FREEZE-DRYING OF DRUG-ADDITIVE BINARY-SYSTEMS .3. CRYSTALLIZATION OF ALPHA-CYCLODEXTRIN INCLUSION COMPLEX IN FREEZING PROCESS

被引：18

作者：

OGUCHI, T ^{[1
]}

OKADA, M ^{[1
]}

YONEMOCHI, E ^{[1
]}

YAMAMOTO, K ^{[1
]}

NAKAI, Y ^{[1
]}

机构：

[1] CHIBA UNIV,FAC PHARMACEUT SCI,1-33 YAYOICHO,CHIBA 260,JAPAN

来源：

INTERNATIONAL JOURNAL OF PHARMACEUTICS | 1990年 / 61卷 / 1-2期

关键词：

Crystallization; Freeze-drying; Inclusion compound; Stoichiometry; α-Cyclodextrin;

D O I：

10.1016/0378-5173(90)90040-B

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The crystallization of α-cyclodextrin (α-CD) inclusion complexes during the process of freeze-drying has been studied. Benzoic acid, salicylic acid, m-hydroxybenzoic acid, p-hydroxybenzoic acid and methyl p-hydroxybenzoate were used as guest molecules. Various amounts of guest compound were dissolved in aqueous α-CD solution. By annealing the binary solutions at -13 to -18°C, the inclusion complex crystallized readily at a molar ratio of 2:1 (α-CD: guest). All inclusion crystals obtained via freeze-drying were of a channel-type structure, while in the coprecipitation method p-hydroxybenzoic acid and methyl p-hydroxybenzoate formed a layer-type inclusion crystal with α-CD. Further, an aqueous binary solution of α-CD and aspirin (2:1 molar ratio) was slowly frozen at -14°C, and then lyophilized. The infrared spectra and the powder X-ray diffractograms indicated that the channel-type inclusion compound of aspirin with α-CD was formed by freeze-drying, although the coprecipitation method did not provide the inclusion compound crystal. It was assumed that the mechanism of solid-phase formation differed between the freezing and coprecipitation processes and that the channel-type structure of α-CD inclusion crystal was preferentially formed during the freezing process. © 1990.

引用

页码：27 / 34

页数：8

共 19 条

[1]

Bender M. L., 1978, CYCLODEXTRIN CHEM, DOI [10.1007/978-3-642-66842-5, DOI 10.1007/978-3-642-66842-5]

[2] LYOPHILIZATION OF PHARMACEUTICALS .4. DETERMINATION OF EUTECTIC TEMPERATURES OF INORGANIC SALTS [J].

DELUCA, P ;

LACHMAN, L .

JOURNAL OF PHARMACEUTICAL SCIENCES, 1965, 54 (10) :1411-&

[3] LYOPHILIZATION OF PHARMACEUTICALS .I. EFFECT OF CERTAIN PHYSICAL-CHEMICAL PROPERTIES [J].

DELUCA, P ;

LACHMAN, L .

JOURNAL OF PHARMACEUTICAL SCIENCES, 1965, 54 (04) :617-&

[4]

HARADA A, 1981, POLYM J, V8, P777

[5] STRUCTURE CHEMISTRY OF CYCLODEXTRIN COMPLEXES [J].

HARATA, K .

JOURNAL OF THE JAPANESE SOCIETY OF STARCH SCIENCE, 1979, 26 (03) :198-209

[6] THE STRUCTURE OF THE CYCLODEXTRIN COMPLEX .21. CRYSTAL-STRUCTURES OF HEPTAKIS(2,6-DI-O-METHYL)-BETA-CYCLODEXTRIN COMPLEXES WITH PARA-IODOPHENOL AND PARA-NITROPHENOL [J].

HARATA, K .

BULLETIN OF THE CHEMICAL SOCIETY OF JAPAN, 1988, 61 (06) :1939-1944

[7] STRUCTURE OF CYCLODEXTRIN COMPLEX .6. CRYSTAL-STRUCTURE OF "ALPHA-CYCLODEXTRIN-META-NITROPHENOL (1-2) COMPLEX [J].

HARATA, K ;

UEDAIRA, H ;

TANAKA, J .

BULLETIN OF THE CHEMICAL SOCIETY OF JAPAN, 1978, 51 (06) :1627-1634

[8] STRUCTURE OF CYCLODEXTRIN COMPLEX .5. CRYSTAL-STRUCTURES OF ALPHA-CYCLODEXTRIN COMPLEXES WITH PARA-NITROPHENOL AND PARA-HYDROXYBENZOIC ACID [J].

HARATA, K .

BULLETIN OF THE CHEMICAL SOCIETY OF JAPAN, 1977, 50 (06) :1416-1424

[9]

Higuchi T., 1965, PHASE SOLUBILITY TEC, V4, P117

[10]

KOBAYASHI M, 1982, SEIZAI TO KIKAI

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