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达那唑可使这种抗蛋白酶严重缺乏的个体血清α1-抗胰蛋白酶水平升高。

Danazol-induced augmentation of serum alpha 1-antitrypsin levels in individuals with marked deficiency of this antiprotease.

作者信息

Gadek J E, Fulmer J D, Gelfand J A, Frank M M, Petty T L, Crystal R G

出版信息

J Clin Invest. 1980 Jul;66(1):82-87. doi: 10.1172/JCI109838.

Abstract

Individuals with serum alpha1-antitrypsin levels below 80 mg/dl are clearly at risk for the development of accelerated panacinar emphysema. One possible approach to the therapy of this disorder would be to raise serum levels of this major antiprotease to establish protease-antiprotease homeostasis within the lung parenchyma. Because danazol, an impeded androgen, elevates levels of C1 inhibitor in patients deficient of that serum antiprotease, we hypothesized that this agent might also increase alpha1-antitrypsin levels in patients with alpha1-antitrypsin deficiency. To evaluate this concept, seven patients with severe emphysema associated with alpha1-antitrypsin deficiency (six PiZ and 1 M(Duarte)Z) and one asymptomatic individual (PiSZ) received 600 mg of danazol daily for 30 d. Five of the six PiZ patients responded to danazol therapy with significant increases in serum alpha1-antitrypsin levels (mean increase of 37%; P < 0.03). The two individuals who were heterozygous for the Z protein increased their serum levels by 85% (PiM(Duarte)Z) and 87% (PiSZ), respectively. These increases in serum alpha1-antitrypsin antigen were accompanied by commensurate increases in serum trypsin inhibition. Crossed immunoelectrophoresis showed no alterations of the microheterogeneity of the alpha1-antitrypsin or the presence of protease-antiprotease complexes in serum during danazol therapy. These data demonstrate that serum alpha1-antitrypsin levels can be augmented by danazol therapy in PiZ individuals as well as those heterozygotes with severe deficiency of alpha1-antitrypsin. The clinical relevance of these increases in serum alpha1-antitrypsin remains speculative, but these findings suggest that danazol may provide a means of improving the protease-antiprotease balance in these individuals and thus impede the progression of their lung disease.

摘要

血清α1 -抗胰蛋白酶水平低于80mg/dl的个体显然有发生快速全腺泡型肺气肿的风险。治疗这种疾病的一种可能方法是提高这种主要抗蛋白酶的血清水平,以在肺实质内建立蛋白酶 -抗蛋白酶平衡。因为达那唑,一种甾体雄激素,能提高缺乏该血清抗蛋白酶患者的C1抑制剂水平,我们推测这种药物也可能增加α1 -抗胰蛋白酶缺乏患者的α1 -抗胰蛋白酶水平。为了评估这一概念,7例患有与α1 -抗胰蛋白酶缺乏相关的严重肺气肿患者(6例PiZ型和1例M(Duarte)Z型)以及1例无症状个体(PiSZ型)每天接受600mg达那唑治疗,持续30天。6例PiZ型患者中有5例对达那唑治疗有反应,血清α1 -抗胰蛋白酶水平显著升高(平均升高37%;P<0.03)。两名Z蛋白杂合个体的血清水平分别升高了85%(PiM(Duarte)Z型)和87%(PiSZ型)。血清α1 -抗胰蛋白酶抗原的这些升高伴随着血清胰蛋白酶抑制的相应增加。交叉免疫电泳显示,在达那唑治疗期间,血清中α1 -抗胰蛋白酶的微异质性没有改变,也没有蛋白酶 -抗蛋白酶复合物的存在。这些数据表明,达那唑治疗可使PiZ个体以及α1 -抗胰蛋白酶严重缺乏的杂合子的血清α1 -抗胰蛋白酶水平升高。血清α1 -抗胰蛋白酶升高的临床相关性仍属推测,但这些发现表明,达那唑可能提供一种改善这些个体蛋白酶 -抗蛋白酶平衡的方法,从而阻止其肺部疾病的进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f42/371508/fbb7ad0b2eb1/jcinvest00691-0094-a.jpg

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