Your search keyword '"Everett, John K"' showing total 284 results

1. Use of HSC-targeted LNP to generate a mouse model of lethal α-thalassemia and treatment via lentiviral gene therapy

Author

Chappell, Maxwell E., Breda, Laura, Tricoli, Lucas, Guerra, Amaliris, Jarocha, Danuta, Castruccio Castracani, Carlo, Papp, Tyler E., Tanaka, Naoto, Hamilton, Nolan, Triebwasser, Michael P., Ghiaccio, Valentina, Fedorky, Megan T., Gollomp, Kandace L., Bochenek, Veronica, Roche, Aoife M., Everett, John K., Cook, Emma J., Bushman, Frederic D., Teawtrakul, Nattiya, Glentis, Stavros, Kattamis, Antonis, Mui, Barbara L., Tam, Ying K., Weissman, Drew, Abdulmalik, Osheiza, Parhiz, Hamideh, and Rivella, Stefano

Published

2024

2. Modulation of AAV transduction and integration targeting by topoisomerase poisons

Author

Kasimsetty, Aradhana, Hwang, Young, Everett, John K., McFarland, Alexander G., Zolnoski, Sonja A., Lu, Tianyu, Roche, Aoife M., Martínez-García, Pedro Manuel, Sabatino, Denise E., and Bushman, Frederic D.

Published

2024

3. Analysis of vector genome integrations in multicentric lymphoma after AAV gene therapy in a severe hemophilia A dog

Author

Van Gorder, Lucas, Doshi, Bhavya S., Willis, Elinor, Nichols, Timothy C., Cook, Emma, Everett, John K., Merricks, Elizabeth P., Arruda, Valder R., Bushman, Frederic D., Callan, Mary Beth, and Samelson-Jones, Benjamin J.

Published

2023

4. Outcomes of hematopoietic stem cell gene therapy for Wiskott-Aldrich syndrome

Author

Labrosse, Roxane, Chu, Julia I., Armant, Myriam A., Everett, John K., Pellin, Danilo, Kareddy, Niharika, Frelinger, Andrew L., Henderson, Lauren A., O’Connell, Amy E., Biswas, Amlan, Coenen-van der Spek, Jet, Miggelbrink, Alexandra, Fiorini, Claudia, Adhikari, Hriju, Berry, Charles C., Cantu, Vito Adrian, Fong, Johnson, Jaroslavsky, Jason, Karadeniz, Derin F., Li, Quan-Zhen, Reddy, Shantan, Roche, Aoife M., Zhu, Chengsong, Whangbo, Jennifer S., Dansereau, Colleen, Mackinnon, Brenda, Morris, Emily, Koo, Stephanie M., London, Wendy B., Baris, Safa, Ozen, Ahmet, Karakoc-Aydiner, Elif, Despotovic, Jenny M., Forbes Satter, Lisa R., Saitoh, Akihiko, Aizawa, Yuta, King, Alejandra, Nguyen, Mai Anh Thi, Vu, Vy Do Uyen, Snapper, Scott B., Galy, Anne, Notarangelo, Luigi D., Bushman, Frederic D., Williams, David A., and Pai, Sung-Yun

Published

2023

5. Antigen-driven clonal selection shapes the persistence of HIV-1 infected CD4+ T cells in vivo

Author

Simonetti, Francesco R, Zhang, Hao, Soroosh, Garshasb P, Duan, Jiayi, Rhodehouse, Kyle, Hill, Alison L, Beg, Subul A, McCormick, Kevin, Raymond, Hayley E, Nobles, Christopher L, Everett, John K, Kwon, Kyungyoon J, White, Jennifer A, Lai, Jun, Margolick, Joseph B, Hoh, Rebecca, Deeks, Steven G, Bushman, Frederic D, Siliciano, Janet D, and Siliciano, Robert F

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Sexually Transmitted Infections, Clinical Research, HIV/AIDS, 2.1 Biological and endogenous factors, Aetiology, Infection, Adult, CD4-Positive T-Lymphocytes, Clonal Selection, Antigen-Mediated, Female, HIV Infections, HIV-1, Humans, Male, Virus Integration, Virus Latency, gag Gene Products, Human Immunodeficiency Virus, AIDS/HIV, Adaptive immunity, Clonal selection, T cells, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Clonal expansion of infected CD4+ T cells is a major mechanism of HIV-1 persistence and a barrier to achieving a cure. Potential causes are homeostatic proliferation, effects of HIV-1 integration, and interaction with antigens. Here, we show that it is possible to link antigen responsiveness, the full proviral sequence, the integration site, and the T cell receptor β-chain (TCRβ) sequence to examine the role of recurrent antigenic exposure in maintaining the HIV-1 reservoir. We isolated CMV- and Gag-responding CD4+ T cells from 10 treated individuals. Proviral populations in CMV-responding cells were dominated by large clones, including clones harboring replication-competent proviruses. TCRβ repertoires showed high clonality driven by converging adaptive responses. Although some proviruses were in genes linked to HIV-1 persistence (BACH2, STAT5B, MKL1), the proliferation of infected cells under antigenic stimulation occurred regardless of the site of integration. Paired TCRβ and integration site analysis showed that infection could occur early or late in the course of a clone's response to antigen and could generate infected cell populations too large to be explained solely by homeostatic proliferation. Together, these findings implicate antigen-driven clonal selection as a major factor in HIV-1 persistence, a finding that will be a difficult challenge to eradication efforts.

Published

2021

6. Autologous T cell therapy for MAGE-A4+ solid cancers in HLA-A*02+ patients: a phase 1 trial

Author

Hong, David S., Van Tine, Brian A., Biswas, Swethajit, McAlpine, Cheryl, Johnson, Melissa L., Olszanski, Anthony J., Clarke, Jeffrey M., Araujo, Dejka, Blumenschein, Jr, George R., Kebriaei, Partow, Lin, Quan, Tipping, Alex J., Sanderson, Joseph P., Wang, Ruoxi, Trivedi, Trupti, Annareddy, Thejo, Bai, Jane, Rafail, Stavros, Sun, Amy, Fernandes, Lilliam, Navenot, Jean-Marc, Bushman, Frederic D., Everett, John K., Karadeniz, Derin, Broad, Robyn, Isabelle, Martin, Naidoo, Revashnee, Bath, Natalie, Betts, Gareth, Wolchinsky, Zohar, Batrakou, Dzmitry G., Van Winkle, Erin, Elefant, Erica, Ghobadi, Armin, Cashen, Amanda, Grand’Maison, Anne, McCarthy, Philip, Fracasso, Paula M., Norry, Elliot, Williams, Dennis, Druta, Mihaela, Liebner, David A., Odunsi, Kunle, and Butler, Marcus O.

