Your search keyword '"Bonita Rup"' showing total 8 results

1. Pegunigalsidase alfa, a novel PEGylated enzyme replacement therapy for Fabry disease, provides sustained plasma concentrations and favorable pharmacodynamics: A 1-year Phase 1/2 clinical trial

Author

Kathy Nicholls, Robert B. Colvin, Ahmad Tuffaha, Gustavo Maegawa, Pilar Giraldo, Simeon A. Boyadjiev, Mohamed G. Atta, Derlis E. Gonzalez, Alona Paz, Mali Szlaifer, Laura Barisoni, Ozlem Goker-Alpan, Myrl Holida, Raphael Schiffmann, Sari Alon, Einat Brill-Almon, Martha R. Charney, Derralynn Hughes, Charles Jennette, Bonita Rup, and Raul Chertkoff

Subjects

Adult, Male, medicine.medical_specialty, Internationality, Adolescent, Urology, Renal function, Kidney, Young Adult, Pharmacokinetics, Genetics, Clinical endpoint, medicine, Humans, Enzyme Replacement Therapy, Adverse effect, Genetics (clinical), business.industry, Trihexosylceramides, Heart, Enzyme replacement therapy, Middle Aged, medicine.disease, Fabry disease, medicine.anatomical_structure, Treatment Outcome, Pharmacodynamics, alpha-Galactosidase, Fabry Disease, Female, business, Glomerular Filtration Rate

Abstract

Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM Pegunigalsidase alfa, a novel PEGylated, covalently crosslinked form of α-galactosidase A developed as enzyme replacement therapy (ERT) for Fabry disease (FD), was designed to increase plasma half-life and reduce immunogenicity, thereby enhancing efficacy compared with available products. Symptomatic adults with FD participated in this open-label, 3-month dose-ranging study, followed by a 9-month extension. Three cohorts were enrolled in a stepwise manner, each receiving increased doses of pegunigalsidase alfa: 0.2, 1.0, 2.0 mg/kg, via intravenous infusion every other week. Pharmacokinetic analysis occurred on Day 1 and Months 3, 6, and 12. Kidney biopsies at baseline and Month 6 assessed peritubular capillary globotriaosylceramide (Gb3) content. Renal function, cardiac parameters, and other clinical endpoints were assessed throughout. Treatment-emergent adverse events (AEs) and presence of immunoglobulin G (IgG) antidrug antibodies (ADAs) were assessed. Sixteen patients completed 1 year's treatment. Mean terminal plasma half-life (each cohort) ranged from 53 to 121 hours. All 11 male and 1 of 7 female patients presented with classic FD phenotype, in whom renal peritubular capillary Gb3 inclusions were reduced by 84%. Mean estimated glomerular filtration rate was 111 mL/min/1.73 m 2 at baseline, remaining stable throughout treatment. Three patients developed treatment-induced IgG ADAs; following 1 year's treatment, all became ADA-negative. Nearly all treatment-emergent AEs were mild or moderate. One patient withdrew from the study following a serious related AE. Pegunigalsidase alfa may represent an advance in ERT for FD, based on its unique pharmacokinetics and apparent low immunogenicity.

Published

2018

2. Immunogenicity of glycans on biotherapeutic drugs produced in plant expression systems—The taliglucerase alfa story

Author

Pauline M. Rudd, Raul Chertkoff, Sari Alon, Bat-chen Amit-Cohen, Yoram Tekoah, Einat Almon, and Bonita Rup

