Your search keyword '"Kimberly A. Wodzanowski"' showing total 17 results

1. Synthesis and validation of click-modified NOD1/2 agonists

Author

Ravi Bharadwaj, Madison V. Anonick, Swati Jaiswal, Siavash Mashayekh, Ashley Brown, Kimberly A. Wodzanowski, Kendi Okuda, Neal Silverman, and Catherine L. Grimes

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

NOD1 and NOD2 sense small bacterial peptidoglycan fragments, often called muropeptides, that access the cytosol. These muropeptides include iE-DAP and MDP, the minimal agonists for NOD1 and NOD2, respectively. Here, we synthesized and validated alkyne-modified muropeptides, iE-DAP-Alk and MDP-Alk, for use in click-chemistry reactions. While it has long been known that many cell types respond to extracellular exposure to muropeptides, it is unclear how these innate immune activators access their cytosolic innate immune receptors, NOD1 and NOD2. The subcellular trafficking and transport mechanisms by which muropeptides access these cytosolic innate immune receptors are a major gap in our understanding of these critical host responses. The click-chemistry-enabled agonists developed here will be particularly powerful to decipher the underlying cell biology and biochemistry of NOD1 and NOD2 innate immune sensing.

Published

2023

2. Bacterial Peptidoglycan Fragments Differentially Regulate Innate Immune Signaling

Author

Klare L. Bersch, Kristen E. DeMeester, Rachid Zagani, Shuyuan Chen, Kimberly A. Wodzanowski, Shuzhen Liu, Siavash Mashayekh, Hans-Christian Reinecker, and Catherine L. Grimes

Subjects

Chemistry, QD1-999

Published

2021

3. Multiscale Invasion Assay for Probing Macrophage Response to Gram-Negative Bacteria

Author

Kimberly A. Wodzanowski, Jeffrey L. Caplan, April M. Kloxin, and Catherine L. Grimes

Subjects

biomaterials, bioorthogonal chemistry, invasion model, bacteria-macrophage interactions, click chemistry, live cell imaging, Chemistry, QD1-999

Abstract

The immune system is a complex network of various cellular components that must differentiate between pathogenic bacteria and the commensal bacteria of the human microbiome, where misrecognition is linked to inflammatory disorders. Fragments of bacterial cell wall peptidoglycan bind to pattern recognition receptors within macrophages, leading to immune activation. To study this complex process, a methodology to remodel and label the bacterial cell wall of two different species of bacteria was established using copper (I) catalyzed azide-alkyne cycloaddition (CuAAC) and strain-promoted azide-alkyne cycloaddition (SPAAC). Additionally, an approach for three-dimensional (3D) culture of human macrophages and their invasion with relevant bacteria in a well-defined hydrogel-based synthetic matrix inspired by the microenvironment of the gut was established. Workflows were developed for human monocyte encapsulation and differentiation into macrophages in 3D culture with high viability. Bacteria invaded into macrophages permitted in situ peptidoglycan labeling. Macrophages exhibited biologically-relevant cytokine release in response to bacteria. This molecularly engineered, multi-dimensional bacteria-macrophage co-culture system will prove useful in future studies to observe immunostimulatory, bacterial fragment production and localization in the cell at the carbohydrate level for insights into how the immune system properly senses bacteria.

Published

2022

4. Investigating Peptidoglycan Recycling Pathways in

Author

Kimberly A, Wodzanowski, Stephen N, Hyland, Sreedevi, Chinthamani, Liam-Michael D, Sandles, Kiyonobu, Honma, Ashu, Sharma, and Catherine L, Grimes

Subjects

Cell Wall, Pseudomonas putida, Muramic Acids, Tannerella forsythia, Escherichia coli, Humans, Peptidoglycan

Abstract

The human oral microbiome is the second largest microbial community in humans, harboring over 700 bacterial species, which aid in digestion and protect from growth of disease-causing pathogens. One such oral pathogen

Published

2023

5. Investigating Peptidoglycan Recycling Pathways in Tannerella forsythia with N-Acetylmuramic Acid Bioorthogonal Probes

Author

Kimberly A. Wodzanowski, Stephen N. Hyland, Sreedevi Chinthamani, Liam-Michael D. Sandles, Kiyonobu Honma, Ashu Sharma, and Catherine L. Grimes

Subjects

Infectious Diseases

Published

2022

6. Synthesis and validation of click-modified of NOD1/2 agonists

Author

Ravi Bharadwaj, Madison V. Anonick, Siavash Mashayekh, Ashley Brown, Kimberly A. Wodzanowski, Kendi Okuda, Neal Silverman, and Catherine L. Grimes

