聚谷氨酸-明胶生物胶生物学评价

考察了聚谷氨酸-明胶生物胶的生物性能。从细胞毒性、急性毒性、皮肤刺激、溶血、热源、皮肤致敏等试验对其进行生物学检测。结果发现：聚谷氨酸-明胶生物胶的细胞毒性、急性毒性、皮肤刺激、溶血、热源、皮肤致敏试验均为阴性。这些结果表明聚谷氨酸-明胶生物胶具有良好的生物性能。     

蜂胶提取物的安全性试验研究

目的 探讨蜂胶的乙醇提取物（EEP）的安全性。方法 用0.5％的EEP对家兔进行皮肤急性毒性试验、皮肤刺激试验以及对豚鼠的过敏试验。结果 EEP低剂量、高剂量皮肤破损组和对照组皮肤破损组各有一只家免,在24 h观察到皮肤破损处微红,48 h消失,其余各实验兔的皮肤、毛发、眼、粘膜、呼吸、中枢神经系统均无任何中毒表现;按照皮肤刺激反应强度,评价标准,完整皮肤组平均分为0,判为无刺激性;破损皮肤组平均分值为033＜0.50,亦判为无刺激性;A组空白对照组和B组EEP组动物均无红斑和水肿反应,判为无致敏性。结论 蜂胶提取物EEP在对实验动物体外寄生虫净化中安全、无毒、无刺激。     

复合生物杀菌剂F6-11的安全性毒理学研究

目的：为研究复合生物杀菌剂F6．11毒性,采用动物实验法进行毒理学评价。方法：对复合生物杀菌剂F6-11进行小鼠急性毒性试验、小鼠骨髓嗜多染红细胞微核试验、亚急性毒性试验、家兔多次完整皮肤刺激试验、急性眼刺激试验、豚鼠皮肤变态反应试验、鱼类延长毒性14天试验。结果：复合生物杀菌剂F6—11对小鼠急性毒性LD50〉5000mg／kg．bw,属于实际无毒级物质;小鼠微核试验该杀菌剂各剂量组与阴性对照组比较,微核率无显著性差异（P〉0．05）;亚急性毒性试验动物血常规、生化指标及各脏器均未发现异常;对家兔多次完整皮肤及眼刺激反应积分均为0,均属无刺激性;对豚鼠皮肤变态反应试验组动物与阴性对照组无可见不同．试验组动物皮肤致敏反应积分为0,无致敏作用;鱼类延长毒性14天试验无异常。结论：毒理学研究表明,复合生物杀菌剂F6．11具有良好的使用安全性。     

紫茎泽兰醇提物的毒理学研究

为确保以紫茎泽兰提取物为主要原药的植物源农药的安全性,对紫茎泽兰醇提物进行了小鼠经口急性毒性试验、大白兔急性皮肤和眼刺激试验、小鼠骨髓嗜多染红细胞微核计数及小鼠精子畸形试验等急性毒性和遗传毒性试验。结果表明,受试物对两种性别的小鼠经口急性毒性试验,LD50大于5000mg／kg,对大白兔皮肤无刺激性;小鼠骨髓嗜多染红细胞微核试验及小鼠精子畸形试验结果均为阴牲,受试物未见遗传毒性。     

瑞香狼毒提取物对试验动物急性毒性及活性的初步研究

采用急性经口、眼刺激、皮肤试验方法,研究了瑞香狼毒乙酸乙酯萃取物的急性毒性作用,同时以番茄晚疫病菌为供试菌,研究了瑞香狼毒提取物的抑菌活性.初步研究表明,瑞香狼毒乙酸乙酯萃取物对小白鼠经口急性毒性为低毒,对白兔的急性皮肤刺激属无刺激性,对白兔的眼刺激属轻度刺激性,对鲫鱼的毒性属于中毒级;瑞香狼毒乙酸乙酯萃取物及其分段物流分B、c、D对番茄晚疫病菌有较好的抑制活性,这为瑞香狼毒乙酸乙酯萃取物进一步开发为产品提供了毒理学依据.     

