Your search keyword '"Andrew Berical"' showing total 14 results

1. Rationale and Design of the Awake Prone Position for Early Hypoxemia in COVID-19 Study Protocol: A Clinical Trial

Author

Garrett L Rampon, Justin M Rucci, Andrew Berical, Katherine L. Modzelewski, Steven Q. Simpson, Kari R. Gillmeyer, Nikhil Jagan, James Hudspeth, Craig S. Ross, Nicholas A Bosch, Shijing Jia, Elissa M. Schechter-Perkins, Michael H. Ieong, Gheorghe Doros, Allan J. Walkey, and Michael A Garcia

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, Randomization, Bayesian analysis, Staffing, MEDLINE, 03 medical and health sciences, 0302 clinical medicine, Humans, Multicenter Studies as Topic, Medicine, Prospective Studies, 030212 general & internal medicine, Wakefulness, Hypoxia, Intensive care medicine, Personal protective equipment, Randomized Controlled Trials as Topic, Clinical Study Design, Protocol (science), SARS-CoV-2, business.industry, COVID-19, Bayes Theorem, Advanced life support, Clinical trial, Prone position, Treatment Outcome, 030228 respiratory system, prone position, business

Abstract

The unprecedented public health burdens of coronavirus disease 2019 (COVID-19) have intensified the urgency to identify effective, low-cost treatments that limit the need for advanced life support measures and improve clinical outcomes. However, personal protective equipment and staffing shortages, disease virulence, and infectivity have created significant barriers to traditional clinical trial practices. We present the novel design of a pragmatic, adaptive, multicenter, international, prospective randomized controlled clinical trial evaluating the safety and effectiveness of awake prone positioning in spontaneously breathing patients with COVID-19 (Awake Prone Positioning for Early Hypoxemia in COVID-19 [APPEX-19]). Key innovations of this trial include: 1) a novel smartphone-based communication process that facilitates rapid enrollment and intervention delivery while allowing social distancing and conservation of personal protective equipment; 2) a Bayesian response-adaptive randomization to allow preferential assignment to the most effective intervention and expedite trial completion compared with frequentist designs; 3) remote electronic collection of patient-reported outcomes and electronic medical record data; and 4) pragmatic prospective utilization of patient-reported data and data collected as part of routine clinical care. Clinical trial registered with www.clinicaltrials.gov (NCT04344587).

Published

2021

2. A multimodal iPSC platform for cystic fibrosis drug testing

Author

Andrew Berical, Rhianna E. Lee, Junjie Lu, Mary Lou Beermann, Jake A. Le Suer, Aditya Mithal, Dylan Thomas, Nicole Ranallo, Megan Peasley, Alex Stuffer, Katherine Bukis, Rebecca Seymour, Jan Harrington, Kevin Coote, Hillary Valley, Killian Hurley, Paul McNally, Gustavo Mostoslavsky, John Mahoney, Scott H. Randell, and Finn J. Hawkins

Subjects

Ion Transport, Multidisciplinary, Cystic Fibrosis, Induced Pluripotent Stem Cells, Animals, Cystic Fibrosis Transmembrane Conductance Regulator, Humans, General Physics and Astronomy, Epithelial Cells, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

Cystic fibrosis is a monogenic lung disease caused by dysfunction of the cystic fibrosis transmembrane conductance regulator anion channel, resulting in significant morbidity and mortality. The progress in elucidating the role of CFTR using established animal and cell-based models led to the recent discovery of effective modulators for most individuals with CF. However, a subset of individuals with CF do not respond to these modulators and there is an urgent need to develop novel therapeutic strategies. In this study, we generate a panel of airway epithelial cells using induced pluripotent stem cells from individuals with common or rare CFTR variants representative of three distinct classes of CFTR dysfunction. To measure CFTR function we adapt two established in vitro assays for use in induced pluripotent stem cell-derived airway cells. In both a 3-D spheroid assay using forskolin-induced swelling as well as planar cultures composed of polarized mucociliary airway epithelial cells, we detect genotype-specific differences in CFTR baseline function and response to CFTR modulators. These results demonstrate the potential of the human induced pluripotent stem cell platform as a research tool to study CF and in particular accelerate therapeutic development for CF caused by rare variants.