Published

2023

7. Lentiviral gene therapy for X-linked chronic granulomatous disease.

Author

Kohn, Donald B, Booth, Claire, Kang, Elizabeth M, Pai, Sung-Yun, Shaw, Kit L, Santilli, Giorgia, Armant, Myriam, Buckland, Karen F, Choi, Uimook, De Ravin, Suk See, Dorsey, Morna J, Kuo, Caroline Y, Leon-Rico, Diego, Rivat, Christine, Izotova, Natalia, Gilmour, Kimberly, Snell, Katie, Dip, Jinhua Xu-Bayford, Darwish, Jinan, Morris, Emma C, Terrazas, Dayna, Wang, Leo D, Bauser, Christopher A, Paprotka, Tobias, Kuhns, Douglas B, Gregg, John, Raymond, Hayley E, Everett, John K, Honnet, Geraldine, Biasco, Luca, Newburger, Peter E, Bushman, Frederic D, Grez, Manuel, Gaspar, H Bobby, Williams, David A, Malech, Harry L, Galy, Anne, Thrasher, Adrian J, and Net4CGD consortium

Subjects

Net4CGD consortium, Neutrophils, Hematopoietic Stem Cells, Chromosomes, Human, X, Humans, Lentivirus, Granulomatous Disease, Chronic, Antigens, CD34, Treatment Outcome, Transplantation Conditioning, Comorbidity, Gene Silencing, Genes, Regulator, Genetic Vectors, Adolescent, Child, Child, Preschool, United States, Male, Promoter Regions, Genetic, Young Adult, Patient Safety, Genetic Therapy, United Kingdom, NADPH Oxidases, Genetics, Hematology, Regenerative Medicine, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Gene Therapy, Clinical Trials and Supportive Activities, Infectious Diseases, Clinical Research, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Inflammatory and immune system, Infection, Medical and Health Sciences, Immunology

Abstract

Chronic granulomatous disease (CGD) is a rare inherited disorder of phagocytic cells1,2. We report the initial results of nine severely affected X-linked CGD (X-CGD) patients who received ex vivo autologous CD34+ hematopoietic stem and progenitor cell-based lentiviral gene therapy following myeloablative conditioning in first-in-human studies (trial registry nos. NCT02234934 and NCT01855685). The primary objectives were to assess the safety and evaluate the efficacy and stability of biochemical and functional reconstitution in the progeny of engrafted cells at 12 months. The secondary objectives included the evaluation of augmented immunity against bacterial and fungal infection, as well as assessment of hematopoietic stem cell transduction and engraftment. Two enrolled patients died within 3 months of treatment from pre-existing comorbidities. At 12 months, six of the seven surviving patients demonstrated stable vector copy numbers (0.4-1.8 copies per neutrophil) and the persistence of 16-46% oxidase-positive neutrophils. There was no molecular evidence of either clonal dysregulation or transgene silencing. Surviving patients have had no new CGD-related infections, and six have been able to discontinue CGD-related antibiotic prophylaxis. The primary objective was met in six of the nine patients at 12 months follow-up, suggesting that autologous gene therapy is a promising approach for CGD patients.

Published

2020

8. T cell dynamics and response of the microbiota after gene therapy to treat X-linked severe combined immunodeficiency

Author

Clarke, Erik L, Connell, A Jesse, Six, Emmanuelle, Kadry, Nadia A, Abbas, Arwa A, Hwang, Young, Everett, John K, Hofstaedter, Casey E, Marsh, Rebecca, Armant, Myriam, Kelsen, Judith, Notarangelo, Luigi D, Collman, Ronald G, Hacein-Bey-Abina, Salima, Kohn, Donald B, Cavazzana, Marina, Fischer, Alain, Williams, David A, Pai, Sung-Yun, and Bushman, Frederic D

Subjects

Biological Sciences, Genetics, Regenerative Medicine, Biotechnology, Gene Therapy, Clinical Research, Stem Cell Research, Inflammatory and immune system, Infection, Cell Division, Child, Preschool, Complementarity Determining Regions, Genetic Therapy, Humans, Microbiota, Receptors, Antigen, T-Cell, alpha-beta, T-Lymphocytes, X-Linked Combined Immunodeficiency Diseases, Clinical Sciences

Abstract

BackgroundMutation of the IL2RG gene results in a form of severe combined immune deficiency (SCID-X1), which has been treated successfully with hematopoietic stem cell gene therapy. SCID-X1 gene therapy results in reconstitution of the previously lacking T cell compartment, allowing analysis of the roles of T cell immunity in humans by comparing before and after gene correction.MethodsHere we interrogate T cell reconstitution using four forms of high throughput analysis. (1) Estimation of the numbers of transduced progenitor cells by monitoring unique positions of integration of the therapeutic gene transfer vector. (2) Estimation of T cell population structure by sequencing of the recombined T cell receptor (TCR) beta locus. (3) Metagenomic analysis of microbial populations in oropharyngeal, nasopharyngeal, and gut samples. (4) Metagenomic analysis of viral populations in gut samples.ResultsComparison of progenitor and mature T cell populations allowed estimation of a minimum number of cell divisions needed to generate the observed populations. Analysis of microbial populations showed the effects of immune reconstitution, including normalization of gut microbiota and clearance of viral infections. Metagenomic analysis revealed enrichment of genes for antibiotic resistance in gene-corrected subjects relative to healthy controls, likely a result of higher healthcare exposure.ConclusionsThis multi-omic approach enables the characterization of multiple effects of SCID-X1 gene therapy, including T cell repertoire reconstitution, estimation of numbers of cell divisions between progenitors and daughter T cells, normalization of the microbiome, clearance of microbial pathogens, and modulations in antibiotic resistance gene levels. Together, these results quantify several aspects of the long-term efficacy of gene therapy for SCID-X1. This study includes data from ClinicalTrials.gov numbers NCT01410019, NCT01175239, and NCT01129544.

