut inflammation and loss of epithelial barrier integrity. Keywords: Neutrophils, Endothelium, Fibronectin, Collagen

Published

2017

11. Selective targeting of IL-2 to NKG2D bearing cells for improved immunotherapy

Author

Reza Ghasemi, Eric Lazear, Xiaoli Wang, Saeed Arefanian, Alexander Zheleznyak, Beatriz M. Carreno, Ryuji Higashikubo, Andrew E. Gelman, Daniel Kreisel, Daved H. Fremont, and Alexander Sasha Krupnick

Subjects

Science

Abstract

High-affinity IL-2Rα expressed by Tregs mitigates the potential of IL-2 use in cancer therapy. Here, the authors fuse IL-2 with an NKDG2 binding domain, and show that it induces IL-2 signalling selectively in NKG2D+cells, delaying tumour growth in mice without the side effects of conventional IL-2 therapy.

Published

2016

12. Updated Views on Neutrophil Responses in Ischemia-Reperfusion Injury

Author

Hailey M. Shepherd, Jason M. Gauthier, Yuriko Terada, Wenjun Li, Alexander S. Krupnick, Andrew E. Gelman, and Daniel Kreisel

Subjects

Transplantation, Neutrophil Infiltration, Neutrophils, Reperfusion Injury, Humans, Lung, Lung Transplantation

Abstract

Ischemia-reperfusion injury is an inevitable event during organ transplantation and represents a primary risk factor for the development of early graft dysfunction in lung, heart, liver, and kidney transplant recipients. Recent studies have implicated recipient neutrophils as key mediators of this process and also have found that early innate immune responses after transplantation can ultimately augment adaptive alloimmunity and affect late graft outcomes. Here, we discuss signaling pathways involved in neutrophil recruitment and activation after ischemia-mediated graft injury in solid organ transplantation with an emphasis on lung allografts, which have been the focus of recent studies. These findings suggest novel therapeutic interventions that target ischemia-reperfusion injury-mediated graft dysfunction in transplant recipients.

Published

2023

13. Solving the Conundrum of Eosinophils in Alloimmunity

Author

Cherie Alissa Lynch, Yizhan Guo, Zhongcheng Mei, Daniel Kreisel, Andrew E. Gelman, Elizabeth A. Jacobsen, and Alexander Sasha Krupnick

Subjects

Eosinophils, Transplantation, Mice, Graft Survival, Animals, Humans, Transplantation, Homologous, Organ Transplantation, Lung Transplantation

Abstract

Eosinophils are bone-marrow-derived granulocytes known for their ability to facilitate clearance of parasitic infections and their association with asthma and other inflammatory diseases. The purpose of this review is to discuss the currently available human observational and animal experimental data linking eosinophils to the immunologic response in solid organ transplantation. First, we present observational human studies that demonstrate a link between transplantation and eosinophils yet were unable to define the exact role of this cell population. Next, we describe published experimental models and demonstrate a defined mechanistic role of eosinophils in downregulating the alloimmune response to murine lung transplants. The overall summary of this data suggests that further studies are needed to define the role of eosinophils in multiple solid organ allografts and points to the possibility of manipulating this cell population to improve graft survival.

Published

2023

14. Loss of stromal cell Thy-1 plays a critical role in lipopolysaccharide induced chronic lung allograft dysfunction

Author

Atsushi Hata, Yizhan Guo, Andrew E. Miller, Mika Hata, Zhongcheng Mei, Amir Manafi, Dongge Li, Anirban Banerjee, Eric Lazear, Christine Lau, Andrew E. Gelman, Daniel Kreisel, Ichiro Yoshino, David Wilkes, Thomas H. Barker, and Alexander Sasha Krupnick

Subjects

Lipopolysaccharides, Mice, Inbred C57BL, Pulmonary and Respiratory Medicine, Mice, Transplantation, Animals, Surgery, Stromal Cells, Allografts, Cardiology and Cardiovascular Medicine, Fibrosis, Lung, Lung Transplantation

Abstract

Long-term survival of lung transplants lags behind other solid organs due to early onset of a fibrotic form of chronic rejection known as chronic lung allograft dysfunction (CLAD). Preventing CLAD is difficult as multiple immunologic and physiologic insults contribute to its development. Targeting fibroblast activation, which is the final common pathway leading to CLAD, offers the opportunity to ameliorate fibrosis irrespective of the initiating insult. Thy-1 is a surface glycoprotein that controls fibroblast differentiation and activation.To study the role of Thy-1 in CLAD, we utilized the minor antigen mismatched C57BL/6 (B6More severe CLAD was evident in B6Our findings suggest that the loss of Thy-1 on fibroblasts is a previously unrecognized cause of CLAD and its replacement may offer therapeutic applications for amelioration of this disease post-transplantation in the setting of infectious stress responses.

Published

2022

15. Ischemia reperfusion injury facilitates lung allograft acceptance through IL-33-mediated activation of donor-derived IL-5 producing group 2 innate lymphoid cells

Author

Yizhan Guo, Zhongcheng Mei, Dongge Li, Anirban Banerjee, May A. Khalil, Allen Burke, Jon Ritter, Christine Lau, Daniel Kreisel, Andrew E. Gelman, Elizabeth Jacobsen, Irina G. Luzina, Sergei P. Atamas, and Alexander Sasha Krupnick

Subjects

Mice, Transplantation, Reperfusion Injury, Animals, Immunology and Allergy, Pharmacology (medical), Lymphocytes, Interleukin-5, Allografts, Interleukin-33, Lung, Immunity, Innate

Abstract

Pathways regulating lung alloimmune responses differ from most other solid organs and remain poorly explored. Based on our recent work identifying the unique role of eosinophils in downregulating lung alloimmunity, we sought to define pathways contributing to eosinophil migration and homeostasis. Using a murine lung transplant model, we have uncovered that immunosuppression increases eosinophil infiltration into the allograft in an IL-5-dependent manner. IL-5 production depends on immunosuppression-mediated preservation of donor-derived group 2 innate lymphoid cells (ILC2). We further describe that ischemia reperfusion injury upregulates the expression of IL-33, which functions as the dominant and nonredundant mediator of IL-5 production by graft-resident ILC2. Our work thus identifies unique cellular mechanisms that contribute to lung allograft acceptance. Notably, ischemia reperfusion injury, widely considered to be solely deleterious to allograft survival, can also downregulate alloimmune responses by initiating unique pathways that promote IL-33/IL-5/eosinophil-mediated tolerance.