Abstract

NOD1 and NOD2 sense small bacterial peptidoglycan fragments often called muropeptides. These muropeptides include iE-DAP and MDP, the minimal agonists for NOD1 and NOD2, respectively. Here, we synthesized and validated alkyne-modified muropeptides, iE-DAP-Alk and MDP-Alk, for use in click-chemistry reactions. While it has long been known that many cell types respond to extracellular exposure to muropeptides, it is unclear how these innate immune activators access their cytosolic innate immune receptors, NOD1 and NOD2. The subcellular trafficking and transport mechanisms by which muropeptides access these cytosolic innate immune receptors are a major gap in our understanding of these critical host responses. The clickchemistry-enabled agonists developed here will be particularly powerful to decipher the underlying cell biology and biochemistry of NOD1 and NOD2 innate immune sensing.

Published

2023

7. Bringing Pasteur Back to Life: Studying the Biochemistry of Yeast Fermentation Through Discussion Groups and an At-Home Lab

Author

Kimberly A. Wodzanowski, Madison V. Anonick, Lauren A. Genova, April M. Kloxin, and Catherine L. Grimes

Subjects

General Medicine

Published

2023

8. Methotrexate suppresses psoriatic skin inflammation by inhibiting muropeptide transporter SLC46A2 activity

Author

Ravi Bharadwaj, Christina F. Lusi, Siavash Mashayekh, Abhinit Nagar, Malireddi Subbarao, Griffin I. Kane, Kimberly A. Wodzanowski, Ashley R. Brown, Kendi Okuda, Amanda Monahan, Donggi Paik, Anubhab Nandy, Madison V. Anonick, William E. Goldman, Thirumala-Devi Kanneganti, Megan H. Orzalli, Catherine Leimkuhler Grimes, Prabhani U. Atukorale, and Neal Silverman

Subjects

Infectious Diseases, Immunology, Immunology and Allergy

Published

2023

9. Bacterial Peptidoglycan Fragments Differentially Regulate Innate Immune Signaling

Author

Rachid Zagani, Siavash Mashayekh, Shuzhen Liu, Hans Christian Reinecker, Catherine L. Grimes, Klare L. Bersch, Kimberly A. Wodzanowski, Kristen E. DeMeester, and Shuyuan Chen

Subjects

Innate immune system, 010405 organic chemistry, General Chemical Engineering, Pattern recognition receptor, Disaccharide, General Chemistry, 010402 general chemistry, 01 natural sciences, 0104 chemical sciences, Proinflammatory cytokine, Cell biology, chemistry.chemical_compound, Chemistry, chemistry, Microbiome, Peptidoglycan, Receptor, QD1-999, Muramyl dipeptide, Research Article

Abstract

The human innate immune system responds to both pathogen and commensal bacteria at the molecular level using bacterial peptidoglycan (PG) recognition elements. Traditionally, synthetic and commercially accessible PG monosaccharide units known as muramyl dipeptide (MDP) and N-glycolyl MDP (ng-MDP) have been used to probe the mechanism of innate immune activation of pattern recognition receptors, such as NOD-like receptors. However, bacterial PG is a dynamic and complex structure, with various chemical modifications and trimming mechanisms that result in the production of disaccharide-containing elements. These molecules pose as attractive targets for immunostimulatory screening; however, studies are limited because of their synthetic accessibility. Inspired by disaccharide-containing compounds produced from the gut microbe Lactobacillus acidophilus, a robust and scalable chemical synthesis of PG-based disaccharide ligands was implemented. Together with a monosaccharide PG library, compounds were screened for their ability to stimulate proinflammatory genes in bone-marrow-derived macrophages. The data reveal distinct gene induction patterns for monosaccharide and disaccharide PG units, suggesting that PG innate immune signaling is more complex than a one activator–one pathway program, as biologically relevant fragments induce transcriptional programs to different degrees. These disaccharide molecules will serve as critical immunostimulatory tools to more precisely define specialized innate immune regulatory mechanisms that distinguish between commensal and pathogenic bacteria residing in the microbiome., Synthesis of biologically inspired peptidoglycan fragments reveals a complex immune pathway activating transcriptional programs that induce genes associated with inflammatory bowel disease.

