Your search keyword '"Derek A. Oldridge"' showing total 87 results

1. Transcriptional immunogenomic analysis reveals distinct immunological clusters in paediatric nervous system tumours

Author

Arash Nabbi, Pengbo Beck, Alberto Delaidelli, Derek A. Oldridge, Sumedha Sudhaman, Kelsey Zhu, S. Y. Cindy Yang, David T. Mulder, Jeffrey P. Bruce, Joseph N. Paulson, Pichai Raman, Yuankun Zhu, Adam C. Resnick, Poul H. Sorensen, Martin Sill, Sebastian Brabetz, Sander Lambo, David Malkin, Pascal D. Johann, Marcel Kool, David T. W. Jones, Stefan M. Pfister, Natalie Jäger, and Trevor J. Pugh

Subjects

Paediatric neuro-oncology, Immunogenomics, CNS tumours, Tumour microenvironment, Neuroblastoma, Medicine, Genetics, QH426-470

Abstract

Abstract Background Cancer immunotherapies including immune checkpoint inhibitors and Chimeric Antigen Receptor (CAR) T-cell therapy have shown variable response rates in paediatric patients highlighting the need to establish robust biomarkers for patient selection. While the tumour microenvironment in adults has been widely studied to delineate determinants of immune response, the immune composition of paediatric solid tumours remains relatively uncharacterized calling for investigations to identify potential immune biomarkers. Methods To inform immunotherapy approaches in paediatric cancers with embryonal origin, we performed an immunogenomic analysis of RNA-seq data from 925 treatment-naïve paediatric nervous system tumours (pedNST) spanning 12 cancer types from three publicly available data sets. Results Within pedNST, we uncovered four broad immune clusters: Paediatric Inflamed (10%), Myeloid Predominant (30%), Immune Neutral (43%) and Immune Desert (17%). We validated these clusters using immunohistochemistry, methylation immune inference and segmentation analysis of tissue images. We report shared biology of these immune clusters within and across cancer types, and characterization of specific immune cell frequencies as well as T- and B-cell repertoires. We found no associations between immune infiltration levels and tumour mutational burden, although molecular cancer entities were enriched within specific immune clusters. Conclusions Given the heterogeneity of immune infiltration within pedNST, our findings suggest personalized immunogenomic profiling is needed to guide selection of immunotherapeutic strategies.

Published

2023

2. Genetic predisposition to neuroblastoma results from a regulatory polymorphism that promotes the adrenergic cell state

Author

Nina Weichert-Leahey, Hui Shi, Ting Tao, Derek A. Oldridge, Adam D. Durbin, Brian J. Abraham, Mark W. Zimmerman, Shizhen Zhu, Andrew C. Wood, Deepak Reyon, J. Keith Joung, Richard A. Young, Sharon J. Diskin, John M. Maris, and A. Thomas Look

Subjects

Genetics, Oncology, Medicine

Abstract

Childhood neuroblastomas exhibit plasticity between an undifferentiated neural crest–like mesenchymal cell state and a more differentiated sympathetic adrenergic cell state. These cell states are governed by autoregulatory transcriptional loops called core regulatory circuitries (CRCs), which drive the early development of sympathetic neuronal progenitors from migratory neural crest cells during embryogenesis. The adrenergic cell identity of neuroblastoma requires LMO1 as a transcriptional cofactor. Both LMO1 expression levels and the risk of developing neuroblastoma in children are associated with a single nucleotide polymorphism, G/T, that affects a GATA motif in the first intron of LMO1. Here, we showed that WT zebrafish with the GATA genotype developed adrenergic neuroblastoma, while knock-in of the protective TATA allele at this locus reduced the penetrance of MYCN-driven tumors, which were restricted to the mesenchymal cell state. Whole genome sequencing of childhood neuroblastomas demonstrated that TATA/TATA tumors also exhibited a mesenchymal cell state and were low risk at diagnosis. Thus, conversion of the regulatory GATA to a TATA allele in the first intron of LMO1 reduced the neuroblastoma-initiation rate by preventing formation of the adrenergic cell state. This mechanism was conserved over 400 million years of evolution, separating zebrafish and humans.

Published

2023

3. Proteomic profiling of MIS-C patients indicates heterogeneity relating to interferon gamma dysregulation and vascular endothelial dysfunction

Author

Caroline Diorio, Rawan Shraim, Laura A. Vella, Josephine R. Giles, Amy E. Baxter, Derek A. Oldridge, Scott W. Canna, Sarah E. Henrickson, Kevin O. McNerney, Frances Balamuth, Chakkapong Burudpakdee, Jessica Lee, Tomas Leng, Alvin Farrel, Michele P. Lambert, Kathleen E. Sullivan, E. John Wherry, David T. Teachey, Hamid Bassiri, and Edward M. Behrens

Subjects

Science

Abstract

Multi-inflammatory syndrome in children (MIS-C) can be associated with SARS-CoV-2 infection but can also be similar to other inflammatory syndromes. Here the authors characterise the plasma proteome phenotype in MIS-C and compare to other SARS-CoV-2 related syndromes and find disproportionately high IFN-γ responses in MIS-C patients.

Published

2021

4. Correction for Merenstein et al., 'Signatures of COVID-19 Severity and Immune Response in the Respiratory Tract Microbiome'

Author

Carter Merenstein, Guanxiang Liang, Samantha A. Whiteside, Ana G. Cobián-Güemes, Madeline S. Merlino, Louis J. Taylor, Abigail Glascock, Kyle Bittinger, Ceylan Tanes, Jevon Graham-Wooten, Layla A. Khatib, Ayannah S. Fitzgerald, Shantan Reddy, Amy E. Baxter, Josephine R. Giles, Derek A. Oldridge, Nuala J. Meyer, E. John Wherry, John E. McGinniss, Frederic D. Bushman, and Ronald G. Collman

Subjects

Microbiology, QR1-502

Published

2022

5. Overview of methods for enhancing bone regeneration in distraction osteogenesis: Potential roles of biometals

Author

Ye Li, Qi Pan, Jiankun Xu, Xuan He, Helen A. Li, Derek A. Oldridge, Gang Li, and Ling Qin

Subjects

Distraction osteogenesis (DO), Biodegradable, Magnesium (Mg), Biometal, Bone regeneration, Diseases of the musculoskeletal system, RC925-935

Abstract

Background: Distraction osteogenesis (DO) is a functional tissue engineering approach that applies gradual mechanical traction on the bone tissues after osteotomy to stimulate bone regeneration. However, DO still has disadvantages that limit its clinical use, including long treatment duration Methods: Review the current methods of promoting bone formation and consolidation in DO with particular interest on biometal. Results: Numerous approaches, including physical therapy, gene therapy, growth factor-based therapy, stem-cell-based therapy, and improved distraction devices, have been explored to reduce the DO treatment duration with some success. Nevertheless, no approach to date is widely accepted in clinical practice due to various reasons, such as high expense, short biologic half-life, and lack of effective delivery methods. Biometals, including calcium (Ca), magnesium (Mg), zinc (Zn), copper (Cu), manganese (Mn), and cobalt (Co) have attracted attention in bone regeneration attributed to their biodegradability and bioactive components released during in vivo degradation. Conclusion: This review summarizes the current therapies accelerating bone formation in DO and the beneficial role of biometals in bone regeneration, particularly focusing on the use of biometal Mg and its alloy in promoting bone formation in DO. Translational potential: The potential clinical applications using Mg-based devices to accelerate DO are promising. Mg stimulates expression of multiple intrinsic biological factors and the development of Mg as an implantable component in DO may be used to argument bone formation and consolidation in DO.

Published

2021

6. Alpha-Fetoprotein-Producing Lung Hepatoid Adenocarcinoma with Brain Metastasis Treated with S-1

Author

Yuki Muroyama, Hiroyuki Tamiya, Goh Tanaka, Wakae Tanaka, Alexander C. Huang, Derek A. Oldridge, Keisuke Matsusaka, Yutaka Takazawa, Taisuke Jo, Tetsuo Ushiku, and Takahide Nagase

Subjects

hepatoid adenocarcinoma, alpha-fetoprotein, lung, s-1, 5-fluorouracil, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Lung hepatoid adenocarcinoma (HAC) is a rare primary lung carcinoma pathologically characterized by hepatocellular carcinoma-like tumor cells, the majority of which produce alpha-fetoprotein (AFP). The clinical prognosis of lung HAC is generally poor, and effective therapeutic regimens for inoperable or recurrent cases have not been established. Here, we report a case of AFP-producing lung HAC with brain metastasis with long-term disease control, treated with the 5-fluorouracil-derived regimen S-1. The patient was a 66-year-old male admitted to the hospital with alexia. Chest X-ray revealed a massive tumor in the left upper lobe, and a head CT scan revealed a metastasis in the left parietal lobe. The laboratory data showed a remarkably elevated AFP level (97,561 ng/mL). Pathological assessment of the resected brain tumor revealed HAC, which was compatible with the lung biopsies. Together with the absence of other metastatic lesions, a final diagnosis of primary lung HAC, stage IV T4N3M1b, was given. The patient first underwent non-small cell lung cancer chemotherapy regimens (carboplatin and paclitaxel as the first line, and pemetrexed as the second line), but had clinical progression. After third-line oral S-1 (tegafur/gimeracil/oteracil) administration, the serum AFP level significantly dropped and the patient achieved long-term disease control without relapse, surviving more than 19 months after disease presentation. The autopsy result was consistent with the diagnosis of primary lung HAC, and immunohistochemical staining was AFP+, glypican 3+, and spalt-like transcription factor 4+. Here, we report the case of a rare primary lung HAC with apparent disease control on S-1 therapy, together with a literature review.

Published

2020

7. Signaling Through FcγRIIA and the C5a-C5aR Pathway Mediate Platelet Hyperactivation in COVID-19

Author

Sokratis A. Apostolidis, Amrita Sarkar, Heather M. Giannini, Rishi R. Goel, Divij Mathew, Aae Suzuki, Amy E. Baxter, Allison R. Greenplate, Cécile Alanio, Mohamed Abdel-Hakeem, Derek A. Oldridge, Josephine R. Giles, Jennifer E. Wu, Zeyu Chen, Yinghui Jane Huang, Jonathan Belman, Ajinkya Pattekar, Sasikanth Manne, Oliva Kuthuru, Jeanette Dougherty, Brittany Weiderhold, Ariel R. Weisman, Caroline A. G. Ittner, Sigrid Gouma, Debora Dunbar, Ian Frank, Alexander C. Huang, Laura A. Vella, The UPenn COVID Processing Unit, John P. Reilly, Scott E. Hensley, Lubica Rauova, Liang Zhao, Nuala J. Meyer, Mortimer Poncz, Charles S. Abrams, E. John Wherry, Sharon Adamski, Zahidul Alam, Mary M. Addison, Katelyn T. Byrne, Aditi Chandra, Hélène C. Descamps, Nicholas Han, Yaroslav Kaminskiy, Shane C. Kammerman, Justin Kim, Jacob T. Hamilton, Nune Markosyan, Julia Han Noll, Dalia K. Omran, Eric Perkey, Elizabeth M. Prager, Dana Pueschl, Austin Rennels, Jennifer B. Shah, Jake S. Shilan, Nils Wilhausen, and Ashley N. Vanderbeck

Subjects

platelet, COVID - 19, FcγRIIa, complement, fostamatinib, Immunologic diseases. Allergy, RC581-607

Abstract

Patients with COVID-19 present with a wide variety of clinical manifestations. Thromboembolic events constitute a significant cause of morbidity and mortality in patients infected with SARS-CoV-2. Severe COVID-19 has been associated with hyperinflammation and pre-existing cardiovascular disease. Platelets are important mediators and sensors of inflammation and are directly affected by cardiovascular stressors. In this report, we found that platelets from severely ill, hospitalized COVID-19 patients exhibited higher basal levels of activation measured by P-selectin surface expression and had poor functional reserve upon in vitro stimulation. To investigate this question in more detail, we developed an assay to assess the capacity of plasma from COVID-19 patients to activate platelets from healthy donors. Platelet activation was a common feature of plasma from COVID-19 patients and correlated with key measures of clinical outcome including kidney and liver injury, and APACHEIII scores. Further, we identified ferritin as a pivotal clinical marker associated with platelet hyperactivation. The COVID-19 plasma-mediated effect on control platelets was highest for patients that subsequently developed inpatient thrombotic events. Proteomic analysis of plasma from COVID-19 patients identified key mediators of inflammation and cardiovascular disease that positively correlated with in vitro platelet activation. Mechanistically, blocking the signaling of the FcγRIIa-Syk and C5a-C5aR pathways on platelets, using antibody-mediated neutralization, IgG depletion or the Syk inhibitor fostamatinib, reversed this hyperactivity driven by COVID-19 plasma and prevented platelet aggregation in endothelial microfluidic chamber conditions. These data identified these potentially actionable pathways as central for platelet activation and/or vascular complications and clinical outcomes in COVID-19 patients. In conclusion, we reveal a key role of platelet-mediated immunothrombosis in COVID-19 and identify distinct, clinically relevant, targetable signaling pathways that mediate this effect.