Published

2022

3. Generation of Airway Epithelial Cell Air-Liquid Interface Cultures from Human Pluripotent Stem Cells

Author

Finn Hawkins, Darrell Kotton, Brian Davis, Taylor Matte, Jake LeSuer, Shingo Suzuki, Mary Lou Beermann, and Andrew Berical

Subjects

Pluripotent Stem Cells, General Immunology and Microbiology, Cystic Fibrosis, General Chemical Engineering, General Neuroscience, Cystic Fibrosis Transmembrane Conductance Regulator, Humans, Cell Differentiation, Epithelial Cells, Lung, General Biochemistry, Genetics and Molecular Biology

Abstract

Diseases of the conducting airway such as asthma, cystic fibrosis (CF), primary ciliary dyskinesia (PCD), and viral respiratory infections are major causes of morbidity and mortality worldwide. In vitro platforms using human bronchial epithelial cells (HBECs) have been instrumental to our understanding of the airway epithelium in health and disease. Access to HBECs from individuals with rare genetic diseases or rare mutations is a bottleneck in lung research. Induced pluripotent stem cells (iPSCs) are readily generated by "reprogramming" somatic cells and retain the unique genetic background of the individual donor. Recent advances allow for the directed differentiation of iPSCs to lung epithelial progenitor cells, alveolar type 2 cells, as well as the cells of the conducting airway epithelium via basal cells, the major airway stem cells. Here we outline a protocol for the maintenance and expansion of iPSC-derived airway basal cells (hereafter iBCs) as well as their trilineage differentiation in air-liquid interface (ALI) cultures. iBCs are maintained and expanded as epithelial spheres suspended in droplets of extracellular matrix cultured in a primary basal cell medium supplemented with inhibitors of TGF-ß and BMP signaling pathways. iBCs within these epithelial spheres express key basal markers TP63 and NGFR, can be purified by fluorescence activated cell sorting (FACS), and when plated on porous membranes in standard ALI culture conditions, differentiate into a functional airway epithelium. ALI cultures derived from healthy donors are composed of basal, secretory and multiciliated cells and demonstrate epithelial barrier integrity, motile cilia, and mucus secretion. Cultures derived from individuals with CF or PCD recapitulate the dysfunctional CFTR-mediated chloride transport or immotile cilia, the respective disease-causing epithelial defects. Here, we present a protocol for the generation of human cells that can be applied for modeling and understanding airway diseases.

Published

2022

4. Generation of mesenchyme free intestinal organoids from human induced pluripotent stem cells

Author

Finn Hawkins, Amalia Capilla, Aleksander D. Szymaniak, Alexander Stuffer, Marall Vedaie, Dar Heinze, Aditya Mithal, Carlos Villacorta-Martin, Gustavo Mostoslavsky, Darrell N. Kotton, Megan Peasley, Kristine M. Abo, John Mahoney, Anjali Jacob, and Andrew Berical

Subjects

0301 basic medicine, Cystic Fibrosis, Science, Mesenchyme, Cellular differentiation, Genetic Vectors, Induced Pluripotent Stem Cells, Thyroid Nuclear Factor 1, Stem-cell differentiation, General Physics and Astronomy, Biology, Cystic fibrosis, Article, General Biochemistry, Genetics and Molecular Biology, Mesoderm, 03 medical and health sciences, 0302 clinical medicine, Directed differentiation, Intestine, Small, medicine, Organoid, Humans, CDX2 Transcription Factor, Gastrointestinal models, Gene Knock-In Techniques, Progenitor cell, lcsh:Science, Induced pluripotent stem cell, CDX2, Multidisciplinary, Disease model, Cell Differentiation, Epithelial Cells, General Chemistry, medicine.disease, 3. Good health, Cell biology, Intestines, Organoids, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, lcsh:Q

Abstract

Efficient generation of human induced pluripotent stem cell (hiPSC)-derived human intestinal organoids (HIOs) would facilitate the development of in vitro models for a variety of diseases that affect the gastrointestinal tract, such as inflammatory bowel disease or Cystic Fibrosis. Here, we report a directed differentiation protocol for the generation of mesenchyme-free HIOs that can be primed towards more colonic or proximal intestinal lineages in serum-free defined conditions. Using a CDX2eGFP iPSC knock-in reporter line to track the emergence of hindgut progenitors, we follow the kinetics of CDX2 expression throughout directed differentiation, enabling the purification of intestinal progenitors and robust generation of mesenchyme-free organoids expressing characteristic markers of small intestinal or colonic epithelium. We employ HIOs generated in this way to measure CFTR function using cystic fibrosis patient-derived iPSC lines before and after correction of the CFTR mutation, demonstrating their future potential for disease modeling and therapeutic screening applications., Human induced pluripotent stem cell-derived intestinal organoids (HIOs) are powerful tools to study development and diseases of the gastrointestinal tract. Here, the authors develop a directed differentiation protocol to generate mesenchyme-free HIOs that can be patterned towards proximal small intestine or colonic epithelium, and demonstrated their utility in modeling CFTR function.