Published

2021

10. Engaging biochemistry students virtually utilizing problem‐based learning and at home lab activities

Author

Kimberly A. Wodzanowski, Madison V. Anonick, Lauren A. Genova, April M. Kloxin, and Catherine L. Grimes

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2022

11. Protected N-Acetyl Muramic Acid Probes Improve Bacterial Peptidoglycan Incorporation via Metabolic Labeling

Author

Cintia C. Santiago, Stephen N. Hyland, Ashley R Brown, Kimberly A. Wodzanowski, PapaNii Asare-Okai, Julianna L Follmar, and Catherine L. Grimes

Subjects

chemistry.chemical_classification, Glycan, biology, Chemistry, Glycobiology, Bacterial Glycan, Carboxylic acid, General Medicine, Peptidoglycan, Muramic acid, Biochemistry, Bacterial cell structure, Article, carbohydrates (lipids), Cell wall, chemistry.chemical_compound, Cell Wall, Polysaccharides, Molecular Probes, Muramic Acids, biology.protein, Escherichia coli, Molecular Medicine

Abstract

Metabolic glycan probes have emerged as an excellent tool to investigate vital questions in biology. Recently, methodology to incorporate metabolic bacterial glycan probes into the cell wall of a variety of bacterial species has been developed. In order to improve this method, a scalable synthesis of the peptidoglycan precursors is developed here, allowing for access to essential peptidoglycan immunological fragments and cell wall building blocks. The question was asked if masking polar groups of the glycan probe would increase overall incorporation, a common strategy exploited in mammalian glycobiology. Here, we show, through cellular assays, that E. coli do not utilize peracetylated peptidoglycan substrates but do employ methyl esters. The 10-fold improvement of probe utilization indicates that (i) masking the carboxylic acid is favorable for transport and (ii) bacterial esterases are capable of removing the methyl ester for use in peptidoglycan biosynthesis. This investigation advances bacterial cell wall biology, offering a prescription on how to best deliver and utilize bacterial metabolic glycan probes.

Published

2021

12. Localizing Peptidoglycan Synthesis in Helicobacter pylori using Clickable Metabolic Probes

Author

Nina R. Salama, Jennifer A. Taylor, Kristen E. DeMeester, Kimberly A. Wodzanowski, Joe W. Gray, Cintia C. Santiago, Catherine L. Grimes, Waldemar Vollmer, and Jacob Biboy

Subjects

Cell, Health Informatics, Peptidoglycan, Muramic acid, Article, General Biochemistry, Genetics and Molecular Biology, Bacterial cell structure, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, Tandem Mass Spectrometry, medicine, General Pharmacology, Toxicology and Pharmaceutics, 030304 developmental biology, 0303 health sciences, Helicobacter pylori, General Immunology and Microbiology, biology, General Neuroscience, 030302 biochemistry & molecular biology, biology.organism_classification, carbohydrates (lipids), Medical Laboratory Technology, medicine.anatomical_structure, chemistry, Biochemistry, N-Acetylmuramic acid, Muramic Acids, Bacteria, Chromatography, Liquid

Abstract

The bacterial cell wall, composed of peptidoglycan (PG), provides structural integrity for the cell and is responsible for cell shape in most bacteria. Here we present tools to study the cell wall using a clickable PG-specific sugar, 2-alkyne muramic acid (MurNAc-alk), as a metabolic probe. Here we present a new reaction pathway for generating MurNAc-alk. We also include protocols for labeling PG synthesis in Helicobacter pylori, determining the identity of the labeled muropeptides using LC-MS/MS, sample preparation of cells labeled for a short fraction of the doubling time, and visualization using 3D structured illumination microscopy. © 2021 Wiley Periodicals LLC. Basic Protocol 1: Alternative synthesis of MurNAc-alk (direct coupling) Support Protocol 1: Growing Helicobacter pylori in liquid culture Support Protocol 2: Fosfomycin rescue assay Basic Protocol 2: Mass spectrometry (MS) analysis to determine incorporation of MurNAc-alk within the peptidoglycan of H. pylori Support Protocol 3: Hayashi test to determine if SDS is present in the supernatant of peptidoglycan preparations Support Protocol 4: Creating custom cytocentrifuge units for use in a swinging-bucket tabletop centrifuge Basic Protocol 3: Labeling H. pylori with MurNAc-alk or D-Ala-alk Basic Protocol 4: Structured illumination microscopy (SIM) imaging on the DeltaVision OMX.

