Your search keyword '"Jou-Ku Chung"' showing total 19 results

1. Biodistribution of Idursulfase Formulated for Intrathecal Use (Idursulfase-IT) in Cynomolgus Monkeys after Intrathecal Lumbar Administration.

Author

Jou-Ku Chung, Eilish Brown, Bob Crooker, Kathleen J Palmieri, and Thomas G McCauley

Subjects

Medicine, Science

Abstract

Enzyme replacement therapy with intravenous idursulfase (recombinant iduronate-2-sulfatase) is approved for the treatment of Hunter syndrome. Intravenous administration does not, however, treat the neurological manifestations, due to its low central nervous system bioavailability. Using intrathecal-lumbar administration, iduronate-2-sulfatase is delivered directly to the central nervous system. This study investigates the central nervous system biodistribution of intrathecal-lumbar administered iduronate-2-sulfatase in cynomolgus monkeys. Twelve monkeys were administered iduronate-2-sulfatase in one 30 mg intrathecal-lumbar injection. Brain, spinal cord, liver, and kidneys were collected for iduronate-2-sulfatase concentration (measured by an enzyme linked immunosorbent assay) and enzyme activity measurement (via a method utilizing 4-methylumbelliferyl-α-iduronate-2-sulfate) at 1, 2, 5, 12, 24, and 48 hours following administration. The tissue enzyme linked immunosorbent assay confirmed iduronate-2-sulfatase uptake to the brain, spinal cord, kidneys, and liver in a time-dependent manner. In spinal cord and brain, iduronate-2-sulfatase appeared as early as 1 hour following administration, and peak concentrations were observed at ~2 and ~5 hours. Iduronate-2-sulfatase appeared in liver and kidneys 1 hour post intrathecal-lumbar dose with peak concentrations between 5 and 24 hours. Liver iduronate-2-sulfatase concentration was approximately 10-fold higher than kidney. The iduronate-2-sulfatase localization and enzyme activity in the central nervous system, following intrathecal administration, demonstrates that intrathecal-lumbar treatment with iduronate-2-sulfatase may be considered for further investigation as a treatment for Hunter syndrome patients with neurocognitive impairment.

Published

2016

2. Pharmacokinetics and bioavailability of a therapeutic enzyme (idursulfase) in cynomolgus monkeys after intrathecal and intravenous administration.

Author

Hongsheng Xie, Jou-Ku Chung, Mary Ann Mascelli, and Thomas G McCauley

Subjects

Medicine, Science

Abstract

Intravenous enzyme replacement therapy with iduronate-2-sulfatase is an approved treatment for Hunter syndrome, however, conventional intravenous delivery cannot treat the neurologic manifestations of the disease due to its limited central nervous system penetration. Intrathecal administration of iduronate-2-sulfatase for delivery to the central nervous system is currently under investigation. The objective of this study was to evaluate the pharmacokinetics of idursulfase in the central nervous system of cynomolgus monkeys (Macaca fasicularis) after intravenous and intrathecal administration. Twenty-seven monkeys, treatment-naïve to enzyme replacement therapy, were placed into 4 groups according to body weight: Group 1 was administered 0.5 mg/kg idursulfase intravenously, Groups 2-4 were administered an intrathecal formulation (1-, 10-, and 30-mg doses). Blood samples and cerebrospinal fluid (sampled at the cisterna magna or lumbar level) were collected at the same time points for 72 hours post dosing. Following intravenous administration, a high maximum serum concentration and rapid distribution of iduronate-2-sulfatase out of the central compartment were observed (elimination half-life: 4.3 hours). Iduronate-2-sulfatase exposure in the cerebrospinal fluid was limited, suggesting intravenous administration provided minimal penetration of the blood-brain barrier. Following intrathecal administration, a high maximum observed concentration was immediately noted and elimination half-life ranged between 7.8-10 hours and 5.9-6.7 hours (cisterna magna and lumbar sampling, respectively). Cerebrospinal fluid pharmacokinetic profiles at different doses of iduronate-2-sulfatase were similar and the dose/exposure relationship was proportional. After intrathecal administration, movement of iduronate-2-sulfatase from cerebrospinal fluid to serum was observed (systemic bioavailability was 40-83%). The clear penetration of iduronate-2-sulfatase into the cerebrospinal fluid and the dose response suggest that intrathecal delivery of iduronate-2-sulfatase may be suitable for treating the central nervous system manifestations associated with Hunter syndrome.

Published

2015

3. Initial Results from a Phase 1 Single Ascending Dose Clinical Trial of STAR-0215, an Investigational Long-Acting Monoclonal Antibody Plasma Kallikrein Inhibitor for Hereditary Angioedema (HAE), in Healthy Subjects Followed for at Least 3 Months

Author

Christopher Morabito, Chris Stevens, Jou-Ku Chung, Rafif Dagher, Pradeep Bista, Kristine Bernard, Pamela Gustafson, Michele Gunsior, and Andy Nichols

Subjects

Immunology, Immunology and Allergy

Published

2023

4. Abstract 1137: Determination of a recommended Phase 2 dose (RP2D) for SRF388, a first-in-class IL-27-blocking antibody, in patients with advanced solid tumors

Author

Jonathan A. Hill, Kerry F. White, Matthew Rausch, Jou-Ku Chung, Amita Patnaik, Aung Naing, Daniel Morgensztern, Charlene M. Mantia, Nizar M. Tannir, Lon S. Smith, Beth Bowers, Alex Alika, Lauren C. Harshman, and Benjamin H. Lee

