Bioavailability and metabolism of hexavalent chromium compounds †

Intratracheal instillation of ⁵¹CrCl₃ in anaesthetized rabbits resulted in partial absorption. In blood, the absorbed material was entirely confined to the plasma compartment. Only trace amounts were deposited in liver and kidney. By contrast, after similar application of Na, ⁵¹CrO₄ the bulk of blood radioactivity was present in red blood cells (RBC). Substantial deposition occurred in liver and kidneys. It is concluded that Cr(VI) may enter the body unreduced via the lung and is partially deposited in cells over a prolonged period of time.

Since chromium was accumulated in liver after administration of Cr(VI) we investigated the intracellular disposition of Cr(VI) in the isolated perfused liver. No significant sex differences in chromium distribution were observed. At the end of the experiments (1 h), 60% of the applied dose (312μg Cr/liver) was located in the cytosol, whilst 14% was in the mitochondria, 9% in the microsomal pellet and 2% was associated with the nuclei. Gel chromatography of the cytosolic compartment showed that the overwhelming part of chromium was eluted in fractions with an apparent molecular weight of 6,000 dalton. These fractions exhibited absorption maxima at 410nm and 548nm. It is concluded, that cytosolic reduction might be the main intracellular redox pathway for chromates. This view was confirmed by monitoring the reaction of Cr(VI) with GSH in vitro. GSH reduced Cr(VI) without further cofactors under formation of GSH‐chromium complexes, which possibly represent major intermediates in the metabolism of Cr(VI).     

还原型谷胱甘肽调控shewanella oneidensis MR-1降解亚碲酸盐

探讨了生物活性小分子还原型谷胱甘肽（GSH）调控奥奈达湖希瓦氏菌（shewanella oneidensis）MR-1还原亚碲酸盐的特性及机理.结果表明,生物体系中加入0.1,0.4,1.0mmol/L GSH,与空白对照相比,亚碲酸盐的生物还原效率可分别提高55%、71%和78%,且GSH浓度在0.1~1.0mmol/L范围内与亚碲酸盐的生物还原效率呈正相关.采用单因素实验优化了培养条件,在温度35℃,pH 8.0,GSH浓度为0.4mmol/L的条件下,亚碲酸盐生物还原效率在24h内即可达到97%.采用6种不同呼吸抑制剂实验探讨亚碲酸盐生物还原的电子传递路径,确定GSH在亚碲酸盐生物还原电子传递链上的加速位点为NADH还原酶、甲萘醌和FAD脱氢酶.     

氯代硝基苯胺对鲫鱼(Carassius auratus)血清抗氧化酶的影响

研究了2-氯-4-硝基苯胺、4-氯-3-硝基苯胺，2-氯-5-硝基苯胺对斑马鱼的急性毒性，96hLC50分别为6.99,2.58,8.63mg/L，为阐明氯化硝基苯胺类化合物对水生生物抗氧化酶的早期影响，将鲫鱼暴露于梯度浓度的2-氯-4-硝基苯胺，4-氯-3-硝基苯胺，2-氯-5-硝基苯胺中，研究鲫鱼血清SOD和GSH-PX活性短期（48h)内的变化，研究结果表明，在实验设置浓度下，随着暴露浓度升高，与空白对照组相比，3种化合物对SOD活性表现为先轻微激活后抑制，对GSH-PX活性先激活再抑制后有所回升，表明3种化合物对鲫鱼血清SOD和GSH-PX活性有显著影响，与3种化合物96hLC50相比，引起生化效应的暴露浓度明显降低，且反应快速，可考虑SOD和GSH-PX酶活性相结合作为该类化合物对水环境污染胁迫的敏感生物指示物。     