Published

2021

13. Multiscale Invasion Assay for Probing Macrophage Response to Bacteria

Author

April M. Kloxin, Catherine L. Grimes, and Kimberly A. Wodzanowski

Subjects

biology, Chemistry, Monocyte, Pattern recognition receptor, Pathogenic bacteria, biology.organism_classification, medicine.disease_cause, Bacterial cell structure, Cell biology, chemistry.chemical_compound, Immune system, medicine.anatomical_structure, Gentamicin protection assay, medicine, Peptidoglycan, Bacteria

Abstract

The immune system is a complex network of various cellular components that must differentiate between pathogenic bacteria and the commensal bacteria of the human microbiome, where misrecognition is linked to inflammatory disorders. Fragments of bacterial cell wall peptidoglycan bind to pattern recognition receptors within macrophages, leading to immune activation. To study this complex process, an approach for three-dimensional (3D) culture of human macrophages and their invasion with relevant bacteria in a well-defined hydrogel-based synthetic matrix inspired by the gut was established. Workflows were developed for monocyte encapsulation and differentiation into macrophages in 3D culture with high viability. Bacteria invaded into macrophages permitted in situ peptidoglycan labeling. Macrophages exhibited biologically-relevant cytokine release in response to bacteria. This multi-dimensional bacteria-macrophage co-culture system will prove useful in future studies to observe bacterial fragment production and localization in the cell at the carbohydrate level for insights into how our immune system properly senses bacteria.TOC Figure

Published

2020

14. Bacterial Peptidoglycan Fragments Differentially Regulate Innate Immune Signaling

Author

Rachid Zagani, Kristen E. DeMeester, Kimberly A. Wodzanowski, Klare L. Bersch, Catherine L. Grimes, and Hans Christian Reinecker

Subjects

chemistry.chemical_compound, Innate immune system, chemistry, Disaccharide, Pattern recognition receptor, Peptidoglycan, Microbiome, Receptor, Muramyl dipeptide, Proinflammatory cytokine, Cell biology

Abstract

The human innate immune system responds to both pathogen and commensal bacteria at the molecular level using bacterial peptidoglycan (PG) recognition elements. Traditionally, synthetic and commercially accessible PG monosaccharide units known as muramyl dipeptide (MDP) and N-glycolyl MDP (ng-MDP) have been used to probe the mechanism of innate immune activation of pattern recognition receptors (PRRs) such as NOD-like receptors (NLRs). However, bacterial PG is a dynamic and complex structure, with various chemical modifications and trimming mechanisms that result in the production of disaccharide containing elements. These molecules pose as attractive targets for immunostimulatory screening; however, studies are limited due to their synthetic accessibility. Inspired by disaccharide containing compounds produced from the gut microbe, Lactobacillus acidophilus, a robust and scalable chemical synthesis of PG-based disaccharide ligands was implemented. Together with a monosaccharide PG library, compounds were screened for their ability to stimulate proinflammatory genes in bone marrow derived macrophages (BMDMs). The data reveal a diverse gene induction pattern between monosaccharide and disaccharide PG units, suggesting that PG innate immune signaling is more complex than a one-activator-one pathway program, as biologically relevant fragments induce distinct transcriptional programs. These disaccharide molecules will serve as critical immunostimulatory tools to more precisely define specialized innate immune regulatory mechanisms that distinguish between commensal and pathogenic bacteria residing in the microbiome.

Published

2020

15. Metabolic Incorporation of N ‐Acetyl Muramic Acid Probes into Bacterial Peptidoglycan

Author

Benjamin L. Prather, Hai Liang, Catherine L. Grimes, Kristen E. DeMeester, Kimberly A. Wodzanowski, Cintia C. Santiago, and Junhui Zhou

Subjects

0301 basic medicine, Azides, Peptidoglycan, Muramic acid, 010402 general chemistry, medicine.disease_cause, 01 natural sciences, Catalysis, Article, Bacterial cell structure, 03 medical and health sciences, chemistry.chemical_compound, Biosynthesis, Glucosamine, Escherichia coli, medicine, Fluorescent Dyes, Cycloaddition Reaction, Chemistry, General Medicine, 0104 chemical sciences, 030104 developmental biology, Metabolic Engineering, Biochemistry, Alkynes, Muramic Acids, Click chemistry, Click Chemistry, Bioorthogonal chemistry