Published

2022

8. Signatures of COVID-19 Severity and Immune Response in the Respiratory Tract Microbiome

Author

Carter Merenstein, Guanxiang Liang, Samantha A. Whiteside, Ana G. Cobián-Güemes, Madeline S. Merlino, Louis J. Taylor, Abigail Glascock, Kyle Bittinger, Ceylan Tanes, Jevon Graham-Wooten, Layla A. Khatib, Ayannah S. Fitzgerald, Shantan Reddy, Amy E. Baxter, Josephine R. Giles, Derek A. Oldridge, Nuala J. Meyer, E. John Wherry, John E. McGinniss, Frederic D. Bushman, and Ronald G. Collman

Subjects

SARS-CoV-2, coronavirus, 16S rRNA gene sequencing, redondovirus, anellovirus, respiratory microbiome, Microbiology, QR1-502

Abstract

ABSTRACT Viral infection of the respiratory tract can be associated with propagating effects on the airway microbiome, and microbiome dysbiosis may influence viral disease. Here, we investigated the respiratory tract microbiome in coronavirus disease 2019 (COVID-19) and its relationship to disease severity, systemic immunologic features, and outcomes. We examined 507 oropharyngeal, nasopharyngeal, and endotracheal samples from 83 hospitalized COVID-19 patients as well as non-COVID patients and healthy controls. Bacterial communities were interrogated using 16S rRNA gene sequencing, and the commensal DNA viruses Anelloviridae and Redondoviridae were quantified by qPCR. We found that COVID-19 patients had upper respiratory microbiome dysbiosis and greater change over time than critically ill patients without COVID-19. Oropharyngeal microbiome diversity at the first time point correlated inversely with disease severity during hospitalization. Microbiome composition was also associated with systemic immune parameters in blood, as measured by lymphocyte/neutrophil ratios and immune profiling of peripheral blood mononuclear cells. Intubated patients showed patient-specific lung microbiome communities that were frequently highly dynamic, with prominence of Staphylococcus. Anelloviridae and Redondoviridae showed more frequent colonization and higher titers in severe disease. Machine learning analysis demonstrated that integrated features of the microbiome at early sampling points had high power to discriminate ultimate level of COVID-19 severity. Thus, the respiratory tract microbiome and commensal viruses are disturbed in COVID-19 and correlate with systemic immune parameters, and early microbiome features discriminate disease severity. Future studies should address clinical consequences of airway dysbiosis in COVID-19, its possible use as biomarkers, and the role of bacterial and viral taxa identified here in COVID-19 pathogenesis. IMPORTANCE COVID-19, caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection of the respiratory tract, results in highly variable outcomes ranging from minimal illness to death, but the reasons for this are not well understood. We investigated the respiratory tract bacterial microbiome and small commensal DNA viruses in hospitalized COVID-19 patients and found that each was markedly abnormal compared to that in healthy people and differed from that in critically ill patients without COVID-19. Early airway samples tracked with the level of COVID-19 illness reached during hospitalization, and the airway microbiome also correlated with immune parameters in blood. These findings raise questions about the mechanisms linking SARS-CoV-2 infection and other microbial inhabitants of the airway, including whether the microbiome might regulate severity of COVID-19 disease and/or whether early microbiome features might serve as biomarkers to discriminate disease severity.

Published

2021

9. CAR T-cell therapy is effective for CD19-dim B-lymphoblastic leukemia but is impacted by prior blinatumomab therapy

Author

Vinodh Pillai, Kavitha Muralidharan, Wenzhao Meng, Asen Bagashev, Derek A. Oldridge, Jaclyn Rosenthal, John Van Arnam, Jos J. Melenhorst, Diwakar Mohan, Amanda M. DiNofia, Minjie Luo, Sindhu Cherian, Jonathan R. Fromm, Gerald Wertheim, Andrei Thomas-Tikhonenko, Michele Paessler, Carl H. June, Eline T. Luning Prak, Vijay G. Bhoj, Stephan A. Grupp, Shannon L. Maude, and Susan R. Rheingold

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: Tisagenlecleucel, a chimeric antigen receptor (CAR) T-cell product targeting CD19 is approved for relapsed/refractory B-cell acute lymphoblastic leukemia (B-ALL). However, the impact of pretreatment variables, such as CD19 expression level, on leukemic blasts, the presence of CD19– subpopulations, and especially prior CD19-targeted therapy, on the response to CAR T-cell therapy has not been determined. We analyzed 166 patients treated with CAR T-cell therapy at our institution. Eleven patients did not achieve a minimal residual disease (MRD)– deep remission, whereas 67 patients had a recurrence after achieving a MRD– deep remission: 28 patients with CD19+ leukemia and 39 patients with CD19– leukemia. Return of CD19+ leukemia was associated with loss of CAR T-cell function, whereas CD19– leukemia was associated with continued CAR T-cell function. There were no significant differences in efficacy of CAR T cells in CD19-dim B-ALL, compared with CD19-normal or -bright B-ALL. Consistent with this, CAR T cells recognized and lysed cells with very low levels of CD19 expression in vitro. The presence of dim CD19 or rare CD19– events by flow cytometry did not predict nonresponse or recurrence after CAR T-cell therapy. However, prior therapy with the CD19-directed, bispecific T-cell engager blinatumomab was associated with a significantly higher rate of failure to achieve MRD– remission or subsequent loss of remission with antigen escape. Finally, immunophenotypic heterogeneity and lineage plasticity were independent of underlying clonotype and cytogenetic abnormalities.

Published

2019

10. Molecular Neuropathology in Practice: Clinical Profiling and Integrative Analysis of Molecular Alterations in Glioblastoma

Author

MacLean P. Nasrallah MD, PhD, Zev A. Binder MD, PhD, Derek A. Oldridge MD, PhD, Jianhua Zhao PhD, FACMG, David B. Lieberman MS, CGC, Jacquelyn J. Roth PhD, Christopher D. Watt MD, PhD, Shrey Sukhadia MS, Eva Klinman PhD, Robert D. Daber PhD, Arati Desai MD, Steven Brem MD, Donald M. O’Rourke MD, and Jennifer J. D. Morrissette PhD

Subjects

Pathology, RB1-214

Abstract

Molecular profiling of glioblastoma has revealed complex cytogenetic, epigenetic, and molecular abnormalities that are necessary for diagnosis, prognosis, and treatment. Our neuro-oncology group has developed a data-driven, institutional consensus guideline for efficient and optimal workup of glioblastomas based on our routine performance of molecular testing. We describe our institution’s testing algorithm, assay development, and genetic findings in glioblastoma, to illustrate current practices and challenges in neuropathology related to molecular and genetic testing. We have found that coordination of test requisition, tissue handling, and incorporation of results into the final pathologic diagnosis by the neuropathologist improve patient care. Here, we present analysis of O 6 -methylguanine-DNA-methyltransferase promoter methylation and next-generation sequencing results of 189 patients, obtained utilizing our internal processes led by the neuropathology team. Our institutional pathway for neuropathologist-driven molecular testing has streamlined the management of glioblastoma samples for efficient return of results for incorporation of genomic data into the pathological diagnosis and optimal patient care.

Published

2019

11. IgA deficiency destabilizes homeostasis toward intestinal microbes and increases systemic immune dysregulation

Author

Peyton E. Conrey, Lidiya Denu, Kaitlin C. O’Boyle, Isaiah Rozich, Jamal Green, Jeffrey Maslanka, Jean-Bernard Lubin, Tereza Duranova, Brittany L. Haltzman, Lauren Gianchetti, Derek A. Oldridge, Nina De Luna, Laura A. Vella, David Allman, Jonathan M. Spergel, Ceylan Tanes, Kyle Bittinger, Sarah E. Henrickson, and Michael A. Silverman

Subjects

Immunology, General Medicine

Abstract

The ability of most patients with selective immunoglobulin A (IgA) deficiency (SIgAD) to remain apparently healthy has been a persistent clinical conundrum. Compensatory mechanisms, including IgM, have been proposed, yet it remains unclear how secretory IgA and IgM work together in the mucosal system and, on a larger scale, whether the systemic and mucosal anti-commensal responses are redundant or have unique features. To address this gap in knowledge, we developed an integrated host-commensal approach combining microbial flow cytometry and metagenomic sequencing (mFLOW-Seq) to comprehensively define which microbes induce mucosal and systemic antibodies. We coupled this approach with high-dimensional immune profiling to study a cohort of pediatric patients with SIgAD and household control siblings. We found that mucosal and systemic antibody networks cooperate to maintain homeostasis by targeting a common subset of commensal microbes. In IgA-deficiency, we find increased translocation of specific bacterial taxa associated with elevated levels of systemic IgG targeting fecal microbiota. Associated features of immune system dysregulation in IgA-deficient mice and humans included elevated levels of inflammatory cytokines, enhanced follicular CD4 T helper cell frequency and activation, and an altered CD8 T cell activation state. Although SIgAD is clinically defined by the absence of serum IgA, the symptomatology and immune dysregulation were concentrated in the SIgAD participants who were also fecal IgA deficient. These findings reveal that mucosal IgA deficiency leads to aberrant systemic exposures and immune responses to commensal microbes, which increase the likelihood of humoral and cellular immune dysregulation and symptomatic disease in patients with IgA deficiency.

Published

2023

12. Human T follicular helper clones seed the germinal center–resident regulatory pool

Author

Carole Le Coz, Derek A. Oldridge, Ramin S. Herati, Nina De Luna, James Garifallou, Emylette Cruz Cabrera, Jonathan P. Belman, Dana Pueschl, Luisa V. Silva, Ainsley V. C. Knox, Whitney Reid, Samuel Yoon, Karen B. Zur, Steven D. Handler, Hakon Hakonarson, E. John Wherry, Michael Gonzalez, and Neil Romberg

Subjects

Immunology, General Medicine

Abstract

The mechanisms by which FOXP3 + T follicular regulatory (Tfr) cells simultaneously steer antibody formation toward microbe or vaccine recognition and away from self-reactivity remain incompletely understood. To explore underappreciated heterogeneity in human Tfr cell development, function, and localization, we used paired TCRVA / TCRVB sequencing to distinguish tonsillar Tfr cells that are clonally related to natural regulatory T cells (nTfr) from those likely induced from T follicular helper (Tfh) cells (iTfr). The proteins iTfr and nTfr cells differentially expressed were used to pinpoint their in situ locations via multiplex microscopy and establish their divergent functional roles. In silico analyses and in vitro tonsil organoid tracking models corroborated the existence of separate T reg -to-nTfr and Tfh-to-iTfr developmental trajectories. Our results identify human iTfr cells as a distinct CD38 + , germinal center–resident, Tfh-descended subset that gains suppressive function while retaining the capacity to help B cells, whereas CD38 − nTfr cells are elite suppressors primarily localized in follicular mantles. Interventions differentially targeting specific Tfr cell subsets may provide therapeutic opportunities to boost immunity or more precisely treat autoimmune diseases.

Published

2023

13. Supplementary Table 1 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

List of imputation results at the 6p22.3 region.

Published

2023

14. Supplementary Figure 4 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

rs6939340 genotype and expression of 6p22.3 gene products.

Published

2023

15. Supplementary Figure 7 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Depletion of the long isoform of CASC15 does not impact neuroblastoma cell viability.

Published

2023

16. Supplementary Table 2 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Full Table for the CASC15-S Cox Statistical Model.

Published

2023

17. Supplementary Methods from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Supplementary Methods

Published

2023

18. Supplementary Figure 1 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Evidence supporting multiple lncRNA transcript isoforms mapping to chromosome 6p22.3.

Published

2023

19. Supplementary Figure 5 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Additional expression data for CASC15 isoforms in neuroblastoma cell lines and patients.

Published

2023

20. Supplementary Figure Legends from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Supplementary Figure Legends

Published

2023

21. Supplementary Figure 2 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Bioinformatical support for CASC15-S as a long noncoding transcript.

Published

2023

22. Supplementary Figure 8 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Cell viability assays for neuroblastoma cell lines stably depleted of CASC15-S.