SO2吸入对小鼠组织谷胱甘肽氧化还原系统的影响

从SO2吸入对雄性小鼠组织谷胱甘肽氧化还原系统中的抗氧化酶谷胱甘肽硫转移酶(GST)和葡萄糖6-磷酸脱氢酶(G6PD)以及还原型谷胱甘肽(GSH)和脂质过氧化物(TBARS)的影响探讨SO2的毒性作用机理.将昆明种纯系雄性小鼠60只随机分成3大组,每组20只,每一大组再随机分成SO2吸入组和对照组(SO2吸入组10只,对照组10只).吸入组吸入SO2浓度分别为(22±2)mg/m3,(64±3)mg/m3和(148±23)mg/m3.分别检测其脑、肺、心、肝、肾组织中GST、G6PD的活性以及GSH、TBARS的含量变化.当SO2浓度为(148±23)mg/m3时,脑、肺、心、肝、肾组织中GST和G6PD活性以及GSH含量均比对照组达到极显著(P<0.01)或显著降低(P<0.05),而脑和肺、心、肝、肾组织中TBARS水平则是显著(P<0.05)或极显著升高(P<0.01),且各指标与SO2浓度间有显著的剂量依赖关系.SO2吸入可使谷胱甘肽氧化还原系统中的关键性酶GST和G6PD活性发生显著降低,可使抗氧化物质GSH含量显著下降,而脂质过氧化物TBARS则显著升高,最终使谷胱甘肽氧化还原系统发生大的变化,导致氧化损伤.图2表2参16     

Investigation of metallothionein level,reduced GSH level,MDA level,and metal content in two different tissues of freshwater mussels from Atatürk Dam Lake coast,Turkey

Atatürk Dam Lake is one of the important freshwater ecosystems in the world in terms of the size of the surface area and the biodiversity. The objective of this study was to determine the effects of metal pollution in the Atatürk Dam Lake on some biochemical markers in the gills and digestive glands of mussels (Unio mancus). Mussel samples were collected in July-2018 from four stations. The metal residues (Cd, Cu, Pb, Zn, and Ni) in the tissues were determined by ICP-MS. The MT, reduced GSH, and MDA levels were analysed using the proposed spectrophotometric methods. According to the results, toxic metals such as Cd and Pb in both tissues were determined mostly in mussels collected from St1. The highest MT and MDA levels in the gills were determined in St3 and St2 respectively, while the highest MT and MDA levels in the digestive glands were determined in St1. Although there was no significant difference in the reduced GSH level in the gills among the stations, the highest reduced GSH level in the digestive glands was determined in St4. These results indicated that mussels are appropriate sentinel organisms for metal contamination with effects on oxidative stress and metal exposure biomarkers.     

Mercuric chloride induced proteotoxicity and structural destabilization in marine fish (Therapon jarbua)

The reaction byproducts derived from lipid peroxidation (LPO), as well as superoxide dismutase (SOD), catalase (CAT), and glutathione peroxidase (GPx) enzyme activities were measured in tissues of marine fish (Therapon jarbua) exposed to mercuric chloride (HgCl) in water dispersions of 0.125 or 0.25 ppm. LPO was significantly increased in various tissues relative to control values after 96-h exposure. SOD and GPx activities significantly decreased after exposure to first two doses but significantly elevated CAT in Dose II kidney and liver tissues. The elevated levels of LPO, decreased activities of SOD and GPx, and increased CAT activities in all tissues examined in T. jarbua are an index of oxidative stress in fish. Structural analysis by scanning electron microscopy studies revealed the structural deformation in HgCl₂-exposed animals. These observations suggest that HgCl acts as a mediator in free radical generation. The increase in CAT and decrease in SOD and GPx activities in these tissues may be an adaptive response.     

不同价态无机砷对罗非鱼肝脏砷积累及GSH/GST解毒代谢的影响

低剂量中长期暴露下的氧化胁迫是砷对水生生物致毒的重要机制之一。本文通过对罗非鱼进行32 d的食物相砷暴露,测定不同时间点罗非鱼肝脏中谷胱甘肽(glutathione,GSH)含量和谷胱甘肽巯基转移酶(glutathione S-transferase,GST)活性,揭示不同价态无机砷对罗非鱼肝脏中GSH/GST的影响机制。经三价砷(As(III))暴露后,砷含量在2 d内显著增加而在随后的30 d内无显著性差异; 0～2 d内GSH含量显著增加,后降低,13 d后GSH含量均低于空白组; 0～6 d GST活性均大于空白组,6～8 d GST活性降低,8 d后活性高于空白组,且32 d达到最大值。经五价砷(As(V))暴露后,罗非鱼肝脏中砷含量逐渐增加,在20 d时达到最大值而后无显著性差异; 0～2 d时GSH含量降低,随后逐渐增加,在16 d达到最大值,16 d后GSH含量均低于空白组; 0～8 d时GST被大量诱导合成,8～20 d时GST合成被抑制,20 d后活性增加,在32 d达到最大值。As(III)和As(V)对罗非鱼GSH/GST的不同影响与其在罗非鱼体内的积累量有关。As(III)暴露后各时间点罗非鱼肝脏中的砷含量与GSH含量呈统计学正相关,而As(V)暴露无明显相关性。这是因为As(V)进入罗非鱼肝脏后会还原为As(III),进而GSH作为可提供巯基的还原剂而被大量消耗。另外,As(III)暴露后各时间点罗非鱼肝脏中的砷含量与GST活性呈显著负相关,而As(V)暴露却呈现出很强的滞后性,这是由于进入生物体内的As(V)需转化为As(III)后,才可直接作用于酶系统。可见,不同形态砷对水生生物的致毒机制需进一步深入研究。     

