Your search keyword '"Patricia Brown-Augsburger"' showing total 27 results

1. The Therapeutic Monoclonal Antibody Bamlanivimab Does Not Enhance SARS-CoV-2 Infection by FcR-Mediated Mechanisms

Author

Robert W. Cross, Christopher M. Wiethoff, Patricia Brown-Augsburger, Shawn Berens, Jamie Blackbourne, Ling Liu, Xiaohua Wu, Jonathan Tetreault, Carter Dodd, Ramtin Sina, Derrick R. Witcher, Deanna Newcomb, Denzil Frost, Angela Wilcox, Viktoriya Borisevich, Krystle N. Agans, Courtney Woolsey, Abhishek N. Prasad, Daniel J. Deer, Joan B. Geisbert, Natalie S. Dobias, Karla A. Fenton, Beth Strifler, Philip Ebert, Richard Higgs, Anne Beall, Sumit Chanda, Laura Riva, Xin Yin, and Thomas W. Geisbert

Subjects

bamlanivimab, antibody-dependent enhancement, SARS-CoV-2, COVID-19, monoclonal antibodies, Medicine

Abstract

As part of the non-clinical safety package characterizing bamlanivimab (SARS-CoV-2 neutralizing monoclonal antibody), the risk profile for antibody-dependent enhancement of infection (ADE) was evaluated in vitro and in an African green monkey (AGM) model of COVID-19. In vitro ADE assays in primary human macrophage, Raji, or THP-1 cells were used to evaluate enhancement of viral infection. Bamlanivimab binding to C1q, FcR, and cell-based effector activity was also assessed. In AGMs, the impact of bamlanivimab pretreatment on viral loads and clinical and histological pathology was assessed to evaluate enhanced SARS-CoV-2 replication or pathology. Bamlanivimab did not increase viral replication in vitro, despite a demonstrated effector function. In vivo, no significant differences were found among the AGM groups for weight, temperature, or food intake. Treatment with bamlanivimab reduced viral loads in nasal and oral swabs and BAL fluid relative to control groups. Viral antigen was not detected in lung tissue from animals treated with the highest dose of bamlanivimab. Bamlanivimab did not induce ADE of SARS-CoV-2 infection in vitro or in an AGM model of infection at any dose evaluated. The findings suggest that high-affinity monoclonal antibodies pose a low risk of mediating ADE in patients and support their safety profile as a treatment of COVID-19 disease.

Published

2023

2. Supplementary Methods and Figure Legends from LY2875358, a Neutralizing and Internalizing Anti-MET Bivalent Antibody, Inhibits HGF-Dependent and HGF-Independent MET Activation and Tumor Growth

Author

Jirong Lu, Peter Vaillancourt, Ying Tang, Julian Davies, Irene Denning, Yong Wang, Lihua Huang, Chi-Kin Chow, Volker Wacheck, Patricia Brown-Augsburger, Darryl W. Ballard, Kelly M. Credille, Jason R. Manro, Jinqi Xia, Jonathan W. Tetreault, Jennifer R. Stephens, Victoria L. Peek, Paul Cornwell, S. Betty Yan, Mark A. Wortinger, Wei Zeng, and Ling Liu

Abstract

Supplementary Methods and Supplementary Figure Legends

Published

2023

3. Supplementary Tables from LY2875358, a Neutralizing and Internalizing Anti-MET Bivalent Antibody, Inhibits HGF-Dependent and HGF-Independent MET Activation and Tumor Growth

Author

Jirong Lu, Peter Vaillancourt, Ying Tang, Julian Davies, Irene Denning, Yong Wang, Lihua Huang, Chi-Kin Chow, Volker Wacheck, Patricia Brown-Augsburger, Darryl W. Ballard, Kelly M. Credille, Jason R. Manro, Jinqi Xia, Jonathan W. Tetreault, Jennifer R. Stephens, Victoria L. Peek, Paul Cornwell, S. Betty Yan, Mark A. Wortinger, Wei Zeng, and Ling Liu

Abstract

Supplementary Tables. Supplementary Table S1. Summary of cell lines used. Supplementary Table S2. Summary of Repeat-Dose Toxicity Study with LY2875358

Published

2023

4. Data from LY2875358, a Neutralizing and Internalizing Anti-MET Bivalent Antibody, Inhibits HGF-Dependent and HGF-Independent MET Activation and Tumor Growth

Author

Jirong Lu, Peter Vaillancourt, Ying Tang, Julian Davies, Irene Denning, Yong Wang, Lihua Huang, Chi-Kin Chow, Volker Wacheck, Patricia Brown-Augsburger, Darryl W. Ballard, Kelly M. Credille, Jason R. Manro, Jinqi Xia, Jonathan W. Tetreault, Jennifer R. Stephens, Victoria L. Peek, Paul Cornwell, S. Betty Yan, Mark A. Wortinger, Wei Zeng, and Ling Liu

Abstract

Purpose: MET, the receptor for hepatocyte growth factor (HGF), has been implicated in driving tumor proliferation and metastasis. High MET expression is correlated with poor prognosis in multiple cancers. Activation of MET can be induced either by HGF-independent mechanisms such as gene amplification, specific genetic mutations, and transcriptional upregulation or by HGF-dependent autocrine or paracrine mechanisms.Experimental Design/Results: Here, we report on LY2875358, a novel humanized bivalent anti-MET antibody that has high neutralization and internalization activities, resulting in inhibition of both HGF-dependent and HGF-independent MET pathway activation and tumor growth. In contrast to other bivalent MET antibodies, LY2875358 exhibits no functional agonist activity and does not stimulate biologic activities such as cell proliferation, scattering, invasion, tubulogenesis, or apoptosis protection in various HGF-responsive cells and no evidence of inducing proliferation in vivo in a monkey toxicity study. LY2875358 blocks HGF binding to MET and HGF-induced MET phosphorylation and cell proliferation. In contrast to the humanized one-armed 5D5 anti-MET antibody, LY2875358 induces internalization and degradation of MET that inhibits cell proliferation and tumor growth in models where MET is constitutively activated. Moreover, LY2875358 has potent antitumor activity in both HGF-dependent and HGF-independent (MET-amplified) xenograft tumor models. Together, these findings indicate that the mechanism of action of LY2875358 is different from that of the one-armed MET antibody.Conclusions: LY2875358 may provide a promising therapeutic strategy for patients whose tumors are driven by both HGF-dependent and HGF-independent MET activation. LY2875358 is currently being investigated in multiple clinical studies. Clin Cancer Res; 20(23); 6059–70. ©2014 AACR.

