Litcius/Paper detail

L-Type amino acid transporter 1 as a target for drug delivery

Elena Puris, Mikko Gynther, Seppo Auriola, Kristiina M. Huttunen

2020Pharmaceutical Research201 citationsDOIOpen Access PDF

Abstract

Abstract Our growing understanding of membrane transporters and their substrate specificity has opened a new avenue in the field of targeted drug delivery. The L-type amino acid transporter 1 (LAT1) has been one of the most extensively investigated transporters for delivering drugs across biological barriers. The transporter is predominantly expressed in cerebral cortex, blood-brain barrier, blood-retina barrier, testis, placenta, bone marrow and several types of cancer. Its physiological function is to mediate Na + and pH independent exchange of essential amino acids: leucine, phenylalanine, etc. Several drugs and prodrugs designed as LAT1 substrates have been developed to improve targeted delivery into the brain and cancer cells. Thus, the anti-parkinsonian drug, L-Dopa, the anti-cancer drug, melphalan and the anti-epileptic drug gabapentin, all used in clinical practice, utilize LAT1 to reach their target site. These examples provide supporting evidence for the utility of the LAT1-mediated targeted delivery of the (pro)drug. This review comprehensively summarizes recent advances in LAT1-mediated targeted drug delivery. In addition, the use of LAT1 is critically evaluated and limitations of the approach are discussed.

Topics & Concepts

Drug deliveryProdrugTransporterPharmacologyDrugAmino acidTargeted drug deliveryMedicineBlood–brain barrierChemistryBiochemistryCentral nervous systemInternal medicineGeneOrganic chemistryAmino Acid Enzymes and MetabolismDrug Transport and Resistance MechanismsEpigenetics and DNA Methylation