Comparison of the effect of lidocaine-epinephrine and prilocaine-felypressine to alter macrophage functions

被引：10

作者：

Azuma, Y ^{[1
]}

Ohura, K ^{[1
]}

机构：

[1] Osaka Dent Univ, Dept Pharmacol, Hirakata, Osaka 5731121, Japan

来源：

INTERNATIONAL IMMUNOPHARMACOLOGY | 2001年 / 1卷 / 05期

关键词：

lidocaine-epinephrine; prilocaine-felypressine; macrophage; epinephrine; superoxide dismutase;

D O I：

10.1016/S1567-5769(01)00027-3

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

In vitro treatment of macrophages with lidocaine-epinephrine or prilocaine-felypressine resulted in inhibition of their adhesion, chemotaxis and phagocytosis. However, prilocaine-felypressine was a much more potent inhibitor of adhesion and phagocytosis than Lidocaine-epinephrine. On the other hand, lidocaine-epinephrine induced transient potentiation of superoxide anion production by macrophages. while prilocaine-felypressine consistently inhibited this. Moreover. lidocaine-epinephrine and prilocaine-felypressine both inhibited the production of hydrogen peroxide. In contrast, epinephrine strongly potentiated superoxide anion production, while markedly inhibiting hydrogen peroxide production. This potentiation by epinephrine was not prevented by adrenergic antagonists. In addition, superoxide dismutase potentiated the production of hydrogen peroxide. which was in part prevented by epinephrine. These results suggest that lidocaine-epinephrine and prilocaine-felypressine inhibit adhesion. chemotaxis, phagocytosis, and the production of hydrogen peroxide by macrophages. In addition, lidocaine-epinephrine evidently differs from prilocaine-felypressine regarding the molecular mechanisms underlying the modulation of superoxide anion production by macrophages. (C) 2001 Elsevier Science B.V. All rights reserved.

引用

页码：911 / 923

页数：13

共 44 条

[11] Antimicrobial effects of lidocaine, bicarbonate, and epinephrine [J].

Epstein, E .

JOURNAL OF THE AMERICAN ACADEMY OF DERMATOLOGY, 1998, 39 (03) :518-519

[12]

FELDMAN JM, 1994, REGION ANESTH, V19, P43

[13] REGULATORY ROLE OF DIVALENT-CATIONS IN HUMAN GRANULOCYTE CHEMOTAXIS - EVIDENCE FOR AN ASSOCIATION BETWEEN CALCIUM EXCHANGES AND MICROTUBULE ASSEMBLY [J].

GALLIN, JI ;

ROSENTHAL, AS .

JOURNAL OF CELL BIOLOGY, 1974, 62 (03) :594-609

[14] ROLE OF PROTEIN-KINASES IN STIMULATION OF HUMAN POLYMORPHONUCLEAR LEUKOCYTE OXIDATIVE-METABOLISM BY VARIOUS AGONISTS - DIFFERENTIAL-EFFECTS OF A NOVEL PROTEIN-KINASE INHIBITOR [J].

GERARD, C ;

MCPHAIL, LC ;

MARFAT, A ;

STIMLERGERARD, NP ;

BASS, DA ;

MCCALL, CE .

JOURNAL OF CLINICAL INVESTIGATION, 1986, 77 (01) :61-65

[15]

HAINES KA, 1990, J IMMUNOL, V144, P4757

[16] Efficacy of lipid soluble, membrane-protective agents against hydrogen peroxide cytotoxicity in cardiac myocytes [J].

Horwitz, LD ;

Wallner, JS ;

Decker, DE ;

Buxser, SE .

FREE RADICAL BIOLOGY AND MEDICINE, 1996, 21 (06) :743-753

[17]

HU WS, 1980, AM J VET RES, V41, P447

[18] EFFECTS OF LIDOCAINE ON INTRACELLULAR CA-2+ AND TENSION IN AIRWAY SMOOTH-MUSCLE [J].

KAI, T ;

NISHIMURA, J ;

KOBAYASHI, S ;

TAKAHASHI, S ;

YOSHITAKE, J ;

KANAIDE, H .

ANESTHESIOLOGY, 1993, 78 (05) :954-965

[19] PROTEIN-KINASE-C ACTIVITY IS NOT INVOLVED IN N-FORMYLMETHIONYL-LEUCYL-PHENYLALANINE-INDUCED PHOSPHOLIPASE-D ACTIVATION IN HUMAN NEUTROPHILS, BUT IS ESSENTIAL FOR CONCOMITANT NADPH OXIDASE ACTIVATION - STUDIES WITH A STAUROSPORINE ANALOG WITH IMPROVED SELECTIVITY FOR PROTEIN-KINASE-C [J].

KESSELS, GCR ;

KRAUSE, KH ;

VERHOEVEN, AJ .

BIOCHEMICAL JOURNAL, 1993, 292 :781-785

[20]

Kouno Motokazu, 1999, Folia Pharmacologica Japonica, V113, P357, DOI 10.1254/fpj.113.357

← 1 2 3 4 5 →