Subjects

Cancer Research, Oncology

Abstract

SRF388 is a first-in-class, anti-IL-27 antibody developed to enhance immune responses within the tumor microenvironment. Preclinical studies have demonstrated that IL-27 pathway blockade can inhibit tumor growth in mouse models of liver cancer and lung cancer metastases. There is also evidence that IL-27 pathway inhibition is accompanied by activation of the innate and adaptive arms of the immune system. An ongoing Phase I trial has shown good tolerability at all dose levels tested and preliminary monotherapy antitumor activity with SRF388 (NCT04374877). Here, we describe the preclinical and clinical data used to select a RP2D and characterize cytokine and chemokine changes observed in patients after treatment with SRF388. To guide selection of the RP2D, the relationship between maximal effective dose (MaxED), pharmacokinetics (PK), and whole blood inhibition of IL-27-mediated phosphorylation of STAT1 by SRF388 was evaluated in a mouse model of liver cancer. The concentration of SRF388 associated with optimal antitumor activity was ~20-fold above the concentration needed for complete inhibition (> 90%) of whole blood phosphorylated STAT1 (pSTAT1). These PK and activity relationships were also defined in patients during the dose-escalation phase of the trial and integrated with safety and efficacy data to select a monotherapy RP2D. In patients, PK were linear, no dose-limiting toxicities were reported, complete pSTAT1 inhibition was achieved throughout the first cycle at 0.3 mg/kg, and 1 patient experienced a confirmed partial response per RECIST version 1.1 at a dose of 10 mg/kg. In the MaxED mouse model, the area under the concentration versus time curve (AUC) associated with significant antitumor activity was 1720 day*μg/mL. In patients, the corresponding target AUC was achieved clinically at 10 mg/kg after a single dose of SRF388. Changes in the concentration of several serum cytokines and chemokines were observed after SRF388 treatment including an increase in IL-27, a phenomenon described for other anti-cytokine antibodies due to altered clearance of the cytokine-antibody complex. Changes in a subset of other serum cytokines/chemokines correlated with a reduction in target lesion size. Taken together, these data support the selection of a monotherapy RP2D of 10 mg/kg intravenously every 4 weeks for SRF388. These data highlight how complementary strategies utilizing preclinical and clinical biomarker evaluations can be employed to establish a monotherapy RP2D and assess biological activity of a first-in-class anti-cytokine antibody, SRF388, for patients with cancer. Citation Format: Jonathan A. Hill, Kerry F. White, Matthew Rausch, Jou-Ku Chung, Amita Patnaik, Aung Naing, Daniel Morgensztern, Charlene M. Mantia, Nizar M. Tannir, Lon S. Smith, Beth Bowers, Alex Alika, Lauren C. Harshman, Benjamin H. Lee. Determination of a recommended Phase 2 dose (RP2D) for SRF388, a first-in-class IL-27-blocking antibody, in patients with advanced solid tumors [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 1137.

Published

2022

5. Results of a phase 1 study of SRF388, a first-in-human, first-in-class, high-affinity anti-IL-27 antibody in advanced solid tumors

Author

Lon Smith, Amita Patnaik, Charlene Mantia, Jou-Ku Chung, Beth Bowers, Daniel Morgensztern, Kerry White, Lauren C. Harshman, Aung Naing, Jonathan A. Hill, Gaia Sciaranghella, Benjamin H. Lee, Toni K. Choueiri, and Nizar M. Tannir

Subjects

Cancer Research, biology, business.industry, medicine.medical_treatment, EBI3, First in human, Immune checkpoint, Proinflammatory cytokine, Cytokine, Oncology, TIGIT, Cancer research, medicine, biology.protein, Antibody, Receptor, business

Abstract

2551 Background: IL-27 is an immunosuppressive cytokine, consisting of two subunits p28 and EBI3, that upregulates immune checkpoint receptors (eg, PD-L1, TIGIT) and downregulates proinflammatory cytokines such as IFNγ, TNFα, and IL-17. SRF388 is a first-in-class, fully human IgG1 antibody to IL-27 that blocks the interaction between IL-27 and its receptor, thereby promoting immune activation in the tumor microenvironment. The IL-27 pathway is activated in hepatocellular carcinoma (HCC) and renal cell carcinoma (RCC), and high circulating levels of EBI3 are associated with inferior outcomes in both. Circulating EBI3 levels may serve as a predictive biomarker of SRF388 activity. Methods: Patients with advanced solid tumors refractory to standard therapy were enrolled in a phase 1 dose-escalation study (accelerated single patient followed by standard 3+3) to establish the preliminary safety of SRF388 as a monotherapy and to identify a dose suitable for expansion (NCT04374877). SRF388 was administered intravenously every 4 weeks. Tumor response was assessed by RECIST v1.1. SRF388 pharmacokinetic (PK) and pharmacodynamic (PD) [phospho-STAT (pSTAT) inhibition] analyses were performed. Results: As of January 26, 2021, 12 patients have received SRF388 at doses ranging from 0.003 to 10 mg/kg with 2 patients undergoing intra-patient dose escalation. Median age was 68 years, 67% were female, and ECOG PS was 0/1 (42%/58%). Median number of prior therapies was 2 (range 1–9), and 75% were anti-PD-(L)1 experienced (n = 9). The only treatment-related adverse events observed across dose levels were low-grade fatigue (n = 1, 8%), nausea (n = 1, 8%) and excess salivation (n = 1, 8%). No dose-limiting toxicities (DLTs) or ≥ Grade 3 related toxicity have occurred. Mean time on study is 12.5 weeks (range 4–40). One patient with RCC who received prior anti-PD-1 has prolonged stable disease for > 9 months. SRF388 PK are linear with estimated T1/2 ranging from 6–19 days. There is evidence of accumulation and no anti-drug antibody development to date. Maximal inhibition of the IL-27 signaling pathway as measured by > 90% pSTAT inhibition in whole blood was achieved starting at 0.3 mg/kg. Given combined evidence of near-complete pathway inhibition and preclinical human equivalent dose modeling projecting biologically active doses, additional slots were opened for RCC and HCC starting at 1 mg/kg. Conclusions: Preliminary results of IL-27 pathway blockade with a first-in-class therapeutic demonstrates that SRF388 is well tolerated at doses that achieve maximal inhibition of downstream pSTAT signaling through the dosing period. Expansions are planned in HCC and RCC. Updated data including the recommended phase 2 dose, clinical outcomes, PK/PD and correlative analyses will be presented. Clinical trial information: NCT04374877.

