RAPID QUANTIFICATION OF C3A AND C5A USING A COMBINATION OF CHROMATOGRAPHIC AND IMMUNOASSAY PROCEDURES

被引：34

作者：

HARTMANN, H

LUBBERS, B

CASARETTO, M

BAUTSCH, W

KLOS, A

KOHL, J

机构：

[1] HANNOVER MED SCH,INST MED MIKROBIOL,HANNOVER,GERMANY

[2] ABION GMBH,JULICH,GERMANY

[3] DEUTSCH WOLLFORSCHUNGSINST AACHEN,AACHEN,GERMANY

来源：

JOURNAL OF IMMUNOLOGICAL METHODS | 1993年 / 166卷 / 01期

关键词：

C3A/C3ADR; C3; C5A/C5ADR; ANAPHYLATOXIN ASSAY; MONOCLONAL ANTIBODY;

D O I：

10.1016/0022-1759(93)90326-3

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

Monoclonal antibodies were isolated which reacted specifically with the complement cleavage products C3a, C3adR, C5a, and C5adR but not with the parent molecules C3 or C5. In both cases the mAbs showed a higher affinity towards the desArg forms. These mAbs were used as capture antibodies in immunoassays for C3a/C3adR and C5a/C5adR. The immunoassays are based on the ABICAP technology which ensures for a rapid measurement. Due to the large binding capacity and the very short diffusion pathways in the gel-matrix the binding equilibrium between capture antibodies and the antigen is reached whilst the sample is flowing through the column. Therefore this test represents an endpoint assay offering the possibility of using a single calibration curve for a large number of measurements. With the C3adR assay concentrations down to 16 ng/ml C3adR can be detected. The lower detection limit of the C5adR assay is 1 ng/ml C5adR. The tests for C3a/C3adR, and C5a/C5adR can be performed in 20 to 25 min and this rapid processing of plasma samples should permit the application of these parameters for diagnostic purposes and patient management.

引用

页码：35 / 44

页数：10

共 31 条

[11] ELEVATED PLASMA-LEVELS OF THE ANAPHYLATOXINS C3A AND C4A ARE ASSOCIATED WITH A FATAL OUTCOME IN SEPSIS [J].

HACK, CE ;

NUIJENS, JH ;

FELTBERSMA, RJF ;

SCHREUDER, WO ;

EERENBERGBELMER, AJM ;

PAARDEKOOPER, J ;

BRONSVELD, W ;

THIJS, LG .

AMERICAN JOURNAL OF MEDICINE, 1989, 86 (01) :20-26

[12] ANAPHYLATOXIN GENERATION IN MULTISYSTEM ORGAN FAILURE [J].

HEIDEMAN, M ;

HUGLI, TE .

JOURNAL OF TRAUMA-INJURY INFECTION AND CRITICAL CARE, 1984, 24 (12) :1038-1043

[13]

HEMMILA I, 1985, CLIN CHEM, V31, P359

[14] INCREASED LEVELS OF PLASMA ANAPHYLATOXINS IN SYSTEMIC LUPUS-ERYTHEMATOSUS PREDICT FLARES OF THE DISEASE AND MAY ELICIT VASCULAR INJURY IN LUPUS CEREBRITIS [J].

HOPKINS, P ;

BELMONT, HM ;

BUYON, J ;

PHILIPS, M ;

WEISSMANN, G ;

ABRAMSON, SB .

ARTHRITIS AND RHEUMATISM, 1988, 31 (05) :632-641

[15]

HUGLI TE, 1984, SPRINGER SEMIN IMMUN, V7, P193

[16] MEASUREMENT OF THE CHEMOTACTIC COMPLEMENT FRAGMENT C5A IN RHEUMATOID SYNOVIAL-FLUIDS BY RADIOIMMUNOASSAY - ROLE OF C5A IN THE ACUTE INFLAMMATORY PHASE [J].

JOSE, PJ ;

MOSS, IK ;

MAINI, RN ;

WILLIAMS, TJ .

ANNALS OF THE RHEUMATIC DISEASES, 1990, 49 (10) :747-752

[17]

KIM BB, 1993, IN PRESS ANAL BIOCH

[18] DETECTION OF NATIVE HUMAN-COMPLEMENT COMPONENTS C-3 AND C5 AND THEIR PRIMARY ACTIVATION PEPTIDES C3A AND C5A (ANAPHYLATOXIC PEPTIDES) BY ELISAS WITH MONOCLONAL-ANTIBODIES [J].

KLOS, A ;

IHRIG, V ;

MESSNER, M ;

GRABBE, J ;

BITTERSUERMANN, D .

JOURNAL OF IMMUNOLOGICAL METHODS, 1988, 111 (02) :241-252

[19]

KOHL J, 1993, COMPLEMENT HLTH DIS, P295

[20] SYNTHETIC PEPTIDES AS ANTAGONISTS OF THE ANAPHYLATOXIN C3A [J].

KRETZSCHMAR, T ;

POHL, M ;

CASARETTO, M ;

PRZEWOSNY, M ;

BAUTSCH, W ;

KLOS, A ;

SAUNDERS, D ;

KOHL, J .

EUROPEAN JOURNAL OF BIOCHEMISTRY, 1992, 210 (01) :185-191

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