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 |
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Main Authors: | , , , , , , , , , , , |
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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 |
Author_xml | – sequence: 1 givenname: Shigenobu surname: Yano fullname: Yano, Shigenobu organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 2 givenname: Sahoko surname: Inoue fullname: Inoue, Sahoko organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 3 givenname: Reiko surname: Nouchi fullname: Nouchi, Reiko organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 4 givenname: Kaoru surname: Mogami fullname: Mogami, Kaoru organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 5 givenname: Yoshie surname: Shinohara fullname: Shinohara, Yoshie organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 6 givenname: Yukiko surname: Yasuda fullname: Yasuda, Yukiko organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 7 givenname: Masako surname: Kato fullname: Kato, Masako organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 8 givenname: Tomoaki surname: Tanase fullname: Tanase, Tomoaki organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 9 givenname: Toyoji surname: Kakuchi fullname: Kakuchi, Toyoji organization: Graduate School of Environmental Earth Science, Hokkaido University, Sapporo 060, Japan – sequence: 10 givenname: Yuji surname: Mikata fullname: Mikata, Yuji organization: Department of Chemistry, Faculty of Science, Nara Women's University, Kitauoya-nishimachi, Nara 630, Japan – sequence: 11 givenname: Takahito surname: Suzuki fullname: Suzuki, Takahito organization: Department of Biology, Faculty of Science, Nara Women's University, Nara 630, Japan – sequence: 12 givenname: Yasuhiro surname: Yamamoto fullname: Yamamoto, Yasuhiro organization: Department of Chemistry, Faculty of Science, Toho University, Funabashi 274, Japan |
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Cites_doi | 10.1128/AAC.30.3.418 10.1099/00221287-138-1-97 10.1016/0010-8545(88)85007-0 10.1007/BF02157171 10.1248/bpb.18.923 10.1039/dt9930001699 10.1002/zaac.18990210137 10.1271/bbb.57.1699 10.1021/ic00198a014 10.1039/dt9930002645 10.1016/S0040-4039(00)84560-8 10.1021/ja01056a023 10.1021/ja00187a011 10.1016/S0021-9258(18)55057-2 10.1021/ic00079a003 10.1021/ic00296a004 10.1016/0040-4039(95)00194-H 10.1107/S0365110X6500004X 10.1021/ja00547a040 |
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Copyright | 1998 Elsevier Science Inc. |
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Keywords | Candida albicans Nickel(II) complexes of N-Glycoside Antifungal nickel(II) complex Amino sugar Crystal structure |
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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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