成团泛菌低分子脂多糖的急性毒性、刺激性、致敏性及遗传毒性评估

本研究对成团泛菌低分子脂多糖(Pantoea agglomerans lipopolysaccharide,LPSp)的安全性进行初步评估.本研究采用一次限量法,用昆明种小鼠进行LPSp急性经口毒性试验,了解LPSp的急性毒性;采用新西兰兔分别进行LPSp急性和多次皮肤刺激性试验以及急性眼刺激性试验,了解LPSp的皮肤和粘膜刺激性;采用豚鼠进行LPSp皮肤变态反应试验,了解LPSp的致敏性;应用平板掺入法进行鼠伤寒沙门氏菌/回复突变试验和小鼠骨髓细胞微核试验考察LPSp的遗传危害.急性毒性试验结果显示,LPSp对小鼠经口一次灌胃的LD50大于5 000 mg/kg体重,属实际无毒级别;LPSp急性和多次皮肤刺激性试验以及急性眼刺激性试验结果显示,皮肤刺激和眼刺激积分均为0分,LPSp对皮肤无刺激性、对眼睛无急性刺激性;在皮肤变态反应试验中,LPSp在各观察时间点的皮肤变态反应积分均为0分,其致敏率均为0%,说明LPSp对豚鼠无致敏性; LPSp的鼠伤寒沙门氏菌/回复突变试验结果呈阴性(P>0.05);LPSp的小鼠骨髓细胞微核试验结果亦呈阴性,LPSp 各剂量组的微核发生率与阴性对照组未见统计学差异(P>0.05),而与阳性对照组有明显差异(P<0.01).本研究结果表明,在本实验剂量范围内,LPSp对小鼠经口毒性极低,属实际无毒级别,对家兔皮肤和眼睛无明显刺激性,对豚鼠无致敏性,对所试菌株和小鼠体细胞无诱变性和致突变性.     

改良丁字带对妇科阴式手术后阴道微生态的影响

目的探讨改良丁字带对比传统丁字带对妇科阴式手术后患者阴道微生态的影响。方法选择妇科阴式手术患者186例作为研究对象,随机分为两组,观察组93例使用改良丁字带固定,对照组93例使用传统丁字带固定。对比分析两组患者术后阴道微生态,敷料污染,引流管阻塞、脱落,皮肤受损,排尿困难等的发生情况。结果观察组阴道微生态失衡发生率为23.66%,敷料污染发生率为29.03%,引流管阻塞发生率为7.52%,皮肤受损发生率为3.23%,均明显低于对照组,差异具有统计学意义(均P0.05)。结论妇科阴式手术后使用改良丁字带固定能够减少手术患者阴道微生态失衡及相关并发症的发生率,提高患者生活质量。     

子宫托对阴道微生态的影响以及应用雌激素的作用

通常将阴道前后壁、膀胱或直肠等盆腔脏器突入阴道内,称为盆腔脏器脱垂,常发生于老年女性。盆腔脏器脱垂及其引起的排尿相关症状严重影响患者的生活质量。目前临床上治疗盆腔脏器脱垂最常用的方法为佩戴子宫托。子宫托治疗盆腔脏器脱垂已有久远的历史。使用子宫托可明显改善盆腔脏器脱垂患者的临床症状,提高患者的生活质量。然而研究显示,对于机体而言,阴道内放置子宫托可在一定程度上影响阴道微生态环境平衡,从而使佩戴子宫托患者的细菌性阴道病患病率增加4.37倍。同时使用雌激素可明显减少由使用子宫托引起的阴道微环境改变、出血、溃疡等症状的发生。现就子宫托对阴道微生态的影响以及应用雌激素的作用做一简要综述。     