Published

2021

6. Results of a first-in-human phase I study of SRF231, a fully human, high-affinity anti-CD47 antibody

Author

Muralidhar Beeram, Demi Niforos, Anna Spreafico, Julia Lester, Alison M. Paterson, Amita Patnaik, Alison M. Schram, Beth Bowers, Marco A. J. Iafolla, Marisa O. Peluso, Alison M. O'Neill, and Jou-Ku Chung

Subjects

Cancer Research, Multiple cancer, biology, business.industry, CD47, First in human, Transmembrane protein, Phase i study, Cell biology, 03 medical and health sciences, Immune recognition, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, biology.protein, Medicine, Antibody, business, 030215 immunology

Abstract

3064 Background: CD47 is a transmembrane protein that acts as a “Don’t Eat Me” signal to evade immune recognition. It is overexpressed in multiple cancer subtypes and is associated with poor prognosis. SRF231 is an investigational, fully human, high-affinity CD47-targeting antibody that delivers an activating signal to myeloid cells and displays favorable preclinical characteristics regarding its receptor occupancy/tumor exposure/efficacy relationship. Methods: In a Phase 1 study, SRF231-101 (NCT03512340), patients with advanced solid and hematologic malignancies who had failed standard therapy were enrolled in dose escalation cohorts (accelerated single-patient followed by standard 3+3) to establish the preliminary safety of SRF231 as a monotherapy and identify a dose and schedule suitable for expansion. In addition to collection of safety data, clinical outcomes were evaluated based on Response Evaluation Criteria in Solid Tumors (RECIST v1.1) and SRF231 pharmacokinetic (PK) and pharmacodynamic (receptor occupancy) analyses were performed. Results: As of January 11, 2020, a total of 46 patients were enrolled, 25 in every-3-week intravenous (IV) dosing schedules and 21 in weekly IV dosing schedules. Weekly dosing schedules also explored the use of a 1.0 mg/kg initiation dose. Other than one patient with recurrent follicular lymphoma, all patients had recurrent/refractory solid tumors. The most common treatment emergent adverse events across dosing schedules were low-grade fatigue (43%), headache (35%), and pyrexia (30%). On every-3-week dosing schedules, 2 dose-limiting toxicities (DLTs) were observed: Grade 3 febrile neutropenia and Grade 3 hemolysis, both at a 12.0 mg/kg dose level. On weekly dosing schedules, 3 DLTs were observed: Grade 4 thrombocytopenia (6.0 mg/kg), Grade 4 amylase and lipase increased (4.0 mg/kg with initiation dose), and Grade 3 fatigue (4.0 mg/kg). The maximum tolerated dose was 9.0 mg/kg on an every-3-week and 4.0 mg/kg on a weekly schedule. Receptor occupancy was maintained at > 90% throughout the dosing period with a 4.0 mg/kg weekly dose schedule. Out of 37 patients who were response evaluable by RECIST, there were no complete or partial responders, although prolonged stable disease has been observed. Conclusions: Preliminary data from a Phase 1 study of SRF231, an anti-CD47 antibody, demonstrate that SRF231 may be administered safely and doses of 4.0 mg/kg weekly maintain > 90% receptor occupancy throughout the dosing period. Updated safety data, clinical outcomes, and PK/pharmacodynamic data will be presented. Clinical trial information: NCT03512340 .

Published

2020

7. Ocular Distribution and Pharmacokinetics of Lifitegrast in Pigmented Rabbits and Mass Balance in Beagle Dogs

Author

Matthew Hunt, Devin Welty, Elizabeth Spencer, Thomas McCauley, and Jou-Ku Chung

Subjects

0301 basic medicine, medicine.medical_specialty, Lifitegrast, genetic structures, Administration, Topical, Phenylalanine, Beagle, Cornea, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Dogs, Pharmacokinetics, Ophthalmology, medicine, Distribution (pharmacology), Animals, Pharmacology (medical), Sulfones, Balance (ability), Pharmacology, business.industry, Volume 2: Drug Delivery, Dry Eye-Ocular Surface, Retina and Ocular Safety Studies, eye diseases, 030104 developmental biology, chemistry, 030221 ophthalmology & optometry, Dry Eye Syndromes, Female, sense organs, Rabbits, Ophthalmic Solutions, business

Abstract

Lifitegrast is approved in the United States for the treatment of dry eye disease (DED). We assessed lifitegrast's ocular distribution/pharmacokinetic profile in rabbits, andFemale pigmented rabbits received a single topical ocular dose of lifitegrast (Formulation No. 1, n = 25; No. 2, n = 25) per eye twice daily (target, 1.75 mg/eye/dose). Blood/ocular tissues were collected on day 5. Beagle dogs received single intravenous (n = 10; target, 3 mg, 262 μCi/animal) and ocular (n = 8, target, 3 mg, 30 μCi/eye) doses ofIn rabbits, lifitegrast CHigh exposure of lifitegrast in rabbit ocular anterior segment tissues and low exposure in posterior segment tissues/plasma suggests that lifitegrast reaches target tissues for DED treatment, with low potential for off-target systemic/ocular effects. Excretion of unchanged

Published

2017

8. Whole Body and CNS Biodistribution of rhHNS in Cynomolgus Monkeys after Intrathecal Lumbar Administration: Treatment Implications for Patients with MPS IIIA