Published

2020

5. Derivation of Airway Basal Stem Cells from Human Pluripotent Stem Cells

Author

Andrew Berical, Taylor Matte, Ruobing Wang, Shingo Suzuki, Mary Lou Beermann, Jyh-Chang Jean, Jason R. Spence, Nadine Matthias, Sarah X.L. Huang, Cristina Barillà, Andras Rab, Finn Hawkins, Thorsten M. Schlaeger, Steven L. Brody, Barry R. Stripp, Amjad Horani, Scott H. Randell, Carlos Villacorta-Martin, Eric J. Sorsher, Joshua Wu, Jake Le Suer, Chantelle Simone-Roach, Gianni Carraro, Yang Tang, Ana M. Crane, Darrell N. Kotton, and Brian R. Davis

Subjects

Pluripotent Stem Cells, Population, Induced Pluripotent Stem Cells, Biology, Regenerative medicine, Article, 03 medical and health sciences, 0302 clinical medicine, Directed differentiation, Genetics, medicine, Humans, Progenitor cell, Induced pluripotent stem cell, education, Lung, 030304 developmental biology, Primary ciliary dyskinesia, 0303 health sciences, education.field_of_study, Cell Differentiation, Epithelial Cells, Cell Biology, respiratory system, medicine.disease, Cell biology, Trachea, Molecular Medicine, Respiratory epithelium, Stem cell, 030217 neurology & neurosurgery

Abstract

The derivation of tissue-specific stem cells from human induced pluripotent stem cells (iPSCs) would have broad reaching implications for regenerative medicine. Here we report the directed differentiation of human iPSCs into airway basal cells (“iBCs”), a population resembling the stem cell of the airway epithelium. Using a dual fluorescent reporter system (NKX2-1(GFP);TP63(tdTomato)) we track and purify these cells as they first emerge as developmentally immature NKX2-1(GFP+) lung progenitors and subsequently augment a TP63 program during subsequent proximal airway epithelial patterning. In response to primary basal cell medium, NKX2-1(GFP+)/ TP63(tdTomato+) cells display the molecular and functional phenotype of airway basal cells, including the capacity to self-renew or undergo multilineage differentiation in vitro and in tracheal xenografts in vivo. iBCs and their differentiated progeny model perturbations that characterize acquired and genetic airway diseases including the mucus metaplasia of asthma, chloride channel dysfunction of cystic fibrosis, and ciliary defects of primary ciliary dyskinesia.

Published

2019

6. High level of PD-1 expression on hepatitis C virus (HCV)-specific CD8+ and CD4+ T cells during acute HCV infection, irrespective of clinical outcome

Author

Raymond T. Chung, William W. Kwok, Gordon J. Freeman, Lia Laura Lewis-Ximenez, Cory M. McMahon, Brian E. Nolan, Georg M. Lauer, Barbara G. McGovern, Julian Schulze zur Wiesch, Bruce D. Walker, Arthur Y. Kim, Andrew Berical, Thomas Kuntzen, Nahel Elias, Todd M. Allen, Paul Klenerman, Jenna Blum, Victoria O. Kasprowicz, Laura L. Reyor, and S. Longworth

Subjects

Adult, CD4-Positive T-Lymphocytes, Male, Adolescent, Hepatitis C virus, Hepacivirus, Programmed Cell Death 1 Receptor, Immunology, CD8-Positive T-Lymphocytes, medicine.disease_cause, Microbiology, Virus, Flaviviridae, CD28 Antigens, Antigens, CD, Predictive Value of Tests, Virology, medicine, Humans, Aged, Immunity, Cellular, biology, T lymphocyte, Hepatitis C, Hepatitis C, Chronic, Middle Aged, medicine.disease, biology.organism_classification, Prognosis, Liver, Insect Science, Pathogenesis and Immunity, Female, Viral disease, Author's Corrections, Apoptosis Regulatory Proteins, CD8, Biomarkers

Abstract

We monitored expression of PD-1 (a mediator of T-cell exhaustion and viral persistence) on hepatitis C virus (HCV)-specific CD8 + and CD4 + T cells from blood and liver during acute and chronic infections and after the resolved infection stage. PD-1 expression on HCV-specific T cells was high early in acute infection irrespective of clinical outcome, and most cells continued to express PD-1 in resolved and chronic stages of infection; intrahepatic expression levels were especially high. Our results suggest that an analysis of PD-1 expression alone is not sufficient to predict infection outcome or to determine T-cell functionality in HCV infection.