Published

2023

23. Supplementary Figure 3 from CASC15-S Is a Tumor Suppressor lncRNA at the 6p22 Neuroblastoma Susceptibility Locus

Author

Kristina A. Cole, John M. Maris, Sharon J. Diskin, Javed Khan, Shahab Asgharzadeh, Robert Seeger, Janahan Gnanchandran, Shile Zhang, Jun S. Wei, Yimei Li, Pichai Raman, Olivia Padovan, Maura Diamond, Lee McDaniel, Juan R. Alvarez-Dominguez, Derek A. Oldridge, Annalise Penikis, and Mike R. Russell

Abstract

Results of Sanger sequencing from 5' and 3'-RACE products of CASC15-S.

Published

2023

24. Cytomegalovirus Latent Infection is Associated with an Increased Risk of COVID-19-Related Hospitalization

Author

Cécile, Alanio, Anurag, Verma, Divij, Mathew, Sigrid, Gouma, Guanxiang, Liang, Thomas, Dunn, Derek A, Oldridge, JoEllen, Weaver, Leticia, Kuri-Cervantes, M Betina, Pampena, Michael R, Betts, Ronald G, Collman, Frederic D, Bushman, Nuala J, Meyer, Scott E, Hensley, Daniel, Rader, E John, Wherry, and Ashley N, Vanderbeck

Subjects

Hospitalization, Infectious Diseases, SARS-CoV-2, Cytomegalovirus Infections, Latent Infection, COVID-19, Cytomegalovirus, Humans, virus diseases, Immunology and Allergy

Abstract

Some risk factors for severe coronavirus disease 2019 (COVID-19) have been identified, including age, race, and obesity. However, 20%–50% of severe cases occur in the absence of these factors. Cytomegalovirus (CMV) is a herpesvirus that infects about 50% of all individuals worldwide and is among the most significant nongenetic determinants of immune system. We hypothesized that latent CMV infection might influence the severity of COVID-19. Our analyses demonstrate that CMV seropositivity is associated with more than twice the risk of hospitalization due to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. Immune profiling of blood and CMV DNA quantitative polymerase chain reaction in a subset of patients for whom respiratory tract samples were available revealed altered T-cell activation profiles in absence of extensive CMV replication in the upper respiratory tract. These data suggest a potential role for CMV-driven immune perturbations in affecting the outcome of SARS-CoV-2 infection and may have implications for the discrepancies in COVID-19 severity between different human populations.

Published

2022

25. Human T follicular helper clones seed the germinal center-resident regulatory pool

Author

Carole Le Coz, Derek A. Oldridge, Ramin S. Herati, Nina De Luna, James Garifallou, Emylette Cruz Cabrera, Jonathan P Belman, Dana Pueschl, Luisa V. Silva, Ainsley V. C. Knox, Samuel Yoon, Karen B. Zur, Steven D. Handler, Hakon Hakonarson, E. John Wherry, Michael Gonzalez, and Neil Romberg

Abstract

How FOXP3+T follicular regulatory (Tfr) cells simultaneously steer antibody formation toward microbe/vaccine recognition and away from self-reactivity remains unsettled. To explore human Tfr cell provenance, function and location heterogeneity, we used pairedTCRVA/TCRVBsequencing to distinguish tonsillar Tfr cells clonally related to natural Tregs (nTfr) from those likely induced from Tfh cells (iTfr). The proteins iTfr and nTfr cells differentially expressed were utilized to pinpoint theirin situlocations via multi-plex microscopy and establish divergent functional roles.In-silicoand tonsil organoid tracking models corroborated the existence of separate Treg-to-nTfr and Tfh-to-iTfr developmental trajectories. In total, we have identified human iTfr cells as a distinct CD38-expressing, GC-resident, Tfh-descended subset that gains suppressive function while retaining capacities for B-cell help whereas CD38-nTfr cells are elite suppressors primarily localized to follicular mantles. Interventions differentially targeting Tfr subsets may provide therapeutic opportunities to boost immunity or more precisely treat autoimmune diseases.One sentence summaryHuman tonsillar Tfr clones descend from either Treg or Tfh lineages and provenance predicts their TCR repertoires, locations and functional characteristics.

Published

2022

26. Transcriptional immunogenomic analysis reveals distinct immunological clusters in pediatric nervous system tumours

Author

Arash Nabbi, Pengbo Beck, Alberto Delaidelli, Derek A. Oldridge, Sumedha Sudhaman, Kelsey Zhu, S.Y. Cindy Yang, David T. Mulder, Jeffrey P. Bruce, Joseph N. Paulson, Pichai Raman, Yuankun Zhu, Adam C. Resnick, Poul H. Sorensen, Martin Sill, Sebastian Brabetz, Sander Lambo, David Malkin, Pascal D. Johann, Marcel Kool, David T.W. Jones, Stefan M. Pfister, Natalie Jäger, and Trevor J. Pugh

Abstract

SummaryTo inform immunotherapy approaches in children, we performed an immunogenomic analysis of RNA-seq data from 925 treatment-naïve pediatric nervous system tumours (pedNST) spanning 12 cancer types from three public data sets. Within pedNST, we uncovered four broad immune clusters: Pediatric Inflamed (10%), Myeloid Predominant (30%), Immune Neutral (43%) and Immune Excluded (17%). We validated these clusters using immunohistochemistry, methylation immune inference, and segmentation analysis of tissue images. We report shared biology of these immune clusters within and across cancer types, and characterization of specific immune-cell frequencies as well as T- and B-cell repertoires. We found no associations between immune infiltration levels and tumour mutational burden, although molecular cancer entities were enriched within specific immune clusters. Given the heterogeneity within pedNST, our findings suggest personalized immunogenomic profiling is needed to guide selection of immunotherapeutic strategies.

Published

2022

27. CD8+ T cells contribute to survival in patients with COVID-19 and hematologic cancer

Author

Divij Mathew, Laura A. Vella, Randall A. Oyer, Jedd D. Wolchok, James Robinson, Cécile Alanio, Susan DeWolf, Kara N. Maxwell, Amy E. Baxter, Erin Bange, Karan Naik, Scott E. Hensley, Justin Kim, Anita Kumar, Tara Perloff, Adam J Widman, Madison E. Weirick, Santosha Vardhana, Madeline A Hwee, Florence Porterfield, Derek A. Oldridge, Krista R Budzik, Samuel J Kerr, Justine V. Cohen, Nicholas Han, Josephine R. Giles, Christopher M McAllister, Ariel R. Weisman, Michael Galantino, Angela DeMichele, Ivan Maillard, Charlotte Roberts, Caroline A. G. Ittner, Paul Wileyto, Ronac Mamtani, Lova Sun, Susan Tollett, Jennifer E. Wu, Olutosin Owoyemi, Sharon Adamski, John P. Reilly, Alexander C. Huang, Sigrid Gouma, Ryan Massa, Allison R. Greenplate, Sawsan R. Boutemine, E. John Wherry, Heather M. Giannini, Tiffanie K. Jones, Carla Wright, Olutwatosin Oniyide, Emily M. Kugler, N. Esther Babady, Alfred L. Garfall, Peter Maslak, Robert H. Vonderheide, Cathy Zheng, R.S. Agyekum, Nuala J. Meyer, and Thomas G. Dunn

Subjects

0301 basic medicine, biology, business.industry, T cell, Cancer, General Medicine, medicine.disease, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Humoral immunity, Immunology, biology.protein, medicine, Cytotoxic T cell, Antibody, Prospective cohort study, business, Survival rate

Abstract

Patients with cancer have high mortality from coronavirus disease 2019 (COVID-19), and the immune parameters that dictate clinical outcomes remain unknown. In a cohort of 100 patients with cancer who were hospitalized for COVID-19, patients with hematologic cancer had higher mortality relative to patients with solid cancer. In two additional cohorts, flow cytometric and serologic analyses demonstrated that patients with solid cancer and patients without cancer had a similar immune phenotype during acute COVID-19, whereas patients with hematologic cancer had impairment of B cells and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)-specific antibody responses. Despite the impaired humoral immunity and high mortality in patients with hematologic cancer who also have COVID-19, those with a greater number of CD8 T cells had improved survival, including those treated with anti-CD20 therapy. Furthermore, 77% of patients with hematologic cancer had detectable SARS-CoV-2-specific T cell responses. Thus, CD8 T cells might influence recovery from COVID-19 when humoral immunity is deficient. These observations suggest that CD8 T cell responses to vaccination might provide protection in patients with hematologic cancer even in the setting of limited humoral responses.

Published

2021

28. Abstract 4648: How inherited mutations affect single cells within the tumor microenvironment in breast tumors stratified by receptor status

Author

Dana Pueschl, Derek A. Oldridge, Jonathan Belman, William Chandler, Anupma Nayak, Bradley Wubbenhorst, John Pluta, Michael Feldman, E. John Wherry, Heather Thorne, Georgia Chenevix-Trench, Kathleen Cuningham Foundation Consortium for Resea kConFab, Susan M. Domchek, and Katherine L. Nathanson

Subjects

Cancer Research, Oncology

Abstract

The tumor microenvironment (TME) plays important roles in tumor progression, therapy response and patient survival. In this comprehensive study, we performed a detailed multiomic single cell analysis of breast cancers with inherited mutations in different genes (BRCA1, BRCA2, PALB2, ATM, CHEK2), and wild type mutation negative (WT) patients, stratified by hormone receptor status, to understand the relationship between inherited mutation and immunogenicity. Using spatial tissue multiplexing (PhenoCycler), single cell RNAseq (10X Genomics) and bulk RNAseq, we evaluated cellular markers within the TME associated with DNA damage as well as phenotypes with tumor suppressive (M1, CD8 T cells, NK cells) or tumor promotive (M2, Treg, CAF) properties. We developed a 43-plex antibody panel and characterized eight tissue microarrays containing 443 patient samples from mutation carriers (BRCA1: n=142, BRCA2: n=118, CHEK2: n=2, TP53: n=3, PALB2: n=7) and WT tumors (n=171). We addressed how the TME differs in mutation carriers versus WT tumors stratified by receptor status. To further investigate immune cell function (cytolytic function, exhaustion, immune checkpoint) as well as pathways involved in immune suppression and/or promotion, we performed scRNA sequencing using isolated single cells from fresh collected BC samples (WT ER: n=3, BRCA2 ER: n=1, CHEK2 ER: n=1, VUS ER: n=1) and bulk RNA (BRCA1: n=17, BRCA2: n=9). To determine immune cell (IC) frequency, we analyzed CD45+ cells detectable in each cohort and their co-expression of markers to determine specific phenotypes. Our data suggest that within BRCA mutation-associated BC, there are two groups: 1) with increased tumor infiltrating lymphocytes (TILs) including CD8+ cytotoxic T cells with high cytolytic function; and 2) with decreased TILs and cytolytic function. The frequency of CD8+ T cells is significantly decreased in breast cancers with BRCA2 mutations compared to BRCA1. Characterizing ER+ CHEK2 BC reveals T cell exhaustion compared to WT ER+ BC. Furthermore, preliminary scRNA results reveal increased fibroblast markers in ER+ CHEK2 and ER+ WT compared to ER+ BRCA2 tumors. Interestingly, cancer associated fibroblast (CAFs) markers (ACTA2, COL1A1, FAP, PDGFRA, PDGFRB, PDPN, THY1) as well as TAMs (CCL2, CD163, CD206, CD68, IL10, LOX, PLOD2, SIGLEC1) are increased in ER+ CHEK2 tumors compared to ER+ WT. These data could provide insights into how the TME associated with ER+ CHEK2 mutations might be driven by CAFs and TAMs with a frequency much higher than in ER+ WT. The detection of immune suppressive (Treg, M2) and immune promotive (M1) phenotypes differs in BRCA1 compared to BRCA2 mutated and WT TNBC. Our findings could decipher the role of DNA repair gene mutations and their effect on cells within the TME that might influence the design of treatment options in patients with inherited mutations based on their receptor status. Citation Format: Dana Pueschl, Derek A. Oldridge, Jonathan Belman, William Chandler, Anupma Nayak, Bradley Wubbenhorst, John Pluta, Michael Feldman, E. John Wherry, Heather Thorne, Georgia Chenevix-Trench, Kathleen Cuningham Foundation Consortium for Resea kConFab, Susan M. Domchek, Katherine L. Nathanson. How inherited mutations affect single cells within the tumor microenvironment in breast tumors stratified by receptor status. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 4648.

