Your search keyword '"Porter, Caroline B. M."' showing total 7 results

1. Tissue-resident memory and circulating T cells are early responders to pre-surgical cancer immunotherapy.

Author

Luoma AM, Suo S, Wang Y, Gunasti L, Porter CBM, Nabilsi N, Tadros J, Ferretti AP, Liao S, Gurer C, Chen YH, Criscitiello S, Ricker CA, Dionne D, Rozenblatt-Rosen O, Uppaluri R, Haddad RI, Ashenberg O, Regev A, Van Allen EM, MacBeath G, Schoenfeld JD, and Wucherpfennig KW

Subjects

CD8-Positive T-Lymphocytes, Humans, Immunotherapy, Lymphocytes, Tumor-Infiltrating, Neoadjuvant Therapy, Tumor Microenvironment, Neoplasms therapy, Programmed Cell Death 1 Receptor

Abstract

Neoadjuvant immune checkpoint blockade has shown promising clinical activity. Here, we characterized early kinetics in tumor-infiltrating and circulating immune cells in oral cancer patients treated with neoadjuvant anti-PD-1 or anti-PD-1/CTLA-4 in a clinical trial (NCT02919683). Tumor-infiltrating CD8 T cells that clonally expanded during immunotherapy expressed elevated tissue-resident memory and cytotoxicity programs, which were already active prior to therapy, supporting the capacity for rapid response. Systematic target discovery revealed that treatment-expanded tumor T cell clones in responding patients recognized several self-antigens, including the cancer-specific antigen MAGEA1. Treatment also induced a systemic immune response characterized by expansion of activated T cells enriched for tumor-infiltrating T cell clonotypes, including both pre-existing and emergent clonotypes undetectable prior to therapy. The frequency of activated blood CD8 T cells, notably pre-treatment PD-1-positive KLRG1-negative T cells, was strongly associated with intra-tumoral pathological response. These results demonstrate how neoadjuvant checkpoint blockade induces local and systemic tumor immunity., Competing Interests: Declaration of interests K.W.W. serves on the SAB of SQZ Biotech, Nextechinvest, Bisou Bioscience Company, and T-Scan Therapeutics and receives sponsored research funding from Novartis. He is a scientific co-founder of Immunitas Therapeutics. J.D.S. reports research support paid to the institution from Merck, BMS, Regeneron, Debiopharm; Consulting/Scientific Advisory Board/Travel fees: Genentech, Immunitas, Debiopharm, BMS, Nanobiotix, Tilos, Castle Biosciences, Astra Zeneca, LEK, Catenion, ACI Clinical, Astellas, Stimit, and Merck KGA; Expert witness fees. Stock options: Immunitas; Equity: Doximity. E.M.V.A. reports Advisory/Consulting: Tango Therapeutics, Genome Medical, Invitae, Enara Bio, Janssen, Manifold Bio, and Monte Rosa; Research support: Novartis, BMS; Equity: Tango Therapeutics, Genome Medical, Syapse, Enara Bio, Manifold Bio, Microsoft, and Monte Rosa; Travel reimbursement: Roche/Genentech; Patents: Institutional patents filed on chromatin mutations and immunotherapy response, and methods for clinical interpretation; intermittent legal consulting on patents for Foaley & Hoag. A.R. is a founder and equity holder of Celsius Therapeutics, an equity holder in Immunitas Therapeutics, and until August 31, 2020, was an SAB member of Syros Pharmaceuticals, Neogene Therapeutics, Asimov, and Thermo Fisher Scientific. From August 1, 2020, A.R. is an employee of Genentech and has equity in Roche., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

2. Increased energy demand from anabolic-catabolic processes drives β-lactam antibiotic lethality.

Author

Lobritz MA, Andrews IW, Braff D, Porter CBM, Gutierrez A, Furuta Y, Cortes LBG, Ferrante T, Bening SC, Wong F, Gruber C, Bakerlee CW, Lambert G, Walker GC, Dwyer DJ, and Collins JJ