Author

Thomas McCauley, Jou-Ku Chung, Kathleen Palmieri, Amir S. Youssef, and Luying Pan

Subjects

Central Nervous System, Male, 0301 basic medicine, positron emission tomography, mucopolysaccharidosis III type A, Sanfilippo syndrome, Pharmacology, lcsh:Chemistry, Mucopolysaccharidosis III, 0302 clinical medicine, Tissue Distribution, lcsh:QH301-705.5, Injections, Spinal, Spectroscopy, lysosomal disorder, General Medicine, Enzyme replacement therapy, Recombinant Proteins, Computer Science Applications, medicine.anatomical_structure, intrathecal administration, Administration, Intravenous, Sulfatases, pharmacokinetics, enzyme replacement therapy, Biodistribution, Central nervous system, Grey matter, Blood–brain barrier, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, recombinant human heparan N-sulfatase, cerebral spinal fluid, Pharmacokinetics, medicine, Animals, Humans, Physical and Theoretical Chemistry, Molecular Biology, business.industry, Organic Chemistry, medicine.disease, Disease Models, Animal, Macaca fascicularis, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, business, 030217 neurology & neurosurgery

Abstract

Mucopolysaccharidosis III type A (MPS IIIA; Sanfilippo syndrome), a genetic lysosomal disorder causing a deficiency of heparan N-sulfatase (HNS), leads to progressive cognitive decline from an early age. An effective enzyme replacement therapy (ERT) for MPS IIIA requires central nervous system (CNS) biodistribution. Recombinant human heparan N-sulfatase (rhHNS), an investigatory ERT for MPS IIIA, has been formulated for intrathecal (IT) administration since intravenous (IV) administration cannot cross the blood brain barrier (BBB) in sufficient amounts to have a therapeutic effect. In this study, systemic and CNS distribution of rhHNS in cynomolgus monkeys following IV and IT administration was evaluated by quantitation of rhHNS in serum, cerebral spinal fluid (CSF) and various tissues, and positron emission tomography (PET) imaging of live animals. Following IV administration, rhHNS levels were low to non-detectable in the CSF, and systemic clearance was rapid (≤2 h). With IT administration, rhHNS was observable in CNS tissues in ≤1 h, with varying Tmax (1–24 h). Appreciable systemic distribution was observed up to 7 days. This provides evidence that in this animal model, intrathecal administration of rhHNS delivers the replacement enzyme to therapeutically relevant tissues for the treatment of Sanfilippo Syndrome type A. Penetration into grey matter and cortex was 3–4 times greater than concentrations in white matter and deeper parenchymal regions, suggesting some limitations of this ERT strategy.

Published

2017

9. Development and verification of a pharmacokinetic model to optimize physiologic replacement of rhIGF-1/rhIGFBP-3 in preterm infants

Author

Ann Hellström, Boubou Hallberg, Jyoti Sharma, David Ley, Adina Tocoian, Jou Ku Chung, Ingrid Hansen-Pupp, Gerald J. Fetterly, Nerissa C. Kreher, Martin A. Graham, and Norman W. Barton

Subjects

Blood Glucose, Male, medicine.medical_specialty, Pediatrics, Time Factors, Population, Phases of clinical research, Gestational Age, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Reference Values, 030225 pediatrics, Internal medicine, medicine, Humans, Computer Simulation, 030212 general & internal medicine, Dosing, Insulin-Like Growth Factor I, education, education.field_of_study, business.industry, Postmenstrual Age, Infant, Newborn, Gestational age, Retinopathy of prematurity, medicine.disease, Recombinant Proteins, Pharmacokinetic analysis, Insulin-Like Growth Factor Binding Protein 3, Infant, Extremely Premature, Pediatrics, Perinatology and Child Health, Female, business, Infant, Premature

Abstract

rhIGF-1/rhIGFBP-3 is being investigated for prevention of retinopathy of prematurity in extremely preterm infants. A population pharmacokinetic model was developed using data from phase I/II (Sections A–C) trials of rhIGF-1/rhIGFBP-3 and additional studies in preterm infants to predict optimal dosing to establish/maintain serum IGF-1 within physiological intrauterine levels. In Section D of the phase II study, infants (gestational age (GA) (wk+d) 23+0 to 27+6) were randomized to rhIGF-1/rhIGFBP-3, administered at the model-predicted dose of 250 µg/kg/d continuous i.v. infusion up to postmenstrual age (PMA) 29 wk+6 d or standard of care. An interim pharmacokinetic analysis was performed for the first 10 treated infants to verify dosing. Serum IGF-1 data were reviewed for 10 treated/9 control infants. Duration of therapy in treated infants ranged 1–34.5 d. At baseline (before infusion and

Published

2016

10. Biodistribution of Idursulfase Formulated for Intrathecal Use (Idursulfase-IT) in Cynomolgus Monkeys after Intrathecal Lumbar Administration

Author

Kathleen Palmieri, Bob Crooker, Eilish Brown, Thomas McCauley, and Jou-Ku Chung

Subjects

0301 basic medicine, Male, Central Nervous System, Time Factors, Idursulfase, Physiology, Drug Evaluation, Preclinical, lcsh:Medicine, Pharmacology, Monkeys, Kidney, Nervous System, 0302 clinical medicine, Cerebrospinal fluid, Medicine and Health Sciences, Tissue Distribution, Enzyme-Linked Immunoassays, lcsh:Science, Injections, Spinal, Mucopolysaccharidosis II, Cerebrospinal Fluid, Mammals, Multidisciplinary, biology, Brain, Hunter syndrome, Enzyme replacement therapy, Body Fluids, medicine.anatomical_structure, Bioassays and Physiological Analysis, Liver, Spinal Cord, Anesthesia, Vertebrates, Female, Anatomy, medicine.drug, Research Article, Biotechnology, Primates, Catheters, Central nervous system, Iduronate Sulfatase, Research and Analysis Methods, 03 medical and health sciences, 030225 pediatrics, medicine, Animals, Humans, Enzyme Replacement Therapy, Immunoassays, Enzyme Assays, business.industry, lcsh:R, Organisms, Biology and Life Sciences, Kidneys, Renal System, Spinal cord, medicine.disease, Enzyme assay, Macaca fascicularis, Neuroanatomy, 030104 developmental biology, Amniotes, biology.protein, Immunologic Techniques, lcsh:Q, Medical Devices and Equipment, business, Biochemical Analysis, Neuroscience