Published

2023

5. First‐in‐Human Study of Bamlanivimab in a Randomized Trial of Hospitalized Patients With COVID‐19

Author

Charles Benson, Emmanuel Chigutsa, Amit Saxena, Paul Klekotka, Peter Chen, Gourab Datta, Ariel Kay, Josh Poorbaugh, Mark J. Mulligan, William A. Fischer, Ying Grace Li, Karen L. Price, Patricia Brown-Augsburger, Ajay Nirula, Robert J. Benschop, Nadine Rouphael, Jenny Y. Chien, Jeffrey Fill, and Michael Dougan

Subjects

Adult, Male, medicine.medical_specialty, Placebo, Antibodies, Monoclonal, Humanized, Antiviral Agents, Article, law.invention, Pharmacokinetics, Randomized controlled trial, Double-Blind Method, law, Internal medicine, Medicine, Humans, Pharmacology (medical), Adverse effect, Fatigue, Aged, Pharmacology, Dose-Response Relationship, Drug, business.industry, Research, Headache, COVID-19, Articles, Middle Aged, COVID-19 Drug Treatment, Clinical trial, Hospitalization, Tolerability, Pharmacodynamics, Monoclonal, Administration, Intravenous, Female, business

Abstract

Therapeutics for patients hospitalized with coronavirus disease 2019 (COVID-19) are urgently needed during the pandemic. Bamlanivimab is a potent neutralizing monoclonal antibody that blocks severe acute respiratory syndrome-coronavirus 2 (SARS-CoV-2) attachment and entry into human cells, which could potentially lead to therapeutic benefit. J2W-MC-PYAA was a randomized, double-blind, sponsor unblinded, placebo-controlled, single ascending dose first-in-human trial (NCT04411628) in hospitalized patients with COVID-19. A total of 24 patients received either placebo or a single dose of bamlanivimab (700 mg, 2,800 mg, or 7,000 mg). The primary objective was assessment of safety and tolerability, including adverse events and serious adverse events, with secondary objectives of pharmacokinetic (PK) and pharmacodynamic analyses. Treatment-emergent adverse event (TEAE) rates were identical in the placebo and pooled bamlanivimab groups (66.7%). There were no apparent dose-related increases in the number or severity of TEAEs. There were no serious adverse events or deaths during the study, and no discontinuations due to adverse events. PKs of bamlanivimab is linear and exposure increased proportionally with dose following single i.v. administration. The half-life was ~ 17 days. These results demonstrate the favorable safety profile of bamlanivimab, and provided the initial critical evaluation of safety, tolerability, and PKs in support of the development of bamlanivimab in several ongoing clinical trials.

Published

2021

6. The therapeutic monoclonal antibody bamlanivimab does not enhance SARS‑CoV-2 infection by FcR-mediated mechanisms

Author

Robert M Cross, Christopher M Wiethoff, Patricia Brown-Augsburger, Shawn Berens, Jamie Blackbourne, Ling Liu, Xiaohua Wu, Jonathan Tetreault, Carter Dodd, Ramtin Sina, Derrick R Witcher, Deanna Newcomb, Denzil Frost, Angela Wilcox, Viktoriya Borisevich, Krystle N Agans, Courtney Woolsey, Abhishek N Prasad, Daniel J Deer, Joan B Geisbert, Natalie S Dobias, Karla A Fenton, Beth Strifler, Philip Ebert, Richard Higgs, Anne Beall, Sumit Chanda, Laura Riva, Xin Yin, and Thomas W Geisbert

Abstract

Background Antibodies targeting envelope glycoproteins have been shown in some instances to enhance infection by subverting Fc receptor and complement function, or by directly inducing fusion with cellular membranes. The potential for antibody dependent enhancement (ADE) of infection raises concern that passive immunization with a therapeutic anti-viral antibody could increase risk of disease. As part of the nonclinical package characterizing the risk profile of the SARS-CoV-2 neutralizing monoclonal antibody bamlanivimab, studies were conducted to evaluate the potential for ADE of infection in vitro and in a non-human primate model of COVID-19. Methods In vitro assays were performed in primary human macrophage, Raji, or THP-1 cells exposed to SARS-CoV-2 in the presence of bamlanivimab ranging from approximately IC50 to more than 100-fold above or below the IC50. Samples were evaluated for demonstration of productive viral infection. Bamlanivimab binding to C1q and FcR were quantified, and activity was studied by cell-based assays. In vivo studies were performed in African green monkeys (AGM) infected with SARS-CoV-2 virus following sub-saturating or saturating doses of bamlanivimab or IgG control. Viral loads, clinical pathology, and histology endpoints were assessed to determine if bamlanivimab enhanced SARS-CoV-2 replication or clinical illness. Mixed model repeated measures were used to evaluate virology statistics. Results Bamlanivimab did not increase viral RNA production in FcγR-expressing cell lines, despite demonstration of effector function. No significant differences were found among the AGM groups in terms of weight, temperature, or food intake. Treatment with bamlanivimab reduced viral loads in nasal and oral swabs and BAL fluid relative to control groups. Viral antigen was not detected in lung tissue from animals treated with the highest dose of bamlanivimab. Microscopic findings along with decreases in viral loads in bamlanivimab-treated animals indicated that ADE of disease was not observed in this study. Conclusions Sub-saturating doses of bamlanivimab treatment do not induce ADE of SARSCoV2 infection in either in vitro or an AGM model of infection. Findings suggest that high affinity monoclonal antibodies pose a low risk of mediating ADE in patients and further supports their safety profile as a treatment of COVID-19 disease.

Published

2022

7. Validation of a de‐immunization strategy for monoclonal antibodies using cynomolgus macaque as a surrogate for human

Author

Derrick R. Witcher, Victor J. Wroblewski, Patricia Brown-Augsburger, Jeffrey S. Boyles, Lukasz K. Chlewicki, Yi Wen, and Natalia Kovalova

Subjects

Male, medicine.drug_class, In silico, Pharmaceutical Science, Monoclonal antibody, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Adalimumab, medicine, Animals, Humans, Pharmacology (medical), Pharmacology, biology, Tumor Necrosis Factor-alpha, Immunogenicity, Antibodies, Monoclonal, General Medicine, Golimumab, Macaca fascicularis, Immunoglobulin G, 030220 oncology & carcinogenesis, Immunology, biology.protein, Female, Immunization, Tumor necrosis factor alpha, Antibody, medicine.drug

Abstract

The immunogenicity of biotherapeutics presents a major challenge during the clinical development of new protein drugs including monoclonal antibodies. To address this, multiple humanization and de-immunization techniques that employ in silico algorithms and in vitro test systems have been proposed and implemented. However, the success of these approaches has been variable and to date, the ability of these techniques to predict immunogenicity has not been systematically tested in humans or other primates. This study tested whether antibody humanization and de-immunization strategies reduce the risk of anti-drug antibody (ADA) development using cynomolgus macaque as a surrogate for human. First human-cyno chimeric antibodies were constructed by grafting the variable domains of the adalimumab and golimumab monoclonal antibodies onto cynomolgus macaque IgG1 and Igκ constant domains followed by framework germlining to cyno to reduce the xenogenic content. Next, B and T cell epitopes and aggregation-prone regions were identified using common in silico methods to select domains with an ADA risk for additional modification. The resultant engineered antibodies had a comparable affinity for TNFα, demonstrated similar biophysical properties, and exhibited significantly reduced ADA levels in cynomolgus macaque compared with the parental antibodies, with a corresponding improvement in the pharmacokinetic profile. Notably, plasma concentrations of the engineered antibodies were quantifiable through 504 hours (chimeric) and 840 hours (germlined/de-immunized), compared with only 336 hours (adalimumab) or 336-672 hours (golimumab). The results point to the significant value in the investment in these engineering strategies as an important guide for monoclonal antibody optimization that can contribute to improved clinical outcomes.