Subjects

Amdinocillin chemistry, Anti-Bacterial Agents chemistry, Escherichia coli metabolism, Escherichia coli Proteins metabolism, Homeostasis drug effects, Microbial Sensitivity Tests, Penicillin-Binding Proteins metabolism, Amdinocillin pharmacology, Anti-Bacterial Agents pharmacology, Escherichia coli drug effects, Escherichia coli Proteins antagonists & inhibitors, Penicillin-Binding Proteins antagonists & inhibitors

Abstract

β-Lactam antibiotics disrupt the assembly of peptidoglycan (PG) within the bacterial cell wall by inhibiting the enzymatic activity of penicillin-binding proteins (PBPs). It was recently shown that β-lactam treatment initializes a futile cycle of PG synthesis and degradation, highlighting major gaps in our understanding of the lethal effects of PBP inhibition by β-lactam antibiotics. Here, we assess the downstream metabolic consequences of treatment of Escherichia coli with the β-lactam mecillinam and show that lethality from PBP2 inhibition is a specific consequence of toxic metabolic shifts induced by energy demand from multiple catabolic and anabolic processes, including accelerated protein synthesis downstream of PG futile cycling. Resource allocation into these processes is coincident with alterations in ATP synthesis and utilization, as well as a broadly dysregulated cellular redox environment. These results indicate that the disruption of normal anabolic-catabolic homeostasis by PBP inhibition is an essential factor for β-lactam antibiotic lethality., Competing Interests: Declaration of interests M.A.L. is a full-time employee and shareholder of F. Hoffmann-La Roche, Ltd. J.J.C. is a scientific co-founder and scientific advisory board chair of Enbiotix, an antibiotics discovery company., (Copyright © 2021 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2022

3. A Distinct Transcriptional Program in Human CAR T Cells Bearing the 4-1BB Signaling Domain Revealed by scRNA-Seq.

Author

Boroughs AC, Larson RC, Marjanovic ND, Gosik K, Castano AP, Porter CBM, Lorrey SJ, Ashenberg O, Jerby L, Hofree M, Smith-Rosario G, Morris R, Gould J, Riley LS, Berger TR, Riesenfeld SJ, Rozenblatt-Rosen O, Choi BD, Regev A, and Maus MV

Subjects

HEK293 Cells, Humans, K562 Cells, RNA-Seq methods, Single-Cell Analysis, Transduction, Genetic, 4-1BB Ligand chemistry, 4-1BB Ligand metabolism, Cell Engineering methods, Protein Domains genetics, RNA, Small Cytoplasmic genetics, Receptors, Chimeric Antigen genetics, Signal Transduction genetics, T-Lymphocytes metabolism, Transcriptome

Abstract

T cells engineered to express chimeric antigen receptors (CARs) targeting CD19 have produced impressive outcomes for the treatment of B cell malignancies, but different products vary in kinetics, persistence, and toxicity profiles based on the co-stimulatory domains included in the CAR. In this study, we performed transcriptional profiling of bulk CAR T cell populations and single cells to characterize the transcriptional states of human T cells transduced with CD3ζ, 4-1BB-CD3ζ (BBζ), or CD28-CD3ζ (28ζ) co-stimulatory domains at rest and after activation by triggering their CAR or their endogenous T cell receptor (TCR). We identified a transcriptional signature common across CARs with the CD3ζ signaling domain, as well as a distinct program associated with the 4-1BB co-stimulatory domain at rest and after activation. CAR T cells bearing BBζ had increased expression of human leukocyte antigen (HLA) class II genes, ENPP2, and interleukin (IL)-21 axis genes, and decreased PD1 compared to 28ζ CAR T cells. Similar to previous studies, we also found BBζ CAR CD8 T cells to be enriched in a central memory cell phenotype and fatty acid metabolism genes. Our data uncovered transcriptional signatures related to costimulatory domains and demonstrated that signaling domains included in CARs uniquely shape the transcriptional programs of T cells., (Copyright © 2020 The American Society of Gene and Cell Therapy. Published by Elsevier Inc. All rights reserved.)

