ORGAN SPECIFIC CYTOKINE THERAPY - LOCAL ACTIVATION OF MONONUCLEAR PHAGOCYTES BY DELIVERY OF AN AEROSOL OF RECOMBINANT INTERFERON-GAMMA TO THE HUMAN LUNG

被引:126
作者
JAFFE, HA
BUHL, R
MASTRANGELI, A
HOLROYD, KJ
SALTINI, C
CZERSKI, D
JAFFE, HS
KRAMER, S
SHERWIN, S
CRYSTAL, RG
机构
[1] NHLBI,PULM BRANCH,BLDG 10,ROOM 6D03,BETHESDA,MD 20892
[2] GENENTECH INC,SAN FRANCISCO,CA 94080
关键词
BRONCHOALVEOLAR LAVAGE; MACROPHAGE; IMMUNE DEFENSE; IP-10; GENE;
D O I
10.1172/JCI115291
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
In the context of the central role of the alveolar macrophage in host defense of the respiratory epithelial surface, and the ability of IFN-gamma to activate mononuclear phagocytes, we have evaluated strategies to use rIFN-gamma to activate human alveolar macrophages in vivo. To accomplish this, rIFN-gamma was administered to nonsmoking normals, the amounts of IFN-gamma quantified in serum and respiratory epithelial lining fluid (ELF) and the status of IFN-gamma related activation of blood monocytes and alveolar macrophages was evaluated by quantifying the expression of mRNA transcripts of IP-10, a gene induced specifically by IFN-gamma. Systemic administration (subcutaneous) of maximally tolerated amounts of rIFN-gamma (250-mu-g) was followed by detectable levels of IFN-gamma in serum but not ELF, the expression of IP-10 transcripts in blood monocytes but not alveolar macrophages, and multiple systemic adverse effects. To circumvent the inability of systemic administration to reach respiratory ELF and activate alveolar macrophages, rIFN-gamma (250-1,000-mu-g) was inhaled as an aerosol once daily for 3 d. Strikingly, while IFN-gamma was not detected in serum it was detectable in respiratory ELF in a dose-dependent fashion. Further, alveolar macrophages, but not blood monocytes, expressed IP-10 mRNA transcripts and, importantly, inhalation of aerosolized rIFN-gamma was not associated with local or systemic adverse effects. Thus, it is feasible to use rIFN-gamma to activate alveolar macrophages by targeting the cytokine directly to the lung. These data suggest a potential strategy for targeted cytokine therapy, without systemic side effects, to augment respiratory tract defenses in individuals at risk for or with lung infection.
引用
收藏
页码:297 / 302
页数:6
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