Abstract

Enzyme replacement therapy with intravenous idursulfase (recombinant iduronate-2-sulfatase) is approved for the treatment of Hunter syndrome. Intravenous administration does not, however, treat the neurological manifestations, due to its low central nervous system bioavailability. Using intrathecal-lumbar administration, iduronate-2-sulfatase is delivered directly to the central nervous system. This study investigates the central nervous system biodistribution of intrathecal-lumbar administered iduronate-2-sulfatase in cynomolgus monkeys. Twelve monkeys were administered iduronate-2-sulfatase in one 30 mg intrathecal-lumbar injection. Brain, spinal cord, liver, and kidneys were collected for iduronate-2-sulfatase concentration (measured by an enzyme linked immunosorbent assay) and enzyme activity measurement (via a method utilizing 4-methylumbelliferyl-α-iduronate-2-sulfate) at 1, 2, 5, 12, 24, and 48 hours following administration. The tissue enzyme linked immunosorbent assay confirmed iduronate-2-sulfatase uptake to the brain, spinal cord, kidneys, and liver in a time-dependent manner. In spinal cord and brain, iduronate-2-sulfatase appeared as early as 1 hour following administration, and peak concentrations were observed at ~2 and ~5 hours. Iduronate-2-sulfatase appeared in liver and kidneys 1 hour post intrathecal-lumbar dose with peak concentrations between 5 and 24 hours. Liver iduronate-2-sulfatase concentration was approximately 10-fold higher than kidney. The iduronate-2-sulfatase localization and enzyme activity in the central nervous system, following intrathecal administration, demonstrates that intrathecal-lumbar treatment with iduronate-2-sulfatase may be considered for further investigation as a treatment for Hunter syndrome patients with neurocognitive impairment.

Published

2016

11. A phase 1/2 study of intrathecal heparan-N-sulfatase in patients with mucopolysaccharidosis IIIA

Author

Ann J. Barbier, Patrick A. J. Haslett, Frits A. Wijburg, Jou-Ku Chung, Fiona Heap, Evelien Tump, Jan Pieter Marchal, Catherine Breen, Luying Pan, Stewart Rust, Nitin Nair, Jessica de Ruijter, Yongchang Qiu, Simon Jones, Other departments, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Other Research, Graduate School, and Paediatric Metabolic Diseases

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Adolescent, Mucopolysaccharidosis, Endocrinology, Diabetes and Metabolism, Gastroenterology, Biochemistry, Antibodies, 03 medical and health sciences, Mucopolysaccharidosis III, Young Adult, 0302 clinical medicine, Cerebrospinal fluid, Endocrinology, Pharmacokinetics, In vivo, Internal medicine, medicine, Genetics, Humans, Adverse effect, Child, Molecular Biology, Injections, Spinal, Dose-Response Relationship, Drug, Chemistry, Enzyme replacement therapy, medicine.disease, 030104 developmental biology, Treatment Outcome, Pharmacodynamics, Child, Preschool, Female, Heparitin Sulfate, Sulfatases, 030217 neurology & neurosurgery

Abstract

Objective This was an open-label, phase 1/2 dose-escalation, safety trial of intrathecal recombinant human heparan -N- sulfatase (rhHNS) administered via intrathecal drug delivery device (IDDD) for treating mucopolysaccharidosis IIIA (NCT01155778). Study design Twelve patients received 10, 45, or 90mg of rhHNS via IDDD once monthly for a total of 6 doses. Primary endpoints included adverse events (AEs) and anti-rhHNS antibodies. Secondary endpoints included standardized neurocognitive assessments, cortical gray matter volume, and pharmacokinetic/pharmacodynamic analyses. Results All patients experienced treatment-emergent AEs; most of mild-to-moderate severity. Seven patients reported a total of 10 serious AEs (SAEs), all but one due to hospitalization to revise a nonfunctioning IDDD. No SAEs were considered related to rhHNS. Anti-rhHNS antibodies were detected in the serum of 6 patients and in the cerebrospinal fluid (CSF) of 2 of these. CSF heparan sulfate levels were elevated at baseline and there were sustained declines in all tested patients following the first rhHNS dose. No impact of anti-rhHNS antibodies on any pharmacodynamic or safety parameters was evident. 4 of 12 patients showed a decline in developmental quotient, 6 were stable, and 2 patients had only a single data point. No dose group showed a clearly different response pattern. Conclusions rhHNS administration via IDDD appeared generally safe and well tolerated. Treatment resulted in consistent declines in CSF heparan sulfate, suggesting in vivo activity in the relevant anatomical compartment. Results of this small study should be interpreted with caution. Future studies are required to assess the potential clinical benefits of rhHNS and to test improved IDDD models.