Subjects

0106 biological sciences, 0301 basic medicine, Male, Glycosylation, Physiology, lcsh:Medicine, Plant Science, Pharmacology, 01 natural sciences, Biochemistry, Pediatrics, Immune Physiology, Medicine and Health Sciences, Macromolecular Structure Analysis, Enzyme-Linked Immunoassays, lcsh:Science, Multidisciplinary, Immune System Proteins, biology, Immunogenicity, food and beverages, Plants, Taliglucerase alfa, medicine.anatomical_structure, Engineering and Technology, Glucosylceramidase, Synthetic Biology, Female, Antibody, Cellular Types, Research Article, Glycan, Protein Structure, Plant Cell Biology, Immunology, Spleen, Enzyme-Linked Immunosorbent Assay, Research and Analysis Methods, Antibodies, 03 medical and health sciences, Antigen, Double-Blind Method, Polysaccharides, Plant Cells, medicine, Humans, Antigens, Immunoassays, Molecular Biology, Biological Products, Gaucher Disease, business.industry, lcsh:R, fungi, Biology and Life Sciences, Proteins, Synthetic Biotherapeutics, Cell Biology, carbohydrates (lipids), 030104 developmental biology, biology.protein, Immunologic Techniques, Clinical safety, lcsh:Q, business, Glucocerebrosidase, 010606 plant biology & botany

Abstract

Plants are a promising alternative for the production of biotherapeutics. Manufacturing in-planta adds plant specific glycans. To understand immunogenic potential of these glycans, we developed a validated method to detect plant specific glycan antibodies in human serum. Using this assay, low prevalence of pre-existing anti-plant glycan antibodies was found in healthy humans (13.5%) and in glucocerebrosidase-deficient Gaucher disease (GD) patients (5%). A low incidence (9% in naïve patient and none in treatment experienced patients) of induced anti-plant glycan antibodies was observed in GD patients after up to 30 months replacement therapy treatment with taliglucerase alfa, a version of human glucocerebrosidase produced in plant cells. Detailed evaluation of clinical safety and efficacy endpoints indicated that anti-plant glycan antibodies did not affect the safety or efficacy of taliglucerase alfa in patients. This study shows the benefit of using large scale human trials to evaluate the immunogenicity risk of plant derived glycans, and indicates no apparent risk related to anti-plant glycan antibodies.

Published

2017

3. Immunogenicity of biologically-derived therapeutics: Assessment and interpretation of nonclinical safety studies

Author

Curtis Maier, James Green, Holly W. Smith, Dan Wierda, Gopi Shankar, Danuta J. Herzyk, Inge A. Ivens, Shalini Gupta, Leslie Abad, Lakshmi Amaravadi, Bonita Rup, Thomas Gelzleichter, Peter Thomas, Christopher Hurst, Rafael A. Ponce, Elizabeth R. Gore, Thomas T. Kawabata, and Barbara Mounho

Subjects

Dose-Response Relationship, Drug, business.industry, Drug Administration Routes, Immunogenicity, Drug Evaluation, Preclinical, Data interpretation, Nonclinical safety, General Medicine, Pharmacology, Toxicology, Bioinformatics, Drug Administration Schedule, Recombinant Proteins, Biopharmaceutics, Species Specificity, Data Interpretation, Statistical, Antibody Formation, Toxicity Tests, Animals, Humans, Medicine, business, Toxicity profile, Clinical evaluation, Antibody formation

Abstract

An evaluation of potential antibody formation to biologic therapeutics during the course of nonclinical safety studies and its impact on the toxicity profile is expected under current regulatory guidance and is accepted standard practice. However, approaches for incorporating this information in the interpretation of nonclinical safety studies are not clearly established. Described here are the immunological basis of anti-drug antibody formation to biopharmaceuticals (immunogenicity) in laboratory animals, and approaches for generating and interpreting immunogenicity data from nonclinical safety studies of biotechnology-derived therapeutics to support their progression to clinical evaluation. We subscribe that immunogenicity testing strategies should be adapted to the specific needs of each therapeutic development program, and data generated from such analyses should be integrated with available clinical and anatomic pathology, pharmacokinetic, and pharmacodynamic data to properly interpret nonclinical studies.