Published

2022

16. Update on the Features and Measurements of Experimental Acute Lung Injury in Animals: An Official American Thoracic Society Workshop Report

Author

Hrishikesh S. Kulkarni, Janet S. Lee, Julie A. Bastarache, Wolfgang M. Kuebler, Gregory P. Downey, Guillermo M. Albaiceta, William A. Altemeier, Antonio Artigas, Jason H. T. Bates, Carolyn S. Calfee, Charles S. Dela Cruz, Robert P. Dickson, Joshua A. Englert, Jeffrey I. Everitt, Michael B. Fessler, Andrew E. Gelman, Kymberly M. Gowdy, Steve D. Groshong, Susanne Herold, Robert J. Homer, Jeffrey C. Horowitz, Connie C. W. Hsia, Kiyoyasu Kurahashi, Victor E. Laubach, Mark R. Looney, Rudolf Lucas, Nilam S. Mangalmurti, Anne M. Manicone, Thomas R. Martin, Sadis Matalon, Michael A. Matthay, Daniel F. McAuley, Sharon A. McGrath-Morrow, Joseph P. Mizgerd, Stephanie A. Montgomery, Bethany B. Moore, Alexandra Noël, Carrie E. Perlman, John P. Reilly, Eric P. Schmidt, Shawn J. Skerrett, Tomeka L. Suber, Charlotte Summers, Benjamin T. Suratt, Masao Takata, Rubin Tuder, Stefan Uhlig, Martin Witzenrath, Rachel L. Zemans, and Gutavo Matute-Bello

Subjects

Pulmonary and Respiratory Medicine, Clinical Biochemistry, Cell Biology, Molecular Biology

Published

2022

17. Supplementary Figure 4 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 30K, Cytotoxicity of NK cells from C57BL/10 and Balb/c mice

Published

2023

18. Supplementary Figure 1 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 36K, T cell depletion in AJ mice

Published

2023

19. Supplementary Figure 2 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 25K, Cytotoxicity of neutrophils and monocytes/macrophages

Published

2023

20. Supplementary Figure 3 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 21K, Strain-specific differences in Yac-1 cytotoxcity

Published

2023

21. Supplementary Figure Legends 1-6 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 33K

Published

2023

22. Supplementary Figure 5 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 76K, Microsatellite mapping of the 129/SvEv.B6-NKC Rag2-/- mouse

Published

2023

23. Supplementary Figure 6 from Strain-Specific Variation in Murine Natural Killer Gene Complex Contributes to Differences in Immunosurveillance for Urethane-Induced Lung Cancer

Author

Alexander S. Krupnick, Robert D. Schreiber, Jack D. Bui, Wayne M. Yokoyama, Samantha M. Taffner, Ming You, Beatriz M. Carreno, Charuhas Deshpande, Kelsey A. Toth, J. Michael White, Haris G. Vikis, Xue Lin, Ryuji Higashikubo, Andrew E. Gelman, and Daniel Kreisel

Abstract

PDF file - 47K, SNP rs13459098 in the Pas-1 locus is of 129 origin in 129/SvEv.B6-NKC Rag2-/- mice

Published

2023

24. Lung epithelial cell–derived C3 protects against pneumonia-induced lung injury

Author

Sanjaya K. Sahu, Ayşe N. Ozantürk, Devesha H. Kulkarni, Lina Ma, Ruteja A. Barve, Linus Dannull, Angel Lu, Marick Starick, Ja’Nia McPhatter, Lorena Garnica, Maxwell Sanfillipo-Burchman, Jeremy Kunen, Xiaobo Wu, Andrew E. Gelman, Steven L. Brody, John P. Atkinson, and Hrishikesh S. Kulkarni

Subjects

Immunology, General Medicine

Abstract

The complement component C3 is a fundamental plasma protein for host defense, produced largely by the liver. However, recent work has demonstrated the critical importance of tissue-specific C3 expression in cell survival. Here, we analyzed the effects of local versus peripheral sources of C3 expression in a model of acute bacterial pneumonia induced by Pseudomonas aeruginosa . Whereas mice with global C3 deficiency had severe pneumonia-induced lung injury, those deficient only in liver-derived C3 remained protected, comparable to wild-type mice. Human lung transcriptome analysis showed that secretory epithelial cells, such as club cells, express high levels of C3 mRNA. Mice with tamoxifen-induced C3 gene ablation from club cells in the lung had worse pulmonary injury compared with similarly treated controls, despite maintaining normal circulating C3 levels. Last, in both the mouse pneumonia model and cultured primary human airway epithelial cells, we showed that stress-induced death associated with C3 deficiency parallels that seen in Factor B deficiency rather than C3a receptor deficiency. Moreover, C3-mediated reduction in epithelial cell death requires alternative pathway component Factor B. Thus, our findings suggest that a pathway reliant on locally derived C3 and Factor B protects the lung mucosal barrier.

Published

2023

25. Lung protective ventilation based on donor size is associated with a lower risk of severe primary graft dysfunction after lung transplantation

Author

Elbert P. Trulock, Bahaa Bedair, Ruben G. Nava, Jennifer Alexander-Brett, Chad A. Witt, Andrew E. Gelman, L.K. Tague, Derek E. Byers, Rodrigo Vazquez-Guillamet, Hrishikesh S. Kulkarni, Ramsey R. Hachem, Daniel Kreisel, and Varun Puri

Subjects

Lung Diseases, Male, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Primary Graft Dysfunction, Lower risk, Gastroenterology, Article, Internal medicine, Humans, Medicine, Lung transplantation, Lung volumes, Aged, Proportional Hazards Models, Retrospective Studies, Mechanical ventilation, Transplantation, business.industry, Proportional hazards model, Body Weight, Total Lung Capacity, Retrospective cohort study, Organ Size, Middle Aged, respiratory system, Respiration, Artificial, Survival Rate, Logistic Models, Breathing, Female, Surgery, Cardiology and Cardiovascular Medicine, business, Lung Transplantation

Abstract

BACKGROUND: Mechanical ventilation immediately after lung transplantation may impact the development of primary graft dysfunction (PGD), particularly in cases of donor-recipient size mismatch as ventilation is typically based on recipient rather than donor size. METHODS: We conducted a retrospective cohort study of adult bilateral lung transplant recipients at our center between January 2010 and January 2017. We defined donor-based lung protective ventilation (dLPV) as 6 to 8 ml/kg of donor ideal body weight and plateau pressure

Published

2021

26. Short telomeres in lung transplantation: Known unknowns

Author

Sravanthi Nandavaram, Satish Chandrashekaran, and Andrew E. Gelman

Subjects

Pulmonary and Respiratory Medicine, Transplantation, Surgery, Cardiology and Cardiovascular Medicine

Published

2022

27. Club Cell Secretory Protein in Lung Disease: Emerging Concepts and Potential Therapeutics

Author

Tereza Martinu, Jamie L. Todd, Andrew E. Gelman, Stefano Guerra, and Scott M. Palmer

Subjects

General Medicine, General Biochemistry, Genetics and Molecular Biology

Abstract

Club cell secretory protein (CCSP), also known as secretoglobin 1A1 (gene name SCGB1A1), is one of the most abundant proteins in the lung, primarily produced by club cells of the distal airway epithelium. At baseline, CCSP is found in large concentrations in lung fluid specimens and can also be detected in the blood and urine. Obstructive lung diseases are generally associated with reduced CCSP levels, thought to be due to decreased CCSP production or club cell depletion. Conversely, several restrictive lung diseases have been found to have increased CCSP levels both in the lung and in the circulation, likely related to club cell dysregulation as well as increasedlung permeability. Recent studies demonstrate multiple mechanisms by which CCSP dampens acute and chronic lung inflammation. Given these anti-inflammatory effects, CCSP represents a novel potential therapeutic modality in lung disease.

Published

2022

28. Innate immunity in lung transplantation

Author

Hailey M. Shepherd, Andrew E. Gelman, Wenjun Li, Daniel Kreisel, Jason M. Gauthier, and Alexander S. Krupnick

Subjects

Graft Rejection, 0301 basic medicine, Pulmonary and Respiratory Medicine, Programmed cell death, Graft failure, medicine.medical_treatment, Primary Graft Dysfunction, Inflammation, 030230 surgery, Lung injury, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Lung transplantation, Transplantation, Innate immune system, business.industry, respiratory system, Immunity, Innate, surgical procedures, operative, 030104 developmental biology, Immunology, Surgery, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Lung Transplantation

Abstract

Innate immune pathways early after pulmonary transplantation have been shown to cause primary graft dysfunction (PGD) and also predispose to late graft failure. Recent studies in animal models have elucidated critical mechanisms governing such innate immune responses. Here, we discuss pathways of inflammatory cell death, triggers for sterile and infectious inflammation, and signaling cascades that mediate lung injury early after transplantation. These studies highlight potential avenues for lung-specific therapies early following lung transplantation to dampen innate immune responses and improve outcomes.

