Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type

Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type

Orlistat, an anti-obesity drug, has two critical issues—the first is its low efficacy due to low water solubility and the second is side effects such as oily spotting due to its lipase inhibition. The present study was designed to propose a solution using a formulation with mesoporous silica to simu...

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Main Authors: Heejun Park, Kwang-Ho Cha, Seung Hyeon Hong, Sharif Md Abuzar, Seungyeol Lee, Eun-Sol Ha, Jeong-Soo Kim, In-Hwan Baek, Min-Soo Kim, Sung-Joo Hwang
Format: Article
Language:English
Published: MDPI AG 2020-04-01
Series:Pharmaceutics
Subjects:
orlistat
mesoporous silica
supercritical melt-adsorption
crystallinity
in vivo evaluation
Online Access:https://www.mdpi.com/1999-4923/12/4/333
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spelling doaj-9dece2e01b9d4e4aa21ee5ea89e1f3f12020-11-25T02:33:48ZengMDPI AGPharmaceutics1999-49232020-04-011233333310.3390/pharmaceutics12040333Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica TypeHeejun Park0Kwang-Ho Cha1Seung Hyeon Hong2Sharif Md Abuzar3Seungyeol Lee4Eun-Sol Ha5Jeong-Soo Kim6In-Hwan Baek7Min-Soo Kim8Sung-Joo Hwang9College of Pharmacy, Pusan National University, 63 Busandaehak-ro, Geumjeong-gu, Busan 46241, KoreaYonsei Institute of Pharmaceutical Sciences & College of Pharmacy, Yonsei University, 85 Songdogwahak-ro, Yeonsu-gu, Incheon 21983, KoreaYonsei Institute of Pharmaceutical Sciences & College of Pharmacy, Yonsei University, 85 Songdogwahak-ro, Yeonsu-gu, Incheon 21983, KoreaYonsei Institute of Pharmaceutical Sciences & College of Pharmacy, Yonsei University, 85 Songdogwahak-ro, Yeonsu-gu, Incheon 21983, KoreaYonsei Institute of Pharmaceutical Sciences & College of Pharmacy, Yonsei University, 85 Songdogwahak-ro, Yeonsu-gu, Incheon 21983, KoreaCollege of Pharmacy, Pusan National University, 63 Busandaehak-ro, Geumjeong-gu, Busan 46241, KoreaDong-A ST Co. Ltd., Giheung-gu, Yongin, Gyeonggi 446-905, KoreaCollege of Pharmacy, Kyungsung University, 309, Suyeong-ro, Nam-gu, Busan 48434, KoreaCollege of Pharmacy, Pusan National University, 63 Busandaehak-ro, Geumjeong-gu, Busan 46241, KoreaYonsei Institute of Pharmaceutical Sciences & College of Pharmacy, Yonsei University, 85 Songdogwahak-ro, Yeonsu-gu, Incheon 21983, KoreaOrlistat, an anti-obesity drug, has two critical issues—the first is its low efficacy due to low water solubility and the second is side effects such as oily spotting due to its lipase inhibition. The present study was designed to propose a solution using a formulation with mesoporous silica to simultaneously overcome two issues. Orlistat was loaded onto mesoporous silica by the supercritical melt-adsorption (SCMA) method, using carbon dioxide (CO<sub>2</sub>). Various types of mesoporous silica were used as adsorbents, and the effects of the pore volume, diameter and particle size of mesoporous silica on the pharmaceutical characteristics were evaluated by various solid-state characterization methods and in vitro and in vivo studies in relation to pharmacological efficacy and the improvement of side effects. The results showed that the pore volume and diameter determine loadable drug amount inside pores and crystallinity. The dissolution was significantly influenced by crystallinity, pore diameter and particle size, and the inhibition of lipase activity was in proportion to the dissolution rate. In vivo studies revealed that the serum triglyceride (TG) concentration was significantly decreased in the group administered amorphous orlistat-loaded Neuisilin<sup>®</sup>UFL2 with the highest in vitro dissolution rate and lipase activity inhibition in comparison to the commercial product. Furthermore, oily spotting tests in rats revealed that undigested oil was adsorbed onto mesoporous silica after orlistat was released in the gastro-intestinal tract, and it correlated with in vitro result that oil adsorption capacity was dependent on the surface area of empty mesoporous silica. Therefore, it was concluded that mesoporous silica type plays a major role in determining the pharmaceutical characteristics of orlistat formulation prepared using SCMA with CO<sub>2</sub> for improving the low solubility and overcoming the side effects.https://www.mdpi.com/1999-4923/12/4/333orlistatmesoporous silicasupercritical melt-adsorptioncrystallinityin vivo evaluation