Published

2018

9. Lentiviral globin gene therapy with reduced-intensity conditioning in adults with β-thalassemia: a phase 1 trial

Author

Boulad, Farid, Maggio, Aurelio, Wang, Xiuyan, Moi, Paolo, Acuto, Santina, Kogel, Friederike, Takpradit, Chayamon, Prockop, Susan, Mansilla-Soto, Jorge, Cabriolu, Annalisa, Odak, Ashlesha, Qu, Jinrong, Thummar, Keyur, Du, Fang, Shen, Lingbo, Raso, Simona, Barone, Rita, Di Maggio, Rosario, Pitrolo, Lorella, Giambona, Antonino, Mingoia, Maura, Everett, John K., Hokama, Pascha, Roche, Aoife M., Cantu, Vito Adrian, Adhikari, Hriju, Reddy, Shantan, Bouhassira, Eric, Mohandas, Narla, Bushman, Frederic D., Rivière, Isabelle, and Sadelain, Michel

Published

2022

10. TET2 regulates early and late transitions in exhausted CD8+T-cell differentiation and limits CAR T-cell function

Author

Dimitri, Alexander J, primary, Baxter, Amy E, additional, Chen, Gregory M, additional, Hopkins, Caitlin R, additional, Rouin, Geoffrey T, additional, Huang, Hua, additional, Kong, Weimin, additional, Holliday, Christopher H, additional, Wiebking, Volker, additional, Bartoszek, Robert, additional, Drury, Sydney, additional, Dalton, Katherine, additional, Koucky, Owen M, additional, Chen, Zeyu, additional, Giles, Josephine R, additional, Jung, In-Young, additional, O'Connor, Roddy, additional, Collins, Sierra, additional, Everett, John K, additional, Amses, Kevin, additional, Sherrill-Mix, Scott, additional, Chandra, Aditi, additional, Goldman, Naomi, additional, Vahedi, Golnaz, additional, Jadlowsky, Julie K, additional, Young, Regina M, additional, Melenhorst, Jan Joseph, additional, Maude, Shannon L, additional, Levine, Bruce L, additional, Frey, Noelle V, additional, Berger, Shelley L, additional, Grupp, Stephan A, additional, Porter, David L, additional, Herbst, Friederike, additional, Porteus, Matthew H, additional, Bushman, Frederic D, additional, Weber, Evan W, additional, Wherry, E. John, additional, Jordan, Martha S, additional, and Fraietta, Joseph A, additional

Published

2024

11. SARS-CoV-2 evolution during prolonged infection in immunocompromised patients

Author

Marques, Andrew D., primary, Graham-Wooten, Jevon, additional, Fitzgerald, Ayannah S., additional, Sobel Leonard, Ashley, additional, Cook, Emma J., additional, Everett, John K., additional, Rodino, Kyle G., additional, Moncla, Louise H., additional, Kelly, Brendan J., additional, Collman, Ronald G., additional, and Bushman, Frederic D., additional

Published

2024

12. INSPIIRED: A Pipeline for Quantitative Analysis of Sites of New DNA Integration in Cellular Genomes

Author

Sherman, Eric, Nobles, Christopher, Berry, Charles C, Six, Emmanuelle, Wu, Yinghua, Dryga, Anatoly, Malani, Nirav, Male, Frances, Reddy, Shantan, Bailey, Aubrey, Bittinger, Kyle, Everett, John K, Caccavelli, Laure, Drake, Mary J, Bates, Paul, Hacein-Bey-Abina, Salima, Cavazzana, Marina, and Bushman, Frederic D

Subjects

Human Genome, Networking and Information Technology R&D (NITRD), Bioengineering, Genetics, Biotechnology, Generic health relevance, SCID-X1, gammaretrovirus, gene therapy, insertional mutagenesis, lentivirus, mutagenesis, recombination, retrovirus, vector, vector driving

Abstract

Integration of new DNA into cellular genomes mediates replication of retroviruses and transposons; integration reactions have also been adapted for use in human gene therapy. Tracking the distributions of integration sites is important to characterize populations of transduced cells and to monitor potential outgrow of pathogenic cell clones. Here, we describe a pipeline for quantitative analysis of integration site distributions named INSPIIRED (integration site pipeline for paired-end reads). We describe optimized biochemical steps for site isolation using Illumina paired-end sequencing, including new technology for suppressing recovery of unwanted contaminants, then software for alignment, quality control, and management of integration site sequences. During library preparation, DNAs are broken by sonication, so that after ligation-mediated PCR the number of ligation junction sites can be used to infer abundance of gene-modified cells. We generated integration sites of known positions in silico, and we describe optimization of sample processing parameters refined by comparison to truth. We also present a novel graph-theory-based method for quantifying integration sites in repeated sequences, and we characterize the consequences using synthetic and experimental data. In an accompanying paper, we describe an additional set of statistical tools for data analysis and visualization. Software is available at https://github.com/BushmanLab/INSPIIRED.

Published

2017

13. INSPIIRED: Quantification and Visualization Tools for Analyzing Integration Site Distributions

Author

Berry, Charles C, Nobles, Christopher, Six, Emmanuelle, Wu, Yinghua, Malani, Nirav, Sherman, Eric, Dryga, Anatoly, Everett, John K, Male, Frances, Bailey, Aubrey, Bittinger, Kyle, Drake, Mary J, Caccavelli, Laure, Bates, Paul, Hacein-Bey-Abina, Salima, Cavazzana, Marina, and Bushman, Frederic D

Subjects

Biotechnology, Networking and Information Technology R&D (NITRD), Human Genome, Genetics, Bioengineering, Cancer, SCID-X1, data visualization, gammaretrovirus, gene therapy, insertional mutagenesis, lentivirus, mutagenesis, recombination, retrovirus, vector, vector driving

Abstract

Analysis of sites of newly integrated DNA in cellular genomes is important to several fields, but methods for analyzing and visualizing these datasets are still under development. Here, we describe tools for data analysis and visualization that take as input integration site data from our INSPIIRED pipeline. Paired-end sequencing allows inference of the numbers of transduced cells as well as the distributions of integration sites in target genomes. We present interactive heatmaps that allow comparison of distributions of integration sites to genomic features and that support numerous user-defined statistical tests. To summarize integration site data from human gene therapy samples, we developed a reproducible report format that catalogs sample population structure, longitudinal dynamics, and integration frequency near cancer-associated genes. We also introduce a novel summary statistic, the UC50 (unique cell progenitors contributing the most expanded 50% of progeny cell clones), which provides a single number summarizing possible clonal expansion. Using these tools, we characterize ongoing longitudinal characterization of a patient from the first trial to treat severe combined immunodeficiency-X1 (SCID-X1), showing successful reconstitution for 15 years accompanied by persistence of a cell clone with an integration site near the cancer-associated gene CCND2. Software is available at https://github.com/BushmanLab/INSPIIRED.