苯酚和对苯二酚对鲫血细胞DNA损伤的研究

酚类可通过水产动物皮肤、鳃吸入或摄入肠道引起肌肉异味;挥发酚对鱼类有一定的急性毒性1 ,这必然会引起人们对食品安全的担忧。       

躯体感觉Ⅱ区皮层内微刺激对猕猴回避性操作式条件反射和针刺镇痛的影响

在七只清醒、可以活动的猕猴上观察了皮层内刺激 S_Ⅱ区对外周痛阈和针刺镇痛的影响,其结果如下:(1)在73次皮层内刺激的实验中有72次引起对侧相应皮肤感受野的痛阈变化,其中54次痛阈明显升高。痛阈升高的效应在停止刺激后常持续0.5—3min。较浅层的刺激,痛阈升高比较明显;不同刺激强度引起的痛阈升高的程度也不相同。(2)一般皮层内刺激 S_Ⅱ区也可导致同侧相应皮肤感受野痛阈升高,但不如对侧痛阈升高明显。(3)皮层内刺激 S_Ⅱ区时,非感受野痛阈几乎没有任何改变。(4)S_Ⅱ区皮层内刺激可增强针刺镇痛效应。     

Concerning the toxicity of two compounds used as mediators in biosensor devices: 7,7,8,8-tetracyanoquinodimethane (TCNQ) and tetrathiafulvalene (TTF).

The lethal dose (LD50) and the maximum tolerated dose (MTD) of TCNQ and TTF were determined experimentally by single-dose administration to CBA-line mice. The effect of the compounds on the blood constitution, accumulation, acute and subacute dermal and eye irritation, skin sensitization and delayed type hypersensitivity reaction were also monitored in mice and guinea pigs. The LD50s were found to be 1225 mg kg-1 (6.0 mmol kg-1) for TCNQ and 710 mg kg-1 (3.5 mmol kg-1) for TTF; MTDs were 750 mg kg-1 (3.7 mmol kg-1) and 450 mg kg-1 (2.2 mmol kg-1), respectively. Mice that had received the MTD showed no significant change in their measured blood parameters after five days for TTF; however, for TCNQ a decrease in the absolute leucocyte number and changes in the leucoformula were apparent by the fifth day. Oral administration to mice for 28 days at a concentration of 10% of the LD50 showed a super-accumulation, and the accumulation index was 0.94 and 0.53 for TCNQ and TTF, respectively. Neither compound caused acute or subacute dermal irritation of guinea pigs and there was no acute eye irritation. Skin sensitization in guinea pigs and delayed-type hypersensitivity reaction in mice indicated that TCNQ and TTF used as ethanol solutions were not allergic. This study indicates that TCNQ and TTF may be regarded as low-toxicity compounds.     

噻吩磺隆的毒性及致突变性

选用大鼠、豚鼠及家兔,采用经口及皮肤,粘膜染毒途径,研究其急性毒性。同时有Ames试验,小鼠骨髓嗜多染红细胞微核试验及小鼠睾丸初级精母细胞染色体畸变试验进行致突变性研究,了解噻吩磺隆的毒性及致突变性。大鼠急性经口LD50大于5000mg／kg,经皮LD50大于2000mg／kg。家兔皮肤刺激试验阴性,轻度眼刺激性和弱致敏性。Ames试验,微核试验及小鼠睾丸初级精母细胞染色体畸变试验结果均为阴性。结论 噻吩磺隆属低毒性农药,在本实验条件下无致突变作用。     

Safety and toxicological evaluation of a novel niacin-bound chromium (III) complex