Published

2023

29. Alpha-Fetoprotein-Producing Lung Hepatoid Adenocarcinoma with Brain Metastasis Treated with S-1

Author

Yutaka Takazawa, Yuki Muroyama, Alexander C. Huang, Goh Tanaka, Takahide Nagase, Keisuke Matsusaka, Wakae Tanaka, Tetsuo Ushiku, Hiroyuki Tamiya, Derek A. Oldridge, and Taisuke Jo

Subjects

0301 basic medicine, medicine.medical_specialty, 5-Fluorouracil, medicine.medical_treatment, Brain tumor, Case Report, lcsh:RC254-282, Gastroenterology, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Carcinoma, Hepatoid adenocarcinoma, Lung, Chemotherapy, business.industry, S-1, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 030104 developmental biology, Pemetrexed, medicine.anatomical_structure, Oncology, Alpha-fetoprotein, 030220 oncology & carcinogenesis, business, medicine.drug, Brain metastasis

Abstract

Lung hepatoid adenocarcinoma (HAC) is a rare primary lung carcinoma pathologically characterized by hepatocellular carcinoma-like tumor cells, the majority of which produce alpha-fetoprotein (AFP). The clinical prognosis of lung HAC is generally poor, and effective therapeutic regimens for inoperable or recurrent cases have not been established. Here, we report a case of AFP-producing lung HAC with brain metastasis with long-term disease control, treated with the 5-fluorouracil-derived regimen S-1. The patient was a 66-year-old male admitted to the hospital with alexia. Chest X-ray revealed a massive tumor in the left upper lobe, and a head CT scan revealed a metastasis in the left parietal lobe. The laboratory data showed a remarkably elevated AFP level (97,561 ng/mL). Pathological assessment of the resected brain tumor revealed HAC, which was compatible with the lung biopsies. Together with the absence of other metastatic lesions, a final diagnosis of primary lung HAC, stage IV T4N3M1b, was given. The patient first underwent non-small cell lung cancer chemotherapy regimens (carboplatin and paclitaxel as the first line, and pemetrexed as the second line), but had clinical progression. After third-line oral S-1 (tegafur/gimeracil/oteracil) administration, the serum AFP level significantly dropped and the patient achieved long-term disease control without relapse, surviving more than 19 months after disease presentation. The autopsy result was consistent with the diagnosis of primary lung HAC, and immunohistochemical staining was AFP+, glypican 3+, and spalt-like transcription factor 4+. Here, we report the case of a rare primary lung HAC with apparent disease control on S-1 therapy, together with a literature review.

Published

2020

30. Efficient recall of Omicron-reactive B cell memory after a third dose of SARS-CoV-2 mRNA vaccine

Author

Rishi R. Goel, Mark M. Painter, Kendall A. Lundgreen, Sokratis A. Apostolidis, Amy E. Baxter, Josephine R. Giles, Divij Mathew, Ajinkya Pattekar, Arnold Reynaldi, David S. Khoury, Sigrid Gouma, Philip Hicks, Sarah Dysinger, Amanda Hicks, Harsh Sharma, Sarah Herring, Scott Korte, Wumesh KC, Derek A. Oldridge, Rachel I. Erickson, Madison E. Weirick, Christopher M. McAllister, Moses Awofolaju, Nicole Tanenbaum, Jeanette Dougherty, Sherea Long, Kurt D’Andrea, Jacob T. Hamilton, Maura McLaughlin, Justine C. Williams, Sharon Adamski, Oliva Kuthuru, Elizabeth M. Drapeau, Miles P. Davenport, Scott E. Hensley, Paul Bates, Allison R. Greenplate, and E. John Wherry

Subjects

Vaccines, Synthetic, COVID-19 Vaccines, SARS-CoV-2, COVID-19, Humans, RNA, Messenger, mRNA Vaccines, Antibodies, Viral, Antibodies, Neutralizing, Article, General Biochemistry, Genetics and Molecular Biology

Abstract

Despite a clear role in protective immunity, the durability and quality of antibody and memory B cell responses induced by mRNA vaccination, particularly by a 3rd dose of vaccine, remains unclear. Here, we examined antibody and memory B cell responses in a cohort of individuals sampled longitudinally for ∼9-10 months after the primary 2-dose mRNA vaccine series, as well as for ∼3 months after a 3rd mRNA vaccine dose. Notably, antibody decay slowed significantly between 6- and 9-months post-primary vaccination, essentially stabilizing at the time of the 3rd dose. Antibody quality also continued to improve for at least 9 months after primary 2-dose vaccination. Spike- and RBD-specific memory B cells were stable through 9 months post-vaccination with no evidence of decline over time, and ∼40-50% of RBD-specific memory B cells were capable of simultaneously recognizing the Alpha, Beta, Delta, and Omicron variants. Omicron-binding memory B cells induced by the first 2 doses of mRNA vaccine were boosted significantly by a 3rd dose and the magnitude of this boosting was similar to memory B cells specific for other variants. Pre-3rd dose memory B cell frequencies correlated with the increase in neutralizing antibody titers after the 3rd dose. In contrast, pre-3rd dose antibody titers inversely correlated with the fold-change of antibody boosting, suggesting that high levels of circulating antibodies may limit reactivation of immunological memory and constrain further antibody boosting by mRNA vaccines. These data provide a deeper understanding of how the quantity and quality of antibody and memory B cell responses change over time and number of antigen exposures. These data also provide insight into potential immune dynamics following recall responses to additional vaccine doses or post-vaccination infections.Graphical Summary

Published

2022

31. mRNA vaccines induce durable immune memory to SARS-CoV-2 and variants of concern

Author

Moses Awofolaju, Amy E. Baxter, Ajinkya Pattekar, J. Han Noll, Derek A. Oldridge, Ian Frank, Alessandro Sette, E. John Wherry, Paul Bates, Daniela Weiskopf, Eline T. Luning Prak, Elizabeth M Drapeau, Oliva Kuthuru, Michael R. Betts, M. M. Addison, Alba Grifoni, S. C. Kammerman, Justine C. Williams, Sokratis A. Apostolidis, Rishi R. Goel, H. C. Descamps, Kendall A. Lundgreen, Scott E. Hensley, J. T. Hamilton, Sherea Long, E. M. Prager, Laura A. Vella, Justin Kim, Nicholas Han, Jacob T. Hamilton, Y. Kaminskiy, Leticia Kuri-Cervantes, D. Pueschl, Josephine R. Giles, Z. Alam, Christopher M McAllister, A. Rennels, Divij Mathew, Nicole Tanenbaum, Sarah Herring, Kurt D'Andrea, Aaron M. Rosenfeld, D. K. Omran, Philip Hicks, Jeanette Dougherty, Maura McLaughlin, N. Markosyan, J. S. Shilan, A. N. Vanderbeck, A. Pattekar, David S. Khoury, Allison R. Greenplate, Miles P. Davenport, A. Chandra, K. T. Byrne, Madison E. Weirick, A. R. Greenplate, Sigrid Gouma, Mark M Painter, Sarah Dysinger, Harsh Sharma, Amanda Hicks, J. B. Shah, Arnold Reynaldi, N. Wilhausen, Wenzhao Meng, Sharon Adamski, S. Adamski, Scott Korte, and E. Perkey

Subjects

Messenger RNA, COVID-19 Vaccines, Multidisciplinary, SARS-CoV-2, T cell, Alpha (ethology), biochemical phenomena, metabolism, and nutrition, Biology, Article, Vaccination, medicine.anatomical_structure, Immunity, Immunology, Humoral immunity, medicine, biology.protein, Humans, mRNA Vaccines, Antibody, Immunologic Memory, CD8

Abstract

SARS-CoV-2 mRNA vaccines have shown remarkable efficacy, especially in preventing severe illness and hospitalization. However, the emergence of several variants of concern and reports of declining antibody levels have raised uncertainty about the durability of immune memory following vaccination. In this study, we longitudinally profiled both antibody and cellular immune responses in SARS-CoV-2 naïve and recovered individuals from pre-vaccine baseline to 6 months post-mRNA vaccination. Antibody and neutralizing titers decayed from peak levels but remained detectable in all subjects at 6 months post-vaccination. Functional memory B cell responses, including those specific for the receptor binding domain (RBD) of the Alpha (B.1.1.7), Beta (B.1.351), and Delta (B.1.617.2) variants, were also efficiently generated by mRNA vaccination and continued to increase in frequency between 3 and 6 months post-vaccination. Notably, most memory B cells induced by mRNA vaccines were capable of cross-binding variants of concern, and B cell receptor sequencing revealed significantly more hypermutation in these RBD variant-binding clones compared to clones that exclusively bound wild-type RBD. Moreover, the percent of variant cross-binding memory B cells was higher in vaccinees than individuals who recovered from mild COVID-19. mRNA vaccination also generated antigen-specific CD8+ T cells and durable memory CD4+ T cells in most individuals, with early CD4+ T cell responses correlating with humoral immunity at later timepoints. These findings demonstrate robust, multi-component humoral and cellular immune memory to SARS-CoV-2 and current variants of concern for at least 6 months after mRNA vaccination. Finally, we observed that boosting of pre-existing immunity with mRNA vaccination in SARS-CoV-2 recovered individuals primarily increased antibody responses in the short-term without significantly altering antibody decay rates or long-term B and T cell memory. Together, this study provides insights into the generation and evolution of vaccine-induced immunity to SARS-CoV-2, including variants of concern, and has implications for future booster strategies.

Published

2021

32. IgA deficiency destabilizes immunological homeostasis towards intestinal microbiota and increases the risk of systemic immune dysregulation

Author

Sarah E. Henrickson, Ceylan Tanes, Lauren Gianchetti, David Allman, Lidiya Denu, Michael A. Silverman, Kaitlin C. O’Boyle, Jonathan M. Spergel, Derek A. Oldridge, Peyton Conrey, Jean-Bernard Lubin, Jamal Green, Brittany L. Haltzman, Jeffrey Maslanka, Laura A. Vella, Kyle Bittinger, and Tereza Duranova

Subjects

Immunoglobulin A, biology, medicine.diagnostic_test, Firmicutes, T cell, Immune dysregulation, medicine.disease_cause, biology.organism_classification, Flow cytometry, medicine.anatomical_structure, Immune system, Immunology, medicine, biology.protein, Antibody, Homeostasis

Abstract

SummaryMammals produce large quantities of mucosal and systemic antibodies that maintain the intestinal barrier, shape the intestinal microbiome and promote lifelong mutualism with commensal microbes. Here, we developed an integrated host-commensal approach combining microbial flow cytometry and 16s rRNA gene sequencing to define the core microbes that induce mucosal and systemic antibodies in pediatric selective Immunoglobulin A (IgA) deficient and household control siblings with CyTOF analysis to determine the impacts of IgA deficiency on host cellular immune phenotype. In healthy controls, mucosal secretory IgA and IgM antibodies coat an overlapping subset of microbes, predominantly Firmicutes and Proteobacteria. Serum IgG antibodies target a similar consortium of fecal microbes, revealing connections between mucosal and systemic antibody networks. Unexpectedly, IgM provides limited compensation for IgA in children lacking intestinal IgA. Furthermore, we find broad systemic immune dysregulation in a subset of children and mice lacking IgA, including enhanced IgG targeting of fecal microbiota, elevated levels of inflammatory and allergic cytokines and alterations in T cell activation state. Thus, IgA tunes systemic interactions between the host and commensal microbiota. Understanding how IgA tunes baseline immune tone has implications for predicting and preventing autoimmune, inflammatory and allergic diseases broadly, as well as providing improved prognostic guidance to patients with IgA deficiency.One Sentence SummaryIgA deficiency impairs immune homeostasis toward microbiota in children, increasing the risk of immune dysregulation.