邻苯二甲酸丁基苄酯对小鼠学习和记忆能力的影响

研究邻苯二甲酸丁基苄酯(BBP)暴露对小鼠脑组织的氧化损伤和对小鼠学习与记忆能力的影响.24只雄性昆明小鼠随机分为4组,每组6只,分别暴露于0,50,250,1250mg/kg的BBP,经口灌胃染毒14d.染毒期间同时进行Morris水迷宫实验,以检测小鼠的学习与记忆能力的改变.实验进行第15d,处死实验动物,取出脑、肝、肾组织,检测ROS水平及MDA和GSH含量.实验结果显示,1250mg/kg浓度BBP染毒组小鼠的学习和记忆能力与对照组相比显著下降(P<0.05);随着BBP染毒浓度的升高,小鼠脑、肝、肾组织中的ROS水平、MDA含量逐渐上升,GSH含量逐渐降低;且在1250mg/kg浓度时与对照组相比具有显著性差异(P<0.05).BBP的暴露可以影响小鼠学习与记忆能力,并对其脑、肝、肾组织产生氧化损伤.     

氯氰菊酯对小鼠脑细胞的氧化损伤及维生素E的抗氧化作用

以昆明小鼠为受试动物,随机分为6组,包括1个阴性对照组、3个氯氰菊酯染毒组、1个维生素E组和1个高剂量氯氰菊酯加维生素E组,染毒组按10,20,40mg/kg 3个剂量水平,维生素E的剂量为100mg/kg,灌胃染毒小鼠7d.以脑组织匀浆测定活性氧(ROS)、还原型谷胱甘肽(GSH)和丙二醛(MDA)的含量;以脑组织细胞测定DNA-蛋白质交联(DPC)系数.随着氯氰菊酯染毒剂量的升高,脑组织的ROS、MDA含量和DPC系数逐渐上升,GSH含量逐渐降低,各指标呈一定的剂量-效应关系.染毒剂量320mg/kg时,ROS含量(841.3±100.34)、GSH含量[(12.54±1.316)nmol/L]和DPC系数(0.054±0.004)有显著差异(P<0.05);染毒剂量340mg/kg时,GSH含量[(10.51±1.545)nmol/L]有显著差异(P<0.05),ROS含量(1014.3±81.67)、MDA含量[(2.849±0.218)μmol/L]和DPC系数(0.079±0.005)有极显著差异(P<0.01).高剂量染毒加维生素E组与高剂量染毒组相比较,脑组织的ROS、MDA含量和DPC系数均有下降,GSH含量上升.脑组织的ROS(719.5±74.56)、GSH[(16.52±1.985)nmol/L]和DPC系数(0.055±0.005)有显著差异(P<0.05),MDA含量[(1.662±0.265)μmol/L]有极显著差异(P<0.01).较高剂量(320mg/kg)的氯氰菊酯能造成小鼠脑组织的氧化损伤,维生素E有抗氧化作用.     

In vivo effects of acute administration of potassium tetranitrodiammine cobaltate(III) on rat erythrocytes

Potassium tetranitrodiammine cobaltate(III) K[Co(NH₃)₂(NO₂)₄] is a coordination complex having Co(III) as the central atom. Cobalt(III) compounds are being advocated for their anticarcinogenic potential. In the present study, we have for the first time evaluated this compound for its toxicity to rat RBC. The parameters studied include the effects of potassium tetranitrodiammine cobaltate(III) on GSH, GST, catalase, G6PD, acid phosphatase, GOT, and GPT. Scanning electron microscopy of RBCs of potassium tetranitrodiammine cobaltate(III) treated rats has also been carried out for evaluating its influence on the red cell morphology. The data showed that potassium tetranitrodiammine cobaltate(III) treatment causes marked biochemical changes in the rat RBCs along with changes in their shapes characterized by the formation of acanthocytes. The results thus suggest that acute administration of potassium tetranitrodiammine cobaltate(III) is potentially toxic to rat RBCs.