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在支气管扩张患者的支气管肺泡灌洗液中发现的人类中性粒细胞胶原酶(MMP-8)与疾病严重程度相关。

Human neutrophil collagenase (MMP-8), identified in bronchiectasis BAL fluid, correlates with severity of disease.

作者信息

Sepper R, Konttinen Y T, Ding Y, Takagi M, Sorsa T

机构信息

Department of Anatomy, University of Helsinki, Finland.

出版信息

Chest. 1995 Jun;107(6):1641-7. doi: 10.1378/chest.107.6.1641.

Abstract

Collagenases in bronchoalveolar lavage fluid (BALF) of patients with bronchiectasis and healthy subjects were characterized using specific functional and immunologic assays. The BAL fluid contained interstitial collagenase and collagenolytic proteinases of bacterial origin. Collagenase activities, obtained after organomercurial activation, correlated with the severity of bronchiectasis. In severe cases, collagenase activities were 3.5 x 10(-7) IU/L/48 h or 4.8 x 10(-6) IU/g/48 h (p < 0.01), in moderate ones 1.74 x 10(-7) IU/L/48 h or 3.35 x 10(-6) IU/g/48 h (p < 0.05), and in mild cases 0.32 x 10(-7) IU/L/48 h or 0.7 x 10(-6) IU/g/48 h (p < 0.05). The corresponding activities in healthy control subjects were 0.08 x 10(-7) IU/L/48 h or 0.13 x 10(-6) IU/g/48 h. The cellular origin of interstitial collagenase was assessed with doxycycline inhibition test utilizing the differential sensitivity of fibroblast-type collagenase/MMP-1 (IC50 = 280 microM) and neutrophil-type collagenase/MMP-8 (IC50 = 26 microM) to the anticollagenolytic, nonantimicrobial doxycycline action. Interstitial collagenase, contained in BALF, was totally inhibited by 100 microM of doxycycline. It can therefore be concluded that most of mammalian collagenase presented in inflamed fluid of bronchiectasis originated from neutrophils. The molecular forms of neutrophil-type collagenase/MMP-8 were confirmed and analyzed by Western-blot, which showed evidence of the proteolytic conversion of the latent 85-kD MMP-8 proenzyme species into active 65-kD molecular weight species. These findings strongly suggest involvement of proteolytic activation pathway of proMMP-8, especially in severe and moderate forms of bronchiectasis. Furthermore, collagenolytic proteases of bacterial origins may also participate in tissue destruction of the lung.

摘要

采用特定的功能和免疫分析方法,对支气管扩张症患者和健康受试者支气管肺泡灌洗液(BALF)中的胶原酶进行了特性分析。BALF中含有间质胶原酶和细菌来源的胶原分解蛋白酶。经有机汞激活后获得的胶原酶活性与支气管扩张的严重程度相关。在严重病例中,胶原酶活性为3.5×10⁻⁷IU/L/48小时或4.8×10⁻⁶IU/g/48小时(p<0.01);中度病例为1.74×10⁻⁷IU/L/48小时或3.35×10⁻⁶IU/g/48小时(p<0.05);轻度病例为0.32×10⁻⁷IU/L/48小时或0.7×10⁻⁶IU/g/48小时(p<0.05)。健康对照受试者的相应活性为0.08×10⁻⁷IU/L/48小时或0.13×10⁻⁶IU/g/48小时。利用成纤维细胞型胶原酶/MMP-1(IC50 = 280微摩尔)和中性粒细胞型胶原酶/MMP-8(IC50 = 26微摩尔)对抗胶原分解、非抗菌强力霉素作用的不同敏感性,通过强力霉素抑制试验评估间质胶原酶的细胞来源。BALF中所含的间质胶原酶可被100微摩尔的强力霉素完全抑制。因此可以得出结论,支气管扩张症炎症液中存在的大多数哺乳动物胶原酶源自中性粒细胞。通过蛋白质免疫印迹法对中性粒细胞型胶原酶/MMP-8的分子形式进行了确认和分析,结果显示有证据表明潜在的85-kD MMP-8前酶物种发生蛋白水解转化为活性65-kD分子量物种。这些发现强烈提示proMMP-8的蛋白水解激活途径参与其中,尤其是在重度和中度支气管扩张症中。此外,细菌来源的胶原分解蛋白酶也可能参与肺部组织破坏。

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