Your search keyword '"Sadeghi, Saman"' showing total 11 results

1. Transforming an Academic Radiochemistry Facility for Positron Emission Tomography Drug cGMP Compliance.

Author

Zhu S, Mosessian S, Kroeger K, Sadeghi S, Slavik R, Kinloch S, Moore M, Allen-Auerbach M, Czernin J, and Phelps M

Subjects

California, Cyclotrons, Drug Approval, Humans, Quality Control, Radiopharmaceuticals, United States, United States Food and Drug Administration, Universities, Drug Industry standards, Facility Regulation and Control standards, Guideline Adherence, Positron-Emission Tomography standards, Radiochemistry methods

Abstract

In light of the United States Food and Drug Administration (FDA) requirement of 21 CFR 212 current Good Manufacturing Practice (cGMP) for FDA-approved position emission tomography (PET) drugs, the University of California Los Angeles (UCLA) Biomedical Cyclotron (BMC) transformed from a pre-cGMP era academic cyclotron and radiochemistry facility to a current cGMP-compliant PET drug manufacturer. In this article, we share the financial and regulatory compliance aspects of the "transformation" required to develop a sustainable quality system to support the production of two PET drugs under Abbreviated New Drug Applications (ANDAs).

Published

2020

2. Production of diverse PET probes with limited resources: 24 18 F-labeled compounds prepared with a single radiosynthesizer.

Author

Collins J, Waldmann CM, Drake C, Slavik R, Ha NS, Sergeev M, Lazari M, Shen B, Chin FT, Moore M, Sadeghi S, Phelps ME, Murphy JM, and van Dam RM

Subjects

Positron-Emission Tomography methods, Radiopharmaceuticals chemistry, Fluorine Radioisotopes chemistry, Radiochemistry methods, Radiopharmaceuticals chemical synthesis

Abstract

New radiolabeled probes for positron-emission tomography (PET) are providing an ever-increasing ability to answer diverse research and clinical questions and to facilitate the discovery, development, and clinical use of drugs in patient care. Despite the high equipment and facility costs to produce PET probes, many radiopharmacies and radiochemistry laboratories use a dedicated radiosynthesizer to produce each probe, even if the equipment is idle much of the time, to avoid the challenges of reconfiguring the system fluidics to switch from one probe to another. To meet growing demand, more cost-efficient approaches are being developed, such as radiosynthesizers based on disposable "cassettes," that do not require reconfiguration to switch among probes. However, most cassette-based systems make sacrifices in synthesis complexity or tolerated reaction conditions, and some do not support custom programming, thereby limiting their generality. In contrast, the design of the ELIXYS FLEX/CHEM cassette-based synthesizer supports higher temperatures and pressures than other systems while also facilitating flexible synthesis development. In this paper, the syntheses of 24 known PET probes are adapted to this system to explore the possibility of using a single radiosynthesizer and hot cell for production of a diverse array of compounds with wide-ranging synthesis requirements, alongside synthesis development efforts. Most probes were produced with yields and synthesis times comparable to literature reports, and because hardware modification was unnecessary, it was convenient to frequently switch among probes based on demand. Although our facility supplies probes for preclinical imaging, the same workflow would be applicable in a clinical setting., Competing Interests: Conflict of interest statement: The Regents of the University of California have licensed technology to Sofie Biosciences, Inc. that was invented by J.C., C.D., M.L., M.M., and R.M.v.D. and have taken equity in Sofie Biosciences as part of the licensing transaction. Furthermore, R.M.v.D. is a founder and consultant of Sofie Biosciences, M.E.P. is a founder and board member, and C.D. and M.M. are employees and owners., (Published under the PNAS license.)

