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Role of alpha-macroglobulin-elastase complexes in the pathogenesis of elastase-induced emphysema in hamsters.

机译:α-巨球蛋白-弹性蛋白酶复合物在弹性蛋白酶诱导的仓鼠肺气肿发病机理中的作用。

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摘要

Radiolabeled, enzymatically active or chloromethyl ketone-inactivated porcine pancreatic elastase was endotracheally instilled into hamsters. Gel filtration of the bronchopulmonary lavage fluid revealed two major radioactive fractions: one, eluting at 780,000 daltons, corresponding to an alpha-macroglobulin-pancreatic elastase complex, and another, at 68,000 daltons, corresponding to an alpha-1-protease inhibitor-pancreatic elastase complex. Elastolytic activity was recovered in the bronchopulmonary lavage fluid up to 4 d after elastase instillation and was associated with the alpha-macroglobulin-pancreatic elastase complex. Small amounts of this complex were recovered 14 d after instillation. When less than 1% (1.5--1.7 micrograms) of the usual dose of elastase was instilled into hamsters, the major radioactive complex was alpha-1-protease inhibitor-pancreatic elastase complex, and little or no elastolytic activity was found in the lavage fluid. In contrast to the instillation of 220 micrograms of elastase, no disease or hemorrhagic reaction was detected with this low dose, and without hemorrhage only insignificant amounts of alpha-macroglobulin-pancreatic elastase complexes were recovered from the lungs. To study the interaction of circulating antiproteases with elastase, hamster plasma was allowed to interact directly with the radiolabeled elastase; alpha-macroglobulin bound much more of the elastase than alpha-1-protease inhibitor, confirming the findings in the lung lavage experiments. The hamster's susceptibility to pancreatic elastase-induced emphysema may depend on the preferential binding of elastase to alpha-macroglobulin, which protects the elastolytic potential, rather than to alpha-1-protease inhibitor, which inactivates elastase. We speculate that if even a fraction of the residual radioactivity found in the hamster lungs as long as 144 d after instillation of elastase represents enzymatically active alpha-macroglobulin-pancreatic elastase complex, this could serve as a source of persistent elastolytic activity, which might explain the progressive nature of the pulmonary lesion.
机译:将经放射性标记的,具有酶活性或氯甲基酮灭活的猪胰弹性蛋白酶经气管内滴入仓鼠。支气管肺灌洗液的凝胶过滤显示出两个主要的放射性级分:一个以780,000道尔顿洗脱,相当于一个α-巨球蛋白-胰弹性蛋白酶复合物;另一个,以68,000道尔顿洗脱,相当于一个α-1蛋白酶抑制剂-胰腺弹性蛋白酶。复杂。弹性蛋白酶滴注后至4 d,在支气管肺灌洗液中恢复了弹性分解活性,并与α-巨球蛋白-胰腺弹性蛋白酶复合物相关。滴注后14 d回收了少量这种复合物。当将通常剂量的弹性蛋白酶的不足1%(1.5--1.7微克)滴入仓鼠时,主要的放射性复合物为α-1-蛋白酶抑制剂-胰弹性蛋白酶复合物,并且在灌洗液中几乎没有或没有发现弹性体液。与滴注220微克的弹性蛋白酶相反,在这种低剂量下未发现任何疾病或出血反应,并且在没有出血的情况下,仅从肺中回收了少量的α-巨球蛋白-胰弹性蛋白酶复合物。为了研究循环的蛋白酶与弹性蛋白酶的相互作用,允许仓鼠血浆直接与放射性标记的弹性蛋白酶相互作用。 α-巨球蛋白比α-1-蛋白酶抑制剂结合更多的弹性蛋白酶,证实了在肺灌洗实验中的发现。仓鼠对胰腺弹性蛋白酶诱导的肺气肿的敏感性可能取决于弹性蛋白酶与α-巨球蛋白的优先结合,后者可以保护弹性蛋白酶的潜力,而不是与α-1蛋白酶抑制剂(其使弹性酶失活)优先结合。我们推测,即使在注入弹性蛋白酶后直到144 d在仓鼠肺中发现的残留放射性的一小部分也代表具有酶活性的α-巨球蛋白-胰弹性蛋白酶复合物,这可以作为持续的弹性蛋白酶活性的来源,这可能解释了肺部病变的进行性。

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