Published

2009

4. Recommendations on risk-based strategies for detection and characterization of antibodies against biotechnology products

Author

Boris Gorovits, Gopi Shankar, Steven J. Swanson, Deborah Finco-Kent, Yuchen Barrett, Shalini Gupta, Holly W. Smith, Bonita Rup, Linda Zuckerman, Gary Taniguchi, Anthony Mire-Sluis, Valerie Quarmby, Michael Moxness, Viswanath Devanarayan, Thomas Parish, Elizabeth Shores, Eugen Koren, and Christopher Stebbins

Subjects

Licensure, Biological Products, biology, business.industry, Immunogenicity, Immunology, Risk Assessment, Antibodies, Biotechnology, Efficacy, Biopharmaceutical industry, Antibody response, biology.protein, Animals, Humans, Immunology and Allergy, Medicine, Antibody, Adverse effect, Risk assessment, business

Abstract

The appropriate evaluation of the immunogenicity of biopharmaceuticals is of major importance for their successful development and licensure. Antibodies elicited by these products in many cases cause no detectable clinical effects in humans. However, antibodies to some therapeutic proteins have been shown to cause a variety of clinical consequences ranging from relatively mild to serious adverse events. In addition, antibodies can affect drug efficacy. In non-clinical studies, anti-drug antibodies (ADA) can complicate interpretation of the toxicity, pharmacokinetic (PK) and pharmacodynamic (PD) data. Therefore, it is important to develop testing strategies that provide valid assessments of antibody responses in both non-clinical and clinical studies. This document provides recommendations for antibody testing strategies stemming from the experience of contributing authors. The recommendations are intended to foster a more unified approach to antibody testing across the biopharmaceutical industry. The strategies proposed are also expected to contribute to better understanding of antibody responses and to further advance immunogenicity evaluation.

Published

2008

5. Therapeutic outcomes, assessments, risk factors and mitigation efforts of immunogenicity of therapeutic protein products

Author

Paolo Vicini, Timothy P. Hickling, Bonita Rup, Liusong Yin, and Xiaoying Chen

Subjects

medicine.medical_specialty, business.industry, Immunogenicity, Immunology, Therapeutic protein, Antibodies, Monoclonal, Autoimmune Diseases, Clinical Practice, Efficacy, Patient safety, Treatment Outcome, Drug development, Risk Factors, Marketed products, Antibody Formation, medicine, Humans, Intensive care medicine, business, Risk assessment

Abstract

Therapeutic protein products (TPPs) are of considerable value in the treatment of a variety of diseases, including cancer, hemophilia, and autoimmune diseases. The success of TPP mainly results from prolonged half-life, increased target specificity and decreased intrinsic toxicity compared with small molecule drugs. However, unwanted immune responses against TPP, such as generation of anti-drug antibody, can impact both drug efficacy and patient safety, which has led to requirements for increased monitoring in regulatory studies and clinical practice, termination of drug development, or even withdrawal of marketed products. We present an overview of current knowledge on immunogenicity of TPP and its impact on efficacy and safety. We also discuss methods for measurement and prediction of immunogenicity and review both product-related and patient-related risk factors that affect its development, and efforts that may be taken to mitigate it. Lastly, we discuss gaps in knowledge and technology and what is needed to fill these.

Published

2015

6. Bioanalytical Methods and Immunogenicity Assays

Author

Bonita Rup, Hendrik Neubert, Boris Gorovits, and Corinna Krinos-Fiorotti

Subjects

Bioanalysis, business.industry, Immunogenicity, Medicine, Computational biology, Pharmacology, business

Published

2014

7. Immunohistochemical detection of bone morphogenetic proteins in bone and soft-tissue sarcomas

Author

John H. Healey, Bonita Rup, Vicki Rosen, Kunio Takaoka, Joseph M. Lane, Pilar Garin-Chesa, Wolfgang J. Rettig, Edward M. Alderman, Andrew G. Huvos, and Hideki Yoshikawa

Subjects

Cancer Research, Pathology, medicine.medical_specialty, animal structures, Soft Tissue Neoplasm, business.industry, Soft tissue, Liposarcoma, medicine.disease, Bone morphogenetic protein, Oncology, embryonic structures, medicine, Osteosarcoma, Sarcoma, Chondrosarcoma, business, Rhabdomyosarcoma

