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11.
This study measured activities of serum enzymes alkaline phosphatase, acid phosphatase, glutamic oxaloacetic transaminase (SGOT), and glutamic pyruvic transaminase (SGPT), markers of liver function in albino rats after continuous ingestion of arsenic trioxide (As203). For the study, treated animals were given AS2O3 (0.2 mg/100 g/day) orally for 180 days. After the completion of treatment, the blood was collected for the estimation of serum biochemical markers. The results obtained were compared with control group. Data showed a significant increase in SGOT and SGPT activity after 60 days of As203 administration. The level of alkaline phosphatase and acid phosphatase increased significantly after 90 and 120 days, respectively. Since the elevation of these serum enzymes is an indicator of hepatic damage, data indicate that As2O3 produces hepatotoxicity. When taken continuously, arsenic was also deposited in liver and blood and affected the enzymatic pathways. Total accumulated arsenic was determined by HG-AAS at 193.7 nm.  相似文献   
12.
溴氰菊酯对大鼠肝微粒体酶的影响   总被引:1,自引:0,他引:1  
本实验研究了溴氰菊酯对雄性大鼠肝微粒体苯胺羟化酶活力和细胞色素P-450含量的影响。结果发现溴氰菊酯在动物体内能降低苯胺羟化酶活力(23.80%)和细胞色素P-450含量(21.18%)。该效应与微粒体脂质过氧化反应无关,亦与肝细胞破坏或内质网膜通透性的改变无关。溴氰菊酯本身对肝微粒体酶并不呈现抑制作用,当用肝微粒体酶诱导剂苯巴比妥诱导肝微粒体酶后,溴氰菊酯降低微粒体酶活性的效应消失。这表明溴氰菊酯降低肝微粒体酶的作用可能与其干扰肝微粒体酶蛋白的合成有关。  相似文献   
13.
预先给小鼠灌胃不同剂量的京尼平甙后,以四氯化碳造模,通过测定小鼠血清中丙氨酸氨基转移酶(ALT)、天氡氨酸氨基转移酶(AST)以及肝脏内GSH的含量并制作组织病理切片,研究了京尼平甙对四氯化碳肝损伤小鼠的保护作用,结果表明,京尼平甙能抑制四氯化碳肝中毒小鼠血清中ALT和AST的活性以及增加肝脏内GSH的含量.然后研究了京尼平甙对正常小鼠肝微粒体内细胞色素P4502E1和细胞色素P4503A活性的影响以及肝脏内谷胱甘肽(GSH)系统的影响,表明京尼平甙对正常小鼠肝微粒体内CYP4502E1具有明显的抑制作用,并能增强肝脏内谷胱甘肽还原酶(GR)以及谷胱甘肽-S-转移酶活性.以上3个酶与自由基形成以及清除有关.图1表3参16  相似文献   
14.
The effects of Ni on hepatic enzymes of tilapia, viz. acid‐ and alkaline phosphatases, catalase and glucose‐6‐phosphatase, both under in vivo and in vitro conditions reflected the following tendencies. In vivo conditions indicated maximal increase in activity for acid phosphatase at 3.00 ppm, equivalent to 28.5%, followed by a slight decrease and increase thereafter. As for alkaline phosphatase, gradual increase in activity was observed with maximal activity at 9 ppm of Ni, equivalent to 16.8%. Catalase demonstrated similar tendencies with maximal activity at 9.0 ppm, equivalent to 101.2%. In the case of glucose‐6‐phosphatase, the tendency was the reverse with maximal inhibition at 9.00 ppm, i.e. 41.9%. In contrast to in vivo conditions, in vitro systems indicated that all investigated enzymes were inhibited in the region of 4–10% except for catalase which demonstrated a slight increase by 5–6% in activity between concentrations of 10–15 ppm of Ni but thereafter continuous inhibitory effects prevailed.

At cellular level, exposure of tilapia to a lethal dose of 9 ppm of Ni indicated not much of an adverse effect except for a slight depletion in fat and glycogen content. In the case of mitochondria, they were normal and a few large secondary lysosomes were observed. In relation to the cell membrane no dramatic change was detected.  相似文献   
15.
三唑醇(triadimenol, TN)是一种广泛使用的手性三唑类杀菌剂,它含有2个手性中心,4个手性对映体,包括对映体A(A1(R,S)和A2(S,R))以及对映体B(B1(R,R)和B2(S,S))。为了研究三唑醇在爬行动物体内的对映选择性行为和潜在的肝毒性,将雄性丽斑麻蜥分别一次经口暴露和28 d长期暴露于三唑醇(100 mg·kg~(-1) body weight),一次经口暴露结果显示,三唑醇进入大脑和肾中的浓度低于肝、性腺、皮肤和尾,B2(S,S)和B1(R,R)对映体具有相似的代谢速率。代谢过程中A1(R,S)的浓度明显高于A2(S,R),并且在暴露后12 h出现二次上升,这可能是A2(S,R)在体内手性转换为A1(R,S)导致。丽斑麻蜥长期(28 d)暴露于三唑醇后,性腺和肾中无明显蓄积现象,皮和尾中浓度显著高于其他组织,各个组织中三唑醇趋向于保持外消旋状态。三唑醇暴露后肝中主要的代谢基因cyp1a1c、yp3a4c、yp2b1和cyp2d3的表达量都出现明显上升,组织病理学分析进一步显示,三唑醇暴露后的肝组织出现组织空泡、血窦阻塞的症状,说明三唑醇对肝组织具有一定的毒性作用。上述结果为手性农药对爬行动物的生态毒理学评价提供了重要依据。  相似文献   
16.