Published

2020

4. Emergence of a High-Plasticity Cell State during Lung Cancer Evolution.

Author

Marjanovic ND, Hofree M, Chan JE, Canner D, Wu K, Trakala M, Hartmann GG, Smith OC, Kim JY, Evans KV, Hudson A, Ashenberg O, Porter CBM, Bejnood A, Subramanian A, Pitter K, Yan Y, Delorey T, Phillips DR, Shah N, Chaudhary O, Tsankov A, Hollmann T, Rekhtman N, Massion PP, Poirier JT, Mazutis L, Li R, Lee JH, Amon A, Rudin CM, Jacks T, Regev A, and Tammela T

Subjects

Animals, Cell Differentiation genetics, Cell Line, Tumor, Cell Proliferation genetics, Cells, Cultured, Disease Models, Animal, Epithelial Cells cytology, Genetic Heterogeneity, Humans, Lung Neoplasms pathology, Mice, Single-Cell Analysis methods, Transcriptome genetics, Cell Plasticity genetics, Epithelial Cells metabolism, Epithelial-Mesenchymal Transition genetics, Lung Neoplasms genetics, Neoplastic Stem Cells metabolism

Abstract

Tumor evolution from a single cell into a malignant, heterogeneous tissue remains poorly understood. Here, we profile single-cell transcriptomes of genetically engineered mouse lung tumors at seven stages, from pre-neoplastic hyperplasia to adenocarcinoma. The diversity of transcriptional states increases over time and is reproducible across tumors and mice. Cancer cells progressively adopt alternate lineage identities, computationally predicted to be mediated through a common transitional, high-plasticity cell state (HPCS). Accordingly, HPCS cells prospectively isolated from mouse tumors and human patient-derived xenografts display high capacity for differentiation and proliferation. The HPCS program is associated with poor survival across human cancers and demonstrates chemoresistance in mice. Our study reveals a central principle underpinning intra-tumoral heterogeneity and motivates therapeutic targeting of the HPCS., Competing Interests: Declaration of Interests T.J. is a member of the Board of Directors of Amgen and Thermo Fisher Scientific, and a co-Founder of Dragonfly Therapeutics and T2 Biosystems. T.J. serves on the Scientific Advisory Board of Dragonfly Therapeutics, SQZ Biotech, and Skyhawk Therapeutics. T.J. also received funding from Calico and currently receives funding from Johnson & Johnson, but this funding did not support the research described in this manuscript. A.R. is a co-founder and equity holder in Celsius Therapeutics and a SAB member for Thermo Fisher, Asimov, Neogene Therapeutics, and Syros Pharmaceuticals, and an equity holder of Immunitas Therapeutics. C.M.R. serves on the SAB of Bridge Medicines and Harpoon Therapeutics, and has consulted regarding oncology drug development with AbbVie, Amgen, Ascentage, Bicycle, Celgene, Daiichi Sankyo, Genentech, Ipsen, Loxo, Pharmamar, and Vavotek. None of the affiliations listed above represent a conflict of interest with the design or execution of this study or interpretation of data presented in this manuscript. Other authors have nothing to disclose., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

5. Transcriptional Atlas of Intestinal Immune Cells Reveals that Neuropeptide α-CGRP Modulates Group 2 Innate Lymphoid Cell Responses.

Author

Xu H, Ding J, Porter CBM, Wallrapp A, Tabaka M, Ma S, Fu S, Guo X, Riesenfeld SJ, Su C, Dionne D, Nguyen LT, Lefkovith A, Ashenberg O, Burkett PR, Shi HN, Rozenblatt-Rosen O, Graham DB, Kuchroo VK, Regev A, and Xavier RJ

Subjects

Animals, Calcitonin Gene-Related Peptide genetics, Cells, Cultured, Computational Biology, Immunity, Innate, Interleukin-5 genetics, Interleukin-5 metabolism, Lectins, C-Type metabolism, Mice, Mice, Inbred BALB C, Mice, Transgenic, Neuropeptides genetics, Receptors, Immunologic metabolism, Sequence Analysis, RNA, Signal Transduction, Single-Cell Analysis, Th2 Cells immunology, Transcriptome, Up-Regulation, Calcitonin Gene-Related Peptide metabolism, Inflammation immunology, Intestines immunology, Lymphocytes immunology, Neuropeptides metabolism