Published

2017

14. A long-term study of AAV gene therapy in dogs with hemophilia A identifies clonal expansions of transduced liver cells

Author

Nguyen, Giang N., Everett, John K., Kafle, Samita, Roche, Aoife M., Raymond, Hayley E., Leiby, Jacob, Wood, Christian, Assenmacher, Charles-Antoine, Merricks, Elizabeth P., Long, C. Tyler, Kazazian, Haig H., Nichols, Timothy C., Bushman, Frederic D., and Sabatino, Denise E.

Published

2021

15. CD19-targeting CAR T cell immunotherapy outcomes correlate with genomic modification by vector integration

Author

Nobles, Christopher L., Sherrill-Mix, Scott, Everett, John K., Reddy, Shantan, Fraietta, Joseph A., Porter, David L., Frey, Noelle, Gill, Saar I., Grupp, Stephan A., Maude, Shannon L., Siegel, Donald L., Levine, Bruce L., June, Carl H., Lacey, Simon F., Melenhorst, J. Joseph, and Bushman, Frederic D.

Subjects

Genes, Chromatin, Immunotherapy, Genomes, Genomics, T cells, Lymphocytic leukemia, Antigens, Chronic lymphocytic leukemia, Acute lymphocytic leukemia, Pediatrics, Health care industry

Abstract

Chimeric antigen receptor-engineered T cells targeting CD19 (CART19) provide an effective treatment for pediatric acute lymphoblastic leukemia but are less effective for chronic lymphocytic leukemia (CLL), focusing attention on improving efficacy. CART19 harbor an engineered receptor, which is delivered through lentiviral vector integration, thereby marking cell lineages and modifying the cellular genome by insertional mutagenesis. We recently reported that vector integration within the host TET2 gene was associated with CLL remission. Here, we investigated clonal population structure and therapeutic outcomes in another 39 patients by high-throughput sequencing of vector-integration sites. Genes at integration sites enriched in responders were commonly found in cell-signaling and chromatin modification pathways, suggesting that insertional mutagenesis in these genes promoted therapeutic T cell proliferation. We also developed a multivariate model based on integration-site distributions and found that data from preinfusion products forecasted response in CLL successfully in discovery and validation cohorts and, in day 28 samples, reported responders to CLL therapy with high accuracy. These data clarify how insertional mutagenesis can modulate cell proliferation in CART19 therapy and how data on integration- site distributions can be linked to treatment outcomes., Introduction Patient T cells engineered to express a CD19-specific chimeric antigen receptor (CART19) have proven effective in inducing long-term remissions in pediatric acute lymphoblastic leukemia (ALL), with complete response rates [...]

Published

2020

16. Chemotherapy-induced reversal of ciltacabtagene autoleucel-associated movement and neurocognitive toxicity

Author

Graham, Charlotte E, primary, Lee, Won-Ho, additional, Wiggin, Hadley R, additional, Supper, Valentina M, additional, Leick, Mark B, additional, Birocchi, Filippo, additional, Yee, Andrew J., additional, Petrichenko, Angelina, additional, Everett, John K, additional, Bushman, Frederic D., additional, Sadrzadeh, Hossein, additional, Rapalino, Otto, additional, Chiu, Daniel, additional, Arrillaga-Romany, Isabel C, additional, Maus, Marcela V, additional, Frigault, Matthew J, additional, and Gallagher, Kathleen M E, additional

Published

2023

17. Figure S8 from Type I Interferon Signaling via the EGR2 Transcriptional Regulator Potentiates CAR T Cell–Intrinsic Dysfunction

Author

Jung, In-Young, primary, Bartoszek, Robert L., primary, Rech, Andrew J., primary, Collins, Sierra M., primary, Ooi, Soon-Keat, primary, Williams, Erik F., primary, Hopkins, Caitlin R., primary, Narayan, Vivek, primary, Haas, Naomi B., primary, Frey, Noelle V., primary, Hexner, Elizabeth O., primary, Siegel, Donald L., primary, Plesa, Gabriela, primary, Porter, David L., primary, Cantu, Adrian, primary, Everett, John K., primary, Guedan, Sonia, primary, Berger, Shelley L., primary, Bushman, Frederic D., primary, Herbst, Friederike, primary, and Fraietta, Joseph A., primary

Published

2023

18. Data from Type I Interferon Signaling via the EGR2 Transcriptional Regulator Potentiates CAR T Cell–Intrinsic Dysfunction

Author

Jung, In-Young, primary, Bartoszek, Robert L., primary, Rech, Andrew J., primary, Collins, Sierra M., primary, Ooi, Soon-Keat, primary, Williams, Erik F., primary, Hopkins, Caitlin R., primary, Narayan, Vivek, primary, Haas, Naomi B., primary, Frey, Noelle V., primary, Hexner, Elizabeth O., primary, Siegel, Donald L., primary, Plesa, Gabriela, primary, Porter, David L., primary, Cantu, Adrian, primary, Everett, John K., primary, Guedan, Sonia, primary, Berger, Shelley L., primary, Bushman, Frederic D., primary, Herbst, Friederike, primary, and Fraietta, Joseph A., primary

Published

2023

19. Table S2 from Type I Interferon Signaling via the EGR2 Transcriptional Regulator Potentiates CAR T Cell–Intrinsic Dysfunction

Author

Jung, In-Young, primary, Bartoszek, Robert L., primary, Rech, Andrew J., primary, Collins, Sierra M., primary, Ooi, Soon-Keat, primary, Williams, Erik F., primary, Hopkins, Caitlin R., primary, Narayan, Vivek, primary, Haas, Naomi B., primary, Frey, Noelle V., primary, Hexner, Elizabeth O., primary, Siegel, Donald L., primary, Plesa, Gabriela, primary, Porter, David L., primary, Cantu, Adrian, primary, Everett, John K., primary, Guedan, Sonia, primary, Berger, Shelley L., primary, Bushman, Frederic D., primary, Herbst, Friederike, primary, and Fraietta, Joseph A., primary

Published

2023

20. Structural genomics is the largest contributor of novel structural leverage

Author

Nair, Rajesh, Liu, Jinfeng, Soong, Ta-Tsen, Acton, Thomas B, Everett, John K, Kouranov, Andrei, Fiser, Andras, Godzik, Adam, Jaroszewski, Lukasz, Orengo, Christine, Montelione, Gaetano T, and Rost, Burkhard

