肿瘤诱导的巨噬细胞II类主要组织相容性复合体分子mRNA表达的调节。
Tumor-induced modulation of macrophage class II MHC molecule mRNA expression.
作者信息
Askew D, Burger C J, Elgert K D
机构信息
Department of Biology, Virginia Polytechnic Institute and State University, Blacksburg 24061-0406.
出版信息
Mol Immunol. 1993 Jul;30(10):911-20. doi: 10.1016/0161-5890(93)90015-4.
Class II MHC protein expression in macrophages (M phi) is reduced during tumor growth. Because regulation of class II MHC proteins occurs during transcription, tumor growth may suppress class II MHC protein expression by suppressing mRNA. The decrease in class II mRNA may result from (i) a decrease in M phi responsiveness to an inducing agent, such as interferon-gamma (IFN-gamma), or (ii) an increase in M phi sensitivity to suppressing agents, such as prostaglandin E2 (PGE2). To determine how tumors induce suppression of class II mRNA, M phi were cultured in the presence of IFN-gamma with or without other factors, and Northern blot analyses were performed. Unstimulated normal host (NH) or tumor-bearing host (TBH) M phi do not express detectable class II mRNA. The addition of IFN-gamma induces class II mRNA expression in NH and TBH M phi, but class II mRNA expression is significantly lower in TBH M phi. Kinetic studies suggested that NH M phi class II mRNA is induced faster and in greater amounts than TBH M phi class II mRNA. There is a decrease in M phi class II mRNA stability during tumor growth that may account for the decreased induction by IFN-gamma. Lipopolysaccharide (LPS) suppresses class II mRNA induction in both NH and TBH IFN-gamma-treated M phi, but TBH M phi are more sensitive to its suppression. PGE2 and tumor-necrosis factor-alpha (TNF-alpha), two factors produced by LPS-stimulated M phi, were tested for their ability to modulate class II mRNA expression in NH and TBH IFN-gamma-treated M phi. PGE2 suppressed class II mRNA expression in both NH and TBH M phi. The addition of TNF-alpha to IFN-gamma-treated M phi suppressed class II mRNA in NH M phi but, surprisingly, had an additive effect on IFN-gamma-induced class II mRNA expression. TNF-alpha did not induce class II mRNA expression in TBH M phi in the absence of IFN-gamma. The cause of the reduced class II mRNA expression during tumor growth is a decreased response to IFN-gamma and an increased sensitivity to PGE2. This change may cause the observed suppression mediated by TBH M phi.
在肿瘤生长过程中,巨噬细胞(M phi)中II类主要组织相容性复合体(MHC)蛋白的表达会降低。由于II类MHC蛋白的调节发生在转录过程中,肿瘤生长可能通过抑制mRNA来抑制II类MHC蛋白的表达。II类mRNA的减少可能是由于:(i)M phi对诱导剂(如γ干扰素(IFN-γ))的反应性降低,或(ii)M phi对抑制因子(如前列腺素E2(PGE2))的敏感性增加。为了确定肿瘤如何诱导II类mRNA的抑制,将M phi在有或没有其他因子存在的情况下与IFN-γ一起培养,并进行Northern印迹分析。未受刺激的正常宿主(NH)或荷瘤宿主(TBH)的M phi不表达可检测到的II类mRNA。添加IFN-γ可诱导NH和TBH的M phi表达II类mRNA,但TBH的M phi中II类mRNA的表达明显较低。动力学研究表明,NH的M phi中II类mRNA的诱导速度更快,量也更多。肿瘤生长过程中M phi II类mRNA稳定性的降低可能是IFN-γ诱导减少的原因。脂多糖(LPS)抑制NH和TBH经IFN-γ处理的M phi中II类mRNA的诱导,但TBH的M phi对其抑制更敏感。检测了LPS刺激的M phi产生的两种因子前列腺素E2(PGE2)和肿瘤坏死因子-α(TNF-α)调节NH和TBH经IFN-γ处理的M phi中II类mRNA表达的能力。PGE2抑制NH和TBH的M phi中II类mRNA的表达。向经IFN-γ处理的M phi中添加TNF-α可抑制NH的M phi中II类mRNA,但令人惊讶的是,对IFN-γ诱导的II类mRNA表达有相加作用。在没有IFN-γ的情况下,TNF-α不会诱导TBH的M phi表达II类mRNA。肿瘤生长过程中II类mRNA表达降低的原因是对IFN-γ的反应性降低和对PGE2的敏感性增加。这种变化可能导致观察到的由TBH的M phi介导的抑制作用。
Zotero 插件