Published

2016

12. Structure-toxicity relationship study of para-halogenated styrene analogues in CYP2E1 transgenic cells

Author

Zhiteng Jiang, Jou Ku Chung, Jiang Zheng, Shuijie Shen, and Wei Yuan

Subjects

Hydrocarbons, Halogenated, Chemistry, Cysteamine, Metabolite, Cytochrome P-450 CYP2E1, General Medicine, Glutathione, CYP2E1, Toxicology, Article, Cell Line, Styrenes, Styrene, Structure-Activity Relationship, chemistry.chemical_compound, Monomer, Styrene oxide, Humans, Structure–activity relationship, Organic chemistry, Cytotoxicity, Cells, Cultured, Protein Binding

Abstract

Styrene is one of the most important industrial intermediates consumed in the world and is mainly used as a monomer for reinforced plastics and rubber. Styrene has been found to be hepatotoxic and pneumotoxic in humans and experimental animals. The toxicity of styrene is suggested to be metabolism-dependent. Styrene-7,8-oxide has been considered as the major metabolite responsible for styrene-induced cytotoxicity. The objective of the study was to investigate the correlation between cytotoxicity of styrene and chemical and biochemical properties of the vinyl group of styrene by development of structure activity relationships (SAR). 4-Fluorostyrene, 4-chlorostyrene and 4-bromostyrene were selected for the SAR study. Cytotoxicity of styrene and the halogenated styrene derivatives with an order of 4-bromostyrene > 4-chlorostyrene > 4-fluorostyrene ≈ styrene was observed in CYP2E1 transgenic cells. Similar orders in the efficiency of the metabolism of styrene and the halogenated styrene analogues to their oxides and in the electrophilicity of the corresponding oxides were observed. Additionally, the order of the potency of cellular glutathione depletion and the degree of protein adduction induced by styrene and the halogenated styrenes were consistent with that of their cytotoxicities. The wild-type cells were less susceptible to the toxicity of the corresponding model compounds than CYP2E1 cells. The present study provided insight into the roles of the biochemical and chemical properties of styrene in its cytotoxicity.

Published

2012

13. rhIGF-1/rhIGFBP-3 in Preterm Infants: A Phase 2 Randomized Controlled Trial

Author

Norman W. Barton, Ajit Mahaveer, Luca A. Ramenghi, Ingrid Hansen-Pupp, Faizah Bhatti, Jason Higginson, Emily Jochim, Alexandra Mangili, Boubou Hallberg, Carlo Dani, Mirjam M. van Weissenbruch, David Ley, Peter Reynolds, Jou Ku Chung, Olachi J. Mezu-Ndubuisi, Lois E.H. Smith, Mark A. Turner, Ann Hellström, Kathryn Beardsall, Neil Marlow, Mohamed Hamdani, Adina Tocoian, Carmen Giannantonio, David B. Dunger, Pediatric surgery, ACS - Diabetes & metabolism, AGEM - Endocrinology, metabolism and nutrition, Amsterdam Neuroscience - Mood, Anxiety, Psychosis, Stress & Sleep, NCA - Neurobiology of mental health, and Amsterdam Reproduction & Development (AR&D)

Subjects

Male, Pediatrics, Severity of Illness Index, law.invention, 0302 clinical medicine, Randomized controlled trial, law, Phase (matter), Medicine, 030212 general & internal medicine, Insulin-Like Growth Factor I, Infusions, Intravenous, bronchopulmonary dysplasia, intraventricular hemorrhage, neonatology, retinopathy of prematurity, Bronchopulmonary Dysplasia, Cerebral Hemorrhage, Female, Gestational Age, Humans, Infant, Extremely Premature, Infant, Newborn, Infant, Premature, Insulin-Like Growth Factor Binding Protein 3, Recombinant Proteins, Retinopathy of Prematurity, Treatment Outcome, Gestational age, Retinopathy of prematurity, 3. Good health, Intraventricular hemorrhage, 030220 oncology & carcinogenesis, Anesthesia, 030211 gastroenterology & hepatology, Intravenous, medicine.medical_specialty, Infusions, Extremely Premature, Article, 03 medical and health sciences, 030225 pediatrics, Severity of illness, Neonatology, Premature, business.industry, Postmenstrual Age, Infant, medicine.disease, Newborn, Bronchopulmonary dysplasia, Pediatrics, Perinatology and Child Health, business

Abstract

Objective: To investigate recombinant human insulin-like growth factor 1 complexed with its binding protein (rhIGF-1/rhIGFBP-3) for the prevention of retinopathy of prematurity (ROP) and other complications of prematurity among extremely preterm infants. Study design: This phase 2 trial was conducted from September 2014 to March 2016. Infants born at a gestational age of 230/7 weeks to 276/7 weeks were randomly allocated to rhIGF-1/rhIGFBP-3 (250 µg/kg/ 24 hours, continuous intravenous infusion from

Published

2018

14. Evidence for cellular protein covalent binding derived from styrene metabolite

Author

Wei Yuan, Hua Jin, Jou Ku Chung, and Jiang Zheng

Subjects

Male, Cytotoxins, Metabolite, Albumin, Proteins, Cytochrome P-450 CYP2E1, General Medicine, Toxicology, Article, Cell Line, Styrene, Mice, chemistry.chemical_compound, chemistry, Biochemistry, Cell culture, Styrene oxide, Microsome, Animals, Epoxy Compounds, Humans, Cytotoxicity, Protein Binding, Cysteine