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Biotechnology, Human Genome, Computational Biology, Databases, Protein, Genomics, Nuclear Magnetic Resonance, Biomolecular, Protein Conformation, Proteins, Proteomics, Environmental Sciences, Information and Computing Sciences, Biophysics, Biological sciences, Environmental sciences

Abstract

The Protein Structural Initiative (PSI) at the US National Institutes of Health (NIH) is funding four large-scale centers for structural genomics (SG). These centers systematically target many large families without structural coverage, as well as very large families with inadequate structural coverage. Here, we report a few simple metrics that demonstrate how successfully these efforts optimize structural coverage: while the PSI-2 (2005-now) contributed more than 8% of all structures deposited into the PDB, it contributed over 20% of all novel structures (i.e. structures for protein sequences with no structural representative in the PDB on the date of deposition). The structural coverage of the protein universe represented by today's UniProt (v12.8) has increased linearly from 1992 to 2008; structural genomics has contributed significantly to the maintenance of this growth rate. Success in increasing novel leverage (defined in Liu et al. in Nat Biotechnol 25:849-851, 2007) has resulted from systematic targeting of large families. PSI's per structure contribution to novel leverage was over 4-fold higher than that for non-PSI structural biology efforts during the past 8 years. If the success of the PSI continues, it may just take another approximately15 years to cover most sequences in the current UniProt database.

Published

2009

21. An ELISA-Based Screening Platform for Ligand–Receptor Discovery

Author

Ozgul, Sinem, primary, von Daake, Sventja, additional, Kakehi, Sumie, additional, Sereni, Davide, additional, Denissova, Natalia, additional, Hanlon, Carlie, additional, Huang, Yuanpeng Janet, additional, Everett, John K., additional, Yin, Cuifeng, additional, Montelione, Gaetano T., additional, and Comoletti, Davide, additional

Published

2019

22. BET bromodomain protein inhibition reverses chimeric antigen receptor extinction and reinvigorates exhausted T cells in chronic lymphocytic leukemia

Author

Kong, Weimin, Dimitri, Alexander, Wang, Wenliang, Jung, In-Young, Ott, Christopher J., Fasolino, Maria, Wang, Yan, Kulikovskaya, Irina, Gupta, Minnal, Yoder, Todd, DeNizio, Jamie E., Everett, John K., Williams, Erik F., Xu, Jun, Scholler, John, Reich, Tyler J., Bhoj, Vijay G., Haines, Kathleen M., Maus, Marcela V., Melenhorst, J. Joseph, Young, Regina M., Jadlowsky, Julie K., Marcucci, Katherine T., Bradner, James E., Levine, Bruce L., Porter, David L., Bushman, Frederic D., Kohli, Rahul M., June, Carl H., Davis, Megan M., Lacey, Simon F., Vahedi, Golnaz, and Fraietta, Joseph A.

Subjects

T cells -- Receptors, Polypeptides -- Health aspects, Antigen receptors, T cell -- Genetic aspects -- Health aspects, Cellular therapy -- Methods, Immunotherapy -- Methods, Chronic lymphocytic leukemia -- Care and treatment, Health care industry

Abstract

Chimeric antigen receptor (CAR) T cells have induced remarkable antitumor responses in B cell malignancies. Some patients do not respond because of T cell deficiencies that hamper the expansion, persistence, and effector function of these cells. We used longitudinal immune profiling to identify phenotypic and pharmacodynamic changes in CD19-directed CAR T cells in patients with chronic lymphocytic leukemia (CLL). CAR expression maintenance was also investigated because this can affect response durability. CAR T cell failure was accompanied by preexisting T cell-intrinsic defects or dysfunction acquired after infusion. In a small subset of patients, CAR silencing was observed coincident with leukemia relapse. Using a small molecule inhibitor, we demonstrated that the bromodomain and extra-terminal (BET) family of chromatin adapters plays a role in downregulating CAR expression. BET protein blockade also ameliorated CAR T cell exhaustion as manifested by inhibitory receptor reduction, enhanced metabolic fitness, increased proliferative capacity, and enriched transcriptomic signatures of T cell reinvigoration. BET inhibition decreased levels of the TET2 methylcytosine dioxygenase, and forced expression of the TET2 catalytic domain eliminated the potency-enhancing effects of BET protein targeting in CAR T cells, providing a mechanism linking BET proteins and T cell dysfunction. Thus, modulating BET epigenetic readers may improve the efficacy of cell-based immunotherapies., Introduction The adoptive transfer of autologous CD19-targeted chimeric antigen receptor (CAR) T cells has shown remarkable activity in patients with B cell malignancies (1-3). Upon treatment with a CAR signaling [...]

Published

2021

23. Disruption of TET2 promotes the therapeutic efficacy of CD19-targeted T cells

Author

Fraietta, Joseph A., Nobles, Christopher L., Sammons, Morgan A., Lundh, Stefan, Carty, Shannon A., Reich, Tyler J., Cogdill, Alexandria P., Morrissette, Jennifer J. D., DeNizio, Jamie E., Reddy, Shantan, Hwang, Young, Gohil, Mercy, Kulikovskaya, Irina, Nazimuddin, Farzana, Gupta, Minnal, Chen, Fang, Everett, John K., Alexander, Katherine A., Lin-Shiao, Enrique, Gee, Marvin H., Liu, Xiaojun, Young, Regina M., Ambrose, David, Wang, Yan, Xu, Jun, Jordan, Martha S., Marcucci, Katherine T., Levine, Bruce L., Garcia, K. Christopher, Zhao, Yangbing, Kalos, Michael, Porter, David L., Kohli, Rahul M., Lacey, Simon F., Berger, Shelley L., Bushman, Frederic D., June, Carl H., and Melenhorst, J. Joseph

Published

2018

24. The HIV-1 Capsid-Targeted Inhibitor GSK878 Alters Selection of Target Sites for HIV DNA Integration

Author

Marquis, Kaitlin A, primary, Everett, John K, additional, Cantu, Vito Adrian, additional, McFarland, Alexander G, additional, Sherrill-Mix, Scott, additional, Krystal, Mark R, additional, Parcella, Kyle E, additional, Gillis, Eric P, additional, Fridell, Robert A, additional, and Bushman, Frederic, additional