Published

2017

3. Production of diverse PET probes with limited resources: 24 18F-labeled compounds prepared with a single radiosynthesizer

Author

Collins, Jeffrey, Waldmann, Christopher M, Drake, Christopher, Slavik, Roger, Ha, Noel S, Sergeev, Maxim, Lazari, Mark, Shen, Bin, Chin, Frederick T, Moore, Melissa, Sadeghi, Saman, Phelps, Michael E, Murphy, Jennifer M, and van Dam, R Michael

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Chemical Sciences, Biomedical Imaging, Generic health relevance, Fluorine Radioisotopes, Positron-Emission Tomography, Radiochemistry, Radiopharmaceuticals, PET tracer, positron-emission tomography, radiochemistry, radiosynthesis module, resource efficiency

Abstract

New radiolabeled probes for positron-emission tomography (PET) are providing an ever-increasing ability to answer diverse research and clinical questions and to facilitate the discovery, development, and clinical use of drugs in patient care. Despite the high equipment and facility costs to produce PET probes, many radiopharmacies and radiochemistry laboratories use a dedicated radiosynthesizer to produce each probe, even if the equipment is idle much of the time, to avoid the challenges of reconfiguring the system fluidics to switch from one probe to another. To meet growing demand, more cost-efficient approaches are being developed, such as radiosynthesizers based on disposable "cassettes," that do not require reconfiguration to switch among probes. However, most cassette-based systems make sacrifices in synthesis complexity or tolerated reaction conditions, and some do not support custom programming, thereby limiting their generality. In contrast, the design of the ELIXYS FLEX/CHEM cassette-based synthesizer supports higher temperatures and pressures than other systems while also facilitating flexible synthesis development. In this paper, the syntheses of 24 known PET probes are adapted to this system to explore the possibility of using a single radiosynthesizer and hot cell for production of a diverse array of compounds with wide-ranging synthesis requirements, alongside synthesis development efforts. Most probes were produced with yields and synthesis times comparable to literature reports, and because hardware modification was unnecessary, it was convenient to frequently switch among probes based on demand. Although our facility supplies probes for preclinical imaging, the same workflow would be applicable in a clinical setting.

Published

2017

4. No-carrier-added electrochemical nucleophilic radiofluorination of aromatics

Author

He, Qinggang, Alfeazi, Ines, and Sadeghi, Saman

Published

2015

5. Electrochemical Radiofluorination of Small Molecules: New Advances.

Author

Hernández‐Valdés, Daniel and Sadeghi, Saman

Subjects

*SMALL molecules, *ACTIVATION energy, *RADIOLABELING, *FLUORIDES, *FLUORINATION

Abstract

The development of new 18F‐based radiopharmaceuticals constantly demands innovations in the search for new radiofluorination methods. [18F]fluoride is the simplest and most convenient chemical form of the isotope for the synthesis of 18F‐based radiopharmaceuticals. The ease of production and handling, as well as the possibility of obtaining high molar activities, makes it the preferred choice for radiofluorination. However, the use of [18F]fluoride in late‐stage radiofluorination comes with challenges, especially for the radiolabeling of electron‐rich molecules where SN2 and SNAr reactions are not suitable. New developments in fluorination chemistry have been extensively studied to overcome these difficulties. Selective electrochemical oxidation of precursors, using a controlled potential, is one method to create reactive intermediates and overcome the activation energy required for nucleophilic fluorination of electron‐rich moieties. This method has been used for years in cold fluorination of organic molecules and more recently has been adapted as an alternative to traditional radiofluorination methods. Although relatively young, this field stands out as a promising route for the synthesis of new PET probes as well as fluorinated pharmaceuticals. This review focuses on recent advances in electrochemical radiofluorination as an alternative for the late‐stage radiolabeling of organic molecules. [ABSTRACT FROM AUTHOR]

Published

2021

6. Production of diverse PET probes with limited resources: 24 F-18-labeled compounds prepared with a single radiosynthesizer

Author

Collins, Jeffrey, Waldmann, Christopher M, Drake, Christopher, Slavik, Roger, Ha, Noel S, Sergeev, Maxim, Lazari, Mark, Shen, Bin, Chin, Frederick T, Moore, Melissa, Sadeghi, Saman, Phelps, Michael E, Murphy, Jennifer M, and van Dam, R Michael

