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The novel BLM3 gene encodes a protein that protects against lethal effects of oxidative damage.

机译:新的BLM3基因编码一种蛋白质,可防止氧化损伤的致命影响。

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Mutational alteration of the BLM3 gene in Saccharomyces cerevisiae confers hypersensitivities to lethal effects of ionizing radiation, anticancer bleomycins and structurally-related phleomycins. Bleomycin is used clinically in the treatment of many types of cancers, including Kaposi's sarcoma. The BLM3 gene was cloned from a genomic library by complementing the drug hypersensitivities conferred by the codominant blm3-1 mutation. The nucleotide sequence of BLM3 encodes a predicted integral protein of 1804 amino acids with seven to ten potential transmembrane domains and additional motifs. The blm3 null mutation was created by gene replacement, and found not to be essential for growth in the absence of the bleomycin-phleomycin antibiotics. Sequence analyses suggest the Blm3p could be a potential member of the major facilitator superfamily (MFS) of permeases. Northern dot blot analyses using a human RNA master tissue blot containing RNA from fifty different fetal and adult tissues revealed sequence homology in adult tissues to BLM3, but no sequence homology in fetal tissues. The function of the Blm3p is presently unknown. We propose several functions for the Blm3p in protecting cells against oxidative agents, including roles in detoxification, transport and defending against DNA damage.
机译:酿酒酵母中BLM3基因的突变使超敏性对电离辐射,抗癌博来霉素和与结构相关的博来霉素具有致命作用。博来霉素在临床上用于治疗多种类型的癌症,包括卡波西氏肉瘤。通过补充由显性blm3-1突变引起的药物超敏性,从基因组文库中克隆了BLM3基因。 BLM3的核苷酸序列编码1804个氨基酸的预测整合蛋白,具有7至10个潜在的跨膜结构域和其他基序。 blm3无效突变是通过基因置换产生的,并且发现在缺少博来霉素-博来霉素抗生素的情况下,blm3突变对于生长不是必需的。序列分析表明,Blm3p可能是通透酶的主要促进子超家族(MFS)的潜在成员。使用包含来自五十种不同胎儿和成年组织的RNA的人RNA主组织印迹进行的Northern dot印迹分析显示,成年组织中的序列与BLM3具有同源性,而胎儿组织中无序列同源性。 Blm3p的功能目前未知。我们提出Blm3p在保护细胞免受氧化剂侵害方面的几种功能,包括在排毒,运输和防御DNA损伤中的作用。

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