Published

2023

25. Type I Interferon Signaling via the EGR2 Transcriptional Regulator Potentiates CAR T Cell–Intrinsic Dysfunction

Author

Jung, In-Young, primary, Bartoszek, Robert L., additional, Rech, Andrew J., additional, Collins, Sierra M., additional, Ooi, Soon-Keat, additional, Williams, Erik F., additional, Hopkins, Caitlin R., additional, Narayan, Vivek, additional, Haas, Naomi B., additional, Frey, Noelle V., additional, Hexner, Elizabeth O., additional, Siegel, Donald L., additional, Plesa, Gabriela, additional, Porter, David L., additional, Cantu, Adrian, additional, Everett, John K., additional, Guedan, Sonia, additional, Berger, Shelley L., additional, Bushman, Frederic D., additional, Herbst, Friederike, additional, and Fraietta, Joseph A., additional

Published

2023

26. Supplementary Data from NPM–ALK-Induced Reprogramming of Mature TCR-Stimulated T Cells Results in Dedifferentiation and Malignant Transformation

Author

Pawlicki, Jan M., primary, Cookmeyer, David L., primary, Maseda, Damian, primary, Everett, John K., primary, Wei, Fang, primary, Kong, Hong, primary, Zhang, Qian, primary, Wang, Hong Y., primary, Tobias, John W., primary, Walter, David M., primary, Zullo, Kelly M., primary, Javaid, Sarah, primary, Watkins, Amanda, primary, Wasik, Mariusz A., primary, Bushman, Frederic D., primary, and Riley, James L., primary

Published

2023

27. Data from NPM–ALK-Induced Reprogramming of Mature TCR-Stimulated T Cells Results in Dedifferentiation and Malignant Transformation

Author

Pawlicki, Jan M., primary, Cookmeyer, David L., primary, Maseda, Damian, primary, Everett, John K., primary, Wei, Fang, primary, Kong, Hong, primary, Zhang, Qian, primary, Wang, Hong Y., primary, Tobias, John W., primary, Walter, David M., primary, Zullo, Kelly M., primary, Javaid, Sarah, primary, Watkins, Amanda, primary, Wasik, Mariusz A., primary, Bushman, Frederic D., primary, and Riley, James L., primary

Published

2023

28. Novel extragenic genomic safe harbors for precise therapeutic T cell engineering

Author

Odak, Ashlesha, primary, Yuan, Han, additional, Feucht, Judith, additional, Cantu, Vito Adrian, additional, Mansilla-Soto, Jorge, additional, Kogel, Friederike, additional, Eyquem, Justin, additional, Everett, John K, additional, Bushman, Frederic D., additional, Leslie, Christina, additional, and Sadelain, Michel, additional

Published

2023

29. Long-Term Outcome of Gene Therapy for X-Linked Severe Combined Immunodeficiency (SCID-X1) Using an Enhancer-Deleted Self-Inactivating Gammaretroviral Vector

Author

Pai, Sung-Yun, primary, Nagarsheth, Nisha, additional, Prockop, Susan, additional, Armant, Myriam, additional, Kohn, Donald B., additional, Marsh, Rebecca A., additional, Booth, Claire, additional, Everett, John K., additional, Bleesing, Jack, additional, Chellapandian, Deepak, additional, Dansereau, Colleen, additional, de Oliveira, Satiro, additional, London, Wendy B., additional, Marinovic, M. Angélica, additional, Moore, Theodore B., additional, Oleastro, Matias, additional, O'Toole, Grainne, additional, Vander Lugt, Mark, additional, Urdinez, Luciano, additional, Walkovich, Kelly J., additional, Walter, Jolan E., additional, Schambach, Axel, additional, Thrasher, Adrian J., additional, Bushman, Frederic D., additional, and Williams, David A, additional

Published

2022

30. Multiple Introductions of SARS-CoV-2 Alpha and Delta Variants into White-Tailed Deer in Pennsylvania

Author

Marques, Andrew D., primary, Sherrill-Mix, Scott, additional, Everett, John K., additional, Adhikari, Hriju, additional, Reddy, Shantan, additional, Ellis, Julie C., additional, Zeliff, Haley, additional, Greening, Sabrina S., additional, Cannuscio, Carolyn C., additional, Strelau, Katherine M., additional, Collman, Ronald G., additional, Kelly, Brendan J., additional, Rodino, Kyle G., additional, Bushman, Frederic D., additional, Gagne, Roderick B., additional, and Anis, Eman, additional

Published

2022

31. Codon influence on protein expression in E. coli correlates with mRNA levels

Author

Boel, Gregory, Letso, Reka, Neely, Helen, Price, W. Nicholson, Wong, Kam-Ho, Su, Min, Luff, Jon D., Valecha, Mayank, Everett, John K., Acton, Thomas B., Xiao, Rong, Montelione, Gaetano T., Aalberts, Daniel P., and Hunt, John F.

Subjects

Messenger RNA -- Research, Codon -- Research, Proteins -- Genetic aspects, Microbiological research, Escherichia coli -- Genetic aspects, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Degeneracy in the genetic code, which enables a single protein to be encoded by a multitude of synonymous gene sequences, has an important role in regulating protein expression, but substantial uncertainty exists concerning the details of this phenomenon. Here we analyse the sequence features influencing protein expression levels in 6,348 experiments using bacteriophage T7 polymerase to synthesize messenger RNA in Escherichia coli. Logistic regression yields a new codon-influence metric that correlates only weakly with genomic codon-usage frequency, but strongly with global physiological protein concentrations and also mRNA concentrations and lifetimes in vivo. Overall, the codon content influences protein expression more strongly than mRNA-folding parameters, although the latter dominate in the initial ~16 codons. Genes redesigned based on our analyses are transcribed with unaltered efficiency but translated with higher efficiency in vitro. The less efficiently translated native sequences show greatly reduced mRNA levels in vivo. Our results suggest that codon content modulates a kinetic competition between protein elongation and mRNA degradation that is a central feature of the physiology and also possibly the regulation of translation in E. coli., Degenerate encoding of 20 amino acids by 61 triplet nucleotide codons enables the same protein sequence to be synthesized by a vast number of synonymous mRNAs. While variations between synonymous [...]