Published

2021

33. mRNA Vaccination Induces Durable Immune Memory to SARS-CoV-2 with Continued Evolution to Variants of Concern

Author

Paul Bates, Ajinkya Pattekar, Michael R. Betts, Scott E. Hensley, Amanda Hicks, Maura McLaughlin, Ian Frank, Aaron M. Rosenfeld, Leticia Kuri-Cervantes, Josephine R. Giles, Miles P. Davenport, Wenzhao Meng, Alba Grifoni, E. John Wherry, Kendall A. Lundgreen, Alessandro Sette, Jacob T. Hamilton, Sharon Adamski, Eline T. Luning Prak, David S. Khoury, Scott Korte, Rishi R. Goel, Elizabeth M Drapeau, Sherea Long, Amy E. Baxter, Sarah Herring, Oliva Kuthuru, Justine C. Williams, Christopher M McAllister, Jeanette Dougherty, Philip Hicks, Daniela Weiskopf, Madison E. Weirick, Mark M Painter, Allison R. Greenplate, Moses Awofolaju, Nicole Tanenbaum, Sigrid Gouma, Sarah Dysinger, Derek A. Oldridge, Divij Mathew, Sokratis A. Apostolidis, Harsh Sharma, and Arnold Reynaldi

Subjects

Vaccination, medicine.anatomical_structure, Immune system, Immunity, T cell, B-cell receptor, Immunology, Humoral immunity, medicine, biology.protein, Biology, Antibody, Memory B cell

Abstract

SARS-CoV-2 mRNA vaccines have shown remarkable efficacy, especially in preventing severe illness and hospitalization. However, the emergence of several variants of concern and reports of declining antibody levels have raised uncertainty about the durability of immune memory following vaccination. In this study, we longitudinally profiled both antibody and cellular immune responses in SARS-CoV-2 naïve and recovered individuals from pre-vaccine baseline to 6 months post-mRNA vaccination. Antibody and neutralizing titers decayed from peak levels but remained detectable in all subjects at 6 months post-vaccination. Functional memory B cell responses, including those specific for the receptor binding domain (RBD) of the Alpha (B.1.1.7), Beta (B.1.351), and Delta (B.1.617.2) variants, were also efficiently generated by mRNA vaccination and continued to increase in frequency between 3 and 6 months post-vaccination. Notably, most memory B cells induced by mRNA vaccines were capable of cross-binding variants of concern, and B cell receptor sequencing revealed significantly more hypermutation in these RBD variant-binding clones compared to clones that exclusively bound wild-type RBD. Moreover, the percent of variant cross-binding memory B cells was higher in vaccinees than individuals who recovered from mild COVID-19. mRNA vaccination also generated antigen-specific CD8+ T cells and durable memory CD4+ T cells in most individuals, with early CD4+ T cell responses correlating with humoral immunity at later timepoints. These findings demonstrate robust, multi-component humoral and cellular immune memory to SARS-CoV-2 and current variants of concern for at least 6 months after mRNA vaccination. Finally, we observed that boosting of pre-existing immunity with mRNA vaccination in SARS-CoV-2 recovered individuals primarily increased antibody responses in the short-term without significantly altering antibody decay rates or long-term B and T cell memory. Together, this study provides insights into the generation and evolution of vaccine-induced immunity to SARS-CoV-2, including variants of concern, and has implications for future booster strategies.GRAPHICAL ABSTRACT

Published

2021

34. Signatures of COVID-19 Severity and Immune Response in the Respiratory Tract Microbiome

Author

Derek A. Oldridge, Ceylan Tanes, Kyle Bittinger, Guanxiang Liang, Madeline S Merlino, Carter Merenstein, Louis J. Taylor, Ronald G. Collman, Josephine R. Giles, Frederic D. Bushman, Abigail L. Glascock, Amy E. Baxter, Jevon Graham-Wooten, Layla A Khatib, John E. McGinniss, Shantan Reddy, E. John Wherry, Samantha A Whiteside, Ana G Cobián-Güemes, Nuala J. Meyer, and Ayannah S. Fitzgerald

Subjects

Adult, Male, Lung microbiome, coronavirus, Oropharynx, Disease, medicine.disease_cause, Microbiology, Anelloviridae, Severity of Illness Index, Article, Immune system, respiratory microbiome, Virology, Nasopharynx, RNA, Ribosomal, 16S, Medicine, Humans, Human virome, Microbiome, Lymphocyte Count, Lung, 16S rRNA gene sequencing, Coronavirus, Aged, Aged, 80 and over, biology, Bacteria, business.industry, redondovirus, SARS-CoV-2, Microbiota, COVID-19, Middle Aged, biology.organism_classification, medicine.disease, QR1-502, medicine.anatomical_structure, Immunology, Dysbiosis, Female, Viral disease, anellovirus, business, Research Article, Respiratory tract

Abstract

Viral infection of the respiratory tract can be associated with propagating effects on the airway microbiome, and microbiome dysbiosis may influence viral disease. Here, we investigated the respiratory tract microbiome in coronavirus disease 2019 (COVID-19) and its relationship to disease severity, systemic immunologic features, and outcomes. We examined 507 oropharyngeal, nasopharyngeal, and endotracheal samples from 83 hospitalized COVID-19 patients as well as non-COVID patients and healthy controls. Bacterial communities were interrogated using 16S rRNA gene sequencing, and the commensal DNA viruses Anelloviridae and Redondoviridae were quantified by qPCR. We found that COVID-19 patients had upper respiratory microbiome dysbiosis and greater change over time than critically ill patients without COVID-19. Oropharyngeal microbiome diversity at the first time point correlated inversely with disease severity during hospitalization. Microbiome composition was also associated with systemic immune parameters in blood, as measured by lymphocyte/neutrophil ratios and immune profiling of peripheral blood mononuclear cells. Intubated patients showed patient-specific lung microbiome communities that were frequently highly dynamic, with prominence of Staphylococcus. Anelloviridae and Redondoviridae showed more frequent colonization and higher titers in severe disease. Machine learning analysis demonstrated that integrated features of the microbiome at early sampling points had high power to discriminate ultimate level of COVID-19 severity. Thus, the respiratory tract microbiome and commensal viruses are disturbed in COVID-19 and correlate with systemic immune parameters, and early microbiome features discriminate disease severity. Future studies should address clinical consequences of airway dysbiosis in COVID-19, its possible use as biomarkers, and the role of bacterial and viral taxa identified here in COVID-19 pathogenesis. IMPORTANCE COVID-19, caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection of the respiratory tract, results in highly variable outcomes ranging from minimal illness to death, but the reasons for this are not well understood. We investigated the respiratory tract bacterial microbiome and small commensal DNA viruses in hospitalized COVID-19 patients and found that each was markedly abnormal compared to that in healthy people and differed from that in critically ill patients without COVID-19. Early airway samples tracked with the level of COVID-19 illness reached during hospitalization, and the airway microbiome also correlated with immune parameters in blood. These findings raise questions about the mechanisms linking SARS-CoV-2 infection and other microbial inhabitants of the airway, including whether the microbiome might regulate severity of COVID-19 disease and/or whether early microbiome features might serve as biomarkers to discriminate disease severity.

Published

2021

35. Rapid induction of antigen-specific CD4+ T cells is associated with coordinated humoral and cellular immunity to SARS-CoV-2 mRNA vaccination

Author

Amy E. Baxter, Kendall A. Lundgreen, Jacob T. Hamilton, Sigrid Gouma, Oliva Kuthuru, Christopher M McAllister, Sarah Dysinger, Divij Mathew, Daniela Weiskopf, Leticia Kuri-Cervantes, Josephine R. Giles, Allison R. Greenplate, Alba Grifoni, Ramin S. Herati, Amanda Hicks, Ajinkya Pattekar, Michael R. Betts, Madison E. Weirick, Derek A. Oldridge, Jeanette Dougherty, Sharon Adamski, Scott E. Hensley, Paul Bates, Scott Korte, Sokratis A. Apostolidis, Alessandro Sette, Mark M Painter, Sherea Long, Kurt D'Andrea, Philip Hicks, E. John Wherry, and Rishi R. Goel

Subjects

Antigens, Differentiation, T-Lymphocyte, Male, Cellular immunity, Cell, Priming (immunology), Tfh, CD8-Positive T-Lymphocytes, Antibodies, Viral, Lymphocyte Activation, Th1, Immunology and Allergy, AIM, Immunity, Cellular, biology, Vaccination, Middle Aged, Infectious Diseases, medicine.anatomical_structure, Spike Glycoprotein, Coronavirus, activation induced markers, Female, Antibody, 2019-nCoV Vaccine mRNA-1273, Adult, COVID-19 Vaccines, Immunology, T cells, Immunization, Secondary, Article, immunological memory, Young Adult, Immune system, Antigens, CD, medicine, Humans, Lectins, C-Type, BNT162 Vaccine, Messenger RNA, SARS-CoV-2, COVID-19, Th1 Cells, Antibodies, Neutralizing, Immunity, Humoral, mRNA vaccine, T follicular helper, biology.protein, Peptides, Immunologic Memory, CD8

Abstract

SARS-CoV-2 mRNA vaccines have shown remarkable clinical efficacy, but questions remain about the nature and kinetics of T cell priming. We performed longitudinal antigen-specific T cell analyses on healthy SARS-CoV-2-naive and recovered individuals prior to and following mRNA prime and boost vaccination. Vaccination induced rapid antigen-specific CD4+ T cell responses in naive subjects after the first dose, whereas CD8+ T cell responses developed gradually and were variable in magnitude. Vaccine-induced Th1 and Tfh cell responses following the first dose correlated with post-boost CD8+ T cells and neutralizing antibodies, respectively. Integrated analysis revealed coordinated immune responses with distinct trajectories in SARS-CoV-2-naive and recovered individuals. Last, whereas booster vaccination improved T cell responses in SARS-CoV-2-naive subjects, the second dose had little effect in SARS-CoV-2-recovered individuals. These findings highlight the role of rapidly primed CD4+ T cells in coordinating responses to the second vaccine dose in SARS-CoV-2-naive individuals., Graphical abstract, SARS-CoV-2 mRNA vaccines have demonstrated remarkable efficacy, but T cell responses to vaccination have not been well studied. In a longitudinal cohort, Painter et al. show that mRNA vaccines activate SARS-CoV-2-specific T cells that could contribute to durable immunity. The findings highlight the central role of T cells in the two-dose vaccine regimen for individuals not previously infected with SARS-CoV-2.

Published

2021

36. Retention of CD19 intron 2 contributes to CART-19 resistance in leukemias with subclonal frameshift mutations in CD19

Author

Ammar S. Naqvi, Matthew R. Gazzara, John M. Maris, Elena Sotillo, Sisi Zheng, Derek A. Oldridge, Asen Bagashev, Deanne Taylor, Stephan A. Grupp, David M. Barrett, Mukta Asnani, Katharina E. Hayer, Andrei Thomas-Tikhonenko, Fadia Ibrahim, Manolis Maragkakis, Kathryn L. Black, Scarlett Y. Yang, Yoseph Barash, and Zissimos Mourelatos

Subjects

Genetics, Cart, Cancer Research, Leukemia, Extramural, Antigens, CD19, Intron, Hematology, Biology, Prognosis, Immunotherapy, Adoptive, Introns, CD19, Frameshift mutation, Oncology, Correspondence, biology.protein, Leukaemia, Humans, Immunotherapy, Frameshift Mutation, Cancer genetics

Published

2019

37. Abstract 6051: Longitudinal single-cell sequencing of high-risk neuroblastoma tumors reveals intrinsic and extrinsic mechanisms of therapy resistance

Author

Yasin Uzun, Liron D. Grossmann, Chia-Hui Chen, Anusha Thadi, Chi-Yun Wu, Peng Gao, Dinh Diep, Lea Surrey, Daniel Martinez, Tasleema Patel, Qi Qiu, Sarah Johnson, Wenbao Yu, Shane Drabings, Changya Chen, Yuxuan Hu, Gregory Chen, Derek A. Oldridge, Kun Zhang, Hao Wu, Kathrin Bernt, Nancy Zhang, John M. Maris, and Kai Tan

Subjects

Cancer Research, Oncology

Abstract

Neuroblastoma is a childhood cancer originating from embryonic neuronal progenitor cells and is the most common cancer diagnosed in infants. Although the majority of patients respond to initial chemotherapy, most high-risk patients suffer relapse due to therapy resistance. Here, we generated single-cell transcriptome and bulk whole-genome sequencing data of diagnosis and post-therapy samples from 23 patients diagnosed with high-risk neuroblastoma. We found two distinct adrenergic populations in the patient samples. Most tumor cells showed a mature sympathoblast phenotype whereas a small fraction was in an undifferentiated state with activation of protein translation, unfolded protein, and oxidative phosphorylation pathways. We found that therapy-resistant tumor cells in these two subpopulations had distinct characteristics. The more mature resistant subpopulation upregulated genes associated with epithelial-to-mesenchymal transition, including TWIST1, PLCB1 and CD276. The undifferentiated resistant subpopulation upregulated Ras signal transduction and TP53 pathway genes. Analysis of the immune microenvironment revealed that most tumor-associated macrophages became more immunosuppressive post-therapy via multiple newly gained signaling interactions including the complement signaling pathway. We discovered a limited infiltration of T lymphocytes in the tumor microenvironment, and chemotherapy induced an effector state with upregulated mTOR signaling and metabolism. Overall, our study revealed subpopulations of tumor cells in neuroblastoma that responded differently to induction chemotherapy. Our findings uncovered distinct molecular signatures of the resistant cells and their interactions with the immune microenvironment, paving the way for developing novel therapies for high-risk neuroblastoma. Citation Format: Yasin Uzun, Liron D. Grossmann, Chia-Hui Chen, Anusha Thadi, Chi-Yun Wu, Peng Gao, Dinh Diep, Lea Surrey, Daniel Martinez, Tasleema Patel, Qi Qiu, Sarah Johnson, Wenbao Yu, Shane Drabings, Changya Chen, Yuxuan Hu, Gregory Chen, Derek A. Oldridge, Kun Zhang, Hao Wu, Kathrin Bernt, Nancy Zhang, John M. Maris, Kai Tan. Longitudinal single-cell sequencing of high-risk neuroblastoma tumors reveals intrinsic and extrinsic mechanisms of therapy resistance [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 6051.