Published

2020

8. Correlation between antidrug antibodies, pre-existing antidrug reactivity, and immunogenetics (MHC class II alleles) in cynomolgus macaque

Author

Lukasz K. Chlewicki, Victor J Wroblewski, Patricia Brown-Augsburger, Natalia Kovalova, and Michael D Knierman

Subjects

Male, 0301 basic medicine, Genes, MHC Class II, Immunology, Population, Immunogenetics, Drug Hypersensitivity, 03 medical and health sciences, 0302 clinical medicine, Immune system, Gene Frequency, Antibodies, Bispecific, Genetics, Animals, education, Phylogeny, MHC class II, education.field_of_study, biology, Immunogenicity, Haplotype, Macaca fascicularis, 030104 developmental biology, Haplotypes, Drug development, biology.protein, Antibody, 030215 immunology

Abstract

Immunogenicity of biomolecules is one of the largest concerns in biological therapeutic drug development. Adverse immune responses as a result of immunogenicity to biotherapeutics range from mild hypersensitivity reactions to potentially life-threatening anaphylactic reactions and can negatively impact human health and drug efficacy. Numerous confounding patient-, product- or treatment-related factors can influence the development of an immune reaction against therapeutic proteins. The goal of this study was to investigate the relationship between pre-existing drug reactivity (PE-ADA), individual immunogenetics (MHC class II haplotypes), and development of treatment-induced antidrug antibodies (TE-ADA) in cynomolgus macaque. PE-ADA refers to the presence of antibodies immunoreactive against the biotherapeutic in treatment-naïve individuals. We observed that PE-ADA frequency against four different bispecific antibodies in naïve cynomolgus macaque is similar to that reported in humans. Additionally, we report a trend towards an increased incidence of TE-ADA development in macaques with high PE-ADA levels. In order to explore the relationship between MHC class II alleles and risk of ADA development, we obtained full-length MHC class II sequences from 60 cynomolgus macaques in our colony. We identified a total of 248 DR, DP, and DQ alleles and 236 unique haplotypes in our cohort indicating a genetically complex set of animals potentially reflective of the human population. Based on our observations, we propose the evaluation of the magnitude/frequency of pre-existing reactivity and consideration of MHC class II genetics as additional useful tools to understand the immunogenic potential of biotherapeutics.

Published

2019

9. The neutralizing antibody, LY-CoV555, protects against SARS-CoV-2 infection in nonhuman primates

Author

Krithika Muthuraman, Richard E. Higgs, Carl L. Hansen, Maren de Vries, Mark J. Mulligan, Kizzmekia S. Corbett, Ping Xiang, Nicole V. Johnson, Jory A. Goldsmith, Jason S. McLellan, John R. Mascola, Marissa H. Piper, Lucas Kraft, Jamie L. Blackbourne, Samuel J. Hinshaw, Davide Pellacani, Stefanie Žentelis, Christopher M. Wiethoff, Solmaz Sobhanifar, David R. Martinez, Franz J. Triana, Thomas P. Cujec, Barney S. Graham, Robert W. Cross, Ching-Lin Hsieh, Beverly A. Heinz, Denisa Foster, Ralph S. Baric, Sean A. Tycho, Jorg Hendle, David Collins, Eun Sung Yang, Ester Falconer, Daniel Wrapp, Andrew C. Adams, Roza Bidshahri, A. Pustilnik, Yuri Hwang, Adil Mohamed, Julian Davies, Yi Zhang, Patricia Brown-Augsburger, Bryan Edward Jones, Shawn J. Berens, Kevin R. Jepson, Bryan C. Barnhart, Kathryn Westendorf, Lingshu Wang, Viktoriya Borisevich, Meike Dittmann, Maia A. Smith, Deepa Balasubramaniam, Thomas W. Geisbert, Rodrigo Goya, Hayley M. Belli, Olubukola M. Abiona, and Marie I. Samanovic

Subjects

Antibodies, Viral, Article, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, medicine, Animals, Respiratory system, Neutralizing antibody, 030304 developmental biology, 0303 health sciences, biology, business.industry, SARS-CoV-2, COVID-19, General Medicine, biology.organism_classification, Virology, Antibodies, Neutralizing, Macaca mulatta, 3. Good health, Vaccination, Rhesus macaque, medicine.anatomical_structure, Viral replication, 030220 oncology & carcinogenesis, Spike Glycoprotein, Coronavirus, biology.protein, Antibody, business, Respiratory tract

Abstract

Severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) poses a public health threat for which preventive and therapeutic agents are urgently needed. Neutralizing antibodies are a key class of therapeutics that may bridge widespread vaccination campaigns and offer a treatment solution in populations less responsive to vaccination. Here, we report that high-throughput microfluidic screening of antigen-specific B cells led to the identification of LY-CoV555 (also known as bamlanivimab), a potent anti-spike neutralizing antibody from a hospitalized, convalescent patient with coronavirus disease 2019 (COVID-19). Biochemical, structural, and functional characterization of LY-CoV555 revealed high-affinity binding to the receptor-binding domain, angiotensin-converting enzyme 2 binding inhibition, and potent neutralizing activity. A pharmacokinetic study of LY-CoV555 conducted in cynomolgus monkeys demonstrated a mean half-life of 13 days and a clearance of 0.22 ml hour-1 kg-1, consistent with a typical human therapeutic antibody. In a rhesus macaque challenge model, prophylactic doses as low as 2.5 mg/kg reduced viral replication in the upper and lower respiratory tract in samples collected through study day 6 after viral inoculation. This antibody has entered clinical testing and is being evaluated across a spectrum of COVID-19 indications, including prevention and treatment.

Published

2020

10. LY-CoV555, a rapidly isolated potent neutralizing antibody, provides protection in a non-human primate model of SARS-CoV-2 infection

Author

Mark J. Mulligan, Kizzmekia S. Corbett, Marissa H. Piper, Nicole V. Johnson, Jory A. Goldsmith, Roza Bidshahri, Carl L. Hansen, Robert W. Cross, Daniel Wrapp, A. Pustilnik, Yuri Hwang, Julian Davies, Adil Mohamed, Kathryn Westendorf, Beverly A. Heinz, Olubukola M. Abiona, Lucas Kraft, Jamie L. Blackbourne, Andrew C. Adams, Marie I. Samanovic, Samuel J. Hinshaw, Bryan Edward Jones, Sean A. Tycho, Christopher M. Wiethoff, Shawn J. Berens, Krithika Muthuraman, Stefanie Zentelis, Thomas W. Geisbert, Richard E. Higgs, Ralph S. Baric, Lingshu Wang, Jorg Hendle, Maia A. Smith, Hayley M. Belli, Meike Dittmann, Deepa Balasubramaniam, Solmaz Sobhanifar, Rodrigo Goya, Denisa Foster, John R. Mascola, Viktoriya Borisevich, Thomas P. Cujec, Barney S. Graham, Ping Xiang, Jason S. McLellan, Davide Pellacani, David R. Martinez, Maren de Vries, Patricia Brown-Augsburger, Franz J. Triana, David Collins, Ester Falconer, Kevin R. Jepson, Bryan C. Barnhart, and Ching-Lin Hsieh

Subjects

Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Medicine, skin and connective tissue diseases, Neutralizing antibody, Research Articles, biology, business.industry, fungi, Antiviral antibody, respiratory system, biology.organism_classification, Virology, respiratory tract diseases, STM r-articles, body regions, Coronavirus, Rhesus macaque, medicine.anatomical_structure, Viral replication, biology.protein, Antibody, business, Research Article, Respiratory tract

