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沙利度胺:跨门和遗传终点缺乏致突变活性。

Thalidomide: lack of mutagenic activity across phyla and genetic endpoints.

作者信息

Ashby J, Tinwell H, Callander R D, Kimber I, Clay P, Galloway S M, Hill R B, Greenwood S K, Gaulden M E, Ferguson M J, Vogel E, Nivard M, Parry J M, Williamson J

机构信息

Zeneca CTL, Macclesfield, Cheshire, UK.

出版信息

Mutat Res. 1997 Dec 12;396(1-2):45-64. doi: 10.1016/s0027-5107(97)00174-7.

Abstract

The human and rabbit teratogen thalidomide has been tested for mutagenicity in a wide range of assays, ranging from bacterial gene mutation assays conducted in vitro to in vivo cytogenetic assays conducted using rabbits, and including a variety of human-derived tissues. Thalidomide was not mutagenic to 6 strains of Salmonella when tested both in the presence and absence of Aroclor-induced rat liver S9 mix. This inactivity was confirmed in strains TA98 and TA100 using a 1-h pre-incubation assay protocol with the same S9 mix (10% S9), and additionally, in strain TA98 using 3 concentrations of S9 (4%, 10% and 30% S9 in S9 mix). Thalidomide was not clastogenic either to cultured human lymphocytes (whole blood cultures, minus S9 mix) or to Chinese hamster ovary (CHO) cells treated in vitro. Further, no cytotoxicity was observed in purified human lymphocytes when exposed to thalidomide up to the limit of its solubility in the medium in the presence and absence of liver S9 from Aroclor-induced pregnant rabbit. The CHO assays were conducted without metabolic activation and in the presence of a variety of sources of auxiliary metabolic activation (PB/beta NP-induced rat liver S9 mix, pooled male and female human liver S9 mix, uninduced and Aroclor-induced pregnant rabbit liver S9 mix and foetal rabbit S9 mix). Thalidomide did not induce micronuclei in isolated human lymphocytes (minus S9 mix) and it was non-mutagenic to mouse lymphoma L5178Y TK+/- cells when tested to the limits of its solubility in the culture medium (+/- S9 mix). No indication of recombinogenic or clastogenic activity was observed for thalidomide when tested in Drosophila. In addition, it failed to induce chromosome aberrations in grasshopper neuroblasts when tested in the presence and absence of Aroclor-induced rat liver S9 mix. Some unusual chromosome morphologies were observed in the grasshopper cytogenetic preparations indicating a potential of thalidomide to interact with chromosomal proteins. However, this potential was not evident in the human lymphocyte micronucleus assay, and thalidomide was apparently not reactive to the proteins of the mouse skin, as it gave negative results in a mouse local lymph node assay for skin sensitizing agents. Thalidomide was inactive in bone marrow micronucleus assays conducted using males and females from two strains of mice, and female New Zealand white rabbits. It is concluded that thalidomide is neither a mutagen nor an aneugen. This conclusion is discussed within the context of the results of earlier mutagenicity studies, the recent claim that thalidomide may be a heritable germ cell mutagen to humans, and the current interest in thalidomide for the treatment of immune system-related diseases.

摘要

已在广泛的检测中对人类和兔致畸剂沙利度胺的致突变性进行了测试,这些检测范围从体外进行的细菌基因突变检测到使用兔子进行的体内细胞遗传学检测,还包括各种人类来源的组织。在有和没有多氯联苯诱导的大鼠肝S9混合物存在的情况下进行测试时,沙利度胺对6株沙门氏菌没有致突变性。使用相同的S9混合物(10% S9)通过1小时预孵育检测方案在TA98和TA100菌株中证实了这种无活性,此外,在TA98菌株中使用3种浓度的S9(S9混合物中分别为4%、10%和30% S9)进行了测试。沙利度胺对培养的人类淋巴细胞(全血培养物,不含S9混合物)或体外处理的中国仓鼠卵巢(CHO)细胞没有致断裂作用。此外,当在有和没有多氯联苯诱导的怀孕兔肝脏S9存在的情况下,将纯化的人类淋巴细胞暴露于沙利度胺直至其在培养基中的溶解度极限时,未观察到细胞毒性。CHO检测在没有代谢激活的情况下以及在存在多种辅助代谢激活来源(多溴联苯/β-萘酚诱导的大鼠肝S9混合物、混合的男性和女性人类肝S9混合物、未诱导和多氯联苯诱导的怀孕兔肝S9混合物以及胎儿兔S9混合物)的情况下进行。沙利度胺在分离的人类淋巴细胞(不含S9混合物)中未诱导微核,并且在测试至其在培养基中的溶解度极限(±S9混合物)时对小鼠淋巴瘤L5178Y TK+/-细胞无致突变性。在果蝇中测试时,未观察到沙利度胺有重组或致断裂活性的迹象。此外,在有和没有多氯联苯诱导的大鼠肝S9混合物存在的情况下进行测试时,它未能在蝗虫神经母细胞中诱导染色体畸变。在蝗虫细胞遗传学制备物中观察到一些异常染色体形态,表明沙利度胺有与染色体蛋白相互作用的潜力。然而,这种潜力在人类淋巴细胞微核检测中并不明显,并且沙利度胺显然对小鼠皮肤蛋白无反应,因为它在小鼠皮肤致敏剂局部淋巴结检测中给出了阴性结果。在使用两种小鼠品系的雄性和雌性以及雌性新西兰白兔进行的骨髓微核检测中,沙利度胺无活性。结论是沙利度胺既不是诱变剂也不是非整倍体诱变剂。在早期致突变性研究结果、最近声称沙利度胺可能是人类可遗传的生殖细胞诱变剂以及目前对沙利度胺治疗免疫系统相关疾病的兴趣的背景下讨论了这一结论。

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