End-to-end continuous manufacturing of conventional compressed tablets: From flow synthesis to tableting through integrated crystallization and filtration

[Display omitted] An end-to-end continuous pharmaceutical manufacturing process was developed for the production of conventional direct compressed tablets on a proof-of-concept level for the first time. The output reaction mixture of the flow synthesis of acetylsalicylic acid was crystallized contin...

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Veröffentlicht in:	International journal of pharmaceutics 2020-05, Vol.581, p.119297-119297, Article 119297
Hauptverfasser:	Domokos, András, Nagy, Brigitta, Gyürkés, Martin, Farkas, Attila, Tacsi, Kornélia, Pataki, Hajnalka, Liu, Yiqing Claire, Balogh, Attila, Firth, Paul, Szilágyi, Botond, Marosi, György, Nagy, Zoltán K., Nagy, Zsombor Kristóf
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Sprache:	eng
Schlagworte:	Aspirin - analysis Aspirin - chemical synthesis Blending Cellulose - analysis Cellulose - chemical synthesis Chemistry, Pharmaceutical - methods Compressive Strength Continuous manufacturing Crystallization Crystallization - methods End-to-end Filtration Filtration - methods Integration Spectroscopy, Near-Infrared - methods Tableting Tablets
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container_title	International journal of pharmaceutics
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creator	Domokos, András Nagy, Brigitta Gyürkés, Martin Farkas, Attila Tacsi, Kornélia Pataki, Hajnalka Liu, Yiqing Claire Balogh, Attila Firth, Paul Szilágyi, Botond Marosi, György Nagy, Zoltán K. Nagy, Zsombor Kristóf
description	[Display omitted] An end-to-end continuous pharmaceutical manufacturing process was developed for the production of conventional direct compressed tablets on a proof-of-concept level for the first time. The output reaction mixture of the flow synthesis of acetylsalicylic acid was crystallized continuously in a mixed suspension mixed product removal crystallizer. The crystallizer was directly connected to a continuous filtration carousel device, thus the crystallization, filtration and drying of acetylsalicylic acid (ASA) was carried out in an integrated 2-step process. Steady state was reached during longer operations and the interaction of process parameters was evaluated in a series of experiments. The filtered crystals were ready for further processing in a following continuous blending and tableting experiment due to the good flowability of the material. The ASA collected during the crystallization-filtration experiments was fed into a continuous twin-screw blender along with microcrystalline cellulose as tableting excipient. After continuous blending Near-Infrared spectroscopy was applied to in-line analyze the drug content of the powder mixture. A belt conveyor carried the mixture towards an eccentric lab-scale tablet press, which continuously produced 500 mg ASA-loaded compressed tablets of 100 mg dose strength. Thus, starting from raw materials, the final drug product was obtained by continuous manufacturing steps with appropriate quality.
doi_str_mv	10.1016/j.ijpharm.2020.119297
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The output reaction mixture of the flow synthesis of acetylsalicylic acid was crystallized continuously in a mixed suspension mixed product removal crystallizer. The crystallizer was directly connected to a continuous filtration carousel device, thus the crystallization, filtration and drying of acetylsalicylic acid (ASA) was carried out in an integrated 2-step process. Steady state was reached during longer operations and the interaction of process parameters was evaluated in a series of experiments. The filtered crystals were ready for further processing in a following continuous blending and tableting experiment due to the good flowability of the material. The ASA collected during the crystallization-filtration experiments was fed into a continuous twin-screw blender along with microcrystalline cellulose as tableting excipient. After continuous blending Near-Infrared spectroscopy was applied to in-line analyze the drug content of the powder mixture. A belt conveyor carried the mixture towards an eccentric lab-scale tablet press, which continuously produced 500 mg ASA-loaded compressed tablets of 100 mg dose strength. Thus, starting from raw materials, the final drug product was obtained by continuous manufacturing steps with appropriate quality.</description><identifier>ISSN: 0378-5173</identifier><identifier>EISSN: 1873-3476</identifier><identifier>DOI: 10.1016/j.ijpharm.2020.119297</identifier><identifier>PMID: 32243964</identifier><language>eng</language><publisher>Netherlands: Elsevier B.V</publisher><subject>Aspirin - analysis ; Aspirin - chemical synthesis ; Blending ; Cellulose - analysis ; Cellulose - chemical synthesis ; Chemistry, Pharmaceutical - methods ; Compressive Strength ; Continuous manufacturing ; Crystallization ; Crystallization - methods ; End-to-end ; Filtration ; Filtration - methods ; Integration ; Spectroscopy, Near-Infrared - methods ; Tableting ; Tablets</subject><ispartof>International journal of pharmaceutics, 2020-05, Vol.581, p.119297-119297, Article 119297</ispartof><rights>2020 The Authors</rights><rights>Copyright © 2020 Elsevier B.V. 