苔藓抑素1和星孢素对T细胞HIV受体蛋白(CD4)的生物合成和表达的不同调节作用

Cell regulation Pub Date : 1991-02-01 DOI:10.1091/mbc.2.2.95
W M Boto, L Brown, J Chrest, W H Adler
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引用次数: 16

摘要

一个结构相关的大环内酯家族,苔藓抑素,最近显示出几个有趣的药理学特性。苔藓虫素是海洋动物叶氏苔藓虫的生物合成产物。为了进一步分析这些极不寻常的生物合成动物产品的生物活性,我们研究了苔藓抑素1 (bryo-1)对正常外周血T淋巴细胞人类免疫缺陷病毒受体CD4稳态表达的影响。用抗CD4单克隆抗体流式细胞术分析,用5 nM的bryo-1孵育细胞导致细胞表面CD4大量丢失。通过northern blot杂交表明,bryo-1对CD4表达的调节不是由于细胞毒性作用:在其调节CD4的培养条件下,bryo-1也刺激了白细胞介素2基因的表达。此外,用纳摩尔量的蛋白激酶C拮抗剂staurosporine孵育淋巴细胞,可抑制bryo-1诱导的CD4表达调节。对[35S]蛋氨酸标记淋巴细胞洗涤剂裂解物的放射免疫沉淀分析结果强烈表明,bryo-1抑制糖基化和CD4表达的方式与tunicamycin相似。
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Distinct modulatory effects of bryostatin 1 and staurosporine on the biosynthesis and expression of the HIV receptor protein (CD4) by T cells.

A family of structurally related macrocyclic lactones, bryostatins, have recently been shown to display several intriguing pharmacologic properties. Bryostatins are biosynthetic products of bryozoa phyllum of marine animals. To extend the analyses of the biological activities of these highly unusual biosynthetic animal products, we have examined the effect of bryostatin 1 (bryo-1) on the steady-state expression of the human immunodeficiency virus receptor, CD4, by normal peripheral blood T lymphocytes. Incubation of the cells with 5 nM bryo-1 caused a substantial loss of CD4 from the cell surface, as analyzed by flow cytometry using anti-CD4 monoclonal antibody. The modulation of CD4 expression by bryo-1 was not due to a cytotoxicity effect: in the culture conditions where it modulated CD4, bryo-1 also stimulated the expression of the interleukin 2 gene, as indicated by northern blot hybridization. In addition, incubation of the lymphocytes with nanomolar amounts of protein kinase C antagonist, staurosporine, resulted in the inhibition of the bryo-1-induced modulation of CD4 expression. The results of radioimmunoprecipitation analysis of detergent lysates of [35S] methionine-labeled lymphocytes strongly suggest that bryo-1 inhibits the glycosylation and expression of CD4 in a manner similar to that of tunicamycin.

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