Chromium is an essential trace element required for normal protein, fat and carbohydrate metabolism. It also helps in energy production and increasing lean body mass. Niacin-bound chromium (NBC) is a unique form of bioavailable chromium that promotes healthy lipid profile. This study was focused on determining the broad spectrum safety of NBC. Acute oral, acute dermal, primary dermal irritation and primary eye irritation toxicities of NBC were evaluated. Ames bacterial reverse mutation assay, mouse lymphoma test and a dose-dependent 90-day subchronic toxicity were also conducted. In safety studies, the acute oral LD(50) of NBC was found to be greater then 5000 mg/kg in both male and female Sprague-Dawley rats. No changes in body weight or adverse effects were observed following necropsy. The acute dermal LD(50) of NBC was found to be >2000 mg/kg. The primary skin irritation test was conducted with NBC on New Zealand Albino rabbits. NBC was classified as slightly irritating. The primary eye irritation test was conducted with NBC on rabbits. NBC was classified as practically non-irritating to the eye. NBC did not induce mutagenic effects in the bacterial reverse mutation test in five Salmonella typhimurium strains (TA1535, TA98, TA100, TA97a and TA102), either with or without metabolic activation. Similarly, NBC did not induce mutagenic effects in the mammalian cell gene mutation test in L5178Y mouse lymphoma cells TK (+/-), either with or without metabolic activation. A dose-dependent 90-day subchronic toxicity study demonstrated no significant changes in selected organ weights individually and as percentages of body and brain weights. NBC supplementation did not cause changes in hepatic lipid peroxidation or DNA fragmentation after 30, 60 or 90 days of treatment. Hematology, clinical chemistry and histopathological evaluations did not show any adverse effects in all organs tested. Taken together, the above results indicate a broad spectrum of safety for NBC.     

Acute and sub-acute toxicity of an insect pheromone, N-heneicosane and combination with insect growth regulator, diflubenzuron, for establishing no observed adverse effect level (NOAEL)

Aedes aegypti mosquito is one of the most notorious vectors of dangerous diseases like dengue hemorrhagic fever and chikangunya. One method of control of the vectors is by the use of semiochemicals or pheromones. The pheromone n-heneicosane (C21) has been proved to be effective in attracting the female Aedes aegypti to lay eggs in the treated water and the growth of the larva is controlled by insect growth regulator diflubenzuron (DB). This study was planned to assess the safety of C21 alone and the combination with DB. Acute toxicity tests were carried out using two doses, viz., 1600 and 3200 mg/kg and two routes of exposure oral and intra-peritoneal. Dermal toxicity test was carried out in both male and female rats at the dose of 3200 mg/kg. Primary skin irritation test was carried out in rabbits. Sub-acute (90 days) dermal toxicity studies in male and female rats at the dose of 1 and 2 mg/kg via the per-cutaneous route were also studied. Sub-acute (90 days) toxicity test through the oral route was carried out, at doses 125, 250 and 500 mg/kg in male and female rats. The calculated LD50 by ip route and dermal route was more than 5 g/kg in mouse and rats of both the sexes. In the primary skin irritation test no significant changes were noted. In the sub-acute toxicity studies even 500 mg/kg dose was not able to produce toxic response in rats when they were dosed daily for 90 days. The established no observed adverse effect level (NOAEL) was more than 500 mg/kg.     

Molecular docking studies,biological and toxicity evaluation of dihydroisoquinoline derivatives as potential anticancer agents

We report a study of a series of isoquinoline derivatives, including their synthesis, in vitro microsomal leucine aminopeptidase (LAP) inhibition and antiproliferative activity on cancer cell lines. Among fourteen tested compounds, one (compound 3b) was determined to have good activity against LAP and significant antiproliferative activity against HL-60 human promyelocytic leukemia, Burkitt’s lymphoma Raji, camptothecin resistant CEM/C2 leukemia cells with mutated catalytic site of topoisomerase I, its parental cell line CCRF/CEM and LoVo colon cancer. Its influence on the cell cycle was also observed. Moreover, we have confirmed that antiproliferative activity towards cancer cells is due to LAP inhibition. Docking simulation based on positioning compound 3b into the LAP active site was performed to explore the possible binding mode. The compound was able to form hydrogen bonds with Gly362 and coordinate zinc ions, which was previously suggested to be essential for inhibitory activity. Compound 3b was also characterized with a good selectivity index for cancer versus normal mammalian cells. Toxicological studies involving examination of skin sensitization, acute skin irritation/corrosion, acute dermal toxicity, acute oral toxicity and acute eye irritation/corrosion established that compound 3b is safe for use.     