Published

2021

29. Selective Imaging of Lung Macrophages Using [11C]PBR28-Based Positron Emission Tomography

Author

Andrew E. Gelman, Kangyun Wu, Kiran Kumar Solingapuram Sai, Elizabeth Arentson, Eugene Agapov, Delphine L. Chen, Michael J. Holtzman, Katherine J. Spayd, Richard A. Pierce, Jeffrey J. Atkinson, Kirby T Moreland, Jacquelyn T. Engle, Derek E. Byers, Richard Laforest, and Kelsey Toth

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Lung, biology, CD68, business.industry, medicine.medical_treatment, Macrophage polarization, Inflammation, respiratory system, Transplantation, medicine.anatomical_structure, Oncology, Neutrophil elastase, medicine, Translocator protein, biology.protein, Lung transplantation, Radiology, Nuclear Medicine and imaging, medicine.symptom, business

Abstract

We tested whether the translocator protein (TSPO)-targeted positron emission tomography (PET) tracer, N-acetyl-N-(2-[11C]methoxybenzyl)-2-phenoxy-5-pyridinamine ([11C]PBR28), could distinguish macrophage dominant from neutrophilic inflammation better than 2-deoxy-2-[18F]fluoro-D-glucose ([18F]FDG) in mouse models of lung inflammation and assessed TSPO association with macrophages in lung tissue from the mouse models and in patients with chronic obstructive pulmonary disease (COPD). MicroPET imaging quantified [11C]PBR28 and [18F]FDG lung uptake in wild-type (Wt) C57BL/6J or heterozygous transgenic monocyte-deficient Wt/opT mice at 49 days after Sendai virus (SeV) infection, during macrophage-dominant inflammation, and in Wt mice at 3 days after SeV infection or 24 h after endotoxin instillation during neutrophilic inflammation. Immunohistochemical staining for TSPO in macrophages and neutrophils was performed using Mac3 and Ly6G for cell identification in mouse lung sections and CD68 and neutrophil elastase (NE) in human lung sections taken from explanted lungs from patients with COPD undergoing lung transplantation and donor lungs rejected for transplantation. Differences in tracer uptake among SeV-infected, endotoxin-treated, and uninfected/untreated control mice and in TSPO staining between neutrophils and macrophage populations in human lung sections were tested using analysis of variance. In Wt mice, [11C]PBR28 uptake (% injected dose/ml lung tissue) increased significantly with macrophage-dominant inflammation at 49 days (D49) after SeV infection compared to controls (p =

Published

2021

30. Pericardial Mitochondrial DNA Levels Are Associated With Atrial Fibrillation After Cardiac Surgery

Author

Richard B. Schuessler, Joshua L. Manghelli, Robert M. MacGregor, Timothy S. Lancaster, Jason M. Gauthier, Spencer J. Melby, Meghan O. Kelly, Andrew E. Gelman, Ralph J. Damiano, Daniel I. Carter, Davide Scozzi, and Ali J. Khiabani

Subjects

Male, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Chemokine, medicine.medical_treatment, Heart Valve Diseases, Inflammation, 030204 cardiovascular system & hematology, DNA, Mitochondrial, Article, 03 medical and health sciences, Postoperative Complications, 0302 clinical medicine, Internal medicine, Atrial Fibrillation, medicine, Humans, Cardiac Surgical Procedures, Coronary Artery Bypass, Aged, Retrospective Studies, biology, business.industry, Pericardial fluid, Atrial fibrillation, Middle Aged, medicine.disease, Cardiac surgery, Cytokine, medicine.anatomical_structure, 030228 respiratory system, Cardiology, biology.protein, Female, Surgery, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Complication, Pericardium, Artery

Abstract

Postoperative atrial fibrillation (POAF) is the most common complication after cardiac surgery, and is associated with increased morbidity and mortality. Inflammation has been implicated as an etiology of POAF. Mitochondrial DNA (mtDNA) has been shown to initiate inflammation. This study analyzed inflammatory mechanisms of POAF by evaluating mtDNA, neutrophils, and cytokines/chemokines in the pericardial fluid and blood after cardiac surgery.Blood and pericardial fluid from patients who underwent coronary artery bypass or heart valve surgery, or both, were collected intraoperatively and at 4, 12, 24, and 48 hours postoperatively. Real-time polymerase chain reaction was used to quantify mtDNA in the pericardial fluid and blood. A Luminex (Luminex Corp, Austin, TX) assay was used to study cytokine and chemokine levels. Flow cytometry was used to analyze neutrophil infiltration and activation in the pericardial fluid.Samples from 100 patients were available for analysis. Postoperatively, mtDNA and multiple cytokine levels were higher in the pericardial fluid versus blood. Patients who had POAF had significantly higher levels of mtDNA in the pericardial fluid compared with patients who did not (P.001, area under the curve 0.74). There was no difference in the mtDNA concentration in the blood between the POAF group and non-POAF group (P = .897). Neutrophil concentration increased in the pericardial fluid over time from a baseline of 0.8% to 56% at 48 hours (P.01).The pericardial space has a high concentration of inflammatory mediators postoperatively. Mitochondrial DNA in the pericardial fluid was strongly associated with the development of POAF. This finding provides insight into a possible mechanism of inflammation that may contribute to POAF, and may offer novel therapeutic targets.

Published

2021

31. Bacterial products in donor airways prevent the induction of lung transplant tolerance

Author

Andrew E. Gelman, Satona Tanaka, Tsuyoshi Takahashi, Jon H. Ritter, Wenjun Li, Ruben G. Nava, Ramsey R. Hachem, Jason M. Gauthier, Ryuji Higashikubo, Ankit Bharat, Daniel Kreisel, Yuriko Terada, Varun Puri, Kohei Hashimoto, and Alexander S. Krupnick

Subjects

Graft Rejection, Adoptive cell transfer, CD11c, 030230 surgery, Major histocompatibility complex, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Animals, Immunology and Allergy, Pharmacology (medical), Lung, Mice, Knockout, Mice, Inbred BALB C, Transplantation, biology, business.industry, Lipopeptide, Mice, Inbred C57BL, TLR2, surgical procedures, operative, medicine.anatomical_structure, chemistry, Immunology, biology.protein, Transplantation Tolerance, business, CD8, Lung Transplantation

Abstract

Although postoperative bacterial infections can trigger rejection of pulmonary allografts, the impact of bacterial colonization of donor grafts on alloimmune responses to transplanted lungs remains unknown. Here, we tested the hypothesis that bacterial products present within donor grafts at the time of implantation promote lung allograft rejection. Administration of the toll-like receptor 2 (TLR2) agonist Pam3 Cys4 to Balb/c wild-type grafts triggered acute cellular rejection after transplantation into B6 wild-type recipients that received perioperative costimulatory blockade. Pam3 Cys4 -triggered rejection was associated with an expansion of CD8+ T lymphocytes and CD11c+ CD11bhi MHC (major histocompatibility complex) class II+ antigen-presenting cells within the transplanted lungs. Rejection was prevented when lungs were transplanted into TLR2-deficient recipients but not when MyD88-deficient donors were used. Adoptive transfer of B6 wild-type monocytes, but not T cells, following transplantation into B6 TLR2-deficient recipients restored the ability of Pam3 Cys4 to trigger acute cellular rejection. Thus, we have demonstrated that activation of TLR2 by a bacterial lipopeptide within the donor airways prevents the induction of lung allograft tolerance through a process mediated by recipient-derived monocytes. Our work suggests that donor lungs harboring bacteria may precipitate an inflammatory response that can facilitate allograft rejection.