Published

2016

7. Pneumococcal Vaccination Strategies. An Update and Perspective

Author

Andrew Berical, Jennifer D. Possick, Drew A. Harris, and Charles S. Dela Cruz

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Immunity, Herd, medicine.medical_specialty, Cost-Benefit Analysis, Pneumococcal conjugate vaccine, Herd immunity, Pneumococcal Vaccines, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, medicine, Humans, 030212 general & internal medicine, Intensive care medicine, Focused Reviews, Immunization Schedule, Randomized Controlled Trials as Topic, Vaccines, Conjugate, business.industry, Pneumonia, Pneumococcal, medicine.disease, Vaccine efficacy, Pneumococcal polysaccharide vaccine, Vaccination, Pneumococcal infections, 030104 developmental biology, Streptococcus pneumoniae, Pneumococcal vaccine, Pneumococcal pneumonia, Immunology, business, medicine.drug

Abstract

Streptococcus pneumoniae is an important global pathogen that causes a wide range of clinical disease in children and adults. Pneumococcal pneumonia is by far the common presentation of noninvasive and invasive pneumococcal disease and affects the young, the elderly, and the immunocompromised disproportionately. Patients with chronic pulmonary diseases are also at higher risk for pneumococcal infections. Substantial progress over the century has been made in the understanding of pneumococcal immunobiology and the prevention of invasive pneumococcal disease through vaccination. Currently, two pneumococcal vaccines are available for individuals at risk of pneumococcal disease: the 23-valent pneumococcal polysaccharide vaccine (PPV23) and the 13-valent pneumococcal protein-conjugate vaccine (PCV13). The goal of pneumococcal vaccination is to stimulate effective antipneumococcal antibody and mucosal immunity response and immunological memory. Vaccination of infants and young children with pneumococcal conjugate vaccine has led to significant decrease in nasal carriage rates and pneumococcal disease in all age groups. Recent pneumococcal vaccine indication and schedule recommendations on the basis of age and risk factors are outlined in this Focused Review. As new pneumococcal vaccine recommendations are being followed, continued efforts are needed to address the vaccine efficacy in the waning immunity of the ever-aging population, the implementation of vaccines using two different vaccines under very specific schedules and their real world clinical and cost effectiveness, and the development of next generation pneumococcal vaccines.

Published

2016

8. Naturally occurring dominant resistance mutations to hepatitis C virus protease and polymerase inhibitors in treatment-naïve patients

Author

Florian Bihl, Raymond T. Chung, Arne Schneidewind, Edward D. Gomperts, Bruce W. Birren, Gerond Lake-Bakaar, David Heckerman, Chad Nusbaum, Zhimin Liu, Niall Lennon, Hugo R. Rosen, James E. Galagan, Bongshin Lee, Sharyne M. Donfield, Andrew Berical, Tony N. Marion, Arthur Y. Kim, Joerg Timm, Vicki M. Park, Michael Koehrsen, Andreas Cerny, Ulrich Spengler, Andrew H. Talal, Margaret A. Madey, Yanming Xing, Eric S. Daar, Laura L. Reyor, Thomas Kuntzen, Ira M. Jacobson, Bruce D. Walker, Jaquelyn Fleckenstein, Jonathan M. Carlson, Marianna Kleyman, Todd M. Allen, Matthew R. Henn, Chinnappa D. Kodira, Aaron M. Berlin, Brian R. Edlin, Timothy Ledlie, Cory M. McMahon, Georg M. Lauer, Sarah Young, Christopher E. Birch, Julian Schulze zur Wiesch, and Andrew Roberts

Subjects

Male, Macrocyclic Compounds, Proline, viruses, Hepacivirus, Hepatitis C virus, Drug resistance, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, Article, Virus, Cohort Studies, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Drug Resistance, Viral, medicine, Humans, Protease Inhibitors, Protease inhibitor (pharmacology), Genetic Testing, Phylogeny, 030304 developmental biology, 0303 health sciences, Hepatology, biology, Ribavirin, virus diseases, Hepatitis C, Viral Load, Phenylthiourea, medicine.disease, biology.organism_classification, Virology, 3. Good health, Thiazoles, chemistry, Mutation, Quinolines, Female, 030211 gastroenterology & hepatology, Carbamates, Oligopeptides, Viral load