Abstract

Background. Bone morphogenetic proteins (BMPs) are potent inducers of bone formation. Functional and immunohistochemical studies have identified BMPs in a subset of osteosarcomas. In the present study, the authors extend the analysis of BMP expression to other bone and soft tissue sarcomas. Methods. Monoclonal antibody AbH3b2/17 against human BMP-2 and BMP-4 was used in avidin-biotin-immunoperoxidase assays with frozen sections of bone tumors (71 specimens), soft tissue sarcomas (69 specimens), and normal tissues. Results. Among bone tumors, BMP was detected in osteosarcomas (17 of 29 samples), malignant fibrous histiocytomas (MFHs) (6 of 6), and the spindle cell sarcomatous components of spindle cell (dedifferentiated) chondrosarcomas (4 of 4), but not in conventional chondrosarcomas (0 of 10) or Ewing's sarcomas (0 of 14). Histologic subtypes of osteosarcoma differed for BMP expression, with 8 of 9 fibrohistiocytic, 9 of 13 osteoblastic, and 0 of 5 chondroblastic lesions showing immunostaining. In all BMP-positive bone tumors, immunostaining was localized in the cytoplasm of primitive mesenchymal cells, with little or no staining in tumor matrix and more mature osteoblastic/chondrocytic cells. Among soft tissue sarcomas, MFHs (11 of 12), liposarcomas (5 of 11), leiomyosarcomas (3 of 9), and malignant schwannomas (3 of 8) showed cytoplasmic BMP immunostaining. Synovial sarcomas (0 of 9), rhabdomyosarcomas (0 of 8), and fibrosarcomas (0 of 7) were BMP-negative. All normal humantissues tested, including the tissues of a 16-week-old fetus, lacked BMP immunoreactivity. Conclusions. Bone morphogenetic protein is expressed in a subset of osteosarcomas, a high proportion of MFHs of bone and soft tissue, and in spindle cell chondrosarcomas. In these tumors, BMP is localized predominantly to the cytoplasm of malignant cells with primitive mesenchymal features; no or little BMP is detected in the more differentiated elements of bone and soft tissue sarcomas, Different histologic types of bone and soft tissue sarcomas may mimic discrete stages of mesenchymal differentiation as defined by BMP expression and histologic criteria.

Published

1994

8. Evaluation of recombinant human factor IX: pharmacokinetic studies in the rat and the dog

Author

James C. Keith, Kyle McCarthy, Bonita Rup, Bibhu Misra, Larry Bush, Thomas Frederick, Robert Faulkner, Thomas J Ferranti, and Robert G. Schaub

Subjects

Male, medicine.medical_specialty, Time Factors, Recombinant Fusion Proteins, Drug Evaluation, Preclinical, Enzyme-Linked Immunosorbent Assay, Pilot Projects, Beagle, Drug Administration Schedule, law.invention, Factor IX, Rats, Sprague-Dawley, Dogs, Pharmacokinetics, Species Specificity, Blood product, law, Internal medicine, medicine, Animals, biology, business.industry, Fissipedia, Hematology, biology.organism_classification, Recombinant Proteins, Rats, Antibody response, Endocrinology, Antibody Formation, Injections, Intravenous, Recombinant DNA, biology.protein, Antibody, business, medicine.drug, Half-Life

Abstract

SummaryThe pharmacokinetics of intravenously administered recombinant human factor IX (rhFIX) were studied in Sprague-Dawley rats and Beagle dogs. Rats received rhFIX (50 IU/kg once daily) for 28 days, and the plasma half-life was 5 h. Anti-Human Factor IX serum antibody levels were found in only 1 of 12 rats. The pharmacokinetic profiles of rhFIX or Mononine™, a purified human plasma-derived factor IX, after single 100 IU/kg IV doses in dogs, were similar. Peak plasma concentrations of rhFIX and Mononine™ were 4–5 μg/ml. The mean plasma half-lives were 13.2 ± 1.6 h for rhFIX and 13.3 ± 1.6 h for Mononine™. Dogs also received rhFIX (40 IU/kg IV, daily) for 28 days or Mononine™ (40 IU/kg IV daily) for 14 days. Anti-human Factor IX serum antibody levels were determined for each compound. Pharmacokinetic half-lives decreased in these treated dogs which developed antihuman Factor IX antibodies. The antibody responses in 28 day rhFIX (40 IU/kg) dogs were similar to 14 day Mononine™ (40 IU/kg) dogs.

Published

1995