Published

2021

32. Mouse Heterotopic Cervical Cardiac Transplantation Utilizing Vascular Cuffs

Author

Daniel Kreisel, Kory J. Lavine, Andrew E. Gelman, Alexander S. Krupnick, Hailey M. Shepherd, and Wenjun Li

Subjects

Graft Rejection, Mice, Transplantation, Heterotopic, General Immunology and Microbiology, Carotid Artery, Common, General Chemical Engineering, General Neuroscience, Animals, Heart Transplantation, General Biochemistry, Genetics and Molecular Biology, Article, Neck

Abstract

Murine models of cardiac transplantation are frequently utilized to study ischemia-reperfusion injury, innate and adaptive immune responses after transplantation, and the impact of immunomodulatory therapies on graft rejection. Heterotopic cervical heart transplantation in mice was first described in 1991 using sutured anastomoses and subsequently modified to include cuff techniques. This modification allowed for improved success rates, and since then, there have been multiple reports that have proposed further technical improvements. However, translation into more widespread utilization remains limited due to the technical difficulty associated with graft anastomoses, which requires precision to achieve adequate length and caliber of the cuffs to avoid vascular anastomotic twisting or excessive tension, which can result in damage to the graft. The present protocol describes a modified technique for performing heterotopic cervical cardiac transplantation in mice which involves cuff placement on the recipient's common carotid artery and the donor's pulmonary artery in alignment with the direction of the blood flow.

Published

2022

33. Role of tertiary lymphoid organs in the regulation of immune responses in the periphery

Author

Amit I. Bery, Hailey M. Shepherd, Wenjun Li, Alexander S. Krupnick, Andrew E. Gelman, and Daniel Kreisel

Subjects

Pharmacology, Cellular and Molecular Neuroscience, Molecular Medicine, Cell Biology, Molecular Biology

Published

2022

34. Necroptosis triggers spatially restricted neutrophil-mediated vascular damage during lung ischemia reperfusion injury

Author

Wenjun Li, Yuriko Terada, Yulia Y. Tyurina, Vladimir A. Tyurin, Amit I. Bery, Jason M. Gauthier, Ryuji Higashikubo, Alice Y. Tong, Dequan Zhou, Felix Nunez-Santana, Emilia Lecuona, Adil Hassan, Kohei Hashimoto, Davide Scozzi, Varun Puri, Ruben G. Nava, Alexander S. Krupnick, Kory J. Lavine, Andrew E. Gelman, Mark J. Miller, Valerian E. Kagan, Ankit Bharat, and Daniel Kreisel

Subjects

Mice, Knockout, Toll-Like Receptor 4, Mice, Multidisciplinary, Neutrophil Infiltration, Neutrophils, Reperfusion Injury, Necroptosis, Animals, Humans, Endothelium, Vascular, Lung

Abstract

Ischemia reperfusion injury represents a common pathological condition that is triggered by the release of endogenous ligands. While neutrophils are known to play a critical role in its pathogenesis, the tissue-specific spatiotemporal regulation of ischemia-reperfusion injury is not understood. Here, using oxidative lipidomics and intravital imaging of transplanted mouse lungs that are subjected to severe ischemia reperfusion injury, we discovered that necroptosis, a nonapoptotic form of cell death, triggers the recruitment of neutrophils. During the initial stages of inflammation, neutrophils traffic predominantly to subpleural vessels, where their aggregation is directed by chemoattractants produced by nonclassical monocytes that are spatially restricted in this vascular compartment. Subsequent neutrophilic disruption of capillaries resulting in vascular leakage is associated with impaired graft function. We found that TLR4 signaling in vascular endothelial cells and downstream NADPH oxidase 4 expression mediate the arrest of neutrophils, a step upstream of their extravasation. Neutrophil extracellular traps formed in injured lungs and their disruption with DNase prevented vascular leakage and ameliorated primary graft dysfunction. Thus, we have uncovered mechanisms that regulate the initial recruitment of neutrophils to injured lungs, which result in selective damage to subpleural pulmonary vessels and primary graft dysfunction. Our findings could lead to the development of new therapeutics that protect lungs from ischemia reperfusion injury.

Published

2022

35. Targeting fatty acid beta-oxidation impairs monocyte differentiation and prolongs heart allograft survival

Author

Yuehui Zhu, Hao Dun, Li Ye, Yuriko Terada, Leah P. Shriver, Gary J. Patti, Daniel Kreisel, Andrew E. Gelman, and Brian W. Wong

Subjects

digestive, oral, and skin physiology, food and beverages

Abstract

Monocytes play an important role in the regulation of alloimmune responses after heart transplantation (HTx). Recent studies have highlighted the importance of immunometabolism in the differentiation and function of myeloid cells. While the importance of glucose metabolism in monocyte differentiation and function has been reported, a role for fatty acid β-oxidation (FAO) has not been explored. Heterotopic HTx was performed using hearts from Balb/c donor mice implanted into C57Bl/6 recipient mice and treated with etomoxir (eto), an irreversible inhibitor of carnitine palmitoyltransferase 1 (Cpt1), a rate-limiting step of FAO, or vehicle control. FAO inhibition prolonged HTx survival, reduced early T cell infiltration/ activation and reduced dendritic cell (DC) and macrophage infiltration to heart allografts of eto-treated HTx recipients. ELISPOT demonstrated eto-treated HTx were less reactive to activated donor antigen presenting cells. FAO inhibition reduced monocyte-to-DC and monocyte-to-macrophage differentiation in vitro and in vivo. Further, FAO inhibition did not alter the survival of heart allografts when transplanted into Ccr2-deficient recipients, suggesting the effects of FAO inhibition on reduced immune cell infiltration and increased heart allograft survival were dependent on monocyte mobilization. Finally, we confirmed the importance of FAO on monocyte differentiation in vivo using conditional deletion of Cpt1a. Our findings demonstrate that targeting FAO attenuates alloimmunity after HTx, in part through impairing monocyte differentiation.

Published

2022

36. Role of tertiary lymphoid organs in the regulation of immune responses in the periphery

Author

Amit I, Bery, Hailey M, Shepherd, Wenjun, Li, Alexander S, Krupnick, Andrew E, Gelman, and Daniel, Kreisel

Subjects

Inflammation, T-Lymphocytes, Immunity, Humans, Lymph Nodes, Germinal Center

Abstract

Tertiary lymphoid organs (TLOs) are collections of immune cells resembling secondary lymphoid organs (SLOs) that form in peripheral, non-lymphoid tissues in response to local chronic inflammation. While their formation mimics embryologic lymphoid organogenesis, TLOs form after birth at ectopic sites in response to local inflammation resulting in their ability to mount diverse immune responses. The structure of TLOs can vary from clusters of B and T lymphocytes to highly organized structures with B and T lymphocyte compartments, germinal centers, and lymphatic vessels (LVs) and high endothelial venules (HEVs), allowing them to generate robust immune responses at sites of tissue injury. Although our understanding of the formation and function of these structures has improved greatly over the last 30 years, their role as mediators of protective or pathologic immune responses in certain chronic inflammatory diseases remains enigmatic and may differ based on the local tissue microenvironment in which they form. In this review, we highlight the role of TLOs in the regulation of immune responses in chronic infection, chronic inflammatory and autoimmune diseases, cancer, and solid organ transplantation.

