Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats

Research output: Contribution to journal › Journal article › Research › peer-review

Standard

Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats. / Michaelsen, Maria Høtoft; Siqueira Jørgensen, Scheyla D.; Abdi, Ismahan Mahad; Wasan, Kishor M.; Rades, Thomas; Müllertz, Anette.

In: European Journal of Pharmaceutics and Biopharmaceutics, Vol. 142, 2019, p. 258-264.

Research output: Contribution to journal › Journal article › Research › peer-review

Harvard

Michaelsen, MH, Siqueira Jørgensen, SD, Abdi, IM, Wasan, KM, Rades, T & Müllertz, A 2019, 'Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats', European Journal of Pharmaceutics and Biopharmaceutics, vol. 142, pp. 258-264. https://doi.org/10.1016/j.ejpb.2019.07.002

APA

Michaelsen, M. H., Siqueira Jørgensen, S. D., Abdi, I. M., Wasan, K. M., Rades, T., & Müllertz, A. (2019). Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats. European Journal of Pharmaceutics and Biopharmaceutics, 142, 258-264. https://doi.org/10.1016/j.ejpb.2019.07.002

Vancouver

Michaelsen MH, Siqueira Jørgensen SD, Abdi IM, Wasan KM, Rades T, Müllertz A. Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats. European Journal of Pharmaceutics and Biopharmaceutics. 2019;142:258-264. https://doi.org/10.1016/j.ejpb.2019.07.002

Author

Michaelsen, Maria Høtoft ; Siqueira Jørgensen, Scheyla D. ; Abdi, Ismahan Mahad ; Wasan, Kishor M. ; Rades, Thomas ; Müllertz, Anette. / Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats. In: European Journal of Pharmaceutics and Biopharmaceutics. 2019 ; Vol. 142. pp. 258-264.

Bibtex

@article{da1be7eb70f94c4b99a266e523474215,

title = "Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats",

abstract = "The effect of drug load and digestion on the solubilization and absorption of fenofibrate in self-nanoemulsifying drug delivery system (SNEDDS) was assessed in a pharmacokinetic study in rats and in an in vitro lipolysis model. SNEDDS containing fenofibrate at 75% of equilibrium solubility (Seq), a super-saturated SNEDDS (super-SNEDDS) containing fenofibrate at 150% of Seq and a super-SNEDDS suspension containing fenofibrate at 100% of Seq and an additional 50% Seq fenofibrate suspended (150% of Seq in total) were used. To assess the effect of lipid digestion on fenofibrate absorption in rats and fenofibrate solubilization during in vitro lipolysis, the lipase inhibitor orlistat was added at 1% (w/w) to the SNEDDS, resulting in six different SNEDDS: SNEDDS, super-SNEDDS and super-SNEDDS suspension with and without orlistat 1% (w/w). In vivo, super-SNEDDS had a higher Cmax and AUC0-30h compared to SNEDDS and super-SNEDDS suspension, both with and without orlistat. While orlistat did not affect fenofibrate absorption in SNEDDS and super-SNEDDS, an increase of Tmax and AUC0-30h for super-SNEDDS suspension was found when orlistat was present. During in vitro lipolysis, the addition of orlistat decreased digestion and lowered drug precipitation. Super-SNEDDS showed significantly increased absorption in rats compared to SNEDDS and super-SNEDDS suspension and the inhibition of digestion resulted in prolonged and increased absorption for the super-SNEDDS suspension.",

keywords = "Absorption, Digestion, Fenofibrate, Orlistat, SNEDDS, Super-SNEDDS, Supersaturation",

author = "Michaelsen, {Maria H{\o}toft} and {Siqueira J{\o}rgensen}, {Scheyla D.} and Abdi, {Ismahan Mahad} and Wasan, {Kishor M.} and Thomas Rades and Anette M{\"u}llertz",

year = "2019",

doi = "10.1016/j.ejpb.2019.07.002",

language = "English",

volume = "142",

pages = "258--264",

journal = "European Journal of Pharmaceutics and Biopharmaceutics",

issn = "0939-6411",

publisher = "Elsevier",

}

RIS

TY - JOUR

T1 - Fenofibrate oral absorption from SNEDDS and super-SNEDDS is not significantly affected by lipase inhibition in rats

AU - Michaelsen, Maria Høtoft

AU - Siqueira Jørgensen, Scheyla D.

