吸烟对男性生殖和遗传毒性的研究进展

吸烟作为一个社会问题受到广泛关注,目前研究认为吸烟可对生殖系统存在有害影响。从吸烟对睾丸功能、精液质量、生殖内分泌功能的影响及吸烟对生殖细胞的遗传毒作用几个方面,总结了近几年国内外有关吸烟对男性生殖与遗传毒性研究进展,为进一步研究吸烟的生殖毒性提供参考。     

铅对雄性生殖毒性的研究进展

从铅对睾丸与附睾形态、精子生成和发育以及生殖内分泌功能等三方面的影响综述了铅对雄性生殖毒性的研究进展;并从铅对睾丸的脂质过氧化损伤,对睾丸标志酶活性的影响,对染色体、DNA及基因的影响以及对CaM、Ca2 -ATP酶活性的影响等方面探讨了铅对雄性生殖毒性作用机理。同时,提出了铅对雄性生殖毒性的研究中存在的若干问题和发展方向。     

丙烯酰胺对小鼠血液毒性的研究

目的 为探明丙烯酰胺对小鼠血液的毒性效应.方法 采用丙烯酰胺溶液连续灌胃小鼠16天,记录小鼠体重、器官系数变化并对小鼠血液成分进行检测.结果 当染毒剂量为120、150 mg/kg时,小鼠体重增重率、肝系数、WBC、LYM、RBC、MCHC、PLT、P-LCR显著降低(P<0.05),GRAN显著增加(P<0.05);...     

蛇毒心脏毒素对动物细胞的遗传损伤和生殖毒性研究

目的 应用眼镜蛇毒心脏毒素（ＣＴＸ）作用于小鼠的骨髓细胞和生殖细胞,以探讨ＣＴＸ对动物体的生殖毒性和遗传毒性。方法 对小鼠腹腔注射不同剂量ＣＴＸ,通过生殖毒性实验和致突变实验,分析孕鼠的胚胎存活率,骨髓细胞和精母细胞的染色体畸变率。结果：ＣＴＸ能影响胎鼠的生长发育,使孕鼠的增重和活胎率均明显地降低（Ｐ〈０．００１）,染色体畸变实验显示ＣＴＸ０．４ｍｇ／ｋｇ剂量上精母细胞多倍体和非整倍体细胞数目增高     

壬基酚对雄性黑斑蛙生殖毒性的研究

通过研究壬基酚对雄性黑斑蛙(Rana nigromaculata)成体的精子和精巢的影响,探讨壬基酚对黑斑蛙的生殖毒性.用不同剂量的壬基酚对雄性黑斑蛙进行处理,对黑斑蛙的精巢系数、精子数、形态结构、畸形率和精巢显微结构等分别进行研究.结果表明,与对照组相比,随着壬基酚浓度的升高,染毒组黑斑蛙的精巢系数下降,精子数减少,精子畸形率明显增大;畸形精子主要表现为其头部出现肥大、弯曲和圆形等现象;精巢显微结构发生变化,表现为生精小管萎缩,生精细胞层次减少,间质区不明显.说明壬基酚对雄性黑斑蛙生殖系统具有毒性效应.     

苦参碱的提取分离及对小鼠的毒性研究

采用酸性乙醇提取、乙醚萃取、硅胶柱层析分离等方法从苦参中分离到苦参碱单体.以小鼠为实验动物进行毒性测定,小鼠的死亡主要集中在48h内,48h后无小鼠的死亡现象.小鼠对苦参碱的耐受量大于30mg.k-g1,小于140mg.k-g1,致死中量LD50为64.01mg.kg-1,回归方程Y=-3.2370+4.5602X,LD50标准误差SE=6.14.适口性的测定表明,苦参碱对小鼠有较好的适口性,可以作为杀鼠剂使用.     

恒定磁场对小鼠精子毒性作用的实验研究

观察不同强度恒定磁场对雄鼠睾丸、附睾重量、精子数量、精子活动度及精子形态的影响. 结果显示睾丸与附睾重量各组无显著差异, 精子数量在实验组与对照组中亦无明显改变. 在 0.12T磁场环境暴露下, 雄鼠精子畸形率增加及活动率下降, 与对照组相比有显著差异. (P< 0.01), 提示磁场对小鼠精子有一定毒性, 并且毒性与其强度有关.     