Published

2021

37. Vendor-specific microbiome controls both acute and chronic murine lung allograft rejection by altering CD4+Foxp3+ regulatory T cell levels

Author

Yizhan Guo, Thomas H. Barker, Anirban Banerjee, Qing Wang, Amir Manafi, Bayan Mahgoub, Oscar Okwudiri Onyema, Daniel Kreisel, Andrew E. Gelman, Zhongcheng Mei, Mark H. Stoler, Dongge Li, David S. Wilkes, and Alexander S. Krupnick

Subjects

Transplantation, Lung, medicine.drug_class, business.industry, Regulatory T cell, Antibiotics, Alloimmunity, FOXP3, Perioperative, medicine.anatomical_structure, Antigen, Immunology, medicine, Immunology and Allergy, Pharmacology (medical), Microbiome, business

Abstract

Despite standardized postoperative care, some lung transplant patients suffer multiple episodes of acute and chronic rejection while others avoid graft problems for reasons that are poorly understood. Using an established model of C57BL/10 to C57BL/6 minor antigen mismatched single lung transplantation, we now demonstrate that the recipient microbiota contributes to variability in the alloimmune response. Specifically, mice from the Envigo facility in Frederick, Maryland contain nearly double the number of CD4+ Foxp3+ regulatory T cells (Tregs ) than mice from the Jackson facility in Bar Harbor, Maine or the Envigo facility in Indianapolis, Indiana (18 vs 9 vs 7%). Lung graft recipients from the Maryland facility thus do not develop acute or chronic rejection. Treatment with broad-spectrum antibiotics decreases Tregs and increases both acute and chronic graft rejection in otherwise tolerant strains of mice. Constitutive depletion of regulatory T cells, using Foxp3-driven expression of diphtheria toxin receptor, leads to the development of chronic rejection and supports the role of Tregs in both acute and chronic alloimmunity. Taken together, our data demonstrate that the microbiota of certain individuals may contribute to tolerance through Treg -dependent mechanisms and challenges the practice of indiscriminate broad-spectrum antibiotic use in the perioperative period.

Published

2019

38. The emerging role of regulatory T cells following lung transplantation

Author

Daniel Kreisel, Andrew E. Gelman, Alexander S. Krupnick, Jason M. Gauthier, and M. Shea Harrison

Subjects

Graft Rejection, 0301 basic medicine, medicine.medical_treatment, Immunology, Biology, medicine.disease_cause, T-Lymphocytes, Regulatory, Autoimmunity, 03 medical and health sciences, 0302 clinical medicine, Transplantation Immunology, medicine, Animals, Humans, Immunology and Allergy, Lung transplantation, Organ system, Lung, Human studies, Cancer, Allografts, medicine.disease, Kidney Transplantation, Liver Transplantation, Transplantation, 030104 developmental biology, medicine.anatomical_structure, Transplantation Tolerance, Solid organ transplantation, Lung Transplantation, 030215 immunology

Abstract

Regulatory T cells (Treg) have proven to be a powerful immunologic force in nearly every organ system and hold therapeutic potential for a wide range of diseases. Insights gained from non-transplant pathologies, such as infection, cancer, and autoimmunity, are now being translated to the field of solid organ transplantation, particularly for livers and kidneys. Recent insights from animal models of lung transplantation have established that Tregs play a vital role in suppressing rejection and facilitating tolerance of lung allografts, and such discoveries are being validated in human studies and preclinical trials. Given that long-term outcomes following lung transplantation remain profoundly limited by chronic rejection, Treg therapy holds the potential to significantly improve patient outcomes and should be aggressively investigated.

Published

2019

39. Increased complement activation is a distinctive feature of severe SARS-CoV-2 infection

Author

Jane A. O’Halloran, C-Hong Chang, Rachel M. Presti, Xiaobo Wu, Rebecca E Schriefer, Alfred H.J. Kim, Vasanthan Kuppuswamy, Hanming Zhang, Parveen Bahel, Henry M. Rinder, John P. Atkinson, George Goshua, Andrew E. Gelman, Sanjaya Kumar Sahu, Hyung J. Chun, Phillip Mudd, Tingting Lei, Lina Ma, Aaron Day, Christina Price, Hrishikesh S. Kulkarni, Alexander B Pine, Charles S. Dela Cruz, Daniel Reynolds, Charles W. Goss, Adriana M Rauseo, Matthew L Meizlish, Ja’Nia McPhatter, Jamal Bajwa, Marlene Cano, and Alfred Ian Lee

Subjects

Male, 0301 basic medicine, Critical Illness, Immunology, Thrombomodulin, Article, law.invention, Cohort Studies, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Von Willebrand factor, law, Humans, Medicine, Prospective Studies, Prospective cohort study, Complement Activation, Research Articles, Aged, biology, business.industry, R-Articles, Patient Acuity, COVID-19, Thrombosis, General Medicine, Middle Aged, Intensive care unit, Complement (complexity), Complement system, Coronavirus, Treatment Outcome, 030104 developmental biology, Respiratory failure, 030220 oncology & carcinogenesis, biology.protein, Alternative complement pathway, Female, Endothelium, Vascular, business, Biomarkers

Abstract

Complement activation has been implicated in the pathogenesis of severe SARS-CoV-2 infection. However, it remains to be determined whether increased complement activation is a broad indicator of critical illness (and thus, no different in COVID-19). It is also unclear which pathways are contributing to complement activation in COVID-19, and if complement activation is associated with certain features of severe SARS-CoV-2 infection, such as endothelial injury and hypercoagulability. To address these questions, we investigated complement activation in the plasma from patients with COVID-19 prospectively enrolled at two tertiary care centers: Washington University School of Medicine (n=134) and Yale School of Medicine (n=49). We compared our patients to two non-COVID cohorts: (a) patients hospitalized with influenza (n=54), and (b) patients admitted to the intensive care unit (ICU) with acute respiratory failure requiring invasive mechanical ventilation (IMV, n=22). We demonstrate that circulating markers of complement activation are elevated in patients with COVID-19 compared to those with influenza and to patients with non-COVID-19 respiratory failure. Further, the results facilitate distinguishing those who are at higher risk of worse outcomes such as requiring ICU admission, or IMV. Moreover, the results indicate enhanced activation of the alternative complement pathway is most prevalent in patients with severe COVID-19 and is associated with markers of endothelial injury (i.e., angiopoietin-2) as well as hypercoagulability (i.e., thrombomodulin and von Willebrand factor). Our findings identify complement activation to be a distinctive feature of COVID-19, and provide specific targets that may be utilized for risk prognostication, drug discovery and personalized clinical trials., Increased complement activation is observed in COVID-19 compared to non-COVID respiratory illness, and is a key marker of organ failure.