Abstract

Resistance mutations to hepatitis C virus (HCV) nonstructural protein 3 (NS3) protease inhibitors in1% of the viral quasispecies may still allow1000-fold viral load reductions upon treatment, consistent with their reported reduced replicative fitness in vitro. Recently, however, an R155K protease mutation was reported as the dominant quasispecies in a treatment-naïve individual, raising concerns about possible full drug resistance. To investigate the prevalence of dominant resistance mutations against specifically targeted antiviral therapy for HCV (STAT-C) in the population, we analyzed HCV genome sequences from 507 treatment-naïve patients infected with HCV genotype 1 from the United States, Germany, and Switzerland. Phylogenetic sequence analysis and viral load data were used to identify the possible spread of replication-competent, drug-resistant viral strains in the population and to infer the consequences of these mutations upon viral replication in vivo. Mutations described to confer resistance to the protease inhibitors Telaprevir, BILN2061, ITMN-191, SCH6 and Boceprevir; the NS5B polymerase inhibitor AG-021541; and to the NS4A antagonist ACH-806 were observed mostly as sporadic, unrelated cases, at frequencies between 0.3% and 2.8% in the population, including two patients with possible multidrug resistance. Collectively, however, 8.6% of the patients infected with genotype 1a and 1.4% of those infected with genotype 1b carried at least one dominant resistance mutation. Viral loads were high in the majority of these patients, suggesting that drug-resistant viral strains might achieve replication levels comparable to nonresistant viruses in vivo.Naturally occurring dominant STAT-C resistance mutations are common in treatment-naïve patients infected with HCV genotype 1. Their influence on treatment outcome should further be characterized to evaluate possible benefits of drug resistance testing for individual tailoring of drug combinations when treatment options are limited due to previous nonresponse to peginterferon and ribavirin.

Published

2008

9. Whole genome pyrosequencing of rare hepatitis C virus genotypes enhances subtype classification and identification of naturally occurring drug resistance variants

Author

Peter Simmonds, Patrick Charlebois, Ruchi M. Newman, Niall J. Lennon, Matthew R. Henn, Brian Weiner, Thomas Kuntzen, Phil Bennett, Donald G. Murphy, Bruce W. Birren, Michael C. Zody, Carla Kuiken, Todd M. Allen, and Andrew Berical

Subjects

Genotype, Hepatitis C virus, Population, Molecular Sequence Data, Genome, Viral, Hepacivirus, Biology, medicine.disease_cause, Genome, Antiviral Agents, 03 medical and health sciences, chemistry.chemical_compound, Major Articles and Brief Reports, Boceprevir, Drug Resistance, Viral, medicine, Immunology and Allergy, Humans, education, Gene, Genotyping, NS5B, Phylogeny, 030304 developmental biology, Genetics, 0303 health sciences, education.field_of_study, Base Sequence, 030306 microbiology, Genetic Variation, Virology, Hepatitis C, 3. Good health, Infectious Diseases, chemistry

Abstract

Hepatitis C virus (HCV) is an enveloped, positive-strand RNA virus belonging to the Hepacivirus genus in the Flaviviridae family. Seven confirmed genotypes (1–7) are generally distinguished by phylogenetic methods and pair-wise distance calculations [1, 2]. On the basis of full genome nucleotide sequences, HCV genotypes diverged from each other by a pair-wise distance of >30%. Individual genotypes can be further divided into more closely related subtypes that diverged by a pair-wise distance of 15%–30%. All viral genotypes retain their repertoire of colinear structural and nonstructural genes, thereby facilitating preliminary genotype classification on the basis of partial genome sequences of short fragments (approximately 300–400 nucleotides) in the structural core/E1 region and the nonstructural NS5B region [3]. However, full genome sequences remain indispensible for the detection of genome recombination events. While only recombinant HCV genotype 2 k/1b viruses have been found to actively circulate in the population so far [4–7], recombinants of genotypes 2/5, 2b/1b, 2b/1a, and 2i/6p have been detected in single isolates from humans [8–11]. Furthermore, the frequency of HCV intergenotype and intragenotype recombination may be underestimated because of the lack of robust detection methods [12, 13]. Although genotyping based on core/E1 or NS5B sequences has resulted in the provisional classification of a large number of subtype variants within each genotype, at least 1 but preferably ≥2 full genome sequences are required to confirm subtype designation [2, 12]. Accurate genotype and subtype classification is clinically important because major genotypes differ considerably in their response rates to treatment with pegylated interferon and ribavirin and with directly acting antiviral drugs (DAAs) that are designed mainly against genotype 1 isolates. The limited efficacy of DAAs against other genotypes has been shown for genotype 3 [14], and treatment response rates for drug regimens containing boceprevir (an NS3 protease inhibitor) or BMS-790052 (an NS5A inhibitor) were found to vary even between subtypes 1a and 1b [15, 16]. Different baseline frequencies of drug resistance mutations may account for these differences [17], and such variation might become more significant if interferon-free regimens containing 1 or more DAAs could indeed displace the current standard of care [18]. Until clinically tolerable DAAs with high barriers to resistance against the complete spectrum of HCV genotypes become available [18, 19], accurate subtype determination and, possibly, drug resistance profiling of the individual's viral population may guide the optimal choice of drugs. Full genome deep sequencing, as performed in this study, allows the identification of drug resistance mutations across the genome that may exist as dominant or minor variants in treatment-naive patients, thereby informing the design of therapeutic regimens.

