脱水视黄醇和5,6-环氧视黄基棕榈酸酯在小鼠淋巴瘤细胞中的光致突变性。
Photomutagenicity of anhydroretinol and 5,6-epoxyretinyl palmitate in mouse lymphoma cells.
作者信息
Mei Nan, Xia Qingsu, Chen Ling, Moore Martha M, Chen Tao, Fu Peter P
机构信息
Division of Genetic, National Center for Toxicological Research, U.S. Food and Drug Administration, Jefferson, Arkansas 72079, USA.
出版信息
Chem Res Toxicol. 2006 Nov;19(11):1435-40. doi: 10.1021/tx0600907.
Retinyl palmitate (RP) is frequently used as an ingredient in cosmetics and other retail products. We previously reported that, under UVA light irradiation, RP is facilely decomposed into multiple products, including anhydroretinol (AR) and 5,6-epoxyretinyl palmitate (5,6-epoxy-RP). We also determined that combined treatment of mouse lymphoma cells with RP and UVA irradiation produced a photomutagenic effect. In this study, we evaluated the photomutagenicity of AR and 5,6-epoxy-RP, in L5178Y/Tk+/- mouse lymphoma cells. Treatment of cells with AR or 5,6-epoxy-RP alone at 10 and 25 microg/mL for 4 h did not show a positive mutagenic response. However, because these doses did not induce the required amount of cytotoxicity for mouse lymphoma assay, we are unable to determine whether or not these two compounds are mutagenic. Treatment of cells with 1-25 microg/mL AR or 5,6-epoxy-RP under UVA light (315-400 nm) for 30 min (1.38 mW/cm2) produced a synergistic photomutagenic effect. At 10 microg/mL (37.3 microM) AR with UVA exposure, the mutant frequency (MF) was about 3-fold higher than that for UVA exposure alone, whereas the MF for 25microg/mL (46.3microM) of 5,6-epoxy-RP + UVA was approximately 2-fold higher than that for UVA exposure alone. Compared with previous results for RP + UVA treatment, the potency of the induced phototoxicity and photomutagenicity was AR > RP > 5,6-epoxy-RP. To elucidate the underlying photomutagenic mechanism, we examined the loss of heterozygosity (LOH) at four microsatellite loci spanning the entire chromosome 11 for mutants induced by AR or 5,6-epoxy-RP. Most mutants lost the Tk+ allele, and more than 70% of the chromosome damage extended to 38 cM in chromosome length. AR + UVA induced about twice as many mutants that lost all four microsatellite markers from the chromosome 11 carrying the Tk+ allele as RP + UVA or 5,6-epoxy-RP + UVA. These results suggest that two of RP's photodecomposition products are photomutagenic in mouse lymphoma cells, causing events that affect a large segment of the chromosome.
视黄醇棕榈酸酯(RP)常用于化妆品及其他零售产品中。我们之前报道过,在紫外线A(UVA)照射下,RP可轻易分解为多种产物,包括脱水视黄醇(AR)和5,6-环氧视黄醇棕榈酸酯(5,6-环氧-RP)。我们还确定,RP与UVA照射联合处理小鼠淋巴瘤细胞会产生光致突变效应。在本研究中,我们评估了AR和5,6-环氧-RP在L5178Y/Tk+/-小鼠淋巴瘤细胞中的光致突变性。单独用10和25μg/mL的AR或5,6-环氧-RP处理细胞4小时未显示出阳性诱变反应。然而,由于这些剂量未诱导出小鼠淋巴瘤检测所需的细胞毒性量,我们无法确定这两种化合物是否具有诱变性。在UVA光(315 - 400nm)下用1 - 25μg/mL的AR或5,6-环氧-RP处理细胞30分钟(1.38mW/cm²)产生了协同光致突变效应。在10μg/mL(37.3μM)AR与UVA照射下,突变频率(MF)比单独UVA照射时高约3倍,而25μg/mL(46.3μM)的5,6-环氧-RP + UVA的MF比单独UVA照射时高约2倍。与之前RP + UVA处理的结果相比,诱导的光毒性和光致突变性的强度为AR > RP > 5,6-环氧-RP。为阐明潜在的光致突变机制,我们检查了由AR或5,6-环氧-RP诱导的突变体在跨越整个11号染色体的四个微卫星位点处的杂合性缺失(LOH)。大多数突变体失去了Tk+等位基因,并且超过70%的染色体损伤在染色体长度上延伸至38cM。AR + UVA诱导的从携带Tk+等位基因的11号染色体上丢失所有四个微卫星标记的突变体数量约为RP + UVA或5,6-环氧-RP + UVA诱导数量的两倍。这些结果表明,RP的两种光分解产物在小鼠淋巴瘤细胞中具有光致突变性,并导致影响染色体大片段的事件发生。
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