Abstract

LY-CoV555, a SARS-CoV-2 spike protein–specific antibody, neutralizes SARS-CoV-2 and protects the airways of nonhuman primates against infection., A monoclonal for SARS-CoV-2 Among the most promising therapeutic options for individuals with coronavirus disease 2019 (COVID-19) are monoclonal antibodies (mAbs). In this study, Jones et al. identified, characterized, and tested one such mAb, LY-CoV555, in vitro and in vivo. They found that LY-CoV555 bound to the severe acute respiratory distress syndrome coronavirus-2 (SARS-CoV-2) spike protein and prevented its interaction with angiotensin-converting enzyme 2. Prophylactic treatment with LY-CoV555 protected the upper and lower respiratory tracts of nonhuman primates from becoming infected with SARS-CoV-2. Together, these data support the clinical use of LY-CoV555 for treating patients with COVID-19., Severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) poses a public health threat for which preventive and therapeutic agents are urgently needed. Neutralizing antibodies are a key class of therapeutics that may bridge widespread vaccination campaigns and offer a treatment solution in populations less responsive to vaccination. Here, we report that high-throughput microfluidic screening of antigen-specific B cells led to the identification of LY-CoV555 (also known as bamlanivimab), a potent anti-spike neutralizing antibody from a hospitalized, convalescent patient with coronavirus disease 2019 (COVID-19). Biochemical, structural, and functional characterization of LY-CoV555 revealed high-affinity binding to the receptor-binding domain, angiotensin-converting enzyme 2 binding inhibition, and potent neutralizing activity. A pharmacokinetic study of LY-CoV555 conducted in cynomolgus monkeys demonstrated a mean half-life of 13 days and a clearance of 0.22 ml hour−1 kg−1, consistent with a typical human therapeutic antibody. In a rhesus macaque challenge model, prophylactic doses as low as 2.5 mg/kg reduced viral replication in the upper and lower respiratory tract in samples collected through study day 6 after viral inoculation. This antibody has entered clinical testing and is being evaluated across a spectrum of COVID-19 indications, including prevention and treatment.

Published

2020

11. Bioequivalence and comparative pharmacodynamics of insulin lispro 200 U/mL relative to insulin lispro (Humalog®) 100 U/mL

Author

Mary E. Seger, Helle Linnebjerg, Amparo de la Peña, Danny Soon, Patricia Brown-Augsburger, Shobha Reddy, Adam Scott, and Michael Allen Dobbins

Subjects

Adult, Male, medicine.medical_specialty, medicine.medical_treatment, Cmax, Pharmaceutical Science, 030209 endocrinology & metabolism, 030204 cardiovascular system & hematology, Pharmacology, Bioequivalence, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Glucose infusion, Pharmacokinetics, Diabetes mellitus, Internal medicine, medicine, Humans, Hypoglycemic Agents, Insulin lispro, Pharmacology (medical), pharmacokinetic, bioequivalence, Cross-Over Studies, Insulin Lispro, Dose-Response Relationship, Drug, business.industry, Insulin, Articles, Middle Aged, medicine.disease, pharmacodynamic, Endocrinology, Therapeutic Equivalency, Area Under Curve, Pharmacodynamics, diabetes mellitus, Glucose Clamp Technique, Female, business, medicine.drug

Abstract

Insulin lispro 200 U/mL (IL200) is a new strength formulation of insulin lispro (Humalog®, IL100), developed as an option for diabetic patients on higher daily mealtime insulin doses. This phase 1, open‐label, 2‐sequence, 4‐period crossover, randomized, 8‐hour euglycemic clamp study aimed to demonstrate the bioequivalence of IL200 and IL100 after subcutaneous administration of 20 U (U) to healthy subjects (n = 38). Pharmacokinetic (PK) and pharmacodynamic (PD) responses were similar in both formulations. All 90%CIs for the ratios of area under the concentration‐versus‐time curve from time zero to the time of the last measurable concentration (AUC0–tlast) and maximum observed drug concentration (Cmax), as well as the total glucose infused throughout the clamp (Gtot) and the maximum glucose infusion rate (Rmax), were contained within 0.80 and 1.25. Time of maximum observed drug concentration (tmax) was similar between formulations, with a median difference of 15 minutes and a 95%CI of the difference that included zero. Inter‐ and intrasubject variability estimates were similar for both formulations. Both formulations were well tolerated. IL200 was bioequivalent to IL100 after subcutaneous administration of 20‐U single doses, and PD responses were comparable between formulation strengths.

Published

2015

12. Disposition of Basal Insulin Peglispro Compared with 20-kDa Polyethylene Glycol in Rats Following a Single Intravenous or Subcutaneous Dose

Author

Anthony T. Murphy, Jennifer A. Martin, Patricia Brown-Augsburger, Victor J. Wroblewski, Bernice Ellis, and Mary Pat Knadler

Subjects

Male, medicine.medical_specialty, Injections, Subcutaneous, Biological Availability, Pharmaceutical Science, Polyethylene glycol, Urine, Polyethylene Glycols, Rats, Sprague-Dawley, chemistry.chemical_compound, Internal medicine, PEG ratio, medicine, Animals, Insulin, Insulin lispro, Tissue Distribution, Feces, Pharmacology, Catabolism, technology, industry, and agriculture, Area under the curve, Rats, Bioavailability, Endocrinology, chemistry, Biochemistry, Injections, Intravenous, medicine.drug

Abstract

Basal insulin peglispro (BIL) comprises insulin lispro covalently bound to a 20-kDa polyethylene glycol (PEG) at lysine B28. The biologic fate of BIL and unconjugated PEG were examined in rats given a single 0.5-mg/kg i.v. or 2-mg/kg s.c. dose of BIL with (14)C label in 20-kDa PEG or (125)I label in lispro. Unconjugated (14)C-labeled 20-kDa PEG was dosed at 10 mg/kg i.v. or s.c. Blood, urine, and feces were collected up to 336 hours after dosing. Radioactivity was measured by scintillation spectrometry, and BIL was quantitated by enzyme-linked immunosorbent assay. Area under the curve and half-life for immunoreactive BIL were lower than those for both (14)C and (125)I after subcutaneous and intravenous administration. The half-lives of (14)C after BIL and PEG dosing were similar. The clearance of immunoreactive BIL was 2.4-fold faster than that of (14)C and 1.6-fold faster than (125)I. After a subcutaneous dose of BIL, immunoreactive BIL accounted for 31% of the circulating (125)I and 16% of the circulating (14)C, indicating extensive catabolism of BIL. Subcutaneous bioavailability of BIL was 23%-29%; bioavailability for unconjugated PEG was 78%. For unconjugated PEG, most of the (14)C dose was recovered in urine. For BIL, ≥86% of (125)I was eliminated in urine and (14)C was eliminated about equally in urine and feces. The major (14)C-labeled catabolism product of BIL in urine was 20-kDa PEG with lysine attached. The attachment of 20-kDa PEG to lispro in BIL led to a different elimination pathway for PEG compared with unconjugated 20-kDa PEG.

Published

2015

13. Subcutaneous Injection Depth Does Not Affect the Pharmacokinetics or Glucodynamics of Insulin Lispro in Normal Weight or Healthy Obese Subjects

Author

Helle Linnebjerg, Linda Morrow, Patricia Brown-Augsburger, Shobha Reddy, Amparo de la Peña, Kwee P. Yeo, Edward Catton, and Debra A. Ignaut

Subjects

Adult, Blood Glucose, Male, medicine.medical_specialty, Injections, Subcutaneous, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Biomedical Engineering, Bioengineering, Body Mass Index, Young Adult, Subcutaneous injection, Pharmacokinetics, Internal medicine, Internal Medicine, medicine, Humans, Hypoglycemic Agents, Insulin lispro, Obesity, Cross-Over Studies, Insulin Lispro, business.industry, Insulin, Body Weight, Original Articles, Middle Aged, Glucose clamp technique, medicine.disease, Crossover study, Healthy Volunteers, Endocrinology, Research Design, Area Under Curve, Glucose Clamp Technique, Female, business, Body mass index, medicine.drug