Abstract

Styrene is one of the most important industrial intermediates consumed in the world. Human exposure to styrene occurs mainly in the reinforced plastics industry, particularly in developing countries. Styrene has been found to be hepatotoxic and pneumotoxic in humans and animals. The biochemical mechanisms of styrene-induced toxicities remain unknown. Albumin and hemoglobin adduction derived from styrene oxide, a major reactive metabolite of styrene, has been reported in blood samples obtained from styrene-exposed workers. The objectives of the current study focused on cellular protein covalent binding of styrene metabolite and its correlation with cytotoxicity induced by styrene. We found that radioactivity was bound to cellular proteins obtained from mouse airway trees after incubation with 14 C-styrene. Microsomal incubation studies showed that the observed protein covalent binding required the metabolic activation of styrene. The observed radioactivity binding in protein samples obtained from the cultured airways and microsomal incubations was significantly suppressed by co-incubation with disulfiram, a CYP2E1 inhibitor, although disulfiram apparently did not show a protective effect against the cytotoxicity of styrene. A 2-fold increase in radioactivity bound to cellular proteins was detected in cells stably transfected with CYP2E1 compared to the wild-type cells after 14 C-styrene exposure. With the polyclonal antibody developed in our lab, we detected cellular protein adduction derived from styrene oxide at cysteinyl residues in cells treated with styrene. Competitive immunoblot studies confirmed the modification of cysteine residues by styrene oxide. Cell culture studies showed that the styrene-induced protein modification and cell death increased with the increasing concentration of styrene exposure. In conclusion, we detected cellular protein covalent modification by styrene oxide in microsomal incubations, cultured cells, and mouse airways after exposure to styrene and found a good correlation between styrene-induced cytotoxicity and styrene oxide-derived cellular protein adduction.

Published

2010

15. Pharmacokinetics and bioavailability of a therapeutic enzyme (idursulfase) in cynomolgus monkeys after intrathecal and intravenous administration

Author

Mary Ann Mascelli, Thomas McCauley, Jou-Ku Chung, and Hongsheng Xie

Subjects

Male, Idursulfase, Biological Availability, lcsh:Medicine, Iduronate Sulfatase, Pharmacology, Cisterna magna, Cerebrospinal fluid, Pharmacokinetics, Medicine, Animals, Humans, Enzyme Replacement Therapy, Dosing, lcsh:Science, Injections, Spinal, Mucopolysaccharidosis II, Multidisciplinary, business.industry, lcsh:R, Hunter syndrome, Enzyme replacement therapy, medicine.disease, Recombinant Proteins, Bioavailability, Macaca fascicularis, Anesthesia, Administration, Intravenous, Female, lcsh:Q, business, medicine.drug, Research Article

Abstract

Intravenous enzyme replacement therapy with iduronate-2-sulfatase is an approved treatment for Hunter syndrome, however, conventional intravenous delivery cannot treat the neurologic manifestations of the disease due to its limited central nervous system penetration. Intrathecal administration of iduronate-2-sulfatase for delivery to the central nervous system is currently under investigation. The objective of this study was to evaluate the pharmacokinetics of idursulfase in the central nervous system of cynomolgus monkeys (Macaca fasicularis) after intravenous and intrathecal administration. Twenty-seven monkeys, treatment-naive to enzyme replacement therapy, were placed into 4 groups according to body weight: Group 1 was administered 0.5 mg/kg idursulfase intravenously, Groups 2–4 were administered an intrathecal formulation (1-, 10-, and 30-mg doses). Blood samples and cerebrospinal fluid (sampled at the cisterna magna or lumbar level) were collected at the same time points for 72 hours post dosing. Following intravenous administration, a high maximum serum concentration and rapid distribution of iduronate-2-sulfatase out of the central compartment were observed (elimination half-life: 4.3 hours). Iduronate-2-sulfatase exposure in the cerebrospinal fluid was limited, suggesting intravenous administration provided minimal penetration of the blood–brain barrier. Following intrathecal administration, a high maximum observed concentration was immediately noted and elimination half-life ranged between 7.8–10 hours and 5.9–6.7 hours (cisterna magna and lumbar sampling, respectively). Cerebrospinal fluid pharmacokinetic profiles at different doses of iduronate-2-sulfatase were similar and the dose/exposure relationship was proportional. After intrathecal administration, movement of iduronate-2-sulfatase from cerebrospinal fluid to serum was observed (systemic bioavailability was 40–83%). The clear penetration of iduronate-2-sulfatase into the cerebrospinal fluid and the dose response suggest that intrathecal delivery of iduronate-2-sulfatase may be suitable for treating the central nervous system manifestations associated with Hunter syndrome.

Published

2015

16. Biodistribution of idursulfase in cynomolgus monkeys after intrathecal-lumbar administration

Author

Thomas McCauley, Jou-Ku Chung, Kathleen Palmieri, Eilish Brown, and Robert Crooker

Subjects

Biodistribution, business.industry, Idursulfase, Endocrinology, Diabetes and Metabolism, Pharmacology, Intrathecal, Biochemistry, Endocrinology, Lumbar, Genetics, Medicine, business, Molecular Biology, medicine.drug

Published

2016

17. ARC15105 is a potent antagonist of von Willebrand factor mediated platelet activation and adhesion

Author

Kathleen E. McGinness, P. Shannon Pendergrast, Robert G. Schaub, Xianbin Tian, Bernd Jilma, Yahye Merhi, Daniel Duerschmied, Jolanta M. Siller-Matula, Jean-François Tanguay, Jou-Ku Chung, and Denisa D. Wagner

Subjects

Blood Platelets, Male, Platelet Function Tests, Swine, Injections, Subcutaneous, Myocardial Infarction, Biological Availability, Pharmacology, Platelet Adhesiveness, Von Willebrand factor, Pharmacokinetics, Drug Stability, von Willebrand Factor, medicine, Animals, Humans, Platelet, Platelet activation, Whole blood, Aged, biology, Dose-Response Relationship, Drug, Chemistry, Quebec, Aptamers, Nucleotide, Middle Aged, Platelet Activation, Adenosine, Bioavailability, Rats, Macaca fascicularis, Cross-Sectional Studies, Coagulation, Austria, Case-Control Studies, Immunology, Injections, Intravenous, biology.protein, Female, Collagen, Cardiology and Cardiovascular Medicine, Aptamers, Peptide, Platelet Aggregation Inhibitors, medicine.drug, Boston, Half-Life, Protein Binding

