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吞噬缺陷——单核细胞/巨噬细胞。

Phagocytic defects--monocytes/macrophages.

作者信息

Douglas S D, Musson R A

出版信息

Clin Immunol Immunopathol. 1986 Jul;40(1):62-8. doi: 10.1016/0090-1229(86)90069-3.

DOI:10.1016/0090-1229(86)90069-3
PMID:3521970
Abstract

Mononuclear phagocytes originate from stem cells in the bone marrow which differentiate from monoblasts into promonocytes, then into circulating blood monocytes. Subsequently the monocytes can develop into macrophages and reside in a variety of tissues. Mononuclear phagocytes have cell surface receptors for a variety of substances (e.g., IgG, complement components, fibronectin, and sugars) and are capable of secreting a number of mediators (enzymes, complement components, coagulation components, and monokines). The tissue macrophages adapt to their environment and express unique differentiated functions that are related to various anatomic sites and organs (e.g., Kupffer cells, pulmonary alveolar macrophages, osteoclasts, microglia). Macrophages have the capacity to become "activated" by both specific and nonspecific immunologic stimuli and the "activated" macrophage has enhanced functional capabilities (e.g., tumoricidal, microbicidal, phagocytosis, secretion of mediators). Abnormal monocyte/macrophage function may be acquired or may be due to genetic or developmental disorders. Because of their central role in host defense (in inflammatory responses, in antigen presentation, and in immunoregulatory networks), monocyte/macrophage dysfunction may result in one or more pathophysiologic consequences: defects in monocyte maturation, deficiencies in the clearance of physiologic substrates in lysosomal diseases (e.g., Gaucher's disease, mucopolysaccharidoses, osteopetrosis, metachromatic leukodystrophy), decreased synthesis and secretion of mediators (complement component deficiencies), defects in microbicidal activity (chronic granulomatous disease) and defects which are acquired following infection and during chemotherapy (e.g., acquired immune deficiency syndrome).

摘要

单核吞噬细胞起源于骨髓中的干细胞,这些干细胞从单核母细胞分化为前单核细胞,然后再分化为循环血液中的单核细胞。随后,单核细胞可发育为巨噬细胞并存在于多种组织中。单核吞噬细胞具有针对多种物质(如免疫球蛋白G、补体成分、纤连蛋白和糖类)的细胞表面受体,并且能够分泌多种介质(酶、补体成分、凝血成分和单核因子)。组织巨噬细胞适应其所处环境,并表达与各种解剖部位和器官相关的独特分化功能(如枯否细胞、肺泡巨噬细胞、破骨细胞、小胶质细胞)。巨噬细胞能够被特异性和非特异性免疫刺激激活,“激活的”巨噬细胞具有增强的功能能力(如杀肿瘤、杀微生物、吞噬作用、介质分泌)。单核细胞/巨噬细胞功能异常可能是后天获得的,也可能是由于遗传或发育障碍所致。由于它们在宿主防御(炎症反应、抗原呈递和免疫调节网络)中起核心作用,单核细胞/巨噬细胞功能障碍可能导致一种或多种病理生理后果:单核细胞成熟缺陷、溶酶体疾病(如戈谢病、黏多糖贮积症、石骨症、异染性脑白质营养不良)中生理底物清除缺陷、介质合成和分泌减少(补体成分缺陷)、杀微生物活性缺陷(慢性肉芽肿病)以及感染后和化疗期间获得的缺陷(如获得性免疫缺陷综合征)。

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Clin Immunol Immunopathol. 1986 Jul;40(1):62-8. doi: 10.1016/0090-1229(86)90069-3.
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Evaluation of Fc-dependent monocyte-macrophage function in bone marrow transplant recipients.骨髓移植受者中Fc依赖性单核细胞-巨噬细胞功能的评估。
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