Published

2022

38. Abstract 3579: T cell intrinsic DNA damage and repair response as a novel marker associated with clinical response to PD-1 blockade

Author

Yuki Muroyama, Sasikanth Manne, Derek A. Oldridge, Nils Wellhausen, Allison R. Greenplate, Lakshmi Chilukuri, Divij Mathew, Caiyue Xu, Ramin S. Herati, Alexander C. Huang, Dmitriy Zamarin, Claire F. Friedman, and E. John Wherry

Subjects

Cancer Research, Oncology

Abstract

Despite the high tumor mutational burden (TMB), immune check point blockade (ICB) still fails in about half of microsatellite instability-high (MSI-H) cancer patients, suggesting underlying immune dysregulation. Immune profiling of peripheral blood from chemotherapy-resistant MSI-H uterine cancer patients treated with nivolumab identified a rapid proliferative CD8 T cell response 2-4 weeks post PD-1 blockade (N = 32). This immunological response, however, did not correlate with clinical response, suggesting additional parameters may be relevant. We focused on DNA damage and repair (DDR) in T cells as potential novel parameters. DDR has been extensively studied in the context of inducing cell death in highly-proliferating tumor cells. However, despite induction of rapid proliferation of T cells upon ICB, whether T cell-intrinsic DDR impacts T cell function, and how the coordination of DDR affects immunological and clinical response to ICBs have been largely unexplored. We hypothesized that the T celI-intrinsic DDR responses to proliferative and genotoxic stress might contribute to the disparity between immunological and clinical response. To test the hypothesis, we developed a novel high-dimensional cytometry platform. This DDR-Immune platform enables simultaneous analysis of T cell differentiation state with changes in major DDR pathways at single-cell resolution. The DDR-Immune platform revealed consistent T cell subset specific patterns of DDR, as well as specific DDR pathways induced by different types of DNA damage, such as γ-irradiation (IR), UV irradiation (UV) or proliferative stress (i.e. anti-CD3/CD28 stimulation). For example, terminally differentiated effector T cells accumulated higher DNA damage and cell death. In contrast, stem cell memory (TSCM) and regulatory T cells (Treg) displayed high DDR with less cell death, suggesting that effective cell-intrinsic DDR against genotoxic stress in T cells confers a survival advantage. We applied the platform to MSI-H uterine cancer cohort to test if T cell-intrinsic DDR distinguish the clinical response. Indeed, we found that in clinical responders but not clinical non-responders, Ki67+ CD8 T cells responding to PD-1 blockade exhibited rapid induction of DDR represented as a spike increase of phosphorylated-ATM (pATM). This likely indicates the T cell ‘fitness’ response to proliferative stress induced by PD-1 blockade. Furthermore, patients with higher induction of pATM in responding CD8 T cells at the peak of the immunological response to PD-1 blockade had longer progression-free survival (PFS). Collectively, the new platform reveals previously unrecognized roles for T cell-intrinsic DDR as a novel determinant of immune responsiveness and clinical outcome to ICB and has potential application to other cancer therapies including chemotherapy and radiotherapy. Citation Format: Yuki Muroyama, Sasikanth Manne, Derek A. Oldridge, Nils Wellhausen, Allison R. Greenplate, Lakshmi Chilukuri, Divij Mathew, Caiyue Xu, Ramin S. Herati, Alexander C. Huang, Dmitriy Zamarin, Claire F. Friedman, E. John Wherry. T cell intrinsic DNA damage and repair response as a novel marker associated with clinical response to PD-1 blockade [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 3579.

Published

2022

39. IMMU-04. Transcriptional analysis reveals distinct microenvironmental subgroups across pediatric nervous system tumors

Author

Arash Nabbi, Pengbo Beck, Alberto Delaidelli, Derek A Oldridge, Sumedha Sudhaman, Kelsey Zhu, S Y Cindy Yang, David T Mulder, Jeffrey P Bruce, Joseph N Paulson, Pichai Raman, Yuankun Zhu, Martin Silll, Sebastian Brabetz, Sander Lambo, Pascal D Johann, Adam C Resnick, Poul H Sorensen, David Malkin, Marcel Kool, David T W Jones, Stefan M Pfister, Natalie Jäger, and Trevor J Pugh

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

INTRODUCTION: Recent clinical trials of immune checkpoint inhibitors indicated 5-11% response rate in pediatric patients depending on cancer type and expression of target proteins. Currently, a systematic analysis characterizing the immune microenvironment of childhood tumors is lacking. The main objective of this study is to uncover the features of immune microenvironment in pediatric nervous system tumors (pedNST). METHODS: We compiled transcriptomes of 925 tumors from three initiatives, Therapeutically Applicable Research To Generate Effective Treatments (TARGET, n = 149), International Cancer Genome Consortium (ICGC, n = 195) and Children Brain Tumor Tissue Network (CBTN, n = 581). We analyzed the performance of immune deconvolution tools and used publicly available datasets to define immune genesets. We conducted a consensus analysis to assign genes to cell-types and identify immunological groups. RESULTS: We found wide variability in immune infiltration across and within cancer types ranging from cold tumors such as medulloblastoma (2.7% infiltrate) to infiltrated entities such as neurofibroma (22.6%). Consensus clustering revealed four distinct immune clusters. The pediatric inflamed group (10%) included MYCN non-amplified neuroblastoma and ATRT. The myeloid-predominant group (30%) showed decreased infiltration of lymphoid cells but enrichment of myeloid cell genesets. The pediatric-cold group (42%) harbored no enrichment of immune genesets and included 72% of ependymomas and 65% of medulloblastomas. The immune excluded group (18%) showed depletion of immune cell-types and included sonic-hedgehog medulloblastoma. 71% of pedNST belonged to the lymphocyte depleted or immunologically quiet clusters, indicating the cold immune microenvironment in pedNST compared to adult cancers. CONCLUSION: We report characteristics of the immune microenvironment in pedNST. We found an overall cold microenvironment with low lymphocyte infiltration in this population compared to common adult cancers. We identified ~10% of tumors harboring a relatively inflamed microenvironment. Our data uncover characteristics of immune infiltration in pediatric tumors with potential implications to guide therapy.

Published

2022

40. Human epigenetic and transcriptional T cell differentiation atlas for identifying functional T cell-specific enhancers

Author

Josephine R. Giles, Sasikanth Manne, Elizabeth Freilich, Derek A. Oldridge, Amy E. Baxter, Sangeeth George, Zeyu Chen, Hua Huang, Lakshmi Chilukuri, Mary Carberry, Lydia Giles, Nan-Ping P. Weng, Regina M. Young, Carl H. June, Lynn M. Schuchter, Ravi K. Amaravadi, Xiaowei Xu, Giorgos C. Karakousis, Tara C. Mitchell, Alexander C. Huang, Junwei Shi, and E. John Wherry

Subjects

Epigenomics, Infectious Diseases, Immunology, Immunology and Allergy, Humans, Cell Differentiation, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Chromatin, Article, Epigenesis, Genetic

Abstract

The clinical benefit of T cell immunotherapies remains limited by incomplete understanding of T cell differentiation and dysfunction. We generated an epigenetic and transcriptional atlas of T cell differentiation from healthy humans that included exhausted CD8 T cells and applied this resource in three ways. First, we identified modules of gene expression and chromatin accessibility, revealing molecular coordination of differentiation after activation and between central memory and effector memory. Second, we applied this healthy molecular framework to three settings - a neoadjuvant anti-PD1 melanoma trial, a basal cell carcinoma scATAC-seq data set, and autoimmune disease-associated SNPs - yielding insights into disease-specific biology. Third, we predicted genome-wide cis-regulatory elements and validated this approach for key effector genes using CRISPR interference, providing functional annotation and demonstrating the ability to identify targets for non-coding cellular engineering. These studies define epigenetic and transcriptional regulation of human T cells and illustrate the utility of interrogating disease in the context of a healthy T cell atlas.

Published

2021

41. Signaling through FcγRIIA and the C5a-C5aR pathway mediates platelet hyperactivation in COVID-19

Author

Jeanette Dougherty, Sasikanth Manne, Amy E. Baxter, Josephine R. Giles, Yinghui Jane Huang, Ajinkya Pattekar, Oliva Kuthuru, Jennifer E. Wu, Aae Suzuki, Nuala J. Meyer, Debora Dunbar, Zeyu Chen, Alexander C. Huang, Ariel R. Weisman, Allison R. Greenplate, Mortimer Poncz, Charles S. Abrams, Ian Frank, Liang Zhao, Caroline A. G. Ittner, Mohamed S. Abdel-Hakeem, Amrita Sarkar, Rishi R. Goel, Sigrid Gouma, Divij Mathew, Sokratis A. Apostolidis, John P. Reilly, Derek A. Oldridge, Cécile Alanio, Scott E. Hensley, Laura A. Vella, E. John Wherry, Heather M. Giannini, Lubica Rauova, and Brittany Weiderhold

Subjects

Adult, Blood Platelets, Male, Morpholines, Immunology, Aminopyridines, Syk, Complement C5a, Inflammation, Fostamatinib, Severity of Illness Index, Article, Thromboembolism, medicine, Humans, Syk Kinase, Immunology and Allergy, Platelet, Platelet activation, Receptor, Anaphylatoxin C5a, Cells, Cultured, biology, Hyperactivation, SARS-CoV-2, business.industry, Receptors, IgG, COVID-19, Platelet Activation, Hospitalization, Ferritin, Pyrimidines, biology.protein, Female, medicine.symptom, Signal transduction, business, Signal Transduction, medicine.drug

Abstract

Patients with COVID-19 present with a wide variety of clinical manifestations. Thromboembolic events constitute a significant cause of morbidity and mortality in patients infected with SARS-CoV-2. Severe COVID-19 has been associated with hyperinflammation and pre-existing cardiovascular disease. Platelets are important mediators and sensors of inflammation and are directly affected by cardiovascular stressors. In this report, we found that platelets from severely ill, hospitalized COVID-19 patients exhibit higher basal levels of activation measured by P-selectin surface expression, and have a poor functional reserve upon in vitro stimulation. Correlating clinical features to the ability of plasma from COVID-19 patients to stimulate control platelets identified ferritin as a pivotal clinical marker associated with platelet hyperactivation. The COVID-19 plasma-mediated effect on control platelets was highest for patients that subsequently developed inpatient thrombotic events. Proteomic analysis of plasma from COVID-19 patients identified key mediators of inflammation and cardiovascular disease that positively correlated with in vitro platelet activation. Mechanistically, blocking the signaling of the FcγRIIa-Syk and C5a-C5aR pathways on platelets, using antibody-mediated neutralization, IgG depletion or the Syk inhibitor fostamatinib, reversed this hyperactivity driven by COVID-19 plasma and prevented platelet aggregation in endothelial microfluidic chamber conditions, thus identifying these potentially actionable pathways as central for platelet activation and/or vascular complications in COVID-19 patients. In conclusion, we reveal a key role of platelet-mediated immunothrombosis in COVID-19 and identify distinct, clinically relevant, targetable signaling pathways that mediate this effect. These studies have implications for the role of platelet hyperactivation in complications associated with SARS-CoV-2 infection., Cover illustration, One-sentence summary: The FcγRIIA and C5a-C5aR pathways mediate platelet hyperactivation in COVID-19

Published

2021

42. Rapid induction of antigen-specific CD4+T cells guides coordinated humoral and cellular immune responses to SARS-CoV-2 mRNA vaccination