Subjects

Fluorine Radioisotopes, Radiochemistry, Positron-Emission Tomography, PET tracer, MD Multidisciplinary, resource efficiency, Radiopharmaceuticals, radiosynthesis module

Abstract

New radiolabeled probes for positron-emission tomography (PET) are providing an ever-increasing ability to answer diverse research and clinical questions and to facilitate the discovery, development, and clinical use of drugs in patient care. Despite the high equipment and facility costs to produce PET probes, many radiopharmacies and radiochemistry laboratories use a dedicated radiosynthesizer to produce each probe, even if the equipment is idle much of the time, to avoid the challenges of reconfiguring the system fluidics to switch from one probe to another. To meet growing demand, more cost-efficient approaches are being developed, such as radiosynthesizers based on disposable "cassettes," that do not require reconfiguration to switch among probes. However, most cassette-based systems make sacrifices in synthesis complexity or tolerated reaction conditions, and some do not support custom programming, thereby limiting their generality. In contrast, the design of the ELIXYS FLEX/CHEM cassette-based synthesizer supports higher temperatures and pressures than other systems while also facilitating flexible synthesis development. In this paper, the syntheses of 24 known PET probes are adapted to this system to explore the possibility of using a single radiosynthesizer and hot cell for production of a diverse array of compounds with wide-ranging synthesis requirements, alongside synthesis development efforts. Most probes were produced with yields and synthesis times comparable to literature reports, and because hardware modification was unnecessary, it was convenient to frequently switch among probes based on demand. Although our facility supplies probes for preclinical imaging, the same workflow would be applicable in a clinical setting.

Published

2017

7. Production of diverse PET probes with limited resources: 24 18F-labeled compounds prepared with a single radiosynthesizer.

Author

Collins, Jeffrey, Waldmann, Christopher M., Drake, Christopher, Slavik, Roger, Ha, Noel S., Sergeev, Maxim, Lazari, Mark, Shen, Bin, Chin, Frederick T., Moore, Melissa, Sadeghi, Saman, Phelps, Michael E., Murphy, Jennifer M., and van Dam, R. Michael

Subjects

POSITRON emission tomography, MOLECULAR probes, RADIOLABELING, RADIOCHEMICAL laboratories, RADIOPHARMACEUTICALS

Abstract

New radiolabeled probes for positron-emission tomography (PET) are providing an ever-increasing ability to answer diverse research and clinical questions and to facilitate the discovery, development, and clinical use of drugs in patient care. Despite the high equipment and facility costs to produce PET probes, many radiopharmacies and radiochemistry laboratories use a dedicated radiosynthesizer to produce each probe, even if the equipment is idle much of the time, to avoid the challenges of reconfiguring the system fluidics to switch from one probe to another. To meet growing demand, more cost-efficient approaches are being developed, such as radiosynthesizers based on disposable "cassettes," that do not require reconfiguration to switch among probes. However, most cassette-based systems make sacrifices in synthesis complexity or tolerated reaction conditions, and some do not support custom programming, thereby limiting their generality. In contrast, the design of the ELIXYS FLEX/CHEM cassette-based synthesizer supports higher temperatures and pressures than other systems while also facilitating flexible synthesis development. In this paper, the syntheses of 24 known PET probes are adapted to this system to explore the possibility of using a single radiosynthesizer and hot cell for production of a diverse array of compounds with wide-ranging synthesis requirements, alongside synthesis development efforts. Most probes were produced with yields and synthesis times comparable to literature reports, and because hardware modification was unnecessary, it was convenient to frequently switch among probes based on demand. Although our facility supplies probes for preclinical imaging, the same workflow would be applicable in a clinical setting. [ABSTRACT FROM AUTHOR]

Published

2017

8. Radiochemistry on electrodes: Synthesis of an 18F-labelled and in vivo stable COX-2 inhibitor.

Author

Lebedev, Artem, Jiao, Jing, Lee, Jason, Yang, Fan, Allison, Nathanael, Herschman, Harvey, and Sadeghi, Saman

Subjects

NONSTEROIDAL anti-inflammatory agents, RADIOCHEMISTRY, POSITRON emission tomography, ELECTRODES, METABOLISM