Abstract

Background: An 8-mm needle length is commonly used for insulin injections; however, recent recommendations suggest shorter needles may help patients avoid intramuscular injections and reduce pain, while maintaining adequate glucose control. The goal of these analyses was to compare the pharmacokinetics (PK) and glucodynamics (GD) of insulin lispro after a 5-mm or an 8-mm injection depth administration in 2 populations: normal weight (study 1) or obese (study 2). Methods: In both open-label, randomized, 2-period crossover euglycemic clamp studies, subjects received single 0.25 U/kg insulin lispro doses on 2 occasions (at 5-mm and 8-mm injection depths); samples for PK and GD analyses were collected up to 6 hours postdose. Noncompartmental PK parameters AUC0-tlast, AUC0-∞, Cmax and GD parameters Gtot, Rmax, tRmax were log-transformed prior to analysis using a mixed effects model. Results: There were no apparent differences between PK profiles at the 5-mm or 8-mm injection depth in either study, demonstrated by the ratios of geometric means of AUC0-tlast, AUC0-∞, and Cmax being close to 1, with 90% confidence intervals (CI) within (0.80, 1.25). There were no apparent differences between GD profiles at either injection depth with the ratios of Gtot and Rmax near unity and 90% CIs that included 1. In both studies, the tRmax values were similar between injection depths, with a small median of pairwise differences and a 90% CI that included zero. Conclusions: Injection depths in the 5-8 mm range did not affect the PK or GD of insulin lispro in normal weight or obese subjects.

Published

2015

14. LY2875358, a Neutralizing and Internalizing Anti-MET Bivalent Antibody, Inhibits HGF-Dependent and HGF-Independent MET Activation and Tumor Growth

Author

Ying Tang, Yong Wang, Julian Davies, Lihua Huang, Patricia Brown-Augsburger, Mark Wortinger, Jonathan Wendell Tetreault, Wei-an Zeng, Volker Wacheck, Jinqi Xia, Paul Cornwell, Chi Kin Chow, Darryl Ballard, Ling Liu, S. Betty Yan, Jason Manro, Jirong Lu, Victoria L. Peek, Peter Edward Vaillancourt, Irene Denning, Jennifer R. Stephens, and Kelly M. Credille

Subjects

Male, Cancer Research, media_common.quotation_subject, Down-Regulation, Antineoplastic Agents, Biology, Antibodies, Monoclonal, Humanized, Mice, Downregulation and upregulation, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Phosphorylation, Receptor, Autocrine signalling, Internalization, Cell Proliferation, media_common, Hepatocyte Growth Factor, Cell growth, Antibodies, Monoclonal, Proto-Oncogene Proteins c-met, Antibodies, Neutralizing, Xenograft Model Antitumor Assays, Molecular biology, Tumor Burden, Enzyme Activation, Disease Models, Animal, Macaca fascicularis, Protein Transport, Oncology, Mechanism of action, Cell culture, Proteolysis, Cancer research, Female, Hepatocyte growth factor, medicine.symptom, medicine.drug

Abstract

Purpose: MET, the receptor for hepatocyte growth factor (HGF), has been implicated in driving tumor proliferation and metastasis. High MET expression is correlated with poor prognosis in multiple cancers. Activation of MET can be induced either by HGF-independent mechanisms such as gene amplification, specific genetic mutations, and transcriptional upregulation or by HGF-dependent autocrine or paracrine mechanisms. Experimental Design/Results: Here, we report on LY2875358, a novel humanized bivalent anti-MET antibody that has high neutralization and internalization activities, resulting in inhibition of both HGF-dependent and HGF-independent MET pathway activation and tumor growth. In contrast to other bivalent MET antibodies, LY2875358 exhibits no functional agonist activity and does not stimulate biologic activities such as cell proliferation, scattering, invasion, tubulogenesis, or apoptosis protection in various HGF-responsive cells and no evidence of inducing proliferation in vivo in a monkey toxicity study. LY2875358 blocks HGF binding to MET and HGF-induced MET phosphorylation and cell proliferation. In contrast to the humanized one-armed 5D5 anti-MET antibody, LY2875358 induces internalization and degradation of MET that inhibits cell proliferation and tumor growth in models where MET is constitutively activated. Moreover, LY2875358 has potent antitumor activity in both HGF-dependent and HGF-independent (MET-amplified) xenograft tumor models. Together, these findings indicate that the mechanism of action of LY2875358 is different from that of the one-armed MET antibody. Conclusions: LY2875358 may provide a promising therapeutic strategy for patients whose tumors are driven by both HGF-dependent and HGF-independent MET activation. LY2875358 is currently being investigated in multiple clinical studies. Clin Cancer Res; 20(23); 6059–70. ©2014 AACR.

Published

2014

15. 2015 White Paper on recent issues in bioanalysis: focus on new technologies and biomarkers (Part 2 - hybrid LBA/LCMS and input from regulatory agencies)

Author

Lin-Zhi Chen, Jan Welink, Ann Lévesque, Timothy V Olah, Jaap Wieling, Stephen Vinter, Natasha Savoie, Olivier Le Blaye, Susan Spitz, Jian Wang, Gustavo Mendes Lima Santos, Mark Bustard, Fabio Garofolo, Leo Kirkovsky, Stephen C. Alley, Sam Haidar, Emma Whale, Hendrik Neubert, Bärbel Witte, Omar F Laterza, Lee Abberley, Nilufer Tampal, Noriko Katori, Brad Ackermann, Julia Heinrich, Surinder Kaur, Michael Skelly, Patricia Brown-Augsburger, Nicola Hughes, and Matthew Szapacs

Subjects

Bioanalysis, Emerging technologies, Clinical Biochemistry, Scientific excellence, Nanotechnology, General Medicine, History, 21st Century, Analytical Chemistry, Biopharmaceutics, Medical Laboratory Technology, Engineering management, White paper, Biopharmaceutical, Humans, Business, General Pharmacology, Toxicology and Pharmaceutics, Biomarkers, Biotechnology

Abstract

The 2015 9th Workshop on Recent Issues in Bioanalysis (9th WRIB) took place in Miami, Florida with participation of over 600 professionals from pharmaceutical and biopharmaceutical companies, biotechnology companies, contract research organizations and regulatory agencies worldwide. It is once again a 5-day week long event – a full immersion bioanalytical week – specifically designed to facilitate sharing, reviewing, discussing and agreeing on approaches to address the most current issues of interest in bioanalysis. The topics covered included both small and large molecules, and involved LCMS, hybrid LBA/LCMS, LBA approaches including the focus on biomarkers and immunogenicity. This 2015 White Paper encompasses recommendations that emerged from the extensive discussions held during the workshop, and is aimed at providing the bioanalytical community with key information and practical solutions on topics and issues addressed, in an effort to advance scientific excellence, improve quality and deliver better regulatory compliance. Due to its length, the 2015 edition of this comprehensive White Paper has been divided into three parts. Part 2 covers the recommendations for hybrid LBA/LCMS and regulatory agencies’ inputs. Part 1 (small molecule bioanalysis using LCMS) and Part 3 (large molecule bioanalysis using LBA, biomarkers and immunogenicity) will be published in volume 7 of Bioanalysis, issues 22 and 24, respectively.

