Stanley E, Lieschke G J, Grail D, Metcalf D, Hodgson G, Gall J A, Maher D W, Cebon J, Sinickas V, Dunn A R
Ludwig Institute for Cancer Research, Melbourne Tumour Biology Branch, Victoria, Australia.
Proc Natl Acad Sci U S A. 1994 Jun 7;91(12):5592-6. doi: 10.1073/pnas.91.12.5592.
Mice homozygous for a disrupted granulocyte/macrophage colony-stimulating factor (GM-CSF) gene develop normally and show no major perturbation of hematopoiesis up to 12 weeks of age. While most GM-CSF-deficient mice are superficially healthy and fertile, all develop abnormal lungs. There is extensive peribronchovascular infiltration with lymphocytes, predominantly B cells. Alveoli contain granular eosinophilic material and lamellar bodies, indicative of surfactant accumulation. There are numerous large intraalveolar phagocytic macrophages. Some mice have subclinical lung infections involving bacterial or fungal organisms, occasionally with focal areas of acute purulent inflammation or lobar pneumonia. Some features of this pathology resemble the human disorder alveolar proteinosis. These observations indicate that GM-CSF is not essential for the maintenance of normal levels of the major types of mature hematopoietic cells and their precursors in blood, marrow, and spleen. However, they implicate GM-CSF as essential for normal pulmonary physiology and resistance to local infection.
粒细胞/巨噬细胞集落刺激因子(GM-CSF)基因缺失的纯合子小鼠发育正常,在12周龄前造血功能未出现重大紊乱。虽然大多数GM-CSF缺陷小鼠表面上健康且可育,但它们的肺部均出现异常。支气管血管周围有大量淋巴细胞浸润,主要是B细胞。肺泡内含有颗粒状嗜酸性物质和板层小体,提示表面活性剂积聚。有大量大的肺泡内吞噬性巨噬细胞。一些小鼠有涉及细菌或真菌的亚临床肺部感染,偶尔伴有局灶性急性化脓性炎症或大叶性肺炎。这种病理学的一些特征类似于人类疾病肺泡蛋白沉积症。这些观察结果表明,GM-CSF对于维持血液、骨髓和脾脏中主要类型成熟造血细胞及其前体的正常水平并非必不可少。然而,这些结果表明GM-CSF对于正常的肺部生理功能和抵抗局部感染至关重要。