Published

2021

40. COVID-19 vaccination in our transplant recipients: The time is now

Author

Robin Vos, Lara Danziger-Isakov, Michelle M. Kittleson, Saima Aslam, Cameron R. Wolfe, Daniel R. Goldstein, and Andrew E. Gelman

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, COVID-19 Vaccines, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Population, 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Interim, vaccine, Pandemic, Medicine, Humans, transplant, 030212 general & internal medicine, education, Adverse effect, Intensive care medicine, Pandemics, Transplantation, education.field_of_study, Minimal risk, business.industry, SARS-CoV-2, pandemic, Vaccination, COVID-19, Organ Transplantation, vaccination, Transplant Recipients, Perspective, Surgery, Cardiology and Cardiovascular Medicine, business

Abstract

We are entering 2021 with an expanding and effective COVID-19 vaccine armamentarium. Recent interim results from COVID-19 vaccine trials, including more than 80,000 participants worldwide, demonstrate remarkable efficacy and low rate of serious adverse events. Based on experience with other vaccines in transplant recipients and knowing the risk of severe COVID-19 in this population, we believe that COVID-19 vaccines provide potential benefit with minimal risk. We strongly support and encourage COVID-19 vaccination of our transplant recipients. ispartof: JOURNAL OF HEART AND LUNG TRANSPLANTATION vol:40 issue:3 pages:169-171 ispartof: location:United States status: published

Published

2020

41. Selective Imaging of Lung Macrophages Using [

Author

Delphine L, Chen, Eugene, Agapov, Kangyun, Wu, Jacquelyn T, Engle, Kiran Kumar, Solingapuram Sai, Elizabeth, Arentson, Katherine J, Spayd, Kirby T, Moreland, Kelsey, Toth, Derek E, Byers, Richard A, Pierce, Jeffrey J, Atkinson, Richard, Laforest, Andrew E, Gelman, and Michael J, Holtzman

Subjects

Mice, Inbred C57BL, Mice, Receptors, GABA, Fluorodeoxyglucose F18, Macrophages, Positron-Emission Tomography, Animals, Humans, Lung

Abstract

We tested whether the translocator protein (TSPO)-targeted positron emission tomography (PET) tracer, N-acetyl-N-(2-[MicroPET imaging quantified [In Wt mice, [PET imaging with [

Published

2020

42. Intercellular Mitochondria Transfer to Macrophages Regulates White Adipose Tissue Homeostasis and Is Impaired in Obesity

Author

Barry L. Hykes, Nicole P. Malvin, Michael R. McAllaster, Andrew E. Gelman, John R. Moley, Wei Zou, Brian Saunders, Bernd H. Zinselmeyer, Xiaoyan Wang, Nidhi Rohatgi, Hongming Ma, Anthony Orvedahl, Marina N. Rowen, John G. Doench, Yongjia Li, Scott A. Handley, Steven L. Teitelbaum, Jonathan R. Brestoff, Craig B. Wilen, Brian S. Kim, Herbert W. Virgin, Madison R. Mack, Jesse W. Williams, Michael S. Diamond, and Dale R. Balce

Subjects

0301 basic medicine, Physiology, Endocrinology, Diabetes and Metabolism, Adipose Tissue, White, Mice, Transgenic, White adipose tissue, Mitochondrion, Article, chemistry.chemical_compound, 03 medical and health sciences, Mice, Endocrinology, 0302 clinical medicine, Adipocyte, Brown adipose tissue, Adipocytes, medicine, Macrophage, Humans, Animals, Homeostasis, Obesity, Molecular Biology, Gene, Mice, Knockout, business.industry, Chemistry, Macrophages, food and beverages, Cell Biology, Metabolism, medicine.disease, Cell biology, Mitochondria, Mice, Inbred C57BL, Crosstalk (biology), 030104 developmental biology, medicine.anatomical_structure, business, 030217 neurology & neurosurgery, Intracellular

Abstract

Summary Recent studies suggest that mitochondria can be transferred between cells to support the survival of metabolically compromised cells. However, whether intercellular mitochondria transfer occurs in white adipose tissue (WAT) or regulates metabolic homeostasis in vivo remains unknown. We found that macrophages acquire mitochondria from neighboring adipocytes in vivo and that this process defines a transcriptionally distinct macrophage subpopulation. A genome-wide CRISPR-Cas9 knockout screen revealed that mitochondria uptake depends on heparan sulfates (HS). High-fat diet (HFD)-induced obese mice exhibit lower HS levels on WAT macrophages and decreased intercellular mitochondria transfer from adipocytes to macrophages. Deletion of the HS biosynthetic gene Ext1 in myeloid cells decreases mitochondria uptake by WAT macrophages, increases WAT mass, lowers energy expenditure, and exacerbates HFD-induced obesity in vivo. Collectively, this study suggests that adipocytes and macrophages employ intercellular mitochondria transfer as a mechanism of immunometabolic crosstalk that regulates metabolic homeostasis and is impaired in obesity.

Published

2020

43. Bronchus-associated lymphoid tissue–resident Foxp3+ T lymphocytes prevent antibody-mediated lung rejection

Author

Wenjun Li, Jason M. Gauthier, Alexander S. Krupnick, Hsi Min Hsiao, Brian W. Wong, Chyi S. Hsieh, Jon H. Ritter, Ramsey R. Hachem, Ryuji Higashikubo, Scott M. Palmer, Andrew E. Gelman, Daniel Kreisel, Francine L. Kelly, Varun Puri, Satona Tanaka, Linh N. Vuong, Alice Y. Tong, William M. Baldwin, and Ankit Bharat

Subjects

0301 basic medicine, Lung, CD40, biology, business.industry, FOXP3, General Medicine, 030230 surgery, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Lymphatic system, Immune system, Immunology, medicine, biology.protein, Respiratory epithelium, Antibody, CXCL13, business

Abstract

Antibody-mediated rejection (AMR) is a principal cause of acute and chronic failure of lung allografts. However, mechanisms mediating this oftentimes fatal complication are poorly understood. Here, we show that Foxp3+ T cells formed aggregates in rejection-free human lung grafts and accumulated within induced bronchus-associated lymphoid tissue (BALT) of tolerant mouse lungs. Using a retransplantation model, we show that selective depletion of graft-resident Foxp3+ T lymphocytes resulted in the generation of donor-specific antibodies (DSA) and AMR, which was associated with complement deposition and destruction of airway epithelium. AMR was dependent on graft infiltration by B and T cells. Depletion of graft-resident Foxp3+ T lymphocytes resulted in prolonged interactions between B and CD4+ T cells within transplanted lungs, which was dependent on CXCR5-CXCL13. Blockade of CXCL13 as well as inhibition of the CD40 ligand and the ICOS ligand suppressed DSA production and prevented AMR. Thus, we have shown that regulatory Foxp3+ T cells residing within BALT of tolerant pulmonary allografts function to suppress B cell activation, a finding that challenges the prevailing view that regulation of humoral responses occurs peripherally. As pulmonary AMR is largely refractory to current immunosuppression, our findings provide a platform for developing therapies that target local immune responses.

