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Dive into the research topics where Sharon Hashmueli is active.

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Featured researches published by Sharon Hashmueli.


PLOS ONE | 2009

A Plant-Derived Recombinant Human Glucocerebrosidase Enzyme—A Preclinical and Phase I Investigation

David Aviezer; Einat Brill-Almon; Yoseph Shaaltiel; Sharon Hashmueli; Daniel Bartfeld; Sarah Mizrachi; Yael Liberman; Arnold I. Freeman; Ari Zimran; Eithan Galun

UNLABELLED Gaucher disease is a progressive lysosomal storage disorder caused by the deficiency of glucocerebrosidase leading to the dysfunction in multiple organ systems. Intravenous enzyme replacement is the accepted standard of treatment. In the current report, we evaluate the safety and pharmacokinetics of a novel human recombinant glucocerebrosidase enzyme expressed in transformed plant cells (prGCD), administered to primates and human subjects. Short term (28 days) and long term (9 months) repeated injections with a standard dose of 60 Units/kg and a high dose of 300 Units/kg were administered to monkeys (n = 4/sex/dose). Neither clinical drug-related adverse effects nor neutralizing antibodies were detected in the animals. In a phase I clinical trial, six healthy volunteers were treated by intravenous infusions with escalating single doses of prGCD. Doses of up to 60 Units/kg were administered at weekly intervals. prGCD infusions were very well tolerated. Anti-prGCD antibodies were not detected. The pharmacokinetic profile of the prGCD revealed a prolonged half-life compared to imiglucerase, the commercial enzyme that is manufactured in a costly mammalian cell system. These studies demonstrate the safety and lack of immunogenicity of prGCD. Following these encouraging results, a pivotal phase III clinical trial for prGCD was FDA approved and is currently ongoing. TRIAL REGISTRATION ClinicalTrials.gov NCT00258778.


Blood | 2011

Pivotal trial with plant cell-expressed recombinant glucocerebrosidase, taliglucerase alfa, a novel enzyme replacement therapy for Gaucher disease

Ari Zimran; Einat Brill-Almon; Raul Chertkoff; Milan Petakov; Francisco Blanco-Favela; Eduardo Terreros Muñoz; Sergio Eduardo Solorio-Meza; Dominick Amato; Gloria Durán; Fiorina Giona; Rene Heitner; Hanna Rosenbaum; Pilar Giraldo; Atul Mehta; Glen Park; Mici Phillips; Deborah Elstein; Gheona Altarescu; Mali Szleifer; Sharon Hashmueli; David Aviezer

Taliglucerase alfa (Protalix Biotherapeutics, Carmiel, Israel) is a novel plant cell-derived recombinant human β-glucocerebrosidase for Gaucher disease. A phase 3, double-blind, randomized, parallel-group, comparison-dose (30 vs 60 U/kg body weight/infusion) multinational clinical trial was undertaken. Institutional review board approvals were received. A 9-month, 20-infusion trial used inclusion/exclusion criteria in treatment-naive adult patients with splenomegaly and thrombocytopenia. Safety end points were drug-related adverse events: Ab formation and hypersensitivity reactions. Primary efficacy end point was reduction in splenic volume measured by magnetic resonance imaging. Secondary end points were: changes in hemoglobin, hepatic volume, and platelet counts. Exploratory parameters included biomarkers and bone imaging. Twenty-nine patients (11 centers) completed the protocol. There were no serious adverse events; drug-related adverse events were mild/moderate and transient. Two patients (6%) developed non-neutralizing IgG Abs; 2 other patients (6%) developed hypersensitivity reactions. Statistically significant spleen reduction was achieved at 9 months: 26.9% (95% confidence interval [CI]: -31.9, -21.8) in the 30-unit dose group and 38.0% (95% CI: -43.4, -32.8) in the 60-unit dose group (both P < .0001); and in all secondary efficacy end point measures, except platelet counts at the lower dose. These results support safety and efficacy of taliglucerase alfa for Gaucher disease.


Plant Biotechnology Journal | 2007

Production of glucocerebrosidase with terminal mannose glycans for enzyme replacement therapy of Gaucher's disease using a plant cell system

Yoseph Shaaltiel; Daniel Bartfeld; Sharon Hashmueli; Gideon Baum; Einat Brill-Almon; Gad Galili; Orly Dym; Israel Silman; Joel L. Sussman; Anthony H. Futerman; David Aviezer


Archive | 2008

Production of high mannose proteins in plant culture

Yoseph Shaaltiel; Gideon Baum; Daniel Bartfeld; Sharon Hashmueli; Ayala Lewkowicz


Molecular Genetics and Metabolism | 2008

6. Novel enzyme replacement therapy for Gaucher disease: On-going phase III clinical trial with recombinant human glucocerebrosidase expressed in plant cells

David Aviezer; Einat Almon-Brill; Yossef Shaaltiel; Gad Galili; Raul Chertkoff; Sharon Hashmueli; Eithan Galun; Ari Zimran


Archive | 2011

Human lysosomal proteins from plant cell culture

Yoseph Shaaltiel; Gideon Baum; Daniel Bartfeld; Sharon Hashmueli; Ayala Lewkowicz


Archive | 2005

System and method for production of antibodies in plant cell culture

Yoseph Shaaltiel; Sharon Hashmueli; Daniel Bartfeld; Gideon Baum; Tal Ratz; Einat Mizrachi; Yehava Forester


Molecular Genetics and Metabolism | 2010

9. Novel enzyme replacement therapy for Gaucher disease: Phase III pivotal clinical trial with plant cell expressed recombinantglucocerebrosidase (prGCD) – taliglucerase alpha

David Aviezer; Einat Almon-Brill; Yoseph Shaaltiel; Raul Chertkoff; Sharon Hashmueli; Ari Zimran


Archive | 2009

Production of high mannose proteins in plant culture and therapeutic uses thereof

Yoseph Shaaltiel; Gideon Baum; Daniel Bartfeld; Sharon Hashmueli; Ayala Lewkowicz


Archive | 2004

Production of iduronate-2-sulphatase in plant culture

Yoseph Shaaltiel; Gideon Baum; Sharon Hashmueli; Ayala Lewkowicz; Daniel Bartfeld

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Daniel Bartfeld

Weizmann Institute of Science

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Ari Zimran

Shaare Zedek Medical Center

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Raul Chertkoff

Shaare Zedek Medical Center

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Einat Brill-Almon

Shaare Zedek Medical Center

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Deborah Elstein

Shaare Zedek Medical Center

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Eithan Galun

Hebrew University of Jerusalem

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Gad Galili

Weizmann Institute of Science

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Gheona Altarescu

Shaare Zedek Medical Center

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