AU - Abdi, Ismahan Mahad

AU - Wasan, Kishor M.

AU - Rades, Thomas

AU - Müllertz, Anette

PY - 2019

Y1 - 2019

N2 - The effect of drug load and digestion on the solubilization and absorption of fenofibrate in self-nanoemulsifying drug delivery system (SNEDDS) was assessed in a pharmacokinetic study in rats and in an in vitro lipolysis model. SNEDDS containing fenofibrate at 75% of equilibrium solubility (Seq), a super-saturated SNEDDS (super-SNEDDS) containing fenofibrate at 150% of Seq and a super-SNEDDS suspension containing fenofibrate at 100% of Seq and an additional 50% Seq fenofibrate suspended (150% of Seq in total) were used. To assess the effect of lipid digestion on fenofibrate absorption in rats and fenofibrate solubilization during in vitro lipolysis, the lipase inhibitor orlistat was added at 1% (w/w) to the SNEDDS, resulting in six different SNEDDS: SNEDDS, super-SNEDDS and super-SNEDDS suspension with and without orlistat 1% (w/w). In vivo, super-SNEDDS had a higher Cmax and AUC0-30h compared to SNEDDS and super-SNEDDS suspension, both with and without orlistat. While orlistat did not affect fenofibrate absorption in SNEDDS and super-SNEDDS, an increase of Tmax and AUC0-30h for super-SNEDDS suspension was found when orlistat was present. During in vitro lipolysis, the addition of orlistat decreased digestion and lowered drug precipitation. Super-SNEDDS showed significantly increased absorption in rats compared to SNEDDS and super-SNEDDS suspension and the inhibition of digestion resulted in prolonged and increased absorption for the super-SNEDDS suspension.

AB - The effect of drug load and digestion on the solubilization and absorption of fenofibrate in self-nanoemulsifying drug delivery system (SNEDDS) was assessed in a pharmacokinetic study in rats and in an in vitro lipolysis model. SNEDDS containing fenofibrate at 75% of equilibrium solubility (Seq), a super-saturated SNEDDS (super-SNEDDS) containing fenofibrate at 150% of Seq and a super-SNEDDS suspension containing fenofibrate at 100% of Seq and an additional 50% Seq fenofibrate suspended (150% of Seq in total) were used. To assess the effect of lipid digestion on fenofibrate absorption in rats and fenofibrate solubilization during in vitro lipolysis, the lipase inhibitor orlistat was added at 1% (w/w) to the SNEDDS, resulting in six different SNEDDS: SNEDDS, super-SNEDDS and super-SNEDDS suspension with and without orlistat 1% (w/w). In vivo, super-SNEDDS had a higher Cmax and AUC0-30h compared to SNEDDS and super-SNEDDS suspension, both with and without orlistat. While orlistat did not affect fenofibrate absorption in SNEDDS and super-SNEDDS, an increase of Tmax and AUC0-30h for super-SNEDDS suspension was found when orlistat was present. During in vitro lipolysis, the addition of orlistat decreased digestion and lowered drug precipitation. Super-SNEDDS showed significantly increased absorption in rats compared to SNEDDS and super-SNEDDS suspension and the inhibition of digestion resulted in prolonged and increased absorption for the super-SNEDDS suspension.

KW - Absorption

KW - Digestion

KW - Fenofibrate

KW - Orlistat

KW - SNEDDS

KW - Super-SNEDDS

KW - Supersaturation

U2 - 10.1016/j.ejpb.2019.07.002

DO - 10.1016/j.ejpb.2019.07.002

M3 - Journal article

C2 - 31276759

AN - SCOPUS:85068411206

VL - 142

SP - 258

EP - 264

JO - European Journal of Pharmaceutics and Biopharmaceutics

JF - European Journal of Pharmaceutics and Biopharmaceutics

SN - 0939-6411

ER -

ID: 241099217

Department of Pharmacy