低浓度84消毒液对小鼠生殖生理的影响

目的：观察低浓度84消毒液对小鼠生殖生理的影响。方法将72只KM小鼠随机分为3组,即：0.5％84消毒液组（ A组）、2.0％84消毒液组（ B组）和生理盐水组（ C组）,每组24只,雌雄各半,各组每天1次灌胃给予相应药物,连续9周。阴道涂片镜检观察雌性小鼠的动情周期。9周后,观察雄性小鼠的精子畸形率;并用ELISA法测定小鼠血清中性激素的水平;并取睾丸（或卵巢）、心、肝、肺、肾进行组织学观察。结果与C组比较,A和B组小鼠体重差异无显著性（ P ＞0.05）;血清性激素水平差异无显著性（ P ＞0.05）;雌性小鼠动情周期差异无显著性（P ＞0.05）;组织学观察未见异常;与C组比较,A组小鼠精子畸形率差异无显著性（P ＞0.05）,B组小鼠精子畸形率显著增高（ P ＝0.041＜0.05）。结论0.5％84消毒液对小鼠的生殖生理无明显影响,在实际使用中要严格控制消毒液浓度。     

氯化二丁基锡对雄性小鼠睾丸和精子质量的影响

成年雄性小鼠腹腔注射 0 0 2 5～ 0 40 μg/kg/d氯化二丁基锡 (DBTCl) ,染毒 7d。实验温度 2 2± 2℃ ,光∶暗 =1 2h∶1 2h。结果表明 ,DBTCl对雄性小鼠生殖系统毒性影响很强。在≥ 0 0 5μg/kg剂量作用下 ,小鼠睾丸重量、精子存活率和密度明显下降 ,精子畸形率明显增加。观察发现 ,在 0 0 2 5～ 0 0 5μg/kg低剂量组中精子头部畸形率较高 ,而在0 2 0～ 0 40 μg/kg高剂量作用下 ,精子尾部的畸形率明显增加。剂量大于 0 1 0 μg/kg处理组小鼠体重明显下降。DBTCl和雄性小鼠生殖指标之间存在剂量 效应关系。DBTCl对精子存活率和精子密度 7d的ED50 值分别为 0 1 7和 0 1 9μg/kg。本项研究为有机锡化合物引起哺乳动物精子畸形的早期诊断提供可能的指标与方法     

伊维菌素对雄性鲫的生殖毒性评价

伊维菌素作为一种广谱、高效的新型抗寄生虫类药物,在我国农、牧、渔业均有广泛应用.为了评价伊维菌素对雄性鲫的生殖毒性效应,本文研究了口灌不同剂量伊维菌素对雄性鲫生殖腺指数、血清及精巢中性激素(睾酮和雌二醇)、血清及脑组织中的γ 氨基丁酸含量、精子超微结构及性腺组织的影响.分别以0、1、3、5倍治疗剂量,即0、0.3、0.9和1.5 mg·kg^-1剂量对鲫进行口灌给药,分别标记为A、B、C、D组,每天1次,连续3 d,停药8 d后对供试鲫各组织进行检测观察.结果表明： 随着给药剂量的增加,供试鲫生殖腺指数逐渐降低,且C和D组显著低于A组;血清及精巢中的睾酮及雌二醇、血清和脑中γ-氨基丁酸含量均表现为先升高再降低趋势,均在B组达到峰值;精子寿命逐渐降低,Ⅱ、Ⅲ和Ⅳ级精子运动时间逐渐减少,C、D组表现尤为明显;精子超微结构和精巢组织未见明显异常.表明正常治疗剂量伊维菌素对生产期雄性鲫未产生明显生殖毒性效应,但高剂量给药可对鲫造成严重的潜在生殖毒性.     

Reproductive and developmental toxicity of the Ginkgo biloba special extract EGb 761® in mice

Extracts from leaves of Ginkgo biloba are among the most widely used and best investigated phytopharmaceuticals worldwide. Almost all clinical trials and the majority of preclinical studies have been performed with a specifically defined extract (EGb 761^®) standardized to contain confined concentrations of active ingredients and limited quantities of potentially harmful substances. Besides pharmaceutical grade extracts poorly characterized Ginkgo preparations are now increasingly appearing on the market as nutraceuticals. While the safety of EGb 761^® has been evaluated in an extensive set of toxicology studies, adverse effects of Ginkgo extracts of non-pharmaceutical quality on reproductive functions in mice have been reported in several publications in recent years. As this species has not previously been used in reproductive toxicity studies with EGb 761^®, the present investigation was conducted to examine the influence of EGb 761^® (100, 350 and 1225 mg/kg/day) on embryo-fetal development in mice during the critical period of organogenesis. During external and internal inspection of the fetuses as well as examination of skeletal and soft tissues no embryotoxic properties were noted. In particular, the incidence of malformations, variations or retardations was not increased and the general condition of dams was not influenced. Thus, the no-observed-effect level (NOEL) was above 1225 mg/kg/day for the dams and the fetuses.     

