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[双链多聚核糖核苷酸的生物学作用及治疗前景:重新评估]

[Biological actions and therapeutic perspectives of double stranded polyribonucleotides: a reappraisal].

作者信息

Thang M N, Guschlbauer W

机构信息

U 245 INSERM, Hôpital Saint-Antoine, Paris, France.

出版信息

Pathol Biol (Paris). 1992 Dec;40(10):1006-14.

PMID:1284399
Abstract

Double-stranded polynucleotides, which are composed of two complementary homopolyribonucleotides containing no genetic information, are synthetic molecules capable of mimicking the action of natural double-stranded RNA or viral RNA on cells. Double-stranded polyribonucleotides act as an alarm system alerting the cell to the presence of an external aggression, e.g. a viral attack. In addition, polyribonucleotides have a more active function in that they trigger cell defense processes through activation of a family of genes, of which some encode cytokines, activation of cytoplasmic enzymes involved in antiviral mechanisms or signal transduction, and activation of nonspecific immune responses. Double-stranded polyribonucleotides containing one mismatched base pair per helix have been found to be especially interesting. The best known example is poly(I).poly(C12U), also called ampligen. Poly(I).poly(C12U) is capable, in experimental models, of limiting the development of viruses (including HIV), reducing tumor growth, eliminating metastases, and, according to one report, preventing steady declines in T-cell counts in HIV-positive patients. Therapeutic doses used in the USA as an experimental drug induced little toxicity. In vitro, poly(I).poly(C12U) acts synergistically with interferon, interleukin 2 or AZT, suggesting that these latter drugs may be effective in lower, less toxic doses when used in combination with poly(I).poly(C12U). The therapeutic activity of poly(I).poly(C12U) holds promise. More extensive prospective studies of this agent are warranted.

摘要

双链多核苷酸由两个不含遗传信息的互补同聚核糖核苷酸组成,是能够模拟天然双链RNA或病毒RNA对细胞作用的合成分子。双链聚核糖核苷酸充当警报系统,提醒细胞存在外部侵袭,例如病毒攻击。此外,聚核糖核苷酸具有更积极的功能,因为它们通过激活一组基因来触发细胞防御过程,其中一些基因编码细胞因子、激活参与抗病毒机制或信号转导的细胞质酶以及激活非特异性免疫反应。已发现每条螺旋含有一个错配碱基对的双链聚核糖核苷酸特别有趣。最著名的例子是聚肌苷酸-聚胞苷酸(12U)[poly(I).poly(C12U)],也称为安普利近。在实验模型中,聚肌苷酸-聚胞苷酸(12U)能够限制病毒(包括HIV)的发展、减少肿瘤生长、消除转移,并且根据一份报告,可防止HIV阳性患者的T细胞计数持续下降。在美国作为实验药物使用的治疗剂量几乎没有毒性。在体外,聚肌苷酸-聚胞苷酸(12U)与干扰素、白细胞介素2或齐多夫定协同作用,这表明当与聚肌苷酸-聚胞苷酸(12U)联合使用时,后几种药物可能以更低、毒性更小的剂量有效。聚肌苷酸-聚胞苷酸(12U)的治疗活性前景广阔。有必要对该药物进行更广泛的前瞻性研究。

相似文献

1
[Biological actions and therapeutic perspectives of double stranded polyribonucleotides: a reappraisal].[双链多聚核糖核苷酸的生物学作用及治疗前景:重新评估]
Pathol Biol (Paris). 1992 Dec;40(10):1006-14.
2
Synergistic inhibition of AZT-resistant HIV by AZT combined with poly(I):poly(C12U), without synergistic toxicity to bone marrow progenitor cell elements.齐多夫定(AZT)与聚肌苷酸:聚胞苷酸(聚(I):聚(C12U))联合使用对AZT耐药的HIV具有协同抑制作用,且对骨髓祖细胞成分无协同毒性。
In Vivo. 1994 May-Jun;8(3):375-81.
3
Clinical studies with ampligen (mismatched double-stranded RNA).使用氨普立明(错配双链RNA)的临床研究。
J Biol Response Mod. 1985 Dec;4(6):669-75.
4
Preclinical studies with Ampligen (mismatched double-stranded RNA).使用Ampligen(错配双链RNA)的临床前研究。
J Biol Response Mod. 1985 Oct;4(5):495-502.
5
Mismatched double-stranded RNA, Ampligen (poly(I): poly(C12U), demonstrates antiviral and immunostimulatory activities in HIV disease.错配双链RNA,氨基比林(聚肌苷酸:聚胞苷酸12尿苷酸),在HIV疾病中显示出抗病毒和免疫刺激活性。
Int J Immunopharmacol. 1991;13 Suppl 1:69-76. doi: 10.1016/0192-0561(91)90127-s.
6
Comparative studies of ampligen (mismatched double-stranded RNA) and interferons.氨力根(错配双链RNA)与干扰素的对比研究。
J Biol Response Mod. 1985 Dec;4(6):613-20.
7
Therapeutic potential of Ampligen.安普利近的治疗潜力。
Am Fam Physician. 1987 Oct;36(4):253-6.
8
Spectroscopic and calorimetric studies on the binding of alkaloids berberine, palmatine and coralyne to double stranded RNA polynucleotides.生物碱小檗碱、巴马汀和珊瑚碱与双链RNA多核苷酸结合的光谱和量热研究。
J Phys Chem B. 2009 Jan 29;113(4):1210-24. doi: 10.1021/jp806597w.
9
[Protective action of double-stranded complexes--interferon inducers in encephalomyocarditis in mice].[双链复合物——小鼠脑心肌炎干扰素诱导剂的保护作用]
Biull Eksp Biol Med. 1984 Apr;97(4):446-8.
10
Ampligen inhibits human herpesvirus-6 in vitro.安普利近在体外可抑制人疱疹病毒6型。
In Vivo. 1994 Jul-Aug;8(4):587-91.

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