Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol

Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol

The aim of this research was to get optimal formula of levofloxacin tablet prepared with variation of PVP K-30 as binder and vivasol as disintegrant. The making of levofloxacin tablets was done by wet granulation. Tablet was prepared with various levels of PVP K-30 and disintegrant vivasol, compr...

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محفوظ في:
التفاصيل البيبلوغرافية
المؤلفون الرئيسيون: Fatmawati, Dina Ayu, Widjaja, Bambang, Setyawan, Dwi
التنسيق: مقال PeerReviewed
اللغة:English
English
منشور في: 2017
الموضوعات:
RS Pharmacy and materia medica
RS1-441 Pharmacy and materia medica
RS200-201 Pharmaceutical dosage forms
الوصول للمادة أونلاين:http://repository.unair.ac.id/75687/3/C-22%20Artikel.pdf
http://repository.unair.ac.id/75687/2/C-22%20Validasi%20dan%20Peer%20Reviewer.pdf
http://repository.unair.ac.id/75687/
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المؤسسة: Universitas Airlangga
اللغة: English
English
id id-langga.75687
record_format dspace
spelling id-langga.756872018-11-21T15:18:35Z http://repository.unair.ac.id/75687/ Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol Fatmawati, Dina Ayu Widjaja, Bambang Setyawan, Dwi RS Pharmacy and materia medica RS1-441 Pharmacy and materia medica RS200-201 Pharmaceutical dosage forms The aim of this research was to get optimal formula of levofloxacin tablet prepared with variation of PVP K-30 as binder and vivasol as disintegrant. The making of levofloxacin tablets was done by wet granulation. Tablet was prepared with various levels of PVP K-30 and disintegrant vivasol, compressed using a hydraulic press with 12 mm punch diameter, for 3 seconds. Physical quality (hardness, friability, and disintegration time) and dissolution rate of tablet was evaluated. The optimization of the formula was done by factorial design of 22 factorial experiments with 2 factors (PVP K-30 and vivasol) and 2 levels (2% and 4%). Optimization results showed that elevated levels of PVP K-30 increased tablet hardness, reduced friability of tablet, decreased disintegrating time, and increased dissolution rate of levofloxacin tablets. Meanwhile, elevated levels of vivasol increased the hardness of tablets, decreased the disintegrating time of tablets, decreased the dissolution rate of levofloxacin tablets, but did not affect the friability of tablets. In conclusion, the optimal tablet that meet the specifications of physical quality (hardness, friability, and disintegrating time) and dissolution rate was made by 2.4 to 3.7% of PVP K-30 and 2.0 to 3.2% vivasol as shown in the feasible area of design space 2017 Article PeerReviewed text en http://repository.unair.ac.id/75687/3/C-22%20Artikel.pdf text en http://repository.unair.ac.id/75687/2/C-22%20Validasi%20dan%20Peer%20Reviewer.pdf Fatmawati, Dina Ayu and Widjaja, Bambang and Setyawan, Dwi (2017) Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol. Jurnal Sains Farmasi & Klinis, 4 (2). pp. 9-15. ISSN 2442-5435
institution Universitas Airlangga
building Universitas Airlangga Library
country Indonesia
collection UNAIR Repository
language English
English
topic RS Pharmacy and materia medica
RS1-441 Pharmacy and materia medica
RS200-201 Pharmaceutical dosage forms
spellingShingle RS Pharmacy and materia medica
RS1-441 Pharmacy and materia medica
RS200-201 Pharmaceutical dosage forms
Fatmawati, Dina Ayu
Widjaja, Bambang
Setyawan, Dwi
Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol
description The aim of this research was to get optimal formula of levofloxacin tablet prepared with variation of PVP K-30 as binder and vivasol as disintegrant. The making of levofloxacin tablets was done by wet granulation. Tablet was prepared with various levels of PVP K-30 and disintegrant vivasol, compressed using a hydraulic press with 12 mm punch diameter, for 3 seconds. Physical quality (hardness, friability, and disintegration time) and dissolution rate of tablet was evaluated. The optimization of the formula was done by factorial design of 22 factorial experiments with 2 factors (PVP K-30 and vivasol) and 2 levels (2% and 4%). Optimization results showed that elevated levels of PVP K-30 increased tablet hardness, reduced friability of tablet, decreased disintegrating time, and increased dissolution rate of levofloxacin tablets. Meanwhile, elevated levels of vivasol increased the hardness of tablets, decreased the disintegrating time of tablets, decreased the dissolution rate of levofloxacin tablets, but did not affect the friability of tablets. In conclusion, the optimal tablet that meet the specifications of physical quality (hardness, friability, and disintegrating time) and dissolution rate was made by 2.4 to 3.7% of PVP K-30 and 2.0 to 3.2% vivasol as shown in the feasible area of design space
format Article
PeerReviewed
author Fatmawati, Dina Ayu
Widjaja, Bambang
Setyawan, Dwi
author_facet Fatmawati, Dina Ayu
Widjaja, Bambang
Setyawan, Dwi
author_sort Fatmawati, Dina Ayu
title Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol
title_short Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol
title_full Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol
title_fullStr Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol
title_full_unstemmed Optimasi Tablet Levofloksasin yang Mengandung Bahan Pengikat PVP K-30 dan Disintegran Vivasol
title_sort optimasi tablet levofloksasin yang mengandung bahan pengikat pvp k-30 dan disintegran vivasol
publishDate 2017
url http://repository.unair.ac.id/75687/3/C-22%20Artikel.pdf
http://repository.unair.ac.id/75687/2/C-22%20Validasi%20dan%20Peer%20Reviewer.pdf
http://repository.unair.ac.id/75687/
_version_ 1681150489680412672

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