We report a case of a twin pregnancy which was complicated by a twin–twin transfusion in which the recipient twin was noted to have an intra-abdominal echogenic mass. This twin died at two days of age of hepatic infarction. The donor twin was healthy at birth, at thirty weeks' gestation, and did not have any subsequent problems. Fetal intra-abdominal echogenicity may be a marker of hepatic infarction. Copyright © 2002 John Wiley & Sons, Ltd.  相似文献   
17.
PFOS致大鼠肝毒性及其作用机制研究   总被引:1,自引:0,他引:1  
通过全氟辛烷磺酸(perfluomoctane sultanate,PFOS)大鼠灌胃染毒实验评价PFOS对肝功能的影响,探讨PFOS肝毒性反应的潜在机制与可能途径。将Sprague Dawley (SD)雄性大鼠随机分为3组,分别以0 mg·kg~(-1)、5 mg·kg~(-1)和10 mg·kg~(-1)PFOS灌胃染毒28 d。以HE和油红染色法观察大鼠肝脏形态改变。ELISA法测定各组谷丙转氨酶(alanine aminotransferase,ALT)、谷草转氨酶(aspartate transaminase,AST)、碱性磷酸酶(alkaline phosphatase,ALP)含量变化。化学比色法测定肝匀浆脂代谢水平和氧化产物含量。RT-PCR法检测肝脏内氧化应激以及脂代谢相关基因表达水平。结果表明,PFOS暴露大鼠体重显著降低而肝脏系数显著增加(P0.05),与对照组相比PFOS组血清肝功能酶均出现随PFOS浓度增加而升高(P0.05)。同时大鼠肝脏谷胱甘肽过氧化物酶(glutathione peroxidase,GSH-px)和丙二醛(malondialdehyde,MDA)水平在高剂量组显著升高(P0.05),超氧化物歧化酶(superoxide dismutase,SOD)含量先显著升高(P0.05)后显著降低(P0.05)。且肝脏中脂代谢水平也随PFOS浓度的增加而出现显著改变(P0.05)。PFOS组基因表达均较对照组显著上升(P0.05)。以上结果说明PFOS具有明显的肝毒性作用,可影响肝脂代谢水平,这可能与PFOS引起的氧化应激所导致的损伤有关。  相似文献   
18.
以鲤鱼肝脏微粒体为实验体系,运用体外实验方法,研究三种含油废水对芳烃羟化酶的活性影响,结果表明,三种含油废水对芳烃羟化酶活性都表现出不同程度的诱导,随着含油量的增大,AHH活性升高,并有相似的变化趋势。芳烃羟化酶活性升高可以作为监测含油废水对水体污染的一种生物指标。  相似文献   
19.
使用环境相关浓度水平(0.05、0.5、5、50 μg· L-1)的布洛芬(Ibuprofen,IBU)对黄颡鱼进行水体暴露,研究IBU对黄颡鱼Ⅰ相代谢酶及其抗氧化系统的影响.结果表明,随着暴露时间的延长,IBU对黄颡鱼肝脏Ⅰ相代谢P450酶系的氨基比林-N-脱甲基酶(APND)、红霉素-N-脱甲基酶(ERND)、7-乙氧基-异吩噁唑酮-脱乙基酶(EROD)和Ⅱ相代谢谷胱甘肽硫转移酶(GST)均表现出先诱导后抑制的作用.暴露24 h时,IBU浓度为5 μg· L-1实验组对Ⅰ相代谢酶APND和ERND的诱导程度最大.当暴露时间达到168 h时,0.5 μg·L-1浓度组中APND和ERND活性均受到极显著抑制.Ⅰ相代谢酶EROD活性在暴露24 h后,除0.05 μg· L-1浓度组无明显变化外,其它浓度组皆受到显著诱导,随着暴露时间延长到168 h时,逐渐恢复到初始水平.GST活性在暴露24 h后,除0.05 μg·L-1浓度组外,其它浓度组均受到最大程度的诱导,过氧化氢酶(CAT)在暴露168 h时被显著诱导.各浓度组丙二醛(MDA)含量在暴露24 h时较对照组显著下降,72 h时其含量达到最高值.其中,ERND响应较为敏感,适合作为布洛芬暴露的生物标记物.  相似文献   
20.
A case of a prenatally recognized hepatic mesenchymal hamartoma is presented and the literature reviewed. These tumors are benign and usually present in early infancy with symptoms that are related to the mass effect on adjacent organs. Radiologic methods used in the past to image this tumor include angiography and ultrasound. However, there is no specific radiologic finding, and, therefore, the diagnosis is usually made during surgery. Once the tumor is removed, the prognosis is generally good. With the increasing use of high resolution ultrasound in prenatal diagnosis, this rare tumor should be considered in the differential diagnosis of any multicystic mass found in the fetal abdomen. The recognition of a mass should then alert the physician to the need for early neonatal intervention.  相似文献   
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