Abstract

Objective— We investigated the stability, pharmacokinetic, and pharmacodynamic profile of the 2 nd generation anti-von Willeband factor aptamer ARC15105. Methods and Results— Platelet plug formation was measured by collagen/adenosine diphosphate-induced closure time with the platelet function analyzer-100 and platelet aggregation by multiple electrode aggregometry. Platelet adhesion was measured on denuded porcine aortas and in a flow chamber. Aptamer stability was assessed by incubation in nuclease rich human, monkey, and rat serum for up to 72 hours. Pharmacokinetic and pharmacodynamic profiles were tested in cynomolgus monkeys after IV and SC administration. The median IC 100 and IC 50 to prolong collagen/adenosine diphosphate-induced closure timewere 27 nmol/L and 12 nmol/L, respectively. ARC15105 (1.3 μmol/L) completely inhibited ristocetin-induced platelet aggregation in whole blood ( P P 90% on denuded porcine aortas ( P 90% ( P 1/2 would be ≈217 hours. Pharmacodynamic analysis confirms that ARC15105 inhibits von Willeband factor activity >90% in blood samples taken 300 hours after a 20 mg/kg IV or SC dose in monkeys. Conclusion— The potency, pharmacokinetic profile, and SC bioavailability of ARC15105 support its clinical investigation for chronic inhibition of von Willeband factor -mediated platelet activation.

Published

2012

18. Investigation of bioactivation and toxicity of styrene in CYP2E1 transgenic cells

Author

Guangxian Liu, Wei Yuan, Jiang Zheng, and Jou-Ku Chung

Subjects

Cell Survival, Metabolite, Epoxide, Toxicology, Ethylbenzene, Styrene, Styrenes, Animals, Genetically Modified, chemistry.chemical_compound, Styrene oxide, Organic chemistry, Animals, Humans, Enzyme Inhibitors, Cytotoxicity, Biotransformation, Cells, Cultured, Chromatography, High Pressure Liquid, Epoxide Hydrolases, Cytochrome P-450 CYP2E1, Glutathione, Acetylcysteine, chemistry, Microsomal epoxide hydrolase, Toxicity, Epoxy Compounds

Abstract

Styrene has been found to be toxic to the respiratory system, and the toxicity of styrene is metabolism-dependent. CYP2E1 is suggested to be one of the cytochrome P450 enzymes responsible for the bioactivation of styrene. Our work focused on the roles of CYP2E1 and epoxide, a metabolite of styrene epoxidation, in the cytotoxicity of styrene. Styrene was found to be more toxic to h2E1 cells than to the wild type, while there was no difference found when styrene oxide was administered. Both soluble and microsomal epoxide hydrolase inhibitors dramatically enhanced styrene toxicity. Glutathione and glutathione ethyl ester showed protection against styrene cytotoxicity. Cytotoxicity of a selection of styrene analogues, such as ethylbenzene, vinylcyclohexane, and ethylcyclohexane, was assessed to determine if unsaturation is required for styrene toxicity. Ethylbenzene and vinylcyclohexane were found to be as toxic as styrene to h2E1 cells, whereas little toxicity of ethylcyclohexane to h2E1 cells was observed. This indicates the importance of vinyl group of styrene in its cytotoxicity, but saturation of the vinyl group does not necessarily eliminate styrene toxicity. An N-acetylcysteine conjugate derived from styrene oxide was identified by LC/MS/MS in the sample obtained from the incubation of h2E1 cell lysate with styrene in the presence of N-acetylcysteine. Formation of the N-acetylcysteine conjugate was found to be NADPH-dependent. These studies provided strong evidence in support of toxic role of styrene epoxide metabolite in styrene toxicity.

Published

2006

19. Whole Body and CNS Biodistribution of rhHNS in Cynomolgus Monkeys after Intrathecal Lumbar Administration: Treatment Implications for Patients with MPS IIIA.

Author

Jou-Ku Chung, Luying Pan, Palmieri, Kathleen, Youssef, Amir S., and McCauley, Thomas G.

Subjects

*SANFILIPPO syndrome, *GENETIC disorders in children, *COGNITION disorders, *CENTRAL nervous system, *BLOOD-brain barrier, *PHARMACOKINETICS, *CEREBROSPINAL fluid, *HEPARAN sulfate, *THERAPEUTICS

Abstract

Mucopolysaccharidosis III type A (MPS IIIA; Sanfilippo syndrome), a genetic lysosomal disorder causing a deficiency of heparan N-sulfatase (HNS), leads to progressive cognitive decline from an early age. An effective enzyme replacement therapy (ERT) for MPS IIIA requires central nervous system (CNS) biodistribution. Recombinant human heparan N-sulfatase (rhHNS), an investigatory ERT for MPS IIIA, has been formulated for intrathecal (IT) administration since intravenous (IV) administration cannot cross the blood brain barrier (BBB) in sufficient amounts to have a therapeutic effect. In this study, systemic and CNS distribution of rhHNS in cynomolgus monkeys following IV and IT administration was evaluated by quantitation of rhHNS in serum, cerebral spinal fluid (CSF) and various tissues, and positron emission tomography (PET) imaging of live animals. Following IV administration, rhHNS levels were low to non-detectable in the CSF, and systemic clearance was rapid (≤2 h). With IT administration, rhHNS was observable in CNS tissues in ≤1 h, with varying Tmax (1-24 h). Appreciable systemic distribution was observed up to 7 days. This provides evidence that in this animal model, intrathecal administration of rhHNS delivers the replacement enzyme to therapeutically relevant tissues for the treatment of Sanfilippo Syndrome type A. Penetration into grey matter and cortex was 3-4 times greater than concentrations in white matter and deeper parenchymal regions, suggesting some limitations of this ERT strategy. [ABSTRACT FROM AUTHOR]

Published

2017