Antifungal nickel(II) complexes derived from amino sugars against pathogenic yeast, Candida albicans

Nickel(II) complexes containing N-glycosides derived from D-glucosamine ( D-GlcN) and ethylenediamine (en) and trimethylenediamine (tn), [Ni( D-GlcN-en) 2]Cl 2·H 2O ( 1) ( D-GlcN-en=1-{(2-aminoethyl)amino}-2-amino-1,2-dideoxy- D-glucose) and [Ni( D-GlcN-tn) 2]Cl 2·4H 2O ( 2) ( D-GlcN-tn=1-{(3-aminop...

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Published in:Journal of inorganic biochemistry Vol. 69; no. 1; pp. 15 - 23
Main Authors: Yano, Shigenobu, Inoue, Sahoko, Nouchi, Reiko, Mogami, Kaoru, Shinohara, Yoshie, Yasuda, Yukiko, Kato, Masako, Tanase, Tomoaki, Kakuchi, Toyoji, Mikata, Yuji, Suzuki, Takahito, Yamamoto, Yasuhiro
Format: Journal Article
Language:English
Published: United States Elsevier Inc 01-02-1998
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Abstract Nickel(II) complexes containing N-glycosides derived from D-glucosamine ( D-GlcN) and ethylenediamine (en) and trimethylenediamine (tn), [Ni( D-GlcN-en) 2]Cl 2·H 2O ( 1) ( D-GlcN-en=1-{(2-aminoethyl)amino}-2-amino-1,2-dideoxy- D-glucose) and [Ni( D-GlcN-tn) 2]Cl 2·4H 2O ( 2) ( D-GlcN-tn=1-{(3-aminopropyl)amino}-2-amino-1,2-dideoxy- D-glucose), are fairly stable in water at room temperature and showed effective antifungal activity against pathogenic yeast, Candida albicans, with the MIC (minimal concentration of inhibition) values of the complexes being 0.25 mM. The results obtained enzyme assays by using preparations of C. albicans chitinase fraction suggested that the sugar complexes 1 and 2 played a role of novel chitinase (chitin-degradation enzyme) inhibitor, where the modes of inhibition were competitive ( K i =1.3 mM for 1, K i =1.8 mM for 2). The newly prepared nickel(II) complex 2 was characterized by elemental analysis, magnetic susceptibility, electronic absorption and circular dichroism spectroscopies, and an X-ray crystallographic analysis.
AbstractList Nickel(II) complexes containing N-glycosides derived from D-glucosamine ( D-GlcN) and ethylenediamine (en) and trimethylenediamine (tn), [Ni( D-GlcN-en) 2]Cl 2·H 2O ( 1) ( D-GlcN-en=1-{(2-aminoethyl)amino}-2-amino-1,2-dideoxy- D-glucose) and [Ni( D-GlcN-tn) 2]Cl 2·4H 2O ( 2) ( D-GlcN-tn=1-{(3-aminopropyl)amino}-2-amino-1,2-dideoxy- D-glucose), are fairly stable in water at room temperature and showed effective antifungal activity against pathogenic yeast, Candida albicans, with the MIC (minimal concentration of inhibition) values of the complexes being 0.25 mM. The results obtained enzyme assays by using preparations of C. albicans chitinase fraction suggested that the sugar complexes 1 and 2 played a role of novel chitinase (chitin-degradation enzyme) inhibitor, where the modes of inhibition were competitive ( K i =1.3 mM for 1, K i =1.8 mM for 2). The newly prepared nickel(II) complex 2 was characterized by elemental analysis, magnetic susceptibility, electronic absorption and circular dichroism spectroscopies, and an X-ray crystallographic analysis.
Nickel(II) complexes containing N-glycosides derived from D-glucosamine (D-GlcN) and ethylenediamine (en) and trimethylenediamine (tn), [Ni(D-GlcN-en)2]Cl2.H2O (1) (D-GlcN-en = 1-¿(2-aminoethyl)amino¿-2-amino-1,2-dideoxy-D-glucose) and [Ni(D-GlcN-tn)2]Cl2.4H2O (2) (D-GlcN-tn = 1-¿(3-aminopropyl)amino¿-2-amino-1,2-dideoxy-D-glucose), are fairly stable in water at room temperature and showed effective antifungal activity against pathogenic yeast, Candida albicans, with the MIC (minimal concentration of inhibition) values of the complexes being 0.25 mM. The results obtained enzyme assays by using preparations of C. albicans chitinase fraction suggested that the sugar complexes 1 and 2 played a role of novel chitinase (chitin-degradation enzyme) inhibitor, where the modes of inhibition were competitive (Ki = 1.3 mM for 1, Ki = 1.8 mM for 2). The newly prepared nickel(II) complex 2 was characterized by elemental analysis, magnetic susceptibility, electronic absorption and circular dichroism spectroscopies, and an X-ray crystallographic analysis.
Author Tanase, Tomoaki
Suzuki, Takahito
Nouchi, Reiko
Mogami, Kaoru
Inoue, Sahoko
Yasuda, Yukiko
Kato, Masako
Yano, Shigenobu
Shinohara, Yoshie
Kakuchi, Toyoji
Mikata, Yuji
Yamamoto, Yasuhiro
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  givenname: Yasuhiro
  surname: Yamamoto
  fullname: Yamamoto, Yasuhiro
  organization: Department of Chemistry, Faculty of Science, Toho University, Funabashi 274, Japan
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Issue 1
Keywords Candida albicans
Nickel(II) complexes of N-Glycoside
Antifungal nickel(II) complex
Amino sugar
Crystal structure
Language English
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Snippet Nickel(II) complexes containing N-glycosides derived from D-glucosamine ( D-GlcN) and ethylenediamine (en) and trimethylenediamine (tn), [Ni( D-GlcN-en) 2]Cl...
Nickel(II) complexes containing N-glycosides derived from D-glucosamine (D-GlcN) and ethylenediamine (en) and trimethylenediamine (tn), [Ni(D-GlcN-en)2]Cl2.H2O...
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SubjectTerms Amino sugar
Antifungal Agents - chemical synthesis
Antifungal Agents - pharmacology
Antifungal nickel(II) complex
Candida albicans
Candida albicans - drug effects
Circular Dichroism
Crystal structure
Crystallography, X-Ray
Diamines
Ethylenediamines
Glucosamine
Kinetics
Microscopy, Phase-Contrast
Models, Molecular
Nickel
Nickel(II) complexes of N-Glycoside
Organometallic Compounds - pharmacology
Spectrophotometry, Infrared
Title Antifungal nickel(II) complexes derived from amino sugars against pathogenic yeast, Candida albicans
URI https://dx.doi.org/10.1016/S0162-0134(97)10004-6
https://www.ncbi.nlm.nih.gov/pubmed/9606935
https://search.proquest.com/docview/79900238
Volume 69
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