Author

Mark M. Painter, Divij Mathew, Rishi R. Goel, Sokratis A. Apostolidis, Ajinkya Pattekar, Oliva Kuthuru, Amy E. Baxter, Ramin S. Herati, Derek A. Oldridge, Sigrid Gouma, Philip Hicks, Sarah Dysinger, Kendall A. Lundgreen, Leticia Kuri-Cervantes, Sharon Adamski, Amanda Hicks, Scott Korte, Josephine R. Giles, Madison E. Weirick, Christopher M. McAllister, Jeanette Dougherty, Sherea Long, Kurt D’Andrea, Jacob T. Hamilton, Michael R. Betts, Paul Bates, Scott E. Hensley, Alba Grifoni, Daniela Weiskopf, Alessandro Sette, Allison R. Greenplate, and E. John Wherry

Subjects

Vaccination, Messenger RNA, medicine.anatomical_structure, Immune system, T cell, Immunology, medicine, biology.protein, Priming (immunology), Biology, Neutralizing antibody, CD8, Proto-oncogene tyrosine-protein kinase Src

Abstract

SummaryThe SARS-CoV-2 mRNA vaccines have shown remarkable clinical efficacy, but questions remain about the nature and kinetics of T cell priming. We performed longitudinal antigen-specific T cell analyses in healthy individuals following mRNA vaccination. Vaccination induced rapid near-maximal antigen-specific CD4+T cell responses in all subjects after the first vaccine dose. CD8+T cell responses developed gradually after the first and second dose and were variable. Vaccine-induced T cells had central memory characteristics and included both Tfh and Th1 subsets, similar to natural infection. Th1 and Tfh responses following the first dose predicted post-boost CD8+T cell and neutralizing antibody levels, respectively. Integrated analysis of 26 antigen-specific T cell and humoral responses revealed coordinated features of the immune response to vaccination. Lastly, whereas booster vaccination improved CD4+and CD8+T cell responses in SARS-CoV-2 naïve subjects, the second vaccine dose had little effect on T cell responses in SARS-CoV-2 recovered individuals. Thus, longitudinal analysis revealed robust T cell responses to mRNA vaccination and highlighted early induction of antigen-specific CD4+T cells.Graphical Abstract

Published

2021

43. Proteomic Profiling of MIS-C Patients Reveals Heterogeneity Relating to Interferon Gamma Dysregulation and Vascular Endothelial Dysfunction

Author

Chakkapong Burudpakdee, E. John Wherry, Rawan Shraim, Caroline Diorio, Fran Balamuth, Laura A. Vella, Kathleen E. Sullivan, Kevin O McNerney, Tomas Leng, Derek A. Oldridge, Edward M. Behrens, Josephine R. Giles, Sarah E. Henrickson, Hamid Bassiri, David T. Teachey, Scott W. Canna, Alvin Farrel, Michele P. Lambert, Amy E. Baxter, and Jessica Lee

Subjects

Proteomics, Thrombotic microangiopathy, Proteome, Inflammation, Disease, Chemokine CXCL9, Group II Phospholipases A2, Asymptomatic, Article, Interferon-gamma, medicine, Humans, Interferon gamma, Vascular Diseases, Endothelial dysfunction, Child, business.industry, COVID-19, medicine.disease, Systemic Inflammatory Response Syndrome, Interleukin-10, Case-Control Studies, Macrophage activation syndrome, Immunology, Endothelium, Vascular, medicine.symptom, business, Biomarkers, medicine.drug

Abstract

Multi-system Inflammatory Syndrome in Children (MIS-C) is a major complication of the Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) pandemic in pediatric patients. Weeks after an often mild or asymptomatic initial infection with SARS-CoV-2 children may present with a severe shock-like picture and marked inflammation. Children with MIS-C present with varying degrees of cardiovascular and hyperinflammatory symptoms. We performed a comprehensive analysis of the plasma proteome of more than 1400 proteins in children with SARS-CoV-2. We hypothesized that the proteome would reflect heterogeneity in hyperinflammation and vascular injury, and further identify pathogenic mediators of disease. Protein signatures demonstrated overlap between MIS-C, and the inflammatory syndromes macrophage activation syndrome (MAS) and thrombotic microangiopathy (TMA). We demonstrate that PLA2G2A is a key marker of MIS-C that associates with TMA. We found that IFNγ responses are dysregulated in MIS-C patients, and that IFNγ levels delineate clinical heterogeneity.

Published

2021

44. Distinct antibody and memory B cell responses in SARS-CoV-2 naïve and recovered individuals after mRNA vaccination

Author

Divij Mathew, E. John Wherry, Kurt D'Andrea, Philip Hicks, Sharon Adamski, Sherea Long, Aaron M. Rosenfeld, Ajinkya Pattekar, Eline T. Luning Prak, Scott Korte, Kendall A. Lundgreen, Oliva Kuthuru, Jacob T. Hamilton, Amanda Hicks, Sigrid Gouma, Derek A. Oldridge, Michael R. Betts, Christopher M McAllister, Leticia Kuri-Cervantes, Josephine R. Giles, Wenzhao Meng, Scott E. Hensley, Paul Bates, Madison E. Weirick, Sarah Dysinger, Allison R. Greenplate, Rishi R. Goel, Sokratis A. Apostolidis, Jeanette Dougherty, Mark M Painter, and Amy E. Baxter

Subjects

Adult, Male, 0301 basic medicine, COVID-19 Vaccines, Immunology, Priming (immunology), Biology, Antibodies, Viral, Article, Serology, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Humans, RNA, Messenger, Memory B cell, Research Articles, B-Lymphocytes, Vaccines, Synthetic, SARS-CoV-2, R-Articles, Vaccination, COVID-19, General Medicine, Middle Aged, Antibodies, Neutralizing, Coronavirus, Titer, 030104 developmental biology, 030220 oncology & carcinogenesis, Spike Glycoprotein, Coronavirus, biology.protein, Female, Antibody

Abstract

Novel mRNA vaccines for SARS-CoV2 have been authorized for emergency use and are currently being administered to millions of individuals worldwide. Despite their efficacy in clinical trials, there is limited data on vaccine-induced immune responses in individuals with a prior SARS-CoV2 infection compared to SARS-CoV2 naïve subjects. Moreover, how mRNA vaccines impact the development of antibodies as well as memory B cells in COVID-19 experienced versus COVID-19 naïve subjects remains poorly understood. In this study, we evaluated antibody responses and antigen-specific memory B cell responses over time in 33 SARS-CoV2 naïve and 11 SARS-CoV2 recovered subjects. mRNA vaccination induced significant antibody and memory B cell responses against full-length SARS-CoV2 spike protein and the spike receptor binding domain (RBD). SARS-CoV2 naïve individuals benefitted from both doses of mRNA vaccine with additional increases in antibodies and memory B cells following booster immunization. In contrast, SARS-CoV2 recovered individuals had a significant immune response after the first dose with no increase in circulating antibodies or antigen-specific memory B cells after the second dose. Moreover, the magnitude of the memory B cell response induced by vaccination was lower in older individuals, revealing an age-dependence to mRNA vaccine-induced B cell memory. Side effects also tended to associate with post-boost antibody levels, but not with post-boost memory B cells, suggesting that side effect severity may be a surrogate of short-term antibody responses. The frequency of pre-vaccine antigen-specific memory B cells in SARS-CoV2 recovered individuals strongly correlated with post-vaccine antibody levels, supporting a key role for memory B cells in humoral recall responses to SARS-CoV2. This observation may have relevance for future booster vaccines and for responses to viral variants that partially escape pre-existing antibodies and require new humoral responses to be generated from memory B cells. Finally, post-boost antibody levels were not correlated with post-boost memory responses in SARS-CoV2 naïve individuals, indicating that short-term antibody levels and memory B cells are complementary immunological endpoints that should be examined in tandem when evaluating vaccine response. Together, our data provide evidence of both serological response and immunological memory following mRNA vaccination that is distinct based on prior SARS-CoV2 exposure. These findings may inform vaccine distribution in a resource-limited setting., Graphical Abstract

Published

2021

45. Deep immune profiling of MIS-C demonstrates marked but transient immune activation compared to adult and pediatric COVID-19

Author

Eileen C. Goodwin, Peyton Conrey, Divij Mathew, E. John Wherry, Heather M. Giannini, Cécile Alanio, Kevin O McNerney, Leticia Kuri-Cervantes, Marcus J. Bolton, Josephine R. Giles, Sigrid Gouma, Samir Sayed, Laura A. Vella, Jessica H. Lee, Julie Chase, Oliva Kuthuru, Claudia P. Arevalo, Scott E. Hensley, Zeyu Chen, Chakkapong Burudpakdee, Sarah E. Henrickson, Derek A. Oldridge, Amy E. Baxter, David T. Teachey, Kurt D'Andrea, Andre Ramos, Caroline Diorio, Hamid Bassiri, Nuala J. Meyer, Elizabeth M. Anderson, M. Betina Pampena, Edward M. Behrens, Yinghui Jane Huang, Sokratis A. Apostolidis, Madison E. Weirick, Jennifer E. Wu, Alexander C. Huang, Cristina Jasen, and Michael R. Betts

Subjects

Adult, Male, 0301 basic medicine, Aging, ARDS, Adolescent, T-Lymphocytes, T cell, Immunology, Disease, Lymphocyte Activation, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Immune system, CX3CR1, medicine, otorhinolaryngologic diseases, Cytotoxic T cell, Humans, 030212 general & internal medicine, Young adult, Child, Research Articles, biology, business.industry, R-Articles, COVID-19, Leukopenia, General Medicine, Flow Cytometry, medicine.disease, Systemic Inflammatory Response Syndrome, Coronavirus, 030104 developmental biology, medicine.anatomical_structure, Concomitant, Child, Preschool, biology.protein, Female, Antibody, business, CD8

Abstract

MIS-C is defined by lymphocyte activation, including elevated plasmablast frequencies and marked activation of CX3CR1+ CD8+ T cells., Pediatric COVID-19 following SARS-CoV-2 infection is associated with fewer hospitalizations and often milder disease than in adults. A subset of children, however, present with Multisystem Inflammatory Syndrome in Children (MIS-C) that can lead to vascular complications and shock, but rarely death. The immune features of MIS-C compared to pediatric COVID-19 or adult disease remain poorly understood. We analyzed peripheral blood immune responses in hospitalized SARS-CoV-2 infected pediatric patients (pediatric COVID-19) and patients with MIS-C. MIS-C patients had patterns of T cell-biased lymphopenia and T cell activation similar to severely ill adults, and all patients with MIS-C had SARS-CoV-2 spike-specific antibodies at admission. A distinct feature of MIS-C patients was robust activation of vascular patrolling CX3CR1+ CD8+ T cells that correlated with the use of vasoactive medication. Finally, whereas pediatric COVID-19 patients with acute respiratory distress syndrome (ARDS) had sustained immune activation, MIS-C patients displayed clinical improvement over time, concomitant with decreasing immune activation. Thus, non-MIS-C versus MIS-C SARS-CoV-2 associated illnesses are characterized by divergent immune signatures that are temporally distinct from one another and implicate CD8+ T cells in the clinical presentation and trajectory of MIS-C.

Published

2021

46. CD8 T cells compensate for impaired humoral immunity in COVID-19 patients with hematologic cancer

Author

Lova Sun, Derek A. Oldridge, Thomas G. Dunn, M. Galantino, Ronac Mamtani, T. Perloff, Anita Kumar, Nicholas Han, Nuala J. Meyer, Peter Maslak, C. Roberts, Santosha Vardhana, Ariel R. Weisman, Caroline A. G. Ittner, Adam J Widman, Randall A. Oyer, E. Wherry, S. Kerr, Divij Mathew, Angela DeMichele, Christopher M McAllister, Amy E. Baxter, Ivan Maillard, C. Wright, Jedd D. Wolchok, James Robinson, Justine V. Cohen, Cécile Alanio, Susan DeWolf, Allison R. Greenplate, K. Budzik, Kara N. Maxwell, Scott E. Hensley, N. E. Babady, Josephine R. Giles, Madison E. Weirick, Justin Kim, K. Naik, Sawsan R. Boutemine, Laura A. Vella, Sharon Adamski, Jennifer E. Wu, Florence Porterfield, Alexander C. Huang, Ryan Massa, S. Tollett, Alfred L. Garfall, Sigrid Gouma, Emily M. Kugler, Heather M. Giannini, Tiffanie K. Jones, Oluwatosin Oniyide, John P. Reilly, Erin Bange, R.S. Agyekum, E. P. Wileyto, Olutosin Owoyemi, Robert H. Vonderheide, and Cathy Zheng

Subjects

business.industry, Cancer, medicine.disease, Serology, Immune system, medicine.anatomical_structure, Humoral immunity, Cohort, Immunology, Medicine, Cytotoxic T cell, business, Viral load, B cell

Abstract

Cancer patients have increased morbidity and mortality from Coronavirus Disease 2019 (COVID-19), but the underlying immune mechanisms are unknown. In a cohort of 100 cancer patients hospitalized for COVID-19 at the University of Pennsylvania Health System, we found that patients with hematologic cancers had a significantly higher mortality relative to patients with solid cancers after accounting for confounders including ECOG performance status and active cancer status. We performed flow cytometric and serologic analyses of 106 cancer patients and 113 non-cancer controls from two additional cohorts at Penn and Memorial Sloan Kettering Cancer Center. Patients with solid cancers exhibited an immune phenotype similar to non-cancer patients during acute COVID-19 whereas patients with hematologic cancers had significant impairment of B cells and SARS-CoV-2-specific antibody responses. High dimensional analysis of flow cytometric data revealed 5 distinct immune phenotypes. An immune phenotype characterized by CD8 T cell depletion was associated with a high viral load and the highest mortality of 71%, among all cancer patients. In contrast, despite impaired B cell responses, patients with hematologic cancers and preserved CD8 T cells had a lower viral load and mortality. These data highlight the importance of CD8 T cells in acute COVID-19, particularly in the setting of impaired humoral immunity. Further, depletion of B cells with anti-CD20 therapy resulted in almost complete abrogation of SARS-CoV-2-specific IgG and IgM antibodies, but was not associated with increased mortality compared to other hematologic cancers, when adequate CD8 T cells were present. Finally, higher CD8 T cell counts were associated with improved overall survival in patients with hematologic cancers. Thus, CD8 T cells likely compensate for deficient humoral immunity and influence clinical recovery of COVID-19. These observations have important implications for cancer and COVID-19-directed treatments, immunosuppressive therapies, and for understanding the role of B and T cells in acute COVID-19.