Efficacy and safety of a new vaginal contraceptive antimicrobial formulation containing high molecular weight poly(sodium 4-styrenesulfonate)

Host cell infection by sexually transmitted disease (STD)-causing microbes and fertilization by spermatozoa may have some mechanisms in common. If so, certain noncytotoxic agents could inhibit the functional activity of both organisms. High molecular mass poly(sodium 4-styrenesulfonate) (T-PSS) may be one of these compounds. T-PSS alone (1 mg/ml) or in a gel (2% or 5% T-PSS) completely prevented conception in the rabbit. Contraception was not due to sperm cytotoxicity or to an effect on sperm migration. However, T-PSS inhibited sperm hyaluronidase (IC(50) = 5.3 microg/ml) and acrosin (IC(50) = 0.3 microg/ml) and caused the loss of acrosomes from spermatozoa (85% maximal loss by 0.5 microg/ml). T-PSS (5% in gel) also reduced sperm penetration into bovine cervical mucus (73% inhibition by 1 mg gel/ml). T-PSS (5% in gel) inhibited human immunodeficiency virus (HIV; IC(50)= 16 microg gel/ml) and herpes simplex viruses (HSV-1 and HSV-2; IC(50) = 1.3 and 1.0 microg gel/ml, respectively). The drug showed high efficacy against a number of clinical isolates and laboratory strains. T-PSS (5% in gel) also inhibited Neisseria gonorrhea (IC(50) < 1.0 gel/ml) and Chlamydia trachomatis (IC(50) = 1.2 microg gel/ml) but had no effect on lactobacilli. These results imply that T-PSS is an effective functional inhibitor of both spermatozoa and certain STD-causing microbes. The noncytotoxic nature should make T-PSS safe for vaginal use. T-PSS was nonmutagenic in vitro and possessed an acute oral toxicity of >5 g/kg (rat). Gel with 10% T-PSS did not irritate the skin or penile mucosa (rabbit) and caused no dermal sensitization (guinea pig). Vaginal administration of the 5% T-PSS gel to the rabbit for 14 consecutive days caused no systemic toxicity and only mild (acceptable) vaginal irritation. T-PSS in gel form is worthy of clinical evaluation as a vaginal contraceptive HIV/STD preventative.     

Efficacy and safety of catnip (Nepeta cataria) as a novel filth fly repellent*

Catnip (Nepeta cataria) is known for its pseudo‐narcotic effects on cats. Recently, it has been reported as an effective mosquito repellent against several Aedes and Culex species, both topically and spatially. Our laboratory bioassays showed that catnip essential oil (at a dosage of 20 mg) resulted in average repellency rates of 96% against stable flies, Stomoxys calcitrans (L.) and 79% against houseflies, Musca domestica (L.), respectively. This finding suggested that the application of repellent could be used as part of filth fly management. Further evaluations of catnip oil toxicity were conducted to provide a broad‐spectrum safety profile of catnip oil use as a potential biting and nuisance insect repellent in urban settings. Acute oral, dermal, inhalation, primary dermal and eye irritation toxicity tests were performed. The acute oral LD₅₀ of catnip oil was found to be 3160 mg/kg body weight (BW) and 2710 mg/kg BW in female and male rats, respectively. The acute dermal LD₅₀ was > 5000 mg/kg BW. The acute inhalation LD₅₀ was observed to be > 10 000 mg/m³. Primary skin irritation tested on New Zealand white rabbits showed that catnip oil is a moderate irritant. Catnip oil was classified as practically non‐irritating to the eye. In comparison with other U.S. Environmental Protection Agency‐approved mosquito repellents (DEET, picaridin and p‐menthane‐3,8‐diol), catnip oil can be considered as a relatively safe repellent, which may cause minor skin irritation.