Inclusion of methotrexate in alkyl-cyclodextrins: effects of host substituents on the stability of complexes

Franco PATTARINO; Lorella GIOVANNELLI; Giovanni Battista GIOVENZANA; Maurizio RINALDI; M. TROTTA

Inclusion of methotrexate in alkyl-cyclodextrins: effects of host substituents on the stability of complexes

Department of Pharmaceutical Sciences

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Abstract

The formation of complexes between an antineoplastic drug, methotrexate (MTX), and a series of native cyclodextrins (αCD, βCD, γCD) and synthetic or commercial β-derivatives (methylated, dimethylated and hydroxypropylated βCDs) was studied using the phase solubility and permeation methods, NMR and DSC. The apparent stability constants determined from the solubility diagram (Kcs) are in excellent agreement (P < 0.00001) with those calculated by the permeation method (Kcp). The degree of substitution (DS) and position of substituents on glucose re- sidues significantly affect the complexing ability of β-inclusion agents. In particular, for dimethyl-derivatives, the presence of the alkyl-groups at the secondary face of CD (positions 2 and 3), sterically prevents host-guest interactions, while a methyl group in position 6 allows an easier association with MTX

Original language	English
Pages (from-to)	465-468
Number of pages	4
Journal	Journal of Drug Delivery Science and Technology
Volume	15
Issue number	6
Publication status	Published - 1 Jan 2005

Cite this

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title = "Inclusion of methotrexate in alkyl-cyclodextrins: effects of host substituents on the stability of complexes",

abstract = "The formation of complexes between an antineoplastic drug, methotrexate (MTX), and a series of native cyclodextrins (αCD, βCD, γCD) and synthetic or commercial β-derivatives (methylated, dimethylated and hydroxypropylated βCDs) was studied using the phase solubility and permeation methods, NMR and DSC. The apparent stability constants determined from the solubility diagram (Kcs) are in excellent agreement (P < 0.00001) with those calculated by the permeation method (Kcp). The degree of substitution (DS) and position of substituents on glucose re- sidues significantly affect the complexing ability of β-inclusion agents. In particular, for dimethyl-derivatives, the presence of the alkyl-groups at the secondary face of CD (positions 2 and 3), sterically prevents host-guest interactions, while a methyl group in position 6 allows an easier association with MTX",

author = "Franco PATTARINO and Lorella GIOVANNELLI and GIOVENZANA, \{Giovanni Battista\} and Maurizio RINALDI and M. TROTTA",

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TY - JOUR

T1 - Inclusion of methotrexate in alkyl-cyclodextrins: effects of host substituents on the stability of complexes

AU - PATTARINO, Franco

AU - GIOVANNELLI, Lorella

AU - GIOVENZANA, Giovanni Battista

AU - RINALDI, Maurizio

AU - TROTTA, M.

PY - 2005/1/1

Y1 - 2005/1/1

N2 - The formation of complexes between an antineoplastic drug, methotrexate (MTX), and a series of native cyclodextrins (αCD, βCD, γCD) and synthetic or commercial β-derivatives (methylated, dimethylated and hydroxypropylated βCDs) was studied using the phase solubility and permeation methods, NMR and DSC. The apparent stability constants determined from the solubility diagram (Kcs) are in excellent agreement (P < 0.00001) with those calculated by the permeation method (Kcp). The degree of substitution (DS) and position of substituents on glucose re- sidues significantly affect the complexing ability of β-inclusion agents. In particular, for dimethyl-derivatives, the presence of the alkyl-groups at the secondary face of CD (positions 2 and 3), sterically prevents host-guest interactions, while a methyl group in position 6 allows an easier association with MTX

AB - The formation of complexes between an antineoplastic drug, methotrexate (MTX), and a series of native cyclodextrins (αCD, βCD, γCD) and synthetic or commercial β-derivatives (methylated, dimethylated and hydroxypropylated βCDs) was studied using the phase solubility and permeation methods, NMR and DSC. The apparent stability constants determined from the solubility diagram (Kcs) are in excellent agreement (P < 0.00001) with those calculated by the permeation method (Kcp). The degree of substitution (DS) and position of substituents on glucose re- sidues significantly affect the complexing ability of β-inclusion agents. In particular, for dimethyl-derivatives, the presence of the alkyl-groups at the secondary face of CD (positions 2 and 3), sterically prevents host-guest interactions, while a methyl group in position 6 allows an easier association with MTX

UR - https://iris.uniupo.it/handle/11579/30412

M3 - Article

SN - 1773-2247

VL - 15

SP - 465

EP - 468

JO - Journal of Drug Delivery Science and Technology

JF - Journal of Drug Delivery Science and Technology

IS - 6

ER -

Inclusion of methotrexate in alkyl-cyclodextrins: effects of host substituents on the stability of complexes

Abstract

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