Abstract

New radiochemistry techniques can yield novel PET tracers for COX-2 and address the shortcomings in in vivo stability and specificity, which have held back clinical translation of tracers to image COX-2 expression. Current techniques limit radiosynthesis to analogs of the COX-2 inhibitors with fluorine-18 added via a carbon chain, or on an aromatic position which renders the radiolabeled analog less specific towards COX-2, resulting in tracers with low in vivo stability or specificity. To solve this problem, we have developed a new high affinity, 18F-labelled COX-2 inhibitor that is radiolabeled directly on a heteroaromatic ring. This molecule exhibits favorable biodistribution and increased metabolic stability. Synthesis of this molecule cannot be achieved by traditional means; consequently, we have developed an automated electrochemical radiosynthesis platform to synthesize up to 5 mCi of radiochemically pure 18F-COX-2ib in 4 hours (2% decay-corrected radiochemical yield). In vitro studies demonstrated clear correlation between COX-2 expression and uptake of the tracer. PET imaging of healthy animals confirmed that the molecule is excreted from blood within an hour, mainly through the hepatobiliary excretion pathway. In vivo metabolism data demonstrated that > 95% of the injected radioactivity remains in the form of the parent molecule 1 hour after injection. [ABSTRACT FROM AUTHOR]

Published

2017

9. Reusable electrochemical cell for rapid separation of [18F]fluoride from [18O]water for flow-through synthesis of 18F-labeled tracers

Author

Sadeghi, Saman, Liang, Vincent, Cheung, Shilin, Woo, Suh, Wu, Curtis, Ly, Jimmy, Deng, Yuliang, Eddings, Mark, and van Dam, R. Michael

Subjects

*ELECTRIC batteries, *SEPARATION (Technology), *FLUORIDES, *WATER, *CHEMICAL synthesis, *RADIOLABELING, *RADIOACTIVE tracers, *BRASS, *PLATINUM, *X-ray photoelectron spectroscopy

Abstract

Abstract: A brass–platinum electrochemical micro-flow cell was developed to extract [18F]fluoride from an aqueous solution and release it into an organic-based solution, suitable for subsequent radio-synthesis, in a fast and reliable manner. This cell does not suffer electrode erosion and is thus reusable while operating faster by enabling increased voltages. By optimizing temperature, trapping and release potentials, flow rates, and electrode materials, an overall [18F]fluoride trapping and release efficiency of 84±5% (n=7) was achieved. X-ray photoelectron spectroscopy (XPS) was used to analyze electrode surfaces of various metal–metal systems and the findings were correlated with the performance of the electrochemical cell. To demonstrate the reactivity of the released [18F]fluoride, the cell was coupled to a flow-through reactor and automated synthesis of [18F]FDG with a repeatable decay-corrected yield of 56±4% (n=4) was completed in <15min. A multi-human dose of 5.92GBq [18F]FDG was also demonstrated. [Copyright &y& Elsevier]

Published

2013

10. Albumin As a Platform for Radiotherapy and Antibody-Recruiting Therapy

Author

Mercanti, Natalie, Valliant, John, Sadeghi, Saman, Rullo, Anthony, and Chemistry and Chemical Biology