Published

2021

47. Overview of methods for enhancing bone regeneration in distraction osteogenesis: Potential roles of biometals

Author

Gang Li, Derek A. Oldridge, Qi Pan, Ye Li, Jiankun Xu, Helen A. Li, Ling Qin, and Xuan He

Subjects

lcsh:Diseases of the musculoskeletal system, In vivo degradation, business.industry, Treatment duration, medicine.medical_treatment, Review Article, Bioinformatics, Biometal, Distraction osteogenesis (DO), Bone regeneration, Mechanical traction, Tissue engineering, Magnesium (Mg), medicine, Distraction osteogenesis, Biodegradable, Orthopedics and Sports Medicine, Bone formation, lcsh:RC925-935, business

Abstract

Background Distraction osteogenesis (DO) is a functional tissue engineering approach that applies gradual mechanical traction on the bone tissues after osteotomy to stimulate bone regeneration. However, DO still has disadvantages that limit its clinical use, including long treatment duration Methods Review the current methods of promoting bone formation and consolidation in DO with particular interest on biometal. Results Numerous approaches, including physical therapy, gene therapy, growth factor-based therapy, stem-cell-based therapy, and improved distraction devices, have been explored to reduce the DO treatment duration with some success. Nevertheless, no approach to date is widely accepted in clinical practice due to various reasons, such as high expense, short biologic half-life, and lack of effective delivery methods. Biometals, including calcium (Ca), magnesium (Mg), zinc (Zn), copper (Cu), manganese (Mn), and cobalt (Co) have attracted attention in bone regeneration attributed to their biodegradability and bioactive components released during in vivo degradation. Conclusion This review summarizes the current therapies accelerating bone formation in DO and the beneficial role of biometals in bone regeneration, particularly focusing on the use of biometal Mg and its alloy in promoting bone formation in DO. Translational potential: The potential clinical applications using Mg-based devices to accelerate DO are promising. Mg stimulates expression of multiple intrinsic biological factors and the development of Mg as an implantable component in DO may be used to argument bone formation and consolidation in DO.

Published

2020

48. Deep immune profiling of COVID-19 patients reveals distinct immunotypes with therapeutic implications

Author

Ariel R. Weisman, Ajinkya Pattekar, Fang Chen, Caroline A. G. Ittner, Cécile Alanio, Sasikanth Manne, Zeyu Chen, E. John Wherry, Holly Ramage, M. Betina Pampena, Scott E. Hensley, Kito Nzingha, Justin Kim, Amy E. Baxter, Jeanette Dougherty, Divij Mathew, Michael R. Betts, Allison R. Greenplate, Claudia P. Arevalo, Yinghui Jane Huang, Leticia Kuri-Cervantes, Josephine R. Giles, Derek A. Oldridge, Nuala J. Meyer, Jennifer E. Wu, Marcus J. Bolton, Laura A. Vella, John P. Reilly, Alexander C. Huang, Elizabeth M. Anderson, Eileen C. Goodwin, Madison E. Weirick, Simon F. Lacey, Sokratis A. Apostolidis, Sara Cherry, Kurt D'Andrea, Nicholas Han, Sigrid Gouma, and Oliva Kuthuru

Subjects

Multidisciplinary, biology, business.industry, R-Articles, T cell, Immunology, Acquired immune system, Virus, medicine.anatomical_structure, Immune system, biology.protein, Medicine, Antibody, business, Cytometry, Research Articles, B-Lymphocyte Subsets, B cell, Research Article

Abstract

Immune profiling of COVID-19 patients Coronavirus disease 2019 (COVID-19) has affected millions of people globally, yet how the human immune system responds to and influences COVID-19 severity remains unclear. Mathew et al. present a comprehensive atlas of immune modulation associated with COVID-19. They performed high-dimensional flow cytometry of hospitalized COVID-19 patients and found three prominent and distinct immunotypes that are related to disease severity and clinical parameters. Arunachalam et al. report a systems biology approach to assess the immune system of COVID-19 patients with mild-to-severe disease. These studies provide a compendium of immune cell information and roadmaps for potential therapeutic interventions. Science , this issue p. eabc8511 , p. 1210

Published

2020

49. Cross-Cohort Analysis Identifies a TEAD4–MYCN Positive Feedback Loop as the Core Regulatory Element of High-Risk Neuroblastoma

Author

Jo Vandesompele, Beatrice Salvatori, Richard A. Young, Brian J. Abraham, A. Thomas Look, Andrea Califano, Javed Khan, Presha Rajbhandari, Robert C. Seeger, Pieter Mestdagh, Jiyang Yu, Daniel Martinez, Claudia Capdevila, Rogier Versteeg, Nina Weichert-Leahey, Antonio Iavarone, Jun Wei, Jose Silva, Mark Yarmarkovich, Mariano J. Alvarez, Ruth Rodriguez-Barrueco, Anna Lasorella, Jo Lynne Harenza, John M. Maris, Shahab Asgharzadeh, Archana Iyer, Derek A. Oldridge, Jan Koster, Gonzalo Lopez, Katleen De Preter, Massachusetts Institute of Technology. Department of Biology, Abraham, Brian Joseph, Young, Richard A, Oncogenomics, and CCA - Cancer biology and immunology

Subjects

Transcriptional Activation, 0301 basic medicine, Proteasome Endopeptidase Complex, Muscle Proteins, Cell Cycle Proteins, Regulatory Sequences, Nucleic Acid, Biology, Article, Neuroblastoma, 03 medical and health sciences, Cell Line, Tumor, MYCN Positive, medicine, Humans, Gene silencing, TEAD4, neoplasms, Neoplasm Staging, Regulation of gene expression, N-Myc Proto-Oncogene Protein, Hippo signaling pathway, Gene Expression Profiling, Computational Biology, Nuclear Proteins, TEA Domain Transcription Factors, medicine.disease, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Gene expression profiling, 030104 developmental biology, Oncology, Cancer research, RNA Interference, N-Myc, Acyltransferases, Transcription Factors

Abstract

High-risk neuroblastomas show a paucity of recurrent somatic mutations at diagnosis. As a result, the molecular basis for this aggressive phenotype remains elusive. Recent progress in regulatory network analysis helped us elucidate disease-driving mechanisms downstream of genomic alterations, including recurrent chromosomal alterations. Our analysis identified three molecular subtypes of high-risk neuroblastomas, consistent with chromosomal alterations, and identified subtype-specific master regulator proteins that were conserved across independent cohorts. A 10-protein transcriptional module—centered around a TEAD4–MYCN positive feedback loop—emerged as the regulatory driver of the high-risk subtype associated with MYCN amplification. Silencing of either gene collapsed MYCN-amplified (MYCNAmp) neuroblastoma transcriptional hallmarks and abrogated viability in vitro and in vivo. Consistently, TEAD4 emerged as a robust prognostic marker of poor survival, with activity independent of the canonical Hippo pathway transcriptional coactivators YAP and TAZ. These results suggest novel therapeutic strategies for the large subset of MYCN-deregulated neuroblastomas. Significance: Despite progress in understanding of neuroblastoma genetics, little progress has been made toward personalized treatment. Here, we present a framework to determine the downstream effectors of the genetic alterations sustaining neuroblastoma subtypes, which can be easily extended to other tumor types. We show the critical effect of disrupting a 10-protein module centered around a YAP/TAZ-independent TEAD4–MYCN positive feedback loop in MYCNAmp neuroblastomas, nominating TEAD4 as a novel candidate for therapeutic intervention. Cancer Discov; 8(5); 582–99. ©2018 AACR. This article is highlighted in the In This Issue feature, p. 517

Published

2018

50. 310 T cell intrinsic DNA damage and repair response as a novel marker associated with clinical response to PD-1 blockade

Author

Ramin S. Herati, Claire F. Friedman, Divij Mathew, Yuki Muroyama, Caiyue Xu, Alexander C. Huang, Allison R. Greenplate, E. John Wherry, D. Zamarin, Lakshmi Chilukuri, Derek A. Oldridge, and Sasikanth Manne

Subjects

Pharmacology, Cancer Research, Chemistry, DNA damage, T cell, Immunology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, body regions, medicine.anatomical_structure, Oncology, Cancer research, medicine, Molecular Medicine, Immunology and Allergy, Pd 1 blockade, RC254-282

Abstract

BackgroundDespite the success of immune checkpoint blockade (ICB), many patients still fail to achieve durable clinical benefit. Previous studies have shown that CD8 T cells are reinvigorated by ICB. However, not all patients with this immunological response experience an effective clinical response, suggesting additional parameters may be relevant.DNA damage and repair (DDR) has been extensively studied in the context of inducing cell death of highly-proliferating tumor cells. However, whether T cell-intrinsic DDR impacts T cell differentiation and function, and how the coordination of DDR affects immunological and clinical response to proliferation-inducing ICBs have been largely unexplored. We hypothesized that the T celI-intrinsic DDR responses to proliferative and genotoxic stress might contribute to the disparity between immunological and clinical response.MethodsTo understand the impact of cell-intrinsic DDR on T cell differentiation and responses to cancer therapies, we developed a novel high-dimensional cytometry platform. This DDR-Immune platform enables simultaneous analysis of T cell differentiation state and multiple DDR pathways at single cell resolution. We then investigated immune reinvigoration and its association with DDR, in a cohort of chemotherapy-resistant hypermutated or microsatellite instability-high (MSI-H) uterine cancer patients treated with nivolumab. Peripheral blood samples were examined every 2–4 weeks after initiating anti-PD-1 treatment (N = 21).ResultsThe DDR-Immune platform revealed consistent T cell subset specific patterns of DDR, as well as specific DDR pathways induced by different types of DNA damage, such as γ-irradiation (IR), UV irradiation (UV) or proliferative stress (i.e. anti-CD3/CD28 stimulation). For example, terminally differentiated effector cells had higher DNA damage accumulation and cell death. In contrast, stem cell memory (TSCM) and regulatory T cells (Treg) displayed high DDR with less cell death, suggesting better cell-intrinsic DDR against genotoxic stress for survival advantage. In hypermutated MSI-H uterine cancer patients, CD8 T cells underwent rapid pharmacodynamic proliferation 2–4 weeks after starting PD-1 blockade, which did not correlate with clinical response. Application of the DDR-Immune platform to this cohort revealed, however, that in clinical responders but not clinical non-responders, Ki67+ CD8 T cells responding to PD-1 blockade had rapid induction of DDR represented as a spike increase of phosphorylated-ATM, presumably adapting T cell ‘fitness’ in response to proliferative stress induced by PD-1 blockade.ConclusionsCollectively, the new platform reveals previously unrecognized roles for T cell-intrinsic DDR as a novel determinant of immune responsiveness and clinical outcome to ICB and have potential application to other cancer therapies including chemotherapy and radiotherapy.Ethics ApprovalThe study was approved by MSKCC Ethics Board, approval number 17–180 (NCT03241745).

Published

2021