离体子宫张力测定在药物生殖毒性研究中的应用

目的:建立药物生殖毒性研究中孕鼠离体子宫平滑肌张力的测定方法。方法:SD大鼠于妊娠第6~15天(GD6-15)给予受试物,在妊娠第20天(GD20)取子宫平滑肌,分别给予不同浓度缩宫素和硫酸镁溶液刺激,选择试验的最佳条件。在此基础上,测定不同剂量组孕鼠离体子宫平滑肌张力的变化情况,采用RM-6240BD多道生理信号采集处理系统分析数据,统计结果。结果:选择0.007 U/m L缩宫素、0.008 mol/m L硫酸镁为最佳刺激浓度。随着受试物剂量的增加,加入缩宫素后,各组妊娠子宫平滑肌的频率和张力均呈逐渐上升的趋势,而加入硫酸镁后,各剂量组妊娠子宫平滑肌的活动幅度、频率和张力均呈现降低的趋势,但各剂量组与溶媒对照组相比均未见明显差异(P0.05)。结论:本研究建立了孕鼠离体子宫平滑肌张力的测定方法,该方法可以更好的反映受试物对孕鼠子宫肌的毒性作用,更加全面的评价受试物的生殖毒性。     

SD大鼠胚胎-胎仔发育毒性试验的基础数据

目的 检测胚胎-胎仔发育毒性试验中SD大鼠妊娠期的体重、生殖功能指标及胎鼠的各项发育指标,为SD大鼠的发育毒性研究提供参考数据.方法 395只SD雌性大鼠,交配成功后,于妊娠第20天剖检孕鼠,检查孕鼠的内脏器官有无异常,称量子宫重量、窝重和胎盘重量,计数黄体数、着床数、活胎数、吸收胎数和死胎数.胎鼠共5272只,将一半胎鼠放人固定液中做内脏检查,另一半胎鼠进行骨骼检查,检查胎鼠外观、内脏和骨骼有无异常和变异.结果 和结论 建立SD大鼠胚胎-胎仔发育毒性试验中各项指标的数据库,求得各指标的正常值及标准差,95％的可信区间,为生殖毒性研究提供正常值的参考依据.     

Influence of copper on the early post-implantation mouse embryo: An in vivo and in vitro study

Summary Female mice were injected intravenously with copper sulphate on either the 7th day (early egg cylinder stage of development), the 8th day (late egg cylinder stage), or the 9th day (early somite stage of development), and examined on the 10th day of gestation. Injection on the 7th day was found to be embryo-lethal; when females were injected on the 8th day, the majority of the surviving embryos exhibited anomalies of the neural tube and/or the heart, while injection on the 9th day resulted in a very low incidence of anomalies. The most common malformations seen on the 10th day involved failure of closure of the neural tube in the head region of the embryo, and various types of anomalies of cardiac rotation and shape. When additional females injected on the 8th day were examined on the 12th day, a high proportion of the fetuses examined had developed exencephaly.A further group of embryos from untreated females were explanted on the 9th day and cultured in vitro in various concentrations of copper sulphate. The lowest levels tested had little obvious effect on neural tube closure. Intermediate doses resulted in, retarded and anomalous embryonic development, while the highest levels employed resulted in neural tube and cardiac anomalies similar to those produced in vivo.The results demonstrate both the direct toxic effect of copper on embryonic development and that the stage of embryonic development at the time of exposure determines both the nature and the extent of the effect.     

Commentary on the Role of Maternal Toxicity on Developmental Toxicity

Maternal mammalian toxicity impacts prenatal development, with general systemic maternal toxicity, from reduced weight gain to morbidity, causative for reduced fetal weights/litter and increased fetal variations (especially skeletal)/litter, but not, in the author's opinion, for increased fetal malformations, reduced litter sizes or full litter losses. Increased fetal malformations are likely due to exposure to specific chemicals which alter specific maternal functions at critical point(s) in pregnancy, typically exaggerated effects from higher doses by drugs under development with known, desired pharmacological effects. Malformations can also be from genetic/epigenetic alterations, specific altered proteins, molecular pathways, etc. Full litter losses are triggered by the mother and are rare in rats. Information to inform maternal (and developmental) toxicity includes ovarian corpora lutea counts, uterine implantation profile, degree of litter reduction (if present), timing and extent of maternal toxicity relative to those of adverse embryofetal effects, etc. The view of maternal toxicity as confounding results in in vivo developmental toxicity studies, worldwide concerns about increased research animal usage, increasing time, labor, costs, and new software and hardware sophistication all drive the interest in development, validation, and performance of in vitro/in silico assays. These assays are fast, inexpensive, responsive to animal use concerns and amenable to mechanistic questions. The strength of these in vitro/in silico assays is considered by many to be the absence of the maternal organism/placenta. These assays inform mechanism and hazard, but NOT risk. The Environmental Protection Agency currently estimates that these new assays are approximately 70% accurate versus the whole animal tests.     