Published

2012

10. Compensatory Mutations Restore the Replication Defects Caused by Cytotoxic T Lymphocyte Escape Mutations in Hepatitis C Virus Polymerase ▿

Author

Peter K. Foote, Matthew R. Henn, Michael Kemper, Katherine Kane, Karen A. Power, C Neumann-Haefelin, Andrew Berical, Laura L. Reyor, Yaoyu E. Wang, Adrianne D. Gladden, Kelsey Hills-Evans, Robert Thimme, Allyson K. Bloom, Cesar Oniangue-Ndza, Georg M. Lauer, Arthur Y. Kim, Thomas Kuntzen, and Todd M. Allen

Subjects

T cell, Immunology, Mutation, Missense, Epitopes, T-Lymphocyte, Hepacivirus, Biology, Viral Nonstructural Proteins, medicine.disease_cause, Virus Replication, Microbiology, Epitope, chemistry.chemical_compound, Suppression, Genetic, Virology, medicine, Cytotoxic T cell, Humans, NS5B, Mutation, virus diseases, CTL, medicine.anatomical_structure, chemistry, Viral replication, HLA-B Antigens, Insect Science, Pathogenesis and Immunity, CD8, T-Lymphocytes, Cytotoxic

Abstract

While human leukocyte antigen B57 (HLA-B57) is associated with the spontaneous clearance of hepatitis C virus (HCV), the mechanisms behind this control remain unclear. Immunodominant CD8 + T cell responses against the B57-restricted epitopes comprised of residues 2629 to 2637 of nonstructural protein 5B (NS5B 2629–2637 ) (KSKKTPMGF) and E2 541–549 (NTRPPLGNW) were recently shown to be crucial in the control of HCV infection. Here, we investigated whether the selection of deleterious cytotoxic T lymphocyte (CTL) escape mutations in the NS5B KSKKTPMGF epitope might impair viral replication and contribute to the B57-mediated control of HCV. Common CTL escape mutations in this epitope were identified from a cohort of 374 HCV genotype 1a-infected subjects, and their impact on HCV replication assessed using a transient HCV replicon system. We demonstrate that while escape mutations at residue 2633 (position 5) of the epitope had little or no impact on HCV replication in vitro , mutations at residue 2629 (position 1) substantially impaired replication. Notably, the deleterious mutations at position 2629 were tightly linked in vivo to upstream mutations at residue 2626, which functioned to restore the replicative defects imparted by the deleterious escape mutations. These data suggest that the selection of costly escape mutations within the immunodominant NS5B KSKKTPMGF epitope may contribute in part to the control of HCV replication in B57-positive individuals and that persistence of HCV in B57-positive individuals may involve the development of specific secondary compensatory mutations. These findings are reminiscent of the selection of deleterious CTL escape and compensatory mutations by HLA-B57 in HIV-1 infection and, thus, may suggest a common mechanism by which alleles like HLA-B57 mediate protection against these highly variable pathogens.

Published

2011

11. Whole genome deep sequencing of HIV-1 reveals the impact of early minor variants upon immune recognition during acute infection

Author

Alexander R. Macalalad, Jenna Rychert, Chanson J. Brumme, Adrianne D. Gladden, Bruce W. Birren, Sarah Young, Bruce D. Walker, Suzane Bazner, Heiko Jessen, Damien C. Tully, Karen L. Axten, Monica Casali, Andrew Berical, Allyson K. Bloom, Jake P. Tinsley, Christian Brander, Niall J. Lennon, Joshua Z. Levin, Yaoyu E. Wang, Zabrina L. Brumme, Christoph Hess, Laura Battis, Christine M. Malboeuf, Florencia Pereyra, Michael Kemper, Michael C Zody, Hendrik Streeck, Carmen Zedlack, Sharvari Gujja, Huldrych F. Günthard, Olivier Gasser, Eric S. Rosenberg, Todd M. Allen, Kenneth H. Mayer, Terrance Shea, Sante Gnerre, Rachel L. Erlich, Ruchi M. Newman, Lisa Green, Marcus Altfeld, Tim Dudek, Matthew R. Henn, Patrick Charlebois, Qiandong Zeng, Elizabeth M. Ryan, Christian L. Boutwell, Karen A. Power, Aaron M. Berlin, and University of Zurich

