BINDING OF HUMAN SERUM AMYLOID-P COMPONENT (HSAP) TO HUMAN NEUTROPHILS

被引：25

作者：

LANDSMANN, P

ROSEN, O

PONTET, M

PRAS, M

LEVARTOWSKY, D

SHEPHARD, EG

FRIDKIN, M

机构：

[1] WEIZMANN INST SCI, DEPT ORGAN CHEM, IL-76100 REHOVOT, ISRAEL

[2] UER BIOMED SAINTS PERES, CHIM BIOL LAB, PARIS, FRANCE

[3] CHAIM SHEBA MED CTR, HELLER INST MED RES, RAMAT GAN, ISRAEL

[4] UNIV CAPE TOWN, SCH MED, LIVER RES CTR, MRC, CAPE TOWN 7925, SOUTH AFRICA

来源：

EUROPEAN JOURNAL OF BIOCHEMISTRY | 1994年 / 223卷 / 03期

关键词：

D O I：

10.1111/j.1432-1033.1994.tb19056.x

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Human serum amyloid P component (hSAP) and human C-reactive protein (hCRP) are normal serum constituents related to the pentraxin family of plasma proteins. hSAP has morphological and immunochemical identity and extensive sequence similarity to the amyloid P (AP) component found in normal tissues and particularly in amyloid deposits. hCRP and its proteolytic products have been previously shown to bind and to interact with various types of human leukocytes. Binding-displacement experiments with I-125-labeled hSAP and hCRP show that both proteins have specific high affinity binding sites on normal human polymorphonuclear leukocytes (PMN) and each can compete efficiently with the binding of the other. Scatchard analysis of hSAP-displacement curves reveals a heterogeneous population of hSAP-binding sites existing on the PMN cells, among them about 300000 low-affinity binding sites with K-d less than or equal to 5X10(-6)M and about 30000 high-affinity binding sites with K-d less than or equal to 5x10(-8)M. hAP was found to be degraded by enzymes from human neutrophils to yield a mixture of low-molecular-mass peptides, similarly to the case of CRP reported previously. The binding of hSAP can be efficiently inhibited by this peptide mixture. The results suggest that both hCRP and hSAP, together with related peptides, may participate in vivo in an unknown mechanism of regulation of human neutrophils.

引用

页码：805 / 811

页数：7

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