Published

2015

16. Development of a Sensitive and Specific in Situ Hybridization Technique for the Cellular Localization of Antisense Oligodeoxynucleotide Drugs in Tissue Sections

Author

Nancy Goebl, Victor J. Wroblewski, Brian R. Berridge, and Patricia Brown-Augsburger

Subjects

040301 veterinary sciences, Survivin, In situ hybridization, Biology, Toxicology, 01 natural sciences, Inhibitor of Apoptosis Proteins, Pathology and Forensic Medicine, 0403 veterinary science, Mice, Fluorescence microscope, Animals, RNA, Messenger, Molecular Biology, In Situ Hybridization, Fluorescence, Cellular localization, Fluorescent Dyes, Paraffin Embedding, Oligonucleotide, 010401 analytical chemistry, RNA, DNA, 04 agricultural and veterinary sciences, Cell Biology, Oligonucleotides, Antisense, Fluorescence, Molecular biology, 0104 chemical sciences, Repressor Proteins, Macaca fascicularis, Hydrazines, biology.protein, Antibody, Oligomer restriction, Microtubule-Associated Proteins, Fluorescein-5-isothiocyanate

Abstract

A sensitive method has been developed for the identification and assessment of phosphorothioate oligonucleotide accumulation in dosed animal tissues using an in situ hybridization approach, which is both sequence specific yet adaptable to every antisense oligonucleotide (ASO), which has been tested to date. Hybridization is accomplished using a digoxigenin-tailed oligonucleotide probe complementary to the ASO target sequence on routinely processed paraffin sections which have been pretreated with a mild target retrieval solution. The DIG-labeled probe is amplified first with an anti-DIG:FITC antibody conjugate followed by an anti:FITC Alexa 488 antibody, then visualized using FITC epifluorescence microscopy. Fluorescent labeling of ASO drug in tissue sections by this method confirms that H&E basophilia previously observed in dosed tissues represents largely intact ASO. However, the fluorescent method enables a wider assessment of tissue distribution in a variety of tissue types due to increased sensitivity and lower signal to noise than can be obtained through an examination of H&E stained tissue sections alone.

Published

2007

17. Development of an Ion-Pair Reverse-Phase Liquid Chromatographic/Tandem Mass Spectrometry Method for the Determination of an 18-Mer Phosphorothioate Oligonucleotide in Mouse Liver Tissue

Author

Bradley L. Ackermann, Patricia Brown-Augsburger, Rosie Z. Yu, Anthony T. Murphy, Stefan Thibodeaux, and Richard S. Geary

Subjects

Spectrometry, Mass, Electrospray Ionization, Protein mass spectrometry, 010402 general chemistry, Tandem mass spectrometry, 01 natural sciences, High-performance liquid chromatography, Phosphates, Mice, chemistry.chemical_compound, Liquid chromatography–mass spectrometry, Liquid–liquid extraction, Animals, Triethylamine, Chromatography, High Pressure Liquid, Spectroscopy, Chromatography, Phosphorothioate Oligonucleotides, 010401 analytical chemistry, Extraction (chemistry), General Medicine, Oligonucleotides, Antisense, Thionucleotides, Atomic and Molecular Physics, and Optics, 0104 chemical sciences, Liver, chemistry

Abstract

A quantitative method for the determination of a partially modified, 2′-ribose alkoxy 18-mer phosphorothioate oligonucleotide in liver tissue has been developed. A liquid:liquid extraction, ion-pair reverse phase chromatographic separation and tandem mass spectrometry were used to achieve a quantitation range of 125 to 10,000 ng g−1 mouse liver tissue. A total cycle time of 5 min was obtained while maintaining separation of three potential impurities. Separations were performed using a Discovery RP-Amide C16, 100 × 2 mm column packed with 5 μm particles. The separation was facilitated by the use of triethylamine (TEA) and hexafluoroisopropanol (HFIP) as ion-pair agents. The method has subsequently been used for the determination of other phosphorothioate oligonucleotides in support of discovery research.

Published

2005

18. Development and validation of a sensitive, specific, and rapid hybridization-ELISA assay for determination of concentrations of a ribozyme in biological matrices

Author

Patricia Brown-Augsburger, Jennifer A. Lockridge, Dimple Kamboj, Kathleen M. Hillgren, Xin Min Yue, and James McSwiggen

Subjects

Male, Analyte, Clinical Biochemistry, Pharmaceutical Science, Enzyme-Linked Immunosorbent Assay, Sensitivity and Specificity, Analytical Chemistry, Microtiter plate, Capillary electrophoresis, Drug Discovery, Animals, RNA, Catalytic, Spectroscopy, Gel electrophoresis, Binding Sites, Chromatography, Base Sequence, Dose-Response Relationship, Drug, biology, Oligonucleotide, Chemistry, Ribozyme, Nucleic Acid Hybridization, Standard curve, Macaca fascicularis, biology.protein, Nucleic acid, Female

Abstract

Ribozymes are RNA or modified RNA polymers capable of catalyzing cleavage reactions in target strands RNA, and are under development as human therapeutics. Previous methods used for quantitation of nucleic acid polymers in serum or plasma required extraction of the polymer followed by capillary electrophoresis, HPLC, or gel electrophoresis. These methods are time consuming and lack sensitivity. A bioanalytical method has been developed that does not require extraction of the ribozyme analyte from serum. This technique relies on hybridization of the ribozyme molecule to two complementary biotin and digoxigenin labeled oligonucleotide probes. Serum containing the ribozyme is mixed with the labeled probes, and the mixture is heated at 75 °C for 5 min to disrupt the ribozyme secondary structure. Samples are then cooled to permit probe annealing and are added to a streptavidin-coated 96-well plate. The bound complex is detected with an anti-digoxigenin alkaline phosphatase (AP) conjugate using PNPP ( p -nitrophenyl phosphate) as a substrate. The amount of colored product is measured on a microtiter plate reader at a wavelength of 405 nm. Concentrations of unknown ribozyme samples are estimated based on a standard curve (0.37–270 ng/ml) prepared in serum. The validated lower and upper limits of quantification are 5.0 and 120 ng/ml, respectively. The assay can be completed in approximately 5 h and does not require extraction procedures or electrophoretic/chromatographic separation. It is therefore a simple, sensitive and rapid technique. This assay has been validated and has been used for quantitation of serum levels of the HEPTAZYME™ ribozyme in mouse, monkey, and human pharmacokinetic studies.

Published

2004

19. Sensitive RIA for the Specific Determination of Insulin Lispro

Author

Ronald R. Bowsher, Ronald E. Chance, William E. Legan, James R. Woodworth, Renee A. Lynch, Patricia Brown-Augsburger, and Paula F. Santa

Subjects

Antiserum, medicine.medical_specialty, endocrine system diseases, biology, Chemistry, Insulin, medicine.medical_treatment, digestive, oral, and skin physiology, Biochemistry (medical), Clinical Biochemistry, nutritional and metabolic diseases, Insulin analog, Radioimmunoassay, Endocrinology, Internal medicine, biology.protein, medicine, Insulin lispro, Antibody, Immunoadsorption, hormones, hormone substitutes, and hormone antagonists, Proinsulin, medicine.drug

Abstract

Insulin lispro is an insulin analog in which the primary sequence has been altered by the inversion of amino acids B28 and B29. To date, it has not been possible to specifically measure insulin lispro in the presence of endogenous insulin because of the high degree of homology between these peptides. However, the specific determination of insulin lispro offers advantages over quantifying total concentrations of immunoreactive insulin. We therefore immunized guinea pigs and screened for antibodies with increased affinity and selectivity for insulin lispro. We prepared a monospecific antiserum by a novel immunoadsorption strategy using despentapeptide insulin. The antiserum was used to develop a competitive RIA for insulin lispro. The RIA has a low limit of quantification (17.2 pmol/L); has no interference from insulin, proinsulin, or C-peptide; and has interassay CVs of 2.6–13.4%. The new RIA is useful for measuring serum concentrations of insulin lispro.