Published

2018

44. Visualization of Monocytic Cells in Regressing Atherosclerotic Plaques by Intravital 2-Photon and Positron Emission Tomography–Based Imaging—Brief Report

Author

Deborah Sultan, Steven L. Brody, Jason M. Gauthier, Hsi-Min Hsiao, Yongjian Liu, Robert J. Gropler, Hannah Luehmann, Daniel Kreisel, Wenjun Li, Andrew E. Gelman, Satona Tanaka, Kory J. Lavine, and Ryuiji Higashikubo

Subjects

Male, 0301 basic medicine, Aortic arch, Pathology, medicine.medical_specialty, CCR2, Time Factors, Intravital Microscopy, Mice, Knockout, ApoE, Receptors, CCR2, Green Fluorescent Proteins, Aortic Diseases, CX3C Chemokine Receptor 1, Aorta, Thoracic, 030204 cardiovascular system & hematology, Aortic arches, Monocytes, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Positron Emission Tomography Computed Tomography, medicine.artery, medicine, Animals, medicine.diagnostic_test, business.industry, Macrophages, Intravital Imaging, Atherosclerosis, Plaque, Atherosclerotic, Cervical aortic arch, Mice, Inbred C57BL, Transplantation, Disease Models, Animal, Luminescent Proteins, Microscopy, Fluorescence, Multiphoton, 030104 developmental biology, medicine.anatomical_structure, Positron emission tomography, Mice, Inbred CBA, Female, Cardiology and Cardiovascular Medicine, business

Abstract

Objective— Aortic arch transplants have advanced our understanding of processes that contribute to progression and regression of atherosclerotic plaques. To characterize the dynamic behavior of monocytes and macrophages in atherosclerotic plaques over time, we developed a new model of cervical aortic arch transplantation in mice that is amenable to intravital imaging. Approach and Results— Vascularized aortic arch grafts were transplanted heterotropically to the right carotid arteries of recipient mice using microsurgical suture techniques. To image immune cells in atherosclerotic lesions during regression, plaque-bearing aortic arch grafts from B6 ApoE-deficient donors were transplanted into syngeneic CX 3 CR1 GFP reporter mice. Grafts were evaluated histologically, and monocytic cells in atherosclerotic plaques in ApoE-deficient grafts were imaged intravitally by 2-photon microscopy in serial fashion. In complementary experiments, CCR2 + cells in plaques were serially imaged by positron emission tomography using specific molecular probes. Plaques in ApoE-deficient grafts underwent regression after transplantation into normolipidemic hosts. Intravital imaging revealed clusters of largely immotile CX 3 CR1 + monocytes/macrophages in regressing plaques that had been recruited from the periphery. We observed a progressive decrease in CX 3 CR1 + monocytic cells in regressing plaques and a decrease in CCR2 + positron emission tomography signal during 4 months. Conclusions— Cervical transplantation of atherosclerotic mouse aortic arches represents a novel experimental tool to investigate cellular mechanisms that contribute to the remodeling of atherosclerotic plaques.

Published

2018

45. PD-1 expression on CD8+ T cells regulates their differentiation within lung allografts and is critical for tolerance induction

Author

Ankit Bharat, Davide Scozzi, Tsuyoshi Takahashi, Wenjun Li, Ryuji Higashikubo, Daniel Kreisel, Jon H. Ritter, Hsi-Min Hsiao, Andrew E. Gelman, Satona Tanaka, and Alexander S. Krupnick

Subjects

Transplantation, Lung, Effector, medicine.medical_treatment, CD11c, 030230 surgery, Biology, Phenotype, 03 medical and health sciences, Tolerance induction, 0302 clinical medicine, medicine.anatomical_structure, Immunology, medicine, Immunology and Allergy, Cytotoxic T cell, Lung transplantation, Pharmacology (medical), CD8, 030215 immunology

Abstract

Immunological requirements for rejection and tolerance induction differ between various organs. While memory CD8+ T cells are considered a barrier to immunosuppression-mediated acceptance of most tissues and organs, tolerance induction after lung transplantation is critically dependent on central memory CD8+ T lymphocytes. Here we demonstrate that costimulation blockade-mediated tolerance after lung transplantation is dependent on programmed cell death 1 (PD-1) expression on CD8+ T cells. In the absence of PD-1 expression, CD8+ T cells form prolonged interactions with graft-infiltrating CD11c+ cells; their differentiation is skewed towards an effector memory phenotype and grafts are rejected acutely. These findings extend the notion that requirements for tolerance induction after lung transplantation differ from other organs. Thus, immunosuppressive strategies for lung transplant recipients need to be tailored based on the unique immunological properties of this organ.

Published

2018

46. Increased Incidence of Clonal Hematopoiesis in Lung Transplant Recipients Involves DNA Damage Response Genes

Author

Karolyn A. Oetjen, Andrew E. Gelman, Anirudh Mahadev, Daniel C. Link, and L.K. Tague

Subjects

Lung, medicine.anatomical_structure, DNA damage, Incidence (epidemiology), Immunology, Clonal hematopoiesis, medicine, Cell Biology, Hematology, Biology, Biochemistry, Gene

Abstract

Lung transplant recipients receive lifelong immunosuppression that includes a calcineurin inhibitor (tacrolimus or cyclosporine), an anti-proliferative agent (mycophenolate or azathioprine) and corticosteroids. They are also known to be at increased risk for a broad spectrum of adverse hematologic events. This includes relatively common complications such as neutropenia and other cytopenias, which occur in over half of patients, as well as rarer events such as de novo hematopoietic malignancy. Certain patterns of clonal hematopoiesis, the expansion of unique somatic clones in hematopoietic stem cells, are known to be associated with cytotoxic therapy and the development of hematologic malignancies. We hypothesized that the stress of transplantation and subsequent immunosuppression provides an environment whereby a unique pattern of clonal hematopoiesis emerges. To evaluate this hypothesis, we designed a custom panel of 59 genes using an error-corrected sequencing assay capable of detecting variant allele frequency (VAF) as low as 0.01. We characterized the overall burden and distribution of clonal hematopoiesis and compared differences among lung transplant recipients (n=73) and age-matched healthy controls (n=19). Clonal hematopoiesis was identified in 51/73 (69.9%) of lung transplant recipients. This was significantly higher than the frequency in the age-matched healthy controls (6/19,31.6% p=0.0071). Additionally, 27/51 (52.9%) of patients with clonal hematopoiesis had multiple variants. The increase in clonal hematopoiesis was mainly due to mutations in DNA damage response (DDR) genes (ATM, PPM1D, SRCAP or TP53), with 29/73 (39.7%) of lung transplant recipients carrying one or more mutation compared with 1/19 (5.3%) of age-matched healthy controls (5.3%, p=0.029). No significant difference in the frequency of clonal hematopoiesis due to non-DDR genes was also observed (48% vs. 26.3%, p=0.121). We first evaluated the relationship between clonal hematopoiesis and lung transplant indication. This is relevant, since interstitial lung disease (ILD), a common indication for lung transplantation, is associated with telomeropathies which are also linked to bone marrow failure and clonal hematopoiesis. However, the frequency of DDR clonal hematopoiesis in ILD patients (17/39, 44%) was similar to that observed in patients with COPD (9/20, 45%). We next investigated the association of immunosuppression with clonal hematopoiesis. Overall, 30/48 patients on mycophenolate (MPA) and 13/19 patients on azathioprine (AZA) had at least 1 clonal hematopoiesis mutation. We found no significant difference in overall clonal hematopoiesis frequency among patients on MPA vs. AZA. However, the frequency of DDR clonal hematopoiesis was significantly higher in patients on AZA (OR 4.04, 95% CI 1.22-13.38, p=0.022) than in patients on MPA. Moreover, when we assessed clonal hematopoiesis burden via Poisson regression, it was increased in patients receiving AZA (1.68, 95% CI 1.08-2.59, p=0.020) when compared to patients on MPA. All lung transplant recipients were maintained on tacrolimus but one, so associations with type of calcineurin inhibitor could not be assessed. Finally, we assessed clonal hematopoiesis in recipients who developed neutropenia (n=24) and found no significant association. To the best of our knowledge, we report the first evidence of increased clonal hematopoiesis in a solid organ transplant population. Our data indicate that azathioprine therapy is associated with the expansion of hematopoietic clones carrying variants in DDR genes. However, azathioprine therapy often represents a failure of MPA therapy, typically due to either hematologic or gastrointestinal toxicity. Therefore, the association noted might reflect MPA intolerance rather than azathioprine therapy. Nevertheless, prior studies show that treatment with genotoxic agents, such as chemotherapy or radiation therapy, provide a fitness advantage to hematopoietic stem/progenitor cells carrying DDR gene variants. Whether azathioprine vs. MPA therapy confers a similar fitness advantage is currently under investigation. Further investigation also is warranted to determine if the presence of clonal hematopoiesis influences lung transplant outcomes. Figure 1 Figure 1. Disclosures No relevant conflicts of interest to declare.

