Hawgood Samuel, Ochs Matthias, Jung Anja, Akiyama Jennifer, Allen Lennell, Brown Cindy, Edmondson Jess, Levitt Stacey, Carlson Elaine, Gillespie Anne Marie, Villar Angela, Epstein Charles J, Poulain Francis R
Cardiovascular Research Institute and Department of Pediatrics, University of California San Francisco, San Francisco, California 94118-1944, USA.
Am J Physiol Lung Cell Mol Physiol. 2002 Nov;283(5):L1002-10. doi: 10.1152/ajplung.00118.2002.
Surfactant proteins-A and -D (SP-A and SP-D) are members of the collectin protein family. Mice singly deficient in SP-A and SP-D have distinct phenotypes. Both have altered inflammatory responses to microbial challenges. To further investigate the functions of SP-A and SP-D in vivo, we developed mice deficient in both proteins by sequentially targeting the closely linked genes in embryonic stem cells using graded resistance to G-418. There is a progressive increase in bronchoalveolar lavage phospholipid, protein, and macrophage content through 24 wk of age. The macrophages from doubly deficient mice express high levels of the matrix metalloproteinase MMP-12 and develop intense but patchy lung inflammation. Stereological analysis demonstrates significant air space enlargement and reduction in alveolar septal tissue per unit volume, consistent with emphysema. These changes qualitatively resemble the lung pathology seen in SP-D-deficient mice. These doubly deficient mice will be useful in dissecting the potential overlap in function between SP-A and SP-D in host defense.
表面活性蛋白A和D(SP-A和SP-D)是凝集素蛋白家族的成员。单独缺乏SP-A和SP-D的小鼠具有不同的表型。两者对微生物攻击的炎症反应均发生改变。为了进一步研究SP-A和SP-D在体内的功能,我们通过利用对G-418的分级抗性依次靶向胚胎干细胞中紧密相连的基因,培育出了两种蛋白均缺乏的小鼠。到24周龄时,支气管肺泡灌洗中的磷脂、蛋白质和巨噬细胞含量逐渐增加。双缺陷小鼠的巨噬细胞表达高水平的基质金属蛋白酶MMP-12,并出现强烈但片状的肺部炎症。体视学分析显示气腔显著扩大,单位体积的肺泡间隔组织减少,与肺气肿一致。这些变化在性质上类似于SP-D缺陷小鼠的肺部病理。这些双缺陷小鼠将有助于剖析SP-A和SP-D在宿主防御中潜在的功能重叠。