Subjects

Viral Diseases, 2405 Parasitology, HIV Infections, CD8-Positive T-Lymphocytes, 10234 Clinic for Infectious Diseases, Biology (General), Oligonucleotide Array Sequence Analysis, Genetics, 0303 health sciences, Viral Vaccine, 2404 Microbiology, 3. Good health, medicine.anatomical_structure, Infectious Diseases, Viral evolution, RNA, Viral, Medicine, Viral load, Research Article, QH301-705.5, T cell, Immune Cells, Immunology, 610 Medicine & health, Viremia, Viral quasispecies, Genome, Viral, Biology, Microbiology, Deep sequencing, 03 medical and health sciences, Immune system, 1311 Genetics, Virology, 1312 Molecular Biology, medicine, Humans, Molecular Biology, 030304 developmental biology, Immune Evasion, 2403 Immunology, 030306 microbiology, Sequence Analysis, RNA, Immunity, Genetic Variation, HIV, Viral Vaccines, RC581-607, medicine.disease, Genomic Structural Variation, 2406 Virology, HIV-1, Parasitology, Clinical Immunology, Immunologic diseases. Allergy, Genome-Wide Association Study

Abstract

Deep sequencing technologies have the potential to transform the study of highly variable viral pathogens by providing a rapid and cost-effective approach to sensitively characterize rapidly evolving viral quasispecies. Here, we report on a high-throughput whole HIV-1 genome deep sequencing platform that combines 454 pyrosequencing with novel assembly and variant detection algorithms. In one subject we combined these genetic data with detailed immunological analyses to comprehensively evaluate viral evolution and immune escape during the acute phase of HIV-1 infection. The majority of early, low frequency mutations represented viral adaptation to host CD8+ T cell responses, evidence of strong immune selection pressure occurring during the early decline from peak viremia. CD8+ T cell responses capable of recognizing these low frequency escape variants coincided with the selection and evolution of more effective secondary HLA-anchor escape mutations. Frequent, and in some cases rapid, reversion of transmitted mutations was also observed across the viral genome. When located within restricted CD8 epitopes these low frequency reverting mutations were sufficient to prime de novo responses to these epitopes, again illustrating the capacity of the immune response to recognize and respond to low frequency variants. More importantly, rapid viral escape from the most immunodominant CD8+ T cell responses coincided with plateauing of the initial viral load decline in this subject, suggestive of a potential link between maintenance of effective, dominant CD8 responses and the degree of early viremia reduction. We conclude that the early control of HIV-1 replication by immunodominant CD8+ T cell responses may be substantially influenced by rapid, low frequency viral adaptations not detected by conventional sequencing approaches, which warrants further investigation. These data support the critical need for vaccine-induced CD8+ T cell responses to target more highly constrained regions of the virus in order to ensure the maintenance of immunodominant CD8 responses and the sustained decline of early viremia., Author Summary The ability of HIV-1 and other highly variable pathogens to rapidly mutate to escape vaccine-induced immune responses represents a major hurdle to the development of effective vaccines to these highly persistent pathogens. Application of next-generation or deep sequencing technologies to the study of host pathogens could significantly improve our understanding of the mechanisms by which these pathogens subvert host immunity, and aid in the development of novel vaccines and therapeutics. Here, we developed a 454 deep sequencing approach to enable the sensitive detection of low-frequency viral variants across the entire HIV-1 genome. When applied to the acute phase of HIV-1 infection we observed that the majority of early, low frequency mutations represented viral adaptations to host cellular immune responses, evidence of strong host immunity developing during the early decline of peak viral load. Rapid viral escape from the most dominant immune responses however correlated with loss of this initial viral control, suggestive of the importance of mounting immune responses against more conserved regions of the virus. These data provide a greater understanding of the early evolutionary events subverting the ability of host immune responses to control early HIV-1 replication, yielding important insight into the design of more effective vaccine strategies.

Published

2011

12. Temporal dynamics of a predominant protease inhibitor-resistance mutation in a treatment-naive, hepatitis C virus-infected individual

Author

Kimon C. Zachary, Joerg Timm, Katherine Kane, Arthur Y. Kim, Laura L. Reyor, Thomas Kuntzen, Todd M. Allen, Brian E. Nolan, Andrew Berical, and Georg M. Lauer

Subjects

Adult, Male, Time Factors, Hepacivirus, Hepatitis C virus, medicine.medical_treatment, HIV Infections, medicine.disease_cause, Virus Replication, Article, Virus, Drug Resistance, Viral, medicine, Immunology and Allergy, Humans, Protease inhibitor (pharmacology), Protease Inhibitors, Phylogeny, NS3, Protease, biology, virus diseases, Hepatitis C, medicine.disease, biology.organism_classification, Resistance mutation, Virology, Infectious Diseases, Immunology, Mutation, RNA, Viral

Abstract

The dramatic antiviral activities of drugs that specifically inhibit hepatitis C virus replication can be tempered by baseline mutations that confer resistance. We describe the kinetics of an R155K mutation in hepatitis C virus (HCV) NS3 protease known to confer resistance to specific protease inhibitors in an individual coinfected with human immunodeficiency virus-1 and HCV. Longitudinal sequences revealed changes in the relative frequency with which this variant was observed independent of HCV replication levels, illustrating that this mutation coexists with wild-type strains in vivo in the absence of drugs. The persistence of drug-resistance mutations argues for baseline resistance genotyping at the time therapy is initiated to accurately predict the efficacy of treatment.

