Current status of rational design of prodrugs targeting the intestinal di/tri-peptide transporter hPEPT1 (SLC15A1)

Lasse Saaby; Carsten Uhd Nielsen; Bente Steffansen; Birger Brodin; S. B.larsen, Larsen

doi:10.1016/S1773-2247(13)50047-5

Current status of rational design of prodrugs targeting the intestinal di/tri-peptide transporter hPEPT1 (SLC15A1)

Lasse Saaby, Carsten Uhd Nielsen, Bente Steffansen, Birger Brodin, S. B.larsen, Larsen

2 Citations (Scopus)

Abstract

The intestinal di/tri-peptide transporter hPEPT1 has broad substrate specificity, accommodating uptake of the majority of investigated di- and tripeptides, as well as of a number of drug compounds. This transport system has a high capacity and it has been hypothesized that hPEPT1-mediated uptake of drug compounds, conjugated with promoieties so as to resemble di- or tripeptides, may be a strategy for increasing the intestinal permeability of compounds with otherwise low bioavailability. Based on the research activities of our group during the last decade, as well as on general research in the field, the present review aims at giving a brief overview of structure-activity relationships for hPEPT1, and to provide a critical evaluation of whether hPEPT1-targeted prodrugs can be rationally designed.

Original language	English
Journal	Journal of Drug Delivery Science and Technology
Volume	23
Issue number	4
Pages (from-to)	307–314
ISSN	1773-2247
DOIs	https://doi.org/10.1016/S1773-2247(13)50047-5
Publication status	Published - 2013

Access to Document

10.1016/S1773-2247(13)50047-5

Cite this

@article{8f4533f102f24c1aab2f5fa614456081,

title = "Current status of rational design of prodrugs targeting the intestinal di/tri-peptide transporter hPEPT1 (SLC15A1)",

abstract = "The intestinal di/tri-peptide transporter hPEPT1 has broad substrate specificity, accommodating uptake of the majority of investigated di- and tripeptides, as well as of a number of drug compounds. This transport system has a high capacity and it has been hypothesized that hPEPT1-mediated uptake of drug compounds, conjugated with promoieties so as to resemble di- or tripeptides, may be a strategy for increasing the intestinal permeability of compounds with otherwise low bioavailability. Based on the research activities of our group during the last decade, as well as on general research in the field, the present review aims at giving a brief overview of structure-activity relationships for hPEPT1, and to provide a critical evaluation of whether hPEPT1-targeted prodrugs can be rationally designed.",

author = "Lasse Saaby and Nielsen, {Carsten Uhd} and Bente Steffansen and Birger Brodin and Larsen, {S. B.larsen,}",

year = "2013",

doi = "10.1016/S1773-2247(13)50047-5",

language = "English",

volume = "23",

pages = "307–314",

journal = "Journal of Drug Delivery Science and Technology",

issn = "1773-2247",

publisher = "Elsevier",

number = "4",

}

TY - JOUR

T1 - Current status of rational design of prodrugs targeting the intestinal di/tri-peptide transporter hPEPT1 (SLC15A1)

AU - Saaby, Lasse

AU - Nielsen, Carsten Uhd

AU - Steffansen, Bente

AU - Brodin, Birger

AU - Larsen, S. B.larsen,

PY - 2013

Y1 - 2013

N2 - The intestinal di/tri-peptide transporter hPEPT1 has broad substrate specificity, accommodating uptake of the majority of investigated di- and tripeptides, as well as of a number of drug compounds. This transport system has a high capacity and it has been hypothesized that hPEPT1-mediated uptake of drug compounds, conjugated with promoieties so as to resemble di- or tripeptides, may be a strategy for increasing the intestinal permeability of compounds with otherwise low bioavailability. Based on the research activities of our group during the last decade, as well as on general research in the field, the present review aims at giving a brief overview of structure-activity relationships for hPEPT1, and to provide a critical evaluation of whether hPEPT1-targeted prodrugs can be rationally designed.

AB - The intestinal di/tri-peptide transporter hPEPT1 has broad substrate specificity, accommodating uptake of the majority of investigated di- and tripeptides, as well as of a number of drug compounds. This transport system has a high capacity and it has been hypothesized that hPEPT1-mediated uptake of drug compounds, conjugated with promoieties so as to resemble di- or tripeptides, may be a strategy for increasing the intestinal permeability of compounds with otherwise low bioavailability. Based on the research activities of our group during the last decade, as well as on general research in the field, the present review aims at giving a brief overview of structure-activity relationships for hPEPT1, and to provide a critical evaluation of whether hPEPT1-targeted prodrugs can be rationally designed.

U2 - 10.1016/S1773-2247(13)50047-5

DO - 10.1016/S1773-2247(13)50047-5

M3 - Journal article

SN - 1773-2247

VL - 23

SP - 307

EP - 314

JO - Journal of Drug Delivery Science and Technology

JF - Journal of Drug Delivery Science and Technology

IS - 4

ER -

Current status of rational design of prodrugs targeting the intestinal di/tri-peptide transporter hPEPT1 (SLC15A1)

Abstract

Access to Document

Fingerprint

Cite this