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内源性产生的干扰素对集落刺激因子-1(CSF-1)作出反应,增强了子代巨噬细胞的功能分化。

Interferon produced endogenously in response to CSF-1 augments the functional differentiation of progeny macrophages.

作者信息

Moore R N, Pitruzzello F J, Robinson R M, Rouse B T

出版信息

J Leukoc Biol. 1985 May;37(5):659-64. doi: 10.1002/jlb.37.5.659.

Abstract

The role of endogenously produced interferon alpha/beta in the functional maturation of newly derived mononuclear phagocytes was investigated. Addition of highly specific anti-interferon alpha + beta antiserum to murine marrow cultures stimulated with colony-stimulating factor-1 (macrophage growth factor) markedly suppressed the capacity of resulting progeny mononuclear phagocytes to ingest opsonized sheep erythrocytes (EAIgG). This impairment was corrected either by direct addition of interferon alpha + beta at a concentration in excess of that neutralized by the antiserum or by the addition of lesser amounts of interferon (33 U/ml) following removal of the anti-interferon from the cultures. Conditioned media from control colony-stimulating factor-stimulated cultures similarly reversed the impairment of maturation resulting from 5 days of growth in the presence of anti-interferon. This enhancement of EAIgG ingestion reflected upon the interferon activity in the conditioned media and was neutralized by anti-interferon. Lastly, the endogenous interferon was found to enhance EAIgG ingestion by a majority of the mononuclear phagocyte progeny and not by a limited subpopulation.

摘要

研究了内源性产生的干扰素α/β在新衍生的单核吞噬细胞功能成熟中的作用。向用集落刺激因子-1(巨噬细胞生长因子)刺激的小鼠骨髓培养物中添加高度特异性的抗干扰素α + β抗血清,显著抑制了由此产生的子代单核吞噬细胞摄取调理化绵羊红细胞(EAIgG)的能力。通过直接添加浓度超过被抗血清中和浓度的干扰素α + β,或在从培养物中去除抗干扰素后添加较少量的干扰素(33 U/ml),可以纠正这种损伤。来自对照集落刺激因子刺激培养物的条件培养基同样逆转了在抗干扰素存在下生长5天导致的成熟损伤。EAIgG摄取的这种增强反映了条件培养基中的干扰素活性,并被抗干扰素中和。最后,发现内源性干扰素可增强大多数单核吞噬细胞子代的EAIgG摄取,而不是有限的亚群。

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