Published

1999

20. Functional domains on elastin and microfibril-associated glycoprotein involved in elastic fibre assembly

Author

Thomas J. Broekelmann, Patricia Brown-Augsburger, Joel Rosenbloom, and Robert P. Mecham

Subjects

Blotting, Western, Fluorescent Antibody Technique, Matrix (biology), Fibrillins, Biochemistry, Desmosine, Extracellular matrix, Immunoglobulin Fab Fragments, Contractile Proteins, Tropoelastin, Animals, Molecular Biology, Cells, Cultured, chemistry.chemical_classification, Extracellular Matrix Proteins, integumentary system, biology, Microfilament Proteins, Antibodies, Monoclonal, Cell Biology, Elastic Tissue, Elastin, Extracellular Matrix, Cartilage, chemistry, biology.protein, Biophysics, Cattle, RNA Splicing Factors, Microfibril, Glycoprotein, Fibrillin, Immunostaining, Research Article

Abstract

Studies in vitro suggest that the C-terminus of tropoelastin mediates elastin polymerization through an interaction with microfibril-associated proteins. In this study we have used cultured auricular chondrocytes as a model system to examine whether this interaction is critical for elastic fibre formation in vivo. Auricular chondrocytes, which deposit an abundant elastic fibre matrix, were cultured in the presence of Fab fragments of antibodies directed against the C-terminus (CTe) or an N-terminal domain (ATe) of tropoelastin. Immunofluorescent staining of the extracellular matrix deposited by the cells showed that the CTe antibody inhibited the deposition of elastin without affecting microfibril structure. Cells grown under identical conditions in the presence of ATe, however, formed fibres that stained normally for both elastin and microfibril proteins. Chondrocytes cultured in the presence of microfibril-associated glycoprotein (MAGP):21–35, an antibody directed against a domain near the N-terminus of MAGP, did not organize tropoelastin into fibres. However, immunostaining for MAGP and fibrillin revealed normal microfibrils. In agreement with the immunofluorescence staining patterns, fewer elastin-specific cross-links, indicative of insoluble elastin, were detected in the extracellular matrix of cells cultured in the presence of CTe. The medium from these cultures, however, contained more soluble elastin, consistent with an antibody-induced alteration of elastin assembly but not its synthesis. Northern analysis of antibody-treated and control cultures substantiated equivalent levels of tropoelastin mRNA. These results confirm that the C-terminus of tropoelastin interacts with microfibrils during the assembly of elastic fibres. Further, the results suggest that the interaction between tropoelastin and microfibrils might be mediated by a domain involving the N-terminal half of MAGP.

Published

1996

21. Biosynthesis of Surfactant Protein D

Author

Patricia Brown-Augsburger, Kevin Rust, Donald Chang, and Edmond C. Crouch

Subjects

biology, Lysyl hydroxylase, Collagen helix, Cell Biology, Tunicamycin, Biochemistry, Dithiothreitol, chemistry.chemical_compound, Protein structure, chemistry, biology.protein, Secretion, Protein disulfide-isomerase, Molecular Biology, Cysteine

Abstract

Surfactant protein D (SP-D) is preferentially secreted as dodecamers consisting of four collagenous trimers cross-linked by disulfide bonds. In these studies, we examined the biosynthesis of wild-type rat SP-D (RrSP-D) and selected mutants by stably transfected CHO-K1 cells to determine the roles of a conserved N-linked oligosaccharide, the collagen helix, and interchain disulfide bonds in SP-D assembly and secretion. The major intracellular form of RrSP-D accumulated in the RER as complexes containing up to four trimeric subunits. Disulfide cross-link formation and RrSP-D secretion were selectively inhibited by 2,2'-dipyridyl, an inhibitor of prolyl and lysyl hydroxylase, and by 2 mM dithiothreitol, but unaffected by tunicamycin or elimination of the consensus sequence for glycosylation at Asn70. Although mutants with serine substituted for Cys15 and Cys20 (RrSP-Dser15/20) are secreted as trimeric subunits, proteins with single cysteine substitutions were retained in the cell. Surprisingly, the secretion of RrSP-Dser15/20 was unaffected by 2,2'-dipyridyl. These studies strongly suggest that the most important and rate-limiting step for the secretion of SP-D involves the association of cross-linked trimeric subunits to form dodecamers stabilized by specific inter-subunit disulfide cross-links. Interference with collagen helix formation prevents secretion by interfering with efficient disulfide cross-linking of the NH2-terminal domain.

Published

1996

22. Site-directed Mutagenesis of Cys-15 and Cys-20 of Pulmonary Surfactant Protein D

Author

Howard G. Welgus, Kevin Rust, Donald Chang, Kevan L. Hartshorn, Patricia Brown-Augsburger, Catherine J. Fliszar, and Edmond C. Crouch

Subjects

Chinese hamster ovary cell, Surfactant protein D, Hemagglutinin (influenza), Cell Biology, Biology, Biochemistry, Serine, Protein structure, biology.protein, Pulmonary Surfactant-Associated Protein D, Site-directed mutagenesis, Molecular Biology, Cysteine

Abstract

Surfactant protein D (SP-D) molecules are preferentially assembled as dodecamers consisting of trimeric subunits associated at their amino termini. The NH2-terminal sequence of each monomer contains two conserved cysteine residues, which participate in interchain disulfide bonds. In order to study the roles of these residues in SP-D assembly and function, we employed site-directed mutagenesis to substitute serine for cysteine 15 and 20 in recombinant rat SP-D (RrSP-D), and have expressed the mutant (RrSP-Dser15/20) in Chinese hamster ovary (CHO-K1) cells. The mutant, which was efficiently secreted, bound to maltosyl-agarose, but unlike RrSP-D, was assembled exclusively as trimers. The constituent monomers showed a decreased mobility on SDS-polyacrylamide gel electrophoresis resulting from an increase in the size and sialylation of the N-linked oligosaccharide at Asn-70. Although RrSP-Dser15/20 contained a pepsin-resistant triple helical domain, it showed a decreased Tm, and acquired susceptibility to proteolytic degradation. Like RrSP-D, RrSP-Dser15/20 bound to the hemagglutinin of influenza A. However, it showed no viral aggregation and did not enhance the binding of influenza A to neutrophils (PMN), augment PMN respiratory burst, or protect PMNs from deactivation. These studies indicate that amino-terminal disulfides are required to stabilize dodecamers, and support our hypothesis that the oligomerization of trimeric subunits contributes to the anti-microbial properties of SP-D.

Published

1996

23. Identification of an Elastin Cross-linking Domain That Joins Three Peptide Chains

Author

Thomas J. Broekelmann, Clarina Tisdale, Carolyn Sloan, Robert P. Mecham, and Patricia Brown-Augsburger

Subjects

Tropoelastin, biology, Lysine, Proteolytic enzymes, Lysyl oxidase, Cell Biology, Biochemistry, Desmosine, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, biology.protein, medicine, Molecular Biology, Peptide sequence, Elastin, Elastic fiber

Abstract

The alignment of elastin molecules in the mature elastic fiber was investigated by purifying and sequencing cross-link-containing peptides generated by proteolytic digestion of incompletely cross-linked insoluble elastin. Peptides of interest were purified by reverse phase and size exclusion high performance liquid chromatography and characterized by amino acid analysis and protein sequencing. One peptide, consisting of the cross-linking domain encoded by exon 10, contained a modified lysine residue that had not condensed to form a polyfunctional cross-link. Although this domain contains the characteristic paired lysine residues found in other cross-linking domains of elastin, protein sequence analysis indicated that the first but not the second lysine had been oxidized by lysyl oxidase. This finding suggests that lysine residues in an individual cross-linking domain may not have equal susceptibility to oxidation by lysyl oxidase. In a second peptide, we found that a major cross-linking site in elastin is formed through the association of sequences encoded by exons 10, 19, and 25 and that the three chains are joined together by one desmosine and two lysinonorleucine cross-links. Past structural studies and computer modeling predict that domains 19 and 25 are linked by a desmosine cross-link, while domain 10 bridges domains 19 and 25 through lysinonorleucine cross-links. These findings, together with the high degree of sequence conservation for these three domains, suggest an important function for these regions of the molecule, possibly nucleating the aggregation and polymerization of tropoelastin monomers in the developing elastic fiber.