Published

2016

32. Polypeptide backbone, Cβ and methyl group resonance assignments of the 24 kDa plectin repeat domain 6 from human protein plectin

Author

Pulavarti, Surya V. S. R. K., Eletsky, Alexander, Huang, Yuanpeng J., Acton, Thomas B., Xiao, Rong, Everett, John K., Montelione, Gaetano T., and Szyperski, Thomas

Published

2015

33. Solution NMR structures of homeodomains from human proteins ALX4, ZHX1, and CASP8AP2 contribute to the structural coverage of the Human Cancer Protein Interaction Network

Author

Xu, Xianzhong, Pulavarti, Surya V. S. R. K., Eletsky, Alexander, Huang, Yuanpeng Janet, Acton, Thomas B., Xiao, Rong, Everett, John K., Montelione, Gaetano T., and Szyperski, Thomas

Published

2014

34. Solution NMR structures of immunoglobulin-like domains 7 and 12 from obscurin-like protein 1 contribute to the structural coverage of the human cancer protein interaction network

Author

Pulavarti, Surya V. S. R. K., Huang, Yuanpeng J., Pederson, Kari, Acton, Thomas B., Xiao, Rong, Everett, John K., Prestegard, James H., Montelione, Gaetano T., and Szyperski, Thomas

Published

2014

35. A phase 1 trial of lentiviral globin gene therapy with reduced intensity conditioning in adults with transfusion dependent β-thalassemia

Author

Boulad, Farid, Maggio, Aurelio, Wang, Xiuyan, Moi, Paolo, Acuto, Santina, Kogel, Friederike, Takpradit, Chayamon, Prockop, Susan, Mansilla-Soto, Jorge, Cabriolu, Annalisa, Odak, Ashlesha, Qu, Jinrong, Thummar, Keyur, Du, Fang, Shen, Lingbo, Raso, Simona, Barone, Rita, Di Maggio, Rosario, Pitrolo, Lorella, Giambona, Antonino, Mingoia, Maura, Everett, John K., Hokama, Pascha, Roche, Aoife M., Cantu, Vito Adrian, Adhikari, Hriju, Reddy, Shantan, Bouhassira, Eric, Mohandas, Narla, Bushman, Frederic D., Rivière, Isabelle, and Sadelain, Michel

Subjects

Adult, Male, Transplantation Conditioning, Adolescent, Genetic Vectors, Lentivirus, beta-Thalassemia, Antigens, CD34, Genetic Therapy, Article, Globins, Young Adult, Transduction, Genetic, Humans, Blood Transfusion, Female

Abstract

The β-thalassemias are inherited anemias that are caused by the absent or insufficient production of the ß chain of hemoglobin. We report 6–8 year follow-up of four adult patients with transfusion-dependent β-thalassemia who were infused with autologous CD34+ cells transduced with the TNS9.3.55 lentiviral globin vector after reduced-intensity conditioning (RIC) in a phase I clinical trial (NCT01639690). Patients were monitored for insertional mutagenesis and the generation of a replication-competent lentivirus (RCL) (safety and tolerability of the infusion product following RIC; primary endpoint) and engraftment of the genetically modified autologous CD34+ cells, the expression of the transduced β-globin gene, and the post-transplant transfusions requirements (efficacy, secondary endpoint). No unexpected safety issues occurred during conditioning and cell product infusion. Hematopoietic gene marking was very stable but low, reducing transfusion requirements in two patients albeit not achieving transfusion independence. Our findings suggest that non-myeloablative conditioning can achieve durable stem cell engraftment but underscore a minimum CD34+ cell transduction requirement for effective therapy. Moderate clonal expansions were associated with integrations near cancer-related genes, suggestive of non-erythroid activity of globin vectors in stem/progenitor cells. These correlative findings highlight the necessity to cautiously monitor patients harboring globin vectors.

Published

2022

36. SARS-CoV-2 Variants Associated with Vaccine Breakthrough in the Delaware Valley through Summer 2021

Author

Marques, Andrew D., primary, Sherrill-Mix, Scott, additional, Everett, John K., additional, Reddy, Shantan, additional, Hokama, Pascha, additional, Roche, Aoife M., additional, Hwang, Young, additional, Glascock, Abigail, additional, Whiteside, Samantha A., additional, Graham-Wooten, Jevon, additional, Khatib, Layla A., additional, Fitzgerald, Ayannah S., additional, Moustafa, Ahmed M., additional, Bianco, Colleen, additional, Rajagopal, Swetha, additional, Helton, Jenna, additional, Deming, Regan, additional, Denu, Lidiya, additional, Ahmed, Azad, additional, Kitt, Eimear, additional, Coffin, Susan E., additional, Newbern, Claire, additional, Mell, Josh Chang, additional, Planet, Paul J., additional, Badjatia, Nitika, additional, Richards, Bonnie, additional, Wang, Zi-Xuan, additional, Cannuscio, Carolyn C., additional, Strelau, Katherine M., additional, Jaskowiak-Barr, Anne, additional, Cressman, Leigh, additional, Loughrey, Sean, additional, Ganguly, Arupa, additional, Feldman, Michael D., additional, Collman, Ronald G., additional, Rodino, Kyle G., additional, Kelly, Brendan J., additional, and Bushman, Frederic D., additional

Published

2022

37. Solution structure of a C-terminal fragment (175–257) of CV_0373 protein from Chromobacterium violaceum adopts a winged helix-turn-helix (wHTH) fold

Author

Yang, Yunhuang, Ramelot, Theresa A., Lee, Hsiau-Wei, Xiao, Rong, Everett, John K., Montelione, Gaetano T., Prestegard, James H., and Kennedy, Michael A.

Published

2014

38. Solution structure of the free Zα domain of human DLM-1 (ZBP1/DAI), a Z-DNA binding domain

Author

Yang, Yunhuang, Ramelot, Theresa A., Lee, Hsiau-Wei, Xiao, Rong, Everett, John K., Montelione, Gaetano T., Prestegard, James H., and Kennedy, Michael A.

Published

2014

39. Introduction of a polar core into the de novo designed protein Top7

Author

Basanta, Benjamin, Chan, Kui K., Barth, Patrick, King, Tiffany, Sosnick, Tobin R., Hinshaw, James R., Liu, Gaohua, Everett, John K., Xiao, Rong, Montelione, Gaetano T., and Baker, David

Published

2016

40. A community resource of experimental data for NMR / X-ray crystal structure pairs

Author

Everett, John K., Tejero, Roberto, Murthy, Sarath B. K., Acton, Thomas B., Aramini, James M., Baran, Michael C., Benach, Jordi, Cort, John R., Eletsky, Alexander, Forouhar, Farhad, Guan, Rongjin, Kuzin, Alexandre P., Lee, Hsiau-Wei, Liu, Gaohua, Mani, Rajeswari, Mao, Binchen, Mills, Jeffrey L., Montelione, Alexander F., Pederson, Kari, Powers, Robert, Ramelot, Theresa, Rossi, Paolo, Seetharaman, Jayaraman, Snyder, David, Swapna, G. V. T., Vorobiev, Sergey M., Wu, Yibing, Xiao, Rong, Yang, Yunhuang, Arrowsmith, Cheryl H., Hunt, John F., Kennedy, Michael A., Prestegard, James H., Szyperski, Thomas, Tong, Liang, and Montelione, Gaetano T.

