The relationship between in vivo nasal drug clearance and in vitro nasal mucociliary clearance: Application to the prediction of nasal drug absorption

Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We previously developed an in vitro method to evaluate MC via the translocation velocity of fluorescent microspheres (VFMS) applied to excised rat na...

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Published inEuropean journal of pharmaceutical sciences Vol. 117; pp. 21 - 26
Main Authors Inoue, Daisuke, Tanaka, Akiko, Kimura, Shunsuke, Kiriyama, Akiko, Katsumi, Hidemasa, Yamamoto, Akira, Ogawara, Ken-ichi, Kimura, Toshikiro, Higaki, Kazutaka, Yutani, Reiko, Sakane, Toshiyasu, Furubayashi, Tomoyuki
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier B.V 30.05.2018
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ISSN0928-0987
1879-0720
1879-0720
DOI10.1016/j.ejps.2018.01.032

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Abstract Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We previously developed an in vitro method to evaluate MC via the translocation velocity of fluorescent microspheres (VFMS) applied to excised rat nasal mucosa. In the present study, the relationship between in vivo nasal MC and in vitro VFMS was examined to optimize our PK model for the prediction of nasal drug absorption. Appropriate inhibitors (propranolol and atropine) and enhancers (terbutaline and acetylcholine chloride) of MC were utilized to modify MC. In vivo clearance of drug from the nasal cavity was determined from the disappearance of fluorescent microspheres (FMS) from the nasal cavity following nasal application to rats. The first order elimination rate constant, kmc, was determined from the disappearance profiles of FMS. kmc was decreased to 35.8% by propranolol and 52.6% by atropine, but increased to 117% by terbutaline and 168% by acetylcholine chloride. A significant linear correlation was observed between kmc and VFMS (r2 = 0.9745, p < 0.001). These results indicate that in vivo kmc can be estimated from the in vitro parameter, VFMS. By introducing linear correlation into our PK model, nasal drug absorption may be precisely estimated, even with changes in MC. [Display omitted]
AbstractList Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We previously developed an in vitro method to evaluate MC via the translocation velocity of fluorescent microspheres (VFMS) applied to excised rat nasal mucosa. In the present study, the relationship between in vivo nasal MC and in vitro VFMS was examined to optimize our PK model for the prediction of nasal drug absorption. Appropriate inhibitors (propranolol and atropine) and enhancers (terbutaline and acetylcholine chloride) of MC were utilized to modify MC. In vivo clearance of drug from the nasal cavity was determined from the disappearance of fluorescent microspheres (FMS) from the nasal cavity following nasal application to rats. The first order elimination rate constant, kmc, was determined from the disappearance profiles of FMS. kmc was decreased to 35.8% by propranolol and 52.6% by atropine, but increased to 117% by terbutaline and 168% by acetylcholine chloride. A significant linear correlation was observed between kmc and VFMS (r2 = 0.9745, p < 0.001). These results indicate that in vivo kmc can be estimated from the in vitro parameter, VFMS. By introducing linear correlation into our PK model, nasal drug absorption may be precisely estimated, even with changes in MC.Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We previously developed an in vitro method to evaluate MC via the translocation velocity of fluorescent microspheres (VFMS) applied to excised rat nasal mucosa. In the present study, the relationship between in vivo nasal MC and in vitro VFMS was examined to optimize our PK model for the prediction of nasal drug absorption. Appropriate inhibitors (propranolol and atropine) and enhancers (terbutaline and acetylcholine chloride) of MC were utilized to modify MC. In vivo clearance of drug from the nasal cavity was determined from the disappearance of fluorescent microspheres (FMS) from the nasal cavity following nasal application to rats. The first order elimination rate constant, kmc, was determined from the disappearance profiles of FMS. kmc was decreased to 35.8% by propranolol and 52.6% by atropine, but increased to 117% by terbutaline and 168% by acetylcholine chloride. A significant linear correlation was observed between kmc and VFMS (r2 = 0.9745, p < 0.001). These results indicate that in vivo kmc can be estimated from the in vitro parameter, VFMS. By introducing linear correlation into our PK model, nasal drug absorption may be precisely estimated, even with changes in MC.
Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We previously developed an in vitro method to evaluate MC via the translocation velocity of fluorescent microspheres (VFMS) applied to excised rat nasal mucosa. In the present study, the relationship between in vivo nasal MC and in vitro VFMS was examined to optimize our PK model for the prediction of nasal drug absorption. Appropriate inhibitors (propranolol and atropine) and enhancers (terbutaline and acetylcholine chloride) of MC were utilized to modify MC. In vivo clearance of drug from the nasal cavity was determined from the disappearance of fluorescent microspheres (FMS) from the nasal cavity following nasal application to rats. The first order elimination rate constant, kmc, was determined from the disappearance profiles of FMS. kmc was decreased to 35.8% by propranolol and 52.6% by atropine, but increased to 117% by terbutaline and 168% by acetylcholine chloride. A significant linear correlation was observed between kmc and VFMS (r2 = 0.9745, p < 0.001). These results indicate that in vivo kmc can be estimated from the in vitro parameter, VFMS. By introducing linear correlation into our PK model, nasal drug absorption may be precisely estimated, even with changes in MC. [Display omitted]
Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We previously developed an in vitro method to evaluate MC via the translocation velocity of fluorescent microspheres (V ) applied to excised rat nasal mucosa. In the present study, the relationship between in vivo nasal MC and in vitro V was examined to optimize our PK model for the prediction of nasal drug absorption. Appropriate inhibitors (propranolol and atropine) and enhancers (terbutaline and acetylcholine chloride) of MC were utilized to modify MC. In vivo clearance of drug from the nasal cavity was determined from the disappearance of fluorescent microspheres (FMS) from the nasal cavity following nasal application to rats. The first order elimination rate constant, k , was determined from the disappearance profiles of FMS. k was decreased to 35.8% by propranolol and 52.6% by atropine, but increased to 117% by terbutaline and 168% by acetylcholine chloride. A significant linear correlation was observed between k and V (r  = 0.9745, p < 0.001). These results indicate that in vivo k can be estimated from the in vitro parameter, V . By introducing linear correlation into our PK model, nasal drug absorption may be precisely estimated, even with changes in MC.
Author Ogawara, Ken-ichi
Kimura, Shunsuke
Kiriyama, Akiko
Katsumi, Hidemasa
Yutani, Reiko
Sakane, Toshiyasu
Kimura, Toshikiro
Furubayashi, Tomoyuki
Yamamoto, Akira
Higaki, Kazutaka
Inoue, Daisuke
Tanaka, Akiko
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  surname: Inoue
  fullname: Inoue, Daisuke
  organization: Department of Pharmaceutics, School of Pharmacy, Shujitsu University, 1-6-1 Nishigawara, Naka-ku, Okayama 703-8516, Japan
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  givenname: Akiko
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  fullname: Tanaka, Akiko
  organization: Department of Biopharmaceutics, Kyoto Pharmaceutical University, 5 Misasagi-nakauchi-cho, Yamashina, Kyoto 607-8414, Japan
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  givenname: Shunsuke
  surname: Kimura
  fullname: Kimura, Shunsuke
  organization: Faculty of Pharmaceutical Sciences, Doshisha Women's College of Liberal Arts, Kodo, Kyotanabe-shi, Kyoto 610-0395, Japan
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  givenname: Akiko
  surname: Kiriyama
  fullname: Kiriyama, Akiko
  organization: Faculty of Pharmaceutical Sciences, Doshisha Women's College of Liberal Arts, Kodo, Kyotanabe-shi, Kyoto 610-0395, Japan
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  givenname: Hidemasa
  surname: Katsumi
  fullname: Katsumi, Hidemasa
  organization: Department of Biopharmaceutics, Kyoto Pharmaceutical University, 5 Misasagi-nakauchi-cho, Yamashina, Kyoto 607-8414, Japan
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  givenname: Akira
  surname: Yamamoto
  fullname: Yamamoto, Akira
  organization: Department of Biopharmaceutics, Kyoto Pharmaceutical University, 5 Misasagi-nakauchi-cho, Yamashina, Kyoto 607-8414, Japan
– sequence: 7
  givenname: Ken-ichi
  surname: Ogawara
  fullname: Ogawara, Ken-ichi
  organization: Department of Pharmaceutics, Faculty of Pharmaceutical Sciences, Okayama University, 1-1-1 Tsushima-naka, Kita-ku, Okayama 700-8530, Japan
– sequence: 8
  givenname: Toshikiro
  surname: Kimura
  fullname: Kimura, Toshikiro
  organization: Department of Pharmaceutics, Faculty of Pharmaceutical Sciences, Okayama University, 1-1-1 Tsushima-naka, Kita-ku, Okayama 700-8530, Japan
– sequence: 9
  givenname: Kazutaka
  surname: Higaki
  fullname: Higaki, Kazutaka
  organization: Department of Pharmaceutics, Faculty of Pharmaceutical Sciences, Okayama University, 1-1-1 Tsushima-naka, Kita-ku, Okayama 700-8530, Japan
– sequence: 10
  givenname: Reiko
  surname: Yutani
  fullname: Yutani, Reiko
  organization: Department of Pharmaceutical Technology, Kobe Pharmaceutical University, 4-19-1 Motoyamakita-machi, Higashinada, Kobe 658-8558, Japan
– sequence: 11
  givenname: Toshiyasu
  surname: Sakane
  fullname: Sakane, Toshiyasu
  organization: Department of Pharmaceutical Technology, Kobe Pharmaceutical University, 4-19-1 Motoyamakita-machi, Higashinada, Kobe 658-8558, Japan
– sequence: 12
  givenname: Tomoyuki
  surname: Furubayashi
  fullname: Furubayashi, Tomoyuki
  email: t-furu@shujitsu.ac.jp
  organization: Department of Pharmaceutics, School of Pharmacy, Shujitsu University, 1-6-1 Nishigawara, Naka-ku, Okayama 703-8516, Japan
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Keywords Prediction system
Nasal residence
Nasal absorption
Nasal formulation
Mucociliary clearance
Mucosal absorption
Language English
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Snippet Drug absorption after nasal application is dependent on drug clearance from the nasal cavity, which is determined by nasal mucociliary clearance (MC). We...
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StartPage 21
SubjectTerms Mucociliary clearance
Mucosal absorption
Nasal absorption
Nasal formulation
Nasal residence
Prediction system
Title The relationship between in vivo nasal drug clearance and in vitro nasal mucociliary clearance: Application to the prediction of nasal drug absorption
URI https://dx.doi.org/10.1016/j.ejps.2018.01.032
https://www.ncbi.nlm.nih.gov/pubmed/29410273
https://www.proquest.com/docview/1999193233
Volume 117
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