collection DOAJ
language English
format Article
sources DOAJ
author Heejun Park
Kwang-Ho Cha
Seung Hyeon Hong
Sharif Md Abuzar
Seungyeol Lee
Eun-Sol Ha
Jeong-Soo Kim
In-Hwan Baek
Min-Soo Kim
Sung-Joo Hwang
spellingShingle Heejun Park
Kwang-Ho Cha
Seung Hyeon Hong
Sharif Md Abuzar
Seungyeol Lee
Eun-Sol Ha
Jeong-Soo Kim
In-Hwan Baek
Min-Soo Kim
Sung-Joo Hwang
Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type
Pharmaceutics
orlistat
mesoporous silica
supercritical melt-adsorption
crystallinity
in vivo evaluation
author_facet Heejun Park
Kwang-Ho Cha
Seung Hyeon Hong
Sharif Md Abuzar
Seungyeol Lee
Eun-Sol Ha
Jeong-Soo Kim
In-Hwan Baek
Min-Soo Kim
Sung-Joo Hwang
author_sort Heejun Park
title Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type
title_short Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type
title_full Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type
title_fullStr Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type
title_full_unstemmed Pharmaceutical Characterization and In Vivo Evaluation of Orlistat Formulations Prepared by the Supercritical Melt-Adsorption Method Using Carbon Dioxide: Effects of Mesoporous Silica Type
title_sort pharmaceutical characterization and in vivo evaluation of orlistat formulations prepared by the supercritical melt-adsorption method using carbon dioxide: effects of mesoporous silica type
publisher MDPI AG
series Pharmaceutics
issn 1999-4923
publishDate 2020-04-01
description Orlistat, an anti-obesity drug, has two critical issues—the first is its low efficacy due to low water solubility and the second is side effects such as oily spotting due to its lipase inhibition. The present study was designed to propose a solution using a formulation with mesoporous silica to simultaneously overcome two issues. Orlistat was loaded onto mesoporous silica by the supercritical melt-adsorption (SCMA) method, using carbon dioxide (CO<sub>2</sub>). Various types of mesoporous silica were used as adsorbents, and the effects of the pore volume, diameter and particle size of mesoporous silica on the pharmaceutical characteristics were evaluated by various solid-state characterization methods and in vitro and in vivo studies in relation to pharmacological efficacy and the improvement of side effects. The results showed that the pore volume and diameter determine loadable drug amount inside pores and crystallinity. The dissolution was significantly influenced by crystallinity, pore diameter and particle size, and the inhibition of lipase activity was in proportion to the dissolution rate. In vivo studies revealed that the serum triglyceride (TG) concentration was significantly decreased in the group administered amorphous orlistat-loaded Neuisilin<sup>®</sup>UFL2 with the highest in vitro dissolution rate and lipase activity inhibition in comparison to the commercial product. Furthermore, oily spotting tests in rats revealed that undigested oil was adsorbed onto mesoporous silica after orlistat was released in the gastro-intestinal tract, and it correlated with in vitro result that oil adsorption capacity was dependent on the surface area of empty mesoporous silica. Therefore, it was concluded that mesoporous silica type plays a major role in determining the pharmaceutical characteristics of orlistat formulation prepared using SCMA with CO<sub>2</sub> for improving the low solubility and overcoming the side effects.
topic orlistat
mesoporous silica
supercritical melt-adsorption
crystallinity
in vivo evaluation
url https://www.mdpi.com/1999-4923/12/4/333
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