Published

1995

24. Microfibril-associated glycoprotein binds to the carboxyl-terminal domain of tropoelastin and is a substrate for transglutaminase

Author

Robert P. Mecham, L Mecham, E G Cleary, Patricia Brown-Augsburger, William R. Abrams, Mark Gibson, J. Rosenbloom, Thomas J. Broekelmann, and Robert W. Mercer

Subjects

chemistry.chemical_classification, Signal peptide, integumentary system, Tropoelastin, biology, Elastic fiber assembly, Cell Biology, Biochemistry, medicine.anatomical_structure, chemistry, biology.protein, Biophysics, medicine, Microfibril, Glycoprotein, Molecular Biology, Fibrillin, Elastin, Elastic fiber

Abstract

Microfibril-associated glycoprotein (MAGP) is an integral component of microfibrillar structures that play a critical role in the organization of elastic fibers in the extracellular matrix. To study possible molecular interactions between MAGP and other elastic fiber components, we have generated native MAGP using a baculovirus expression system and tested its ability to associate with tropoelastin and fibrillin. MAGP produced by SF9 cells underwent processing similar to the mammalian protein, including correct cleavage of the signal peptide and sulfation of tyrosine residues. When tested in solid-phase binding assays, native MAGP specifically bound to tropoelastin but not fibrillin-1. Binding to tropoelastin was divalent cation-independent and was completely blocked by reduction and alkylation of either protein. Antibody inhibition studies indicated that the carboxyl terminus of tropoelastin mediated its interaction with MAGP. In addition to binding to elastin, MAGP was also a substrate for transglutaminase, which might explain its propensity to form high molecular weight aggregates that cannot be dissociated with reduction or denaturation. Together, the results of this study provide new insights into the functional relationship between microfibrillar proteins and have important implications for understanding elastic fiber assembly.

Published

1994

25. Elastic Fibre Assembly: Macromolecular Interactions

Author

Mark Gibson, Robert P. Mecham, Patricia Brown-Augsburger, Thomas J. Broekelmann, and Elaine C. Davis

Subjects

integumentary system, Tropoelastin, biology, Fibrillins, macromolecular substances, Plasma protein binding, Desmosine, Cell biology, Extracellular matrix, chemistry.chemical_compound, chemistry, biology.protein, Binding site, Elastin, Fibrillin

Abstract

To investigate the mechanisms behind elastic fibre assembly, we studied the molecular interactions between elastin and microfibrillar components using solid-phase binding assays. Fibrillin 1, purified from tissue using reductive-saline extraction, showed no binding to microfibril-associated glycoprotein (MAGP) or tropoelastin. MAGP, however, was found to bind specifically to tropoelastin in a divalent-cation independent manner. Antibody inhibition studies indicated that the C-terminus of tropoelastin defined the interactive site with MAGP. MAGP and fibrillin were also substrates for transglutaminase, which may provide an important mechanism for stabilizing microfibrillar structure. In other studies we found that a major cross-linking region in elastin is formed through the association of domains encoded by exons 10, 19 and 25 of tropoelastin and that the three chains are joined together by one desmosine and two lysinonorleucine cross-links.

Published

2007

26. Anabolic and catabolic bone effects of human parathyroid hormone (1-34) are predicted by duration of hormone exposure

Author

Elwood C Black, Janet M. Hock, R.L. Cain, Julie Satterwhite, Patricia Brown-Augsburger, Charles A. Frolik, and Masahiko Sato

Subjects

Male, endocrine system, medicine.medical_specialty, Histology, Anabolism, Physiology, Endocrinology, Diabetes and Metabolism, Injections, Subcutaneous, Osteoporosis, Cmax, Parathyroid hormone, Bone remodeling, Phosphates, Rats, Sprague-Dawley, Pharmacokinetics, Internal medicine, Medicine, Animals, Humans, Dose-Response Relationship, Drug, Tibia, business.industry, Area under the curve, medicine.disease, Peptide Fragments, Rats, Endocrinology, Parathyroid Hormone, Calcium, Bone Remodeling, business, hormones, hormone substitutes, and hormone antagonists, Hormone

Abstract

Parathyroid hormone (PTH)(1-34), given once daily, increases bone mass in a variety of animal models and humans with osteoporosis. However, continuous PTH infusion has been shown to cause bone loss. To determine the pharmacokinetic profile of PTH(1-34) associated with anabolic and catabolic bone responses, PTH(1-34) pharmacokinetic and serum biochemical profiles were evaluated in young male rats using dosing regimens that resulted in either gain or loss of bone mass. Once-daily PTH(1-34) or 6 PTH(1-34) injections within 1 h, for a total daily dose of 80 microg/kg, induced equivalent increases in proximal tibia bone mass. In contrast, 6 PTH(1-34) injections/day over 6 h for a total dose of 80 microg/kg/day or 3 injections/day over 8 h for a total of 240 microg/kg/day decreased tibia bone mass. The PTH(1-34) pharmacokinetics of the different treatment regimens were distinctive. The magnitude of the maximum serum concentrations (Cmax) of PTH(1-34) and area under the curve (AUC) did not predict the catabolic bone outcome. Compared to the anabolic pharmacokinetic profile of a transient increase in PTH(1-34) with rapid decreases in serum calcium and phosphate, the catabolic regimen was associated with PTH(1-34) concentrations remaining above baseline values during the entire 6-h dosing period with a trend toward an increase in serum calcium and a prolonged decrease in phosphate. The pharmacokinetic profiles suggest that the anabolic or catabolic response of bone to PTH(1-34) is determined primarily by the length of time each day that serum concentrations of PTH(1-34) remain above baseline levels of endogenous PTH and only secondarily by the Cmax or AUC of PTH(1-34) achieved.

Published

2003

27. Demonstrating the intrinsic ion channel activity of virally encoded proteins

Author

Marie L. Kelly, James A. Cook, Lawrence H. Pinto, Michele C. Smith, Patricia Brown-Augsburger, and Beverly A. Heinz

Subjects

Viral ion channel, Time Factors, Rhinovirus, viruses, Biophysics, Biology, medicine.disease_cause, Biochemistry, Models, Biological, Virus, Ion Channels, Viral Matrix Proteins, 03 medical and health sciences, Structural Biology, Genetics, Influenza A virus, medicine, Animals, Humans, Molecular Biology, 030304 developmental biology, Ions, 0303 health sciences, Dose-Response Relationship, Drug, 030302 biochemistry & molecular biology, Cell Biology, Orthomyxoviridae, Virology, Endogenous channel, 3. Good health, Cell biology, Ion channel activity, Influenza virus

Abstract

This review summarizes the types of evidence that can be invoked in order to demonstrate that a virally encoded protein possesses ion channel activity that is intrinsic to the life cycle of the virus. Ion channel activity has been proposed to be a key step in the life cycle of influenza virus, and the protein responsible for this activity has been proposed to be the M2 protein encoded by the virus. This review contrasts the evidence supporting the conclusion that the A/M2 protein of influenza A virus has intrinsic ion channel activity with the evidence that the 3AB protein encoded by the human rhinovirus possesses intrinsic ion channel activity.

Published

2003