Abstract

Signaling abnormalities in immune responses in the small intestine can trigger chronic type 2 inflammation involving interaction of multiple immune cell types. To systematically characterize this response, we analyzed 58,067 immune cells from the mouse small intestine by single-cell RNA sequencing (scRNA-seq) at steady state and after induction of a type 2 inflammatory reaction to ovalbumin (OVA). Computational analysis revealed broad shifts in both cell-type composition and cell programs in response to the inflammation, especially in group 2 innate lymphoid cells (ILC2s). Inflammation induced the expression of exon 5 of Calca, which encodes the alpha-calcitonin gene-related peptide (α-CGRP), in intestinal KLRG1 + ILC2s. α-CGRP antagonized KLRG1 + ILC2s proliferation but promoted IL-5 expression. Genetic perturbation of α-CGRP increased the proportion of intestinal KLRG1 + ILC2s. Our work highlights a model where α-CGRP-mediated neuronal signaling is critical for suppressing ILC2 expansion and maintaining homeostasis of the type 2 immune machinery., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

6. Carbon Sources Tune Antibiotic Susceptibility in Pseudomonas aeruginosa via Tricarboxylic Acid Cycle Control.

Author

Meylan S, Porter CBM, Yang JH, Belenky P, Gutierrez A, Lobritz MA, Park J, Kim SH, Moskowitz SM, and Collins JJ

Subjects

Anti-Bacterial Agents chemistry, Biofilms drug effects, Microbial Sensitivity Tests, Pseudomonas aeruginosa metabolism, Anti-Bacterial Agents pharmacology, Carbon metabolism, Citric Acid Cycle drug effects, Pseudomonas aeruginosa drug effects

Abstract

Metabolically dormant bacteria present a critical challenge to effective antimicrobial therapy because these bacteria are genetically susceptible to antibiotic treatment but phenotypically tolerant. Such tolerance has been attributed to impaired drug uptake, which can be reversed by metabolic stimulation. Here, we evaluate the effects of central carbon metabolite stimulations on aminoglycoside sensitivity in the pathogen Pseudomonas aeruginosa. We identify fumarate as a tobramycin potentiator that activates cellular respiration and generates a proton motive force by stimulating the tricarboxylic acid (TCA) cycle. In contrast, we find that glyoxylate induces phenotypic tolerance by inhibiting cellular respiration with acetyl-coenzyme A diversion through the glyoxylate shunt, despite drug import. Collectively, this work demonstrates that TCA cycle activity is important for both aminoglycoside uptake and downstream lethality and identifies a potential strategy for potentiating aminoglycoside treatment of P. aeruginosa infections., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

7. Bactericidal Antibiotics Induce Toxic Metabolic Perturbations that Lead to Cellular Damage.

Author

Belenky P, Ye JD, Porter CB, Cohen NR, Lobritz MA, Ferrante T, Jain S, Korry BJ, Schwarz EG, Walker GC, and Collins JJ

Subjects

DNA Breaks, Double-Stranded, Ampicillin pharmacology, Anti-Bacterial Agents pharmacology, Escherichia coli drug effects, Kanamycin pharmacology, Norfloxacin pharmacology, Oxidative Stress

Abstract

Understanding how antibiotics impact bacterial metabolism may provide insight into their mechanisms of action and could lead to enhanced therapeutic methodologies. Here, we profiled the metabolome of Escherichia coli after treatment with three different classes of bactericidal antibiotics (?-lactams, aminoglycosides, quinolones). These treatments induced a similar set of metabolic changes after 30 min that then diverged into more distinct profiles at later time points. The most striking changes corresponded to elevated concentrations of central carbon metabolites, active breakdown of the nucleotide pool, reduced lipid levels, and evidence of an elevated redox state. We examined potential end-target consequences of these metabolic perturbations and found that antibiotic-treated cells exhibited cytotoxic changes indicative of oxidative stress, including higher levels of protein carbonylation, malondialdehyde adducts, nucleotide oxidation, and double-strand DNA breaks. This work shows that bactericidal antibiotics induce a complex set of metabolic changes that are correlated with the buildup of toxic metabolic by-products., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2015