Published

2009

13. A set of reference sequences for the Hepatitis C genotypes 4d, 4f and 4k covering the full open reading frame

Author

Phil Bennett, Bruce W. Birren, Peter Simmonds, Carla Kuiken, Thomas Kuntzen, Jean Ndjomou, Arne Schneidewind, Andrew Berical, Niall Lennon, Matthew R. Henn, and Todd M. Allen

Subjects

Genotype, Hepacivirus, Hepatitis C virus, Molecular Sequence Data, medicine.disease_cause, Polymerase Chain Reaction, Article, Flaviviridae, Open Reading Frames, Phylogenetics, Virology, medicine, Coding region, Humans, Amino Acid Sequence, Phylogeny, Genetics, Recombination, Genetic, biology, Base Sequence, Hepatitis C, Sequence Analysis, DNA, Reference Standards, biology.organism_classification, medicine.disease, Infectious Diseases, Viral disease, Sequence Alignment

Abstract

Infection with genotype 4 of the Hepatitis C virus is common in Africa and the Mediterranean area, but has also been found at increasing frequencies in injection drug users in Europe and North America. Full length viral sequences to characterize viral diversity and structure have recently become available mostly for subtype 4a, and studies in Egypt and Saudi Arabia, where high proportions of subtype 4a infected patients exist, have begun to establish optimized treatment regimens. However knowledge about other subtype variants of genotype 4 present in less developed African states is lacking. In this study the full coding region from so far poorly characterized variants of HCV genotype 4 was amplified and sequenced using a long range PCR technique. Sequences were analyzed with respect to phylogenetic relationship, possible recombination and prominent sequence characteristics compared to other known HCV strains. We present for the first time two full-length sequences from the HCV genotype 4k, in addition to five strains from HCV genotypes 4d and 4f. Reference sequences for accurate HCV genotyping are required for optimized treatment, and a better knowledge of the global viral sequence diversity is needed to guide vaccines or new drugs effective in the world wide epidemic.

Published

2008

14. Immunologic evidence for lack of heterologous protection following resolution of HCV in patients with non–genotype 1 infection

Author

Lia Laura Lewis-Ximenez, Ansgar W. Lohse, Alysse G. Wurcel, Martin Neukamm, Joerg Timm, Andrea M. Jones, Brian E. Nolan, Bruce D. Walker, Arthur Y. Kim, Todd M. Allen, Cory M. McMahon, Thomas Kuntzen, Steve A. Longworth, Raymond T. Chung, Julian Schulze zur Wiesch, Georg M. Lauer, Andrew Berical, and Victoria O. Kasprowicz

Subjects

Serotype, Adult, CD4-Positive T-Lymphocytes, Male, Genotype, Hepacivirus, Hepatitis C virus, Immunology, Heterologous, Epitopes, T-Lymphocyte, medicine.disease_cause, Biochemistry, Virus, Epitope, Serology, medicine, Humans, Serotyping, Antigens, Viral, Immunobiology, Aged, Cell Proliferation, biology, Cell Biology, Hematology, Hepatitis C, Chronic, Middle Aged, biology.organism_classification, Virology, Female, Peptides, Epitope Mapping

Abstract

Chronic hepatitis C virus (HCV) infection is typically characterized by a lack of virus-specific CD4+ T-cell–proliferative responses, but strong responses have been described in a subset of persons with persistent viremia. One possible explanation for these responses is that they were primed by an earlier resolved infection and do not recognize the current circulating virus. We defined all targeted epitopes using overlapping peptides corresponding to a genotype 1a strain in 44 patients chronically infected with different HCV genotypes (GT). Surprisingly, more HCV-specific CD4+ T-cell responses were detected in patients with chronic non-GT1 infection compared with patients with chronic GT1 infection (P = .017). Notably, we found serologic evidence of a previous exposure to GT1 in 4 patients with non-GT1 infection, and these persons also demonstrated significantly more responses than non-GT1 patients in whom genotype and HCV serotype were identical (P < .001). Comparison of recognition of GT1-specific peptides to peptides representing autologous virus revealed the absence of cross-recognition of the autologous circulating virus. These data indicate that persisent HCV infection can occur in the presence of an HCV-specific T-cell response primed against a heterologous HCV strain, and suggest that clearance of 1 GT does not necessarily protect against subsequent exposure to a second GT.

Published

2007