Published

2021

47. Mechanisms of Graft Rejection and Immune Regulation after Lung Transplant

Author

Alexander S. Krupnick, Hsi Min Hsiao, Andrew E. Gelman, Saeed Arefanian, Tsuyoshi Takahashi, Daniel Kreisel, Jason M. Gauthier, and Wenjun Li

Subjects

Graft Rejection, 0301 basic medicine, Pulmonary and Respiratory Medicine, Lymphoid Tissue, medicine.medical_treatment, 030230 surgery, T-Lymphocytes, Regulatory, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immune Tolerance, medicine, Humans, Lung, Graft rejection, Lymphoid neogenesis, business.industry, Immune regulation, Immunosuppression, respiratory system, State of the Art, respiratory tract diseases, surgical procedures, operative, 030104 developmental biology, medicine.anatomical_structure, Immunology, business, Lung Transplantation

Abstract

Outcomes after lung transplant lag behind those of other solid-organ transplants. A better understanding of the pathways that contribute to rejection and tolerance after lung transplant will be required to develop new therapeutic strategies that take into account the unique immunological features of lungs. Mechanistic immunological investigations in an orthotopic transplant model in the mouse have shed new light on immune responses after lung transplant. Here, we highlight that interactions between immune cells within pulmonary grafts shape their fate. These observations set lungs apart from other organs and help provide the conceptual framework for the development of lung-specific immunosuppression.

Published

2017

48. A Functional Polymorphism in C3 is Associated with Worse CLAD-Free Survival

Author

B. Mittler, Jamal Bajwa, Catherine Chen, Daniel R Calabrese, Chad A. Witt, John P. Atkinson, Howard J. Huang, Ramsey R. Hachem, Andrew E. Gelman, Daniel Kreisel, Derek E. Byers, L.K. Tague, John R. Greenland, and Hrishikesh S. Kulkarni

Subjects

Pulmonary and Respiratory Medicine, Oncology, Transplantation, medicine.medical_specialty, business.industry, Internal medicine, medicine, Surgery, Cardiology and Cardiovascular Medicine, business, Functional polymorphism

Published

2020

49. Perfect timing: circadian rhythms, sleep, and immunity — an NIH workshop summary

Author

Yvonne C. Lee, Mahesh M. Thakkar, Paula Desplats, Albert C. Shaw, Éva Szentirmai, Sanja Jelic, Nicolas Cermakian, Brian S. Kim, Colin Reardon, Ron C. Anafi, Andrew E. Gelman, Shaon Sengupta, Laura A. Solt, Aaron D. Laposky, Christopher M. Depner, Aric A. Prather, Marishka K. Brown, Jeffrey A. Haspel, Monika Haack, Brian J. Prendergast, Wendy E. Walker, and Emmanuel F. Mongodin

Subjects

0301 basic medicine, 1.1 Normal biological development and functioning, T-Lymphocytes, medicine.medical_treatment, Review, Education, 03 medical and health sciences, 0302 clinical medicine, Immune system, Underpinning research, Immunity, Animals, Humans, Medicine, Circadian rhythm, Chronobiology, business.industry, Inflammatory and immune system, Microbiota, Neurosciences, Immune regulation, Cell Differentiation, Chemotaxis, General Medicine, biochemical phenomena, metabolism, and nutrition, Sleep in non-human animals, United States, Circadian Rhythm, 030104 developmental biology, Cytokine, National Institutes of Health (U.S.), Immune System, 030220 oncology & carcinogenesis, Sleep Research, Sleep, business, Neuroscience

Abstract

Recent discoveries demonstrate a critical role for circadian rhythms and sleep in immune system homeostasis. Both innate and adaptive immune responses - ranging from leukocyte mobilization, trafficking, and chemotaxis to cytokine release and T cell differentiation -are mediated in a time of day-dependent manner. The National Institutes of Health (NIH) recently sponsored an interdisciplinary workshop, "Sleep Insufficiency, Circadian Misalignment, and the Immune Response," to highlight new research linking sleep and circadian biology to immune function and to identify areas of high translational potential. This Review summarizes topics discussed and highlights immediate opportunities for delineating clinically relevant connections among biological rhythms, sleep, and immune regulation.

Published

2020

50. Lymphatic drainage from bronchus-associated lymphoid tissue in tolerant lung allografts promotes peripheral tolerance

Author

Jason M. Gauthier, Margaret S. Harrison, Andrew E. Gelman, Ankit Bharat, Brian W. Wong, Yuriko Terada, Alice Y. Tong, Kohei Hashimoto, Alexander S. Krupnick, Christian Corbin Frye, Varun Puri, Kory J. Lavine, Ryuji Higashikubo, Daniel Kreisel, Amit I. Bery, Ruben G. Nava, Jon H. Ritter, and Wenjun Li

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Pathology, Stromal cell, Lymphoid Tissue, High endothelial venules, chemical and pharmacologic phenomena, Bronchi, Mice, Transgenic, Organ transplantation, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Animals, Transplantation, Homologous, Lung, Mice, Inbred BALB C, business.industry, FOXP3, Peripheral tolerance, General Medicine, Transplantation, 030104 developmental biology, medicine.anatomical_structure, Lymphatic system, 030220 oncology & carcinogenesis, Mice, Inbred CBA, Female, Transplantation Tolerance, business, Lung Transplantation, Research Article

Abstract

Tertiary lymphoid organs are aggregates of immune and stromal cells including high endothelial venules and lymphatic vessels that resemble secondary lymphoid organs and can be induced at nonlymphoid sites during inflammation. The function of lymphatic vessels within tertiary lymphoid organs remains poorly understood. During lung transplant tolerance, Foxp3(+) cells accumulate in tertiary lymphoid organs that are induced within the pulmonary grafts and are critical for the local downregulation of alloimmune responses. Here, we showed that tolerant lung allografts could induce and maintain tolerance of heterotopic donor-matched hearts through pathways that were dependent on the continued presence of the transplanted lung. Using lung retransplantation, we showed that Foxp3(+) cells egressed from tolerant lung allografts via lymphatics and were recruited into donor-matched heart allografts. Indeed, survival of the heart allografts was dependent on lymphatic drainage from the tolerant lung allograft to the periphery. Thus, our work indicates that cellular trafficking from tertiary lymphoid organs regulates immune responses in the periphery. We propose that these findings have important implications for a variety of disease processes that are associated with the induction of tertiary lymphoid organs.

Published

2020