Published

2016

41. Solution NMR structure of CD1104B from pathogenic Clostridium difficile reveals a distinct α-helical architecture and provides first structural representative of protein domain family PF14203

Author

Pulavarti, Surya V. S. R. K., Eletsky, Alexander, Lee, Hsiau-Wei, Acton, Thomas B., Xiao, Rong, Everett, John K., Prestegard, James H., Montelione, Gaetano T., and Szyperski, Thomas

Published

2013

42. Long-Term Follow-up Study after Lentiviral Hematopoietic Stem/Progenitor Cell Gene Therapy for Wiskott - Aldrich Syndrome

Author

Magnani, Alessandra, primary, Semeraro, Michaela, additional, ADAM, Frédéric, additional, Booth, Claire, additional, Dupre, Loic, additional, Morris, Emma C, additional, Gabrion, Aurélie, additional, Roudaut, Cecile, additional, Borgel, Delphine, additional, Toubert, Antoine, additional, Clave, Emmanuel, additional, Abdo, Chrystelle, additional, Gorochov, Guy, additional, Petermann, Rachel, additional, Guiot, Mélanie, additional, Miyara, Makoto, additional, Moshous, Despina, additional, Magrin, Elisa, additional, Denis, Adeline, additional, Suarez, Felipe, additional, Lagresle-Peyrou, Chantal, additional, Doto, Aoife, additional, Everett, John K., additional, Trinquand, Amélie, additional, Guisset, Marianne, additional, Xu-Bayford, Jin Hua, additional, Hacein-Bey-Abina, Salima, additional, Kauskot, Alexandre, additional, Elfeky, Reem, additional, Rivat, Christine, additional, Abbas, Sarah, additional, Gaspar, Bobby H, additional, Macintyre, Elizabeth A., additional, Picard, Capucine, additional, Bushman, Frederic D., additional, Galy, Anne, additional, Fischer, Alain, additional, Six, Emmanuelle, additional, Thrasher, Adrian J., additional, and Cavazzana, Marina, additional

Published

2021

43. SARS-CoV-2 variants associated with vaccine breakthrough in the Delaware Valley through summer 2021

Author

Marques, Andrew, primary, Sherrill-Mix, Scott, additional, Everett, John K, additional, Reddy, Shantan, additional, Hokama, Pascha, additional, Roche, Aoife M, additional, Hwang, Young, additional, Glascock, Abigail, additional, Whiteside, Samantha A, additional, Graham-Wooten, Jevon, additional, Khatib, Layla A, additional, Fitzgerald, Ayannah S, additional, Moustafa, Ahmed, additional, Bianco, Colleen, additional, Rajagopal, Swetha, additional, Helton, Jenna, additional, Deming, Regan, additional, Denu, Lidiya, additional, Azad, Ahmed, additional, Kitt, Eimear, additional, Coffin, Susan, additional, Newbern, Claire, additional, Mell, Josh C, additional, Planet, Paul J, additional, Badjatia, Nitika, additional, Wang, Zi-Xuan, additional, Cannuscio, Carolyn C, additional, Strelau, Katherine, additional, Jaskowiak-Barr, Anne, additional, Cressman, Leigh, additional, Loughrey, Sean, additional, Ganguly, Arupa, additional, Feldman, Michael D, additional, Collman, Ronald G, additional, Rodino, Kyle G, additional, Kelly, Brendan J, additional, and Bushman, Frederic D, additional

Published

2021

44. Solution NMR structures provide first structural coverage of the large protein domain family PF08369 and complementary structural coverage of dark operative protochlorophyllide oxidoreductase complexes

Author

Pulavarti, Surya V. S. R. K., He, Yunfen, Feldmann, Erik A., Eletsky, Alexander, Acton, Thomas B., Xiao, Rong, Everett, John K., Montelione, Gaetano T., Kennedy, Michael A., and Szyperski, Thomas

Published

2013

45. Solution NMR structure of the helicase associated domain BVU_0683(627–691) from Bacteroides vulgatus provides first structural coverage for protein domain family PF03457 and indicates domain binding to DNA

Author

Mills, Jeffrey L., Acton, Thomas B., Xiao, Rong, Everett, John K., Montelione, Gaetano T., and Szyperski, Thomas

Published

2013

46. Solution NMR structure of Alr2454 from Nostoc sp. PCC 7120, the first structural representative of Pfam domain family PF11267

Author

Aramini, James M., Petrey, Donald, Lee, Dong Yup, Janjua, Haleema, Xiao, Rong, Acton, Thomas B., Everett, John K., and Montelione, Gaetano T.

Published

2012

47. Solution NMR and X-ray crystal structures of Pseudomonas syringae Pspto_3016 from protein domain family PF04237 (DUF419) adopt a “double wing” DNA binding motif

Author

Feldmann, Erik A., Seetharaman, Jayaraman, Ramelot, Theresa A., Lew, Scott, Zhao, Li, Hamilton, Keith, Ciccosanti, Colleen, Xiao, Rong, Acton, Thomas B., Everett, John K., Tong, Liang, Montelione, Gaetano T., and Kennedy, Michael A.

Published

2012

48. Solution NMR structures reveal unique homodimer formation by a winged helix-turn-helix motif and provide first structures for protein domain family PF10771

Author

Eletsky, Alexander, Petrey, Donald, Zhang, Qiangfeng Cliff, Lee, Hsiau-Wei, Acton, Thomas B., Xiao, Rong, Everett, John K., Prestegard, James H., Honig, Barry, Montelione, Gaetano T., and Szyperski, Thomas

Published

2012

49. Solution NMR structures reveal a distinct architecture and provide first structures for protein domain family PF04536

Author

Eletsky, Alexander, Acton, Thomas B., Xiao, Rong, Everett, John K., Montelione, Gaetano T., and Szyperski, Thomas

Published

2012

50. Solution NMR structure of Dsy0195 homodimer from Desulfitobacterium hafniense: first structure representative of the YabP domain family of proteins involved in spore coat assembly

Author

Yang, Yunhuang, Ramelot, Theresa A., Cort, John R., Wang, Huang, Ciccosanti, Colleen, Jiang, Mei, Janjua, Haleema, Acton, Thomas B., Xiao, Rong, Everett, John K., Montelione, Gaetano T., and Kennedy, Michael A.

Published

2011