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加速老化后粘合剂对汽车坐垫革顶层涂饰性能的影响
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作者 Ibrahim Eryazici Bradley Hageman +3 位作者 Joseph Hoefler Edwin Nungesser richard rosen 李瑞(译) 《中国皮革》 CAS 2018年第8期29-35,共7页
在购买新车过程中,皮革座椅的选择被视为一种不能用低价替代品代替的高端选择。为了保持优质地位.对皮革座椅的舒适性、关观性和耐久性寄予了较高的期望。陶氏化学公司开发了一种丙烯酸类顶层粘合剂。当其与传统的聚氨酯分散液(PUD... 在购买新车过程中,皮革座椅的选择被视为一种不能用低价替代品代替的高端选择。为了保持优质地位.对皮革座椅的舒适性、关观性和耐久性寄予了较高的期望。陶氏化学公司开发了一种丙烯酸类顶层粘合剂。当其与传统的聚氨酯分散液(PUD)粘合剂结合使用时可以显示优良性能。然而,当前顶层涂层的座椅材料在经受一系列加速老化条件处理后不能保持其性能要求。本文对比了全成品汽车装饰用皮革在经过一系列加速老化条件(热、水解和几种氙灯老化)下性能的变化情况。对较宽范围内的PUD化学成分以及化学反应的类型进行考察,判断丙烯酸类顶层粘合剂和每一种材料混合用作标准家具革筛选配方所产生的影响。对每种加速老化条件处理前后的样品进行颜色、光泽和耐折性的评估。分析数据表明:使用石英过滤器的氙孤方法处理的样品其性能最低,且测试时间与性能成比例下降。同样地.一种类似于氙弧方法处理但借助辅助灯和过滤器等设备的处理结果表明其可导致相同的破坏,但此结果需要相当长的时间处理后才可获得。置于水解和干热条件下样品产生的变化最小。这些数据也证明可以根据不同的老化条件选择PUD粘合剂。不考虑某一特殊类别PUD粘合剂的优点和缺点,PUD-丙烯酸类粘合剂的调节效果较强。这表明当2种化学品一同用于皮革家具顶层涂饰时,在加速老化条件处理后可以产生协同效应。 展开更多
关键词 加速老化 涂饰性能 汽车坐垫革 粘合剂 顶层 丙烯酸类 陶氏化学公司 PUD
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Beta-adrenergic agonist protects retinal pigment epithelium against hydroxycholoroquine toxicity via c AMP-PKA signal pathway
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作者 Ruihua Zhang Dan-Ning Hu richard rosen 《International Journal of Ophthalmology(English edition)》 SCIE CAS 2020年第4期552-559,共8页
AIM: To test our hypothesis that activation of protein kinase A(PKA) signal pathway by β-adrenergic agonist plays an important role in the protecting of cultured retinal pigment epithelial(RPE) cells against the hydr... AIM: To test our hypothesis that activation of protein kinase A(PKA) signal pathway by β-adrenergic agonist plays an important role in the protecting of cultured retinal pigment epithelial(RPE) cells against the hydroxychloroquine(HCQ) toxicity. METHODS: Cultured human RPE cells were treated with 1) HCQ, 2) HCQ with salbutamol(a β2-adrenergic receptor agonist), and 3) HCQ with salbutamol and a PKA inhibitor, and compared these to 4) untreated cells(controls). After treated for 24 h, cell vacuolation, cells viability, PKA and PKA kinase activity levels were determined by the measurement of the size of vacuoles using Image J software, the cell counting with a dye-exclusion testing, Western blot and PKA kinase detection, respectively. RESULTS: Cell vacuolation and cell death of cultured RPE cells were significantly increased by the treatment of HCQ. Salbutamol significantly elevated PKA and PKA activity levels and this was associated with the inhibition of the vacuolation and cell death. The PKA inhibitor significantly decreased the PKA levels and eliminated the protective effects of salbutamol on HCQ-treated RPE cells. CONCLUSION: The PKA pathway plays an important role in the protective effects of β2-adrenergic agonist on the RPE cells against HCQ toxicity. These findings reveal a novel potential strategy against HCQ retinopathy by treatment with PKA activating medications. 展开更多
关键词 hydroxycholoroquine retinal PIGMENT EPITHELIAL cells RETINOPATHY protein kinase A VACUOLATION
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