圈养小熊猫繁殖行为变化及繁殖行为对策

In order to investigate the change of reproductive behaviors and understand reproductive strategies of both male and female red pandas, one-year behavioral observation was conducted through the focal sampling method in the Chengdu Research Base of Giant Panda Breeding from December 1999 to November 2000. Our results indicated that reproductive behaviors showed significant differences between the estrous and non-estrous seasons. Frequencies of the rubbing anogenital, sniffing and licking marking were much higher in estrus than in non-estrus. Bleating only appeared in the estrus and can be regarded as an estrous indicator.The result also demonstrated that both male and females applied different reproductive behavioral strategies. Frequencies of activity, rubbing anogenital, licking and sniffing marking, and bleat were much higher in the male than in the female. However, those of resting and investigating were much lower in the male than in the female. This indicated that the male was more active than the female during the estrus and might imply that the male acts mainly as an estrous message sender, and the female as a message receiver in the estrous season.     

小型哺乳动物的繁殖投入与繁殖成功率

动物的繁殖活动关系到整个种群的生存与灭绝, 繁殖投入和繁殖成功率是繁殖生态学研究的重要内容。从繁殖投入的划分入手, 综述了小型哺乳动物的繁殖投入和繁殖成功率之间的关系及其影响因素、分子生物学技术在繁殖生态学中的应用等, 阐述了小型哺乳动物能够根据自身的状态调整每次繁殖活动中的时间投入和能量分配, 采取不同的繁殖对策。这些繁殖对策是长期自然选择的结果, 其目的都是为了最大限度地提高自身的适合度。并且指出分子生物学技术在繁殖生态学中的应用将大大加快这一研究领域的快速发展。     

Preclinical Reproductive and Developmental Toxicity Profile of a Glycine Transporter Type 1 (Glyt1) Inhibitor

Bitopertin is a glycine type 1 (GlyT1) inhibitor intended for the treatment of psychiatric disorders. The principle adverse effect in the regulatory reproductive toxicity studies was peri‐natal pup death when rat dams were treated during parturition at a dose resulting in five‐times the human therapeutic exposure (AUC). Cessation of dosing two days before parturition prevented the pup deaths. Investigatory experiments and pharmacokinetic modelling suggested that the neonatal mortality was related to transplacental passage of bitopertin leading to high systemic levels in the newborn pups. Brain levels of bitopertin in the rat fetus and neonate were two‐fold higher than in the mother. As illustrated by knock‐out mice models, GlyT1 function is essential for neonatal pup survival in rodents, but is not necessary for normal prenatal morphological development. The glycine transport systems are immature at birth in the rat, but are functionally well‐developed in the human newborn. While the relevance to humans of the neonatal mortality seen in rats following late gestational exposure is unknown, bitopertin would not be recommended for use during late pregnancy unless the anticipated benefit for the mother outweighs the potential risk to the newborn.     

乙酸铜对雄性小白鼠生殖毒性的影响

以清洁级ICR雄性小白鼠为实验动物,研究不同剂量乙酸铜对小白鼠的生殖毒性。采用小白鼠精子畸形实验及小白鼠骨髓嗜多染红细胞(以下简称PCE)微核实验等方法。分别对成年小白鼠腹腔每天注射0.25~16.00mg/kg8个剂量的乙酸铜,染毒7天。结果表明:乙酸铜对小白鼠的体重增长及睾丸重量具有一定的抑制作用,其中组VI、组VII的最明显。不同剂量的乙酸铜均使雄性小白鼠精子密度(P<0.001)、精子活力明显降低,具有明显的剂量效应。各实验组精子畸形率、PCE微核率均明显高于对照组(P<0.001)(P<0.05或P<0.001),且均随乙酸铜剂量的增加而明显升高。结果表明实验剂量的乙酸铜对ICR雄性小白鼠具有明显的生殖毒性效应。