Abstract

Bacterial cells utilize small carbohydrate building blocks to construct peptidoglycan (PG), a highly conserved mesh-like polymer that serves as a protective coat for the cell. PG production has long been a target for antibiotics, and its breakdown is a source for human immune recognition. A key component of bacterial PG, N-acetyl muramic acid (NAM), is a vital element in many synthetically derived immunostimulatory compounds. However, the exact molecular details of these structures and how they are generated remain unknown due to a lack of chemical probes surrounding the NAM core. A robust synthetic strategy to generate bioorthogonally tagged NAM carbohydrate units is implemented. These molecules serve as precursors for PG biosynthesis and recycling. Escherichia coli cells are metabolically engineered to incorporate the bioorthogonal NAM probes into their PG network. The probes are subsequently modified using copper-catalyzed azide-alkyne cycloaddition to install fluorophores directly into the bacterial PG, as confirmed by super-resolution microscopy and high-resolution mass spectrometry. Here, synthetic notes for key elements of this process to generate the sugar probes as well as streamlined user-friendly metabolic labeling strategies for both microbiology and immunological applications are described. © 2019 by John Wiley & Sons, Inc. Basic Protocol 1: Synthesis of peracetylated 2-azido glucosamine Basic Protocol 2: Synthesis of 2-azido and 2-alkyne NAM Basic Protocol 3: Synthesis of 3-azido NAM methyl ester Basic Protocol 4: Incorporation of NAM probes into bacterial peptidoglycan Basic Protocol 5: Confirmation of bacterial cell wall remodeling by mass spectrometry.

Published

2019

16. Tools for probing host-bacteria interactions in the gut microenvironment: From molecular to cellular levels

Author

Kimberly A. Wodzanowski, Samantha E. Cassel, April M. Kloxin, and Catherine L. Grimes

Subjects

Clinical Biochemistry, Pharmaceutical Science, Models, Biological, Biochemistry, Article, Host-Parasite Interactions, chemistry.chemical_compound, Molecular level, Immune system, Drug Discovery, Animals, Humans, Microbiome, Molecular Biology, Fluorescent Dyes, Bacteria, biology, Host (biology), Organic Chemistry, Therapeutic evaluation, biology.organism_classification, Immunity, Innate, Extracellular Matrix, Cell biology, Intestines, Cellular Microenvironment, chemistry, Molecular Medicine, Peptidoglycan, Function (biology)

Abstract

Healthy function of the gut microenvironment is dependent on complex interactions between the bacteria of the microbiome, epithelial and immune (host) cells, and the surrounding tissue. Misregulation of these interactions is implicated in disease. A range of tools have been developed to study these interactions, from mechanistic studies to therapeutic evaluation. In this Digest, we highlight select tools at the cellular and molecular level for probing specific cell-microenvironment interactions. Approaches are overviewed for controlling and probing cell-cell interactions, from transwell and microfluidic devices to engineered bacterial peptidoglycan fragments, and cell-matrix interactions, from three-dimensional scaffolds to chemical handles for in situ modifications.

Published

2020

17. Catalytic activity and autoprocessing of murine caspase-11 mediate noncanonical inflammasome assembly in response to cytosolic LPS

Author

Daniel C Akuma, Kimberly A Wodzanowski, Ronit Schwartz Wertman, Patrick M Exconde, Víctor R Vázquez Marrero, Chukwuma E Odunze, Daniel Grubaugh, Sunny Shin, Cornelius Taabazuing, and Igor E Brodsky

Subjects

noncanonical inflammasome, caspase-11, LPS, sepsis, caspase-1, pyroptosis, Medicine, Science, Biology (General), QH301-705.5

Abstract

Inflammatory caspases are cysteine protease zymogens whose activation following infection or cellular damage occurs within supramolecular organizing centers (SMOCs) known as inflammasomes. Inflammasomes recruit caspases to undergo proximity-induced autoprocessing into an enzymatically active form that cleaves downstream targets. Binding of bacterial LPS to its cytosolic sensor, caspase-11 (Casp11), promotes Casp11 aggregation within a high-molecular-weight complex known as the noncanonical inflammasome, where it is activated to cleave gasdermin D and induce pyroptosis. However, the cellular correlates of Casp11 oligomerization and whether Casp11 forms an LPS-induced SMOC within cells remain unknown. Expression of fluorescently labeled Casp11 in macrophages revealed that cytosolic LPS induced Casp11 speck formation. Unexpectedly, catalytic activity and autoprocessing were required for Casp11 to form LPS-induced specks in macrophages. Furthermore, both catalytic activity and autoprocessing were required for Casp11 speck formation in an ectopic expression system, and processing of Casp11 via ectopically expressed TEV protease was sufficient to induce Casp11 speck formation. These data reveal a previously undescribed role for Casp11 catalytic activity and autoprocessing in noncanonical inflammasome assembly, and shed new light on the molecular requirements for noncanonical inflammasome assembly in response to cytosolic LPS.

Published

2024