Subjects

immunology, antibody-recruitment, radiochemistry, radiotherapy

Abstract

The aim of this thesis was to develop and evaluate albumin-based conjugates for their use in radiotherapy and antibody-recruiting therapy which may then be combined to enhance therapeutic efficacy of each monotherapy. The approach taken in order to achieve high tumour uptake of the conjugates and minimize doses to healthy tissues involved the intratumoural administration of therapeutic compounds; a technique which has gained popularity in recent years for the treatment of solid tumours. Despite the promise this method of administration holds, it is often limited by the fast clearance of injected compounds from the tumour. Using albumin-based conjugates allows for the exploitation of the enhanced permeation and retention (EPR) effect which aids in the retention of the compound at the site of interest for longer periods of time, thus allowing the opportunity for enhanced therapeutic efficacy. Bovine serum albumin conjugated with DOTA chelators was first synthesized and found to possess 3.9 ± 0.4 chelates per BSA molecule. Radiolabelling of the compound with lutetium- 177 produced the desired product in radiochemical yields of 74 ±2 % with a radiochemical purity >99%. The stability of the compound was evaluated by monitoring the radiochemical purity over 7 days which was found to be >95% pure over the entirety of the testing period, indicating a stable product. The intratumoural administration of [177Lu]Lu-DOTA-BSA in a triple negative breast cancer (TNBC) tumour model revealed significant tumour retention of 52 ± 12 %ID/g and 35 ± 6 %ID/g at 24 h and 72 h post-injection, respectively, while autoradiography displayed a heterogenous dispersion of the compound throughout the tumour. A multidosing therapy study in which animals received two doses of either 4.44, 5.92, or 7.40 MBq of [177Lu]Lu-DOTA-BSA showed promise, with a strong trend observed between the administration of higher doses and a prolonged lifespan. Histological analysis of tumours excised 7 days post-treatment revealed signs iv of necrosis and apoptosis in tumours treated with 7.40 MBq [177Lu]Lu-DOTA-BSA. These preliminary results prove to be a promising approach for use in combination therapy and may be further optimized to enhance its efficacy as a monotherapy. Next, the in vivo evaluation of DNP-BSA was carried out to assess using an intratumourally administered, albumin-based platform for antibody-recruiting in a triple negative breast cancer model. A preliminary antibody-recruiting study administering 35 nmol DNP-BSA three times per week unfortunately did not induce slowed tumour growth nor did it have an impact on lifespan. Treated mice were also unable to tolerate repeated doses of the antigen which indicated too high of a concentration and/or dosing frequency was used. A tolerability study was then carried out in order to determine a treatment schedule which did not lead to adverse effects. Mice treated once per week with low (9 nmol) to moderate (17 nmol) doses of DNP-BSA did not display toxic effects but unfortunately did not exhibit a therapeutic effect nor any indication that an adaptive immune response was achieved. These results suggest that further optimization is required prior to use in combination therapy and moderate doses (17 nmol) DNP should be used to investigate a treatment schedule which is able to induce antibody recruitment. Thesis Master of Science (MSc)

Published

2021

11. Electrochemical nucleophilic synthesis of di-tert-butyl-(4-[18F]fluoro-1,2-phenylene)-dicarbonate.

Author

He, Qinggang, Wang, Ying, Alfeazi, Ines, and Sadeghi, Saman

Subjects

*ELECTROCHEMICAL analysis, *NUCLEOPHILIC reactions, *PHENYLENE compounds, *CARBONATES, *POSITRON emission tomography, *RADIOCHEMISTRY

Abstract

An electrochemical method with the ability to conduct 18 F-fluorination of aromatic molecules through direct nucleophilic fluorination of cationic intermediates is presented in this paper. The reaction was performed on a remote-controlled automatic platform. Nucleophilic electrochemical fluorination of tert-butyloxycarbonyl (Boc) protected catechol, an intermediate model molecule for the positron emission tomography (PET) probe (3,4-dihydroxy-6-[ 18 F]fluoro- l -phenylalanine), was performed. Fluorination was achieved under potentiostatic anodic oxidation in acetonitrile containing Et 3 N·3HF and other supporting electrolytes. Radiofluorination efficiency was influenced by a number of variables, including the concentration of the precursor, concentration of Et 3 N·3HF, type of supporting electrolyte, temperature and time, as well as applied potentials. Radio-fluorination efficiency of 10.4±0.6% ( n =4) and specific activity of up to 43 GBq/mmol was obtained after 1 h electrolysis of 0.1 M of 4- tert -butyl-diboc-catechol in the acetonitrile solution of Et 3 N·3HF (0.033 M) and NBu 4 PF 6 (0.05 M). Density functional theory (DFT) was employed to explain the tert -butyl functional group facilitation of electrochemical oxidation and subsequent fluorination. [ABSTRACT FROM AUTHOR]

Published

2014