TOXIN PRODUCTION BY CLOSTRIDIUM-DIFFICILE IN A DEFINED MEDIUM WITH LIMITED AMINO-ACIDS

被引：34

作者：

YAMAKAWA, K ^{[1
]}

KAMIYA, S ^{[1
]}

MENG, XQ ^{[1
]}

KARASAWA, T ^{[1
]}

NAKAMURA, S ^{[1
]}

机构：

[1] KANAZAWA UNIV,SCH MED,DEPT BACTERIOL,KANAZAWA,ISHIKAWA 920,JAPAN

来源：

JOURNAL OF MEDICAL MICROBIOLOGY | 1994年 / 41卷 / 05期

关键词：

D O I：

10.1099/00222615-41-5-319

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

Basal defined medium (BDM) containing vitamins, minerals and seven amino acids-(/L) tryptophan 0.1 g, methionine 0.2 g, valine 0.3 g, isoleucine 0.3 g, proline 0.3 g, leucine 0.4g and cysteine 0.5 g-which appeared to be essential for good growth of Clostridium difficile was prepared. Addition of glycine 0.2 g/L and threonine 0.4 g/L to BDM produced better growth of strain VPI 10463, and this defined medium was designated minimum amino acid-defined medium (MADM). Production of toxins A and B by strain VPI 10463 in 6 x MADM containing (/L) tryptophan 0.6 g, methionine 1.2 g, valine 1.8 g, isoleucine 1.8 g, proline 1.8 g, leucine 24 g, cysteine 0.5 g, glycine 0.2 g and threonine 0.4 g, was much greater than in MADM. Toxin production by 20 C. difficile strains was examined in two defined media-6 x MADM and complete amino acid-defined medium (CADM) containing 18 amino acids-and one complex medium, modified brain heart infusion medium (m-BHI). Simultaneous production of toxins A and B by all test strains was demonstrated in m-BHI and the two defined media. It was also shown that 6 x MADM was generally better than CADM and as effective as m-BHI for stimulating toxin production by 13 strains. This defined medium would be useful for studies on the physiology, metabolism and pathogenicity of C. difficile.

引用

页码：319 / 323

页数：5

共 25 条

[1]

BANNO Y, 1984, REV INFECT DIS, V6, pS11

[2] ANTIBIOTIC-ASSOCIATED PSEUDOMEMBRANOUS COLITIS DUE TO TOXIN-PRODUCING CLOSTRIDIA [J].

BARTLETT, JG ;

CHANG, TW ;

GURWITH, M ;

GORBACH, SL ;

ONDERDONK, AB .

NEW ENGLAND JOURNAL OF MEDICINE, 1978, 298 (10) :531-534

[3] MOLECULAR, IMMUNOLOGICAL, AND BIOLOGICAL CHARACTERIZATION OF A TOXIN-A-NEGATIVE, TOXIN-B-POSITIVE STRAIN OF CLOSTRIDIUM-DIFFICILE [J].

BORRIELLO, SP ;

WREN, BW ;

HYDE, S ;

SEDDON, SV ;

SIBBONS, P ;

KRISHNA, MM ;

TABAQCHALI, S ;

MANEK, S ;

PRICE, AB .

INFECTION AND IMMUNITY, 1992, 60 (10) :4192-4199

[4] ANTIBIOTIC AND PSEUDOMEMBRANOUS COLITIS [J].

BORRIELLO, SP ;

LARSON, HE .

JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY, 1981, 7 :53-&

[5] MOLECULAR CHARACTERIZATION OF THE CLOSTRIDIUM-DIFFICILE TOXIN-A GENE [J].

DOVE, CH ;

WANG, SZ ;

PRICE, SB ;

PHELPS, CJ ;

LYERLY, DM ;

WILKINS, TD ;

JOHNSON, JL .

INFECTION AND IMMUNITY, 1990, 58 (02) :480-488

[6] NONTOXIGENIC STRAINS OF CLOSTRIDIUM-DIFFICILE LACK THE GENES FOR BOTH TOXIN-A AND TOXIN-B [J].

FLUIT, AC ;

WOLFHAGEN, MJHM ;

VERDONK, GPHT ;

JANSZE, M ;

TORENSMA, R ;

VERHOEF, J .

JOURNAL OF CLINICAL MICROBIOLOGY, 1991, 29 (11) :2666-2667

[7]

GEORGE WL, 1978, LANCET, V1, P802

[8] GROWTH OF CLOSTRIDIUM-DIFFICILE AND PRODUCTION OF TOXINS A AND B IN COMPLEX AND DEFINED MEDIA [J].

HASLAM, SC ;

KETLEY, JM ;

MITCHELL, TJ ;

STEPHEN, J ;

BURDON, DW ;

CANDY, DCA .

JOURNAL OF MEDICAL MICROBIOLOGY, 1986, 21 (04) :293-297

[9] CLONING AND EXPRESSION OF THE TOXIN-B GENE OF CLOSTRIDIUM-DIFFICILE [J].

JOHNSON, JL ;

PHELPS, C ;

BARROSO, L ;

ROBERTS, MD ;

LYERLY, DM ;

WILKINS, TD .

CURRENT MICROBIOLOGY, 1990, 20 (06) :397-401

[10]

LARSON HE, 1978, LANCET, V1, P1063

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