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一种三氮烯化合物与β-干扰素对针对淋巴母细胞的天然免疫的体外联合作用:效应细胞和靶细胞水平的研究

In vitro combined effects of a triazene compound and interferon-beta on natural immunity against lymphoblastoid cells: studies at effector and target cell level.

作者信息

Bonmassar L, D'Atri S, Turriziani M, Giuliani A

机构信息

Istituto Superiore di Sanità, Rome, Italy.

出版信息

Immunopharmacol Immunotoxicol. 1994 Nov;16(4):695-715. doi: 10.3109/08923979409019746.

Abstract

It was shown that Dacarbazine and other triazene compounds render murine leukemias highly immunogenic and susceptible to natural immunity (NI). In addition a pilot clinical study revealed that Dacarbazine can be cytotoxic for bone marrow blasts in patients with acute non-lymphoblastic leukemias through a mechanism that could be, at least in part, of immunological origin. However triazenes depress antigen-dependent responses and NI, whereas interferons, including interferon-beta (IFN), antagonize drug-induced impairment of NI. Therefore the complex interaction between triazenes and IFN on NI effector (i.e. NK) lymphocytes and human target lymphoblastoid cells has been investigated. The results show that: (a) IFN increases NK activity and antagonizes the depressive effects of methyl-triazene-benzoic acid (MTBA, an in vitro active triazene compound) on the NK function; (b) a lymphoblastoid cell line exposed to multiple in vitro treatments with MTBA, shows increased growth rate, augmented chemoresistance to MTBA, and higher susceptibility to NI than parental cells; (c) as expected IFN pretreatment down-regulates the susceptibility of lymphoblastoid cells to NK effectors; (d) however a net "therapeutic gain" was found if the overall influence of MTBA+IFN on target and effector cells is considered.

摘要

已表明达卡巴嗪和其他三氮烯化合物可使鼠白血病具有高度免疫原性,并易受天然免疫(NI)作用。此外,一项初步临床研究显示,达卡巴嗪可通过一种至少部分源于免疫的机制,对急性非淋巴细胞白血病患者的骨髓母细胞产生细胞毒性。然而,三氮烯会抑制抗原依赖性反应和天然免疫,而包括β干扰素(IFN)在内的干扰素则可拮抗药物诱导的天然免疫损伤。因此,对三氮烯与IFN在天然免疫效应细胞(即自然杀伤细胞)和人靶淋巴母细胞上的复杂相互作用进行了研究。结果表明:(a)IFN可增强自然杀伤细胞活性,并拮抗甲基三氮烯苯甲酸(MTBA,一种体外活性三氮烯化合物)对自然杀伤细胞功能的抑制作用;(b)经MTBA多次体外处理的淋巴母细胞系,其生长速率增加,对MTBA的化学抗性增强,且比亲代细胞对天然免疫更敏感;(c)正如预期的那样,IFN预处理可下调淋巴母细胞对自然杀伤细胞效应的敏感性;(d)然而,如果考虑MTBA + IFN对靶细胞和效应细胞的总体影响,则会发现净“治疗增益”。

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