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The output reaction mixture of the flow synthesis of acetylsalicylic acid was crystallized continuously in a mixed suspension mixed product removal crystallizer. The crystallizer was directly connected to a continuous filtration carousel device, thus the crystallization, filtration and drying of acetylsalicylic acid (ASA) was carried out in an integrated 2-step process. Steady state was reached during longer operations and the interaction of process parameters was evaluated in a series of experiments. The filtered crystals were ready for further processing in a following continuous blending and tableting experiment due to the good flowability of the material. The ASA collected during the crystallization-filtration experiments was fed into a continuous twin-screw blender along with microcrystalline cellulose as tableting excipient. After continuous blending Near-Infrared spectroscopy was applied to in-line analyze the drug content of the powder mixture. A belt conveyor carried the mixture towards an eccentric lab-scale tablet press, which continuously produced 500 mg ASA-loaded compressed tablets of 100 mg dose strength. Thus, starting from raw materials, the final drug product was obtained by continuous manufacturing steps with appropriate quality.</description><subject>Aspirin - analysis</subject><subject>Aspirin - chemical synthesis</subject><subject>Blending</subject><subject>Cellulose - analysis</subject><subject>Cellulose - chemical synthesis</subject><subject>Chemistry, Pharmaceutical - methods</subject><subject>Compressive Strength</subject><subject>Continuous manufacturing</subject><subject>Crystallization</subject><subject>Crystallization - methods</subject><subject>End-to-end</subject><subject>Filtration</subject><subject>Filtration - methods</subject><subject>Integration</subject><subject>Spectroscopy, Near-Infrared - methods</subject><subject>Tableting</subject><subject>Tablets</subject><issn>0378-5173</issn><issn>1873-3476</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2020</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqFUc2O0zAQthCI7RYeAeQjlxT_xU65ILTaXZBW4gJny7EnravELrazq_IoPC0OLVw5jWa-n7HnQ-gNJRtKqHx_2PjDcW_StGGE1Rndsq16hla0U7zhQsnnaEW46pqWKn6FrnM-EEIko_wluuKMCb6VYoV-3QbXlNhAcNjGUHyY45zxZMI8GFvm5MMOx2HBHqHCMZixNtMxQc7gcDH9CCV_wHcpTngY4xPOp1D2kH3GJV7wxaTsU5x3e-xDgV0ypYptOuVixtH_NIszNvURgx9L-tO-Qi8GM2Z4falr9P3u9tvN5-bh6_2Xm08PjRWUlUYZ1jkmmGqdIMLI3gFznEkpCGNs26leCKl60wLlVknSb8VAW-bE4DgMreNr9O7se0zxxwy56MlnC-NoAtRbaMY7yTpF6-nWqD1TbYo5Jxj0MfnJpJOmRC-x6IO-xKKXWPQ5lqp7e1kx9xO4f6q_OVTCxzMB6kcfPSSdrYdgwfkEtmgX_X9W_AaPb6Vp</recordid><startdate>20200515</startdate><enddate>20200515</enddate><creator>Domokos, András</creator><creator>Nagy, Brigitta</creator><creator>Gyürkés, Martin</creator><creator>Farkas, Attila</creator><creator>Tacsi, Kornélia</creator><creator>Pataki, Hajnalka</creator><creator>Liu, Yiqing Claire</creator><creator>Balogh, Attila</creator><creator>Firth, Paul</creator><creator>Szilágyi, Botond</creator><creator>Marosi, György</creator><creator>Nagy, Zoltán K.</creator><creator>Nagy, Zsombor Kristóf</creator><general>Elsevier B.V</general><scope>6I.</scope><scope>AAFTH</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>20200515</creationdate><title>End-to-end continuous manufacturing of conventional compressed tablets: From flow synthesis to tableting through integrated crystallization and filtration</title><author>Domokos, András ; 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The output reaction mixture of the flow synthesis of acetylsalicylic acid was crystallized continuously in a mixed suspension mixed product removal crystallizer. The crystallizer was directly connected to a continuous filtration carousel device, thus the crystallization, filtration and drying of acetylsalicylic acid (ASA) was carried out in an integrated 2-step process. Steady state was reached during longer operations and the interaction of process parameters was evaluated in a series of experiments. The filtered crystals were ready for further processing in a following continuous blending and tableting experiment due to the good flowability of the material. The ASA collected during the crystallization-filtration experiments was fed into a continuous twin-screw blender along with microcrystalline cellulose as tableting excipient. After continuous blending Near-Infrared spectroscopy was applied to in-line analyze the drug content of the powder mixture. 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source	MEDLINE; ScienceDirect Journals (5 years ago - present)
subjects	Aspirin - analysis Aspirin - chemical synthesis Blending Cellulose - analysis Cellulose - chemical synthesis Chemistry, Pharmaceutical - methods Compressive Strength Continuous manufacturing Crystallization Crystallization - methods End-to-end Filtration Filtration - methods Integration Spectroscopy, Near-Infrared - methods Tableting Tablets
title	End-to-end continuous manufacturing of conventional compressed tablets: From flow synthesis to tableting through integrated crystallization and filtration
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