TY - JOUR
T1 - May glutamine addiction drive the delivery of antitumor cisplatin-based Pt(IV) prodrugs?
AU - RAVERA, Mauro
AU - GABANO, Elisabetta
AU - Stefano, TINELLO
AU - Ilaria, ZANELLATO
AU - Domenico, OSELLA
PY - 2017/1/1
Y1 - 2017/1/1
N2 - A small series of Pt(IV) prodrugs containing Gln-like (Gln=glutamine) axial ligands has been designed with the aim to take advantage of the increased demand of Gln showed by some cancer cells (glutamine addiction). In complex 4 the Gln, linked through the α-carboxylic group is recognized by the Gln transporters, in particular by the solute carrier transporter SLC1A5. All compounds showed cellular accumulation, as well as antiproliferative activity, related to their lipophilicity, as already demonstrated for the majority of Pt(IV) prodrugs, that enter cells mainly by passive diffusion. On the contrary, when the Gln concentration in cell medium is near or lower to the physiological value, complex 4 acts as a Trojan horse: it enters SLC1A5-overexpressing cells, where, upon reduction, it releases the active metabolite cisplatin and the Gln-containing ligand, thus preventing any possible extrusion by the L-type amino acid transporter LAT1. This selective mechanism could decrease off-target accumulation of 4 and, consequently, Pt-associated side-effects.
AB - A small series of Pt(IV) prodrugs containing Gln-like (Gln=glutamine) axial ligands has been designed with the aim to take advantage of the increased demand of Gln showed by some cancer cells (glutamine addiction). In complex 4 the Gln, linked through the α-carboxylic group is recognized by the Gln transporters, in particular by the solute carrier transporter SLC1A5. All compounds showed cellular accumulation, as well as antiproliferative activity, related to their lipophilicity, as already demonstrated for the majority of Pt(IV) prodrugs, that enter cells mainly by passive diffusion. On the contrary, when the Gln concentration in cell medium is near or lower to the physiological value, complex 4 acts as a Trojan horse: it enters SLC1A5-overexpressing cells, where, upon reduction, it releases the active metabolite cisplatin and the Gln-containing ligand, thus preventing any possible extrusion by the L-type amino acid transporter LAT1. This selective mechanism could decrease off-target accumulation of 4 and, consequently, Pt-associated side-effects.
KW - Anticancer prodrugs
KW - Cancer metabolism
KW - Drug targeting and delivery
KW - Glutamine metabolism
KW - Pt(IV) complexes
KW - Anticancer prodrugs
KW - Cancer metabolism
KW - Drug targeting and delivery
KW - Glutamine metabolism
KW - Pt(IV) complexes
UR - https://iris.uniupo.it/handle/11579/80037
U2 - 10.1016/j.jinorgbio.2016.11.024
DO - 10.1016/j.jinorgbio.2016.11.024
M3 - Article
SN - 0162-0134
VL - 167
SP - 27
EP - 35
JO - Journal of Inorganic Biochemistry
JF - Journal of Inorganic Biochemistry
ER -