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find Keyword "药物毒性" 5 results
  • 心内直视手术中鱼精蛋白毒性反应的发生及处理

    目的 分析心内直视手术中鱼精蛋白毒性反应发生情况、临床特点,探讨处理措施。 方法 2001年1月~2006年1月,连续行1 163例心内直视手术中发生鱼精蛋白毒性反应31例,其中轻度反应(血压下降lt;30mmHg)26例,中度、重度反应(中度反应血压下降30~49mmHg,重度反应血压下降≥50mmHg)5例;低血压型28例,过敏反应/类过敏反应型2例,肺血管收缩型1例。所有患者均给予立即停止使用鱼精蛋白或减慢鱼精蛋白泵入速度、补充血容量、抗过敏、血管活性药物或再次体外循环治疗。 结果 26例出现轻度鱼精蛋白毒性反应者经停止使用或减慢鱼精蛋白泵入速度及相应治疗后,均很快好转;5例出现中度、重度鱼精蛋白毒性反应者,经停止使用鱼精蛋白、抗过敏、补充血容量、血管活性药物和再次体外循环支持, 4例好转,1例死亡。27例门诊随访3个月,恢复正常学习和工作。 结论 心内直视手术中鱼精蛋白毒性反应发生率高,中度、重度反应者死亡率高。鱼精蛋白毒性反应的发生与其用量和使用方法密切有关,充分认识鱼精蛋白毒性反应的临床特点,精确鱼精蛋白用量和改进使用方法能在一定程度上防治毒性反应的发生。

    Release date:2016-08-30 06:15 Export PDF Favorites Scan
  • Experimental tests of ophthalmic drugs and related issues

    Release date:2016-09-02 05:46 Export PDF Favorites Scan
  • 氯喹中毒性眼部损害一例

    Release date:2021-07-21 02:11 Export PDF Favorites Scan
  • Retinal toxicity study of different-dose intravitreal ganciclovir in albino rabbit

    ObjectiveTo explore safe dosage of single intravitreal injection of ganciclovir (IVG) in healthy rabit eyes, and to explore retinal toxicity of different dosage of ganciclovir after continues intravitreal injection into the vitreous cavity of healthy albino rabbit eyes. MethodsTen healthy New Zealand albino rabbits were divided into 5 groups with 2 rabbits in each group. Each group was injected with 1 mg/0.025 ml, 2 mg/0.025 ml, 5 mg/0.025 ml, 10 mg/0.025 ml ganciclovir or 0.025 ml saline (control group). After 1 week of intervention, rabbits were examined by ultra-wide-angle fundus photography, optical coherence tomography (OCT) and full field electroretinogram (ERG). The maximum mixed response of rod and cone cells (Max-R) was measured under dark adaption conditions, cone response (Cone-R) and 30 Hz flicker response (30 Hz-R) were measured under light adaption conditions. Twenty-four healthy New Zealand albino rabbits were randomly divided into a low-dose experimental group, a low-dose control group, a high-dose experimental group, and a high-dose control group, with 6 rabbits in each group, with the right eye as the experimental eye. The rabbits in the high-dose experimental group were continuously injected with ganciclovir 2 mg/0.025 ml, once a week, for a total of 4 times. The rabbits in the low-dose experimental group were injected with 1 mg/0.025 ml ganciclovir, the induction period was 2 times/week, a total of 4 times; the maintenance period was 1 time/week, a total of 2 times. The rabbits in the high-dose control group and the low-dose control group were injected with 0.025 ml normal saline into the vitreous cavity respectively. Full-field ERG examination was performed 1 day before each injection and 1 week after the last injection. Max-R was measured under dark-adapted conditions, and Cone-R and 30 Hz-R were measured under light-adapted conditions. OCT was recorded before the first injection and one week after the last injection. One week after the last injection, the experimental rabbits in each group were sacrificed for hematoxylin-eosin staining, and the retinal structure was observed under a light microscope. The comparison of a-wave and b-wave amplitude of Max-R, Cone-R and 30 Hz-R amplitude at different time was performed by two independent sample nonparametric test. ResultsThere were no abnormal results of fundus photography, OCT and ERG after single intravitral injection of 1 mg or 2 mg ganciclovir. One week after single 5 mg IVG, fundus photography of rabbits showed vascular occlusion and preretinal hemorrhage and ERG showed slight decrease of amplitude of Max-R, Cone-R and 30 Hz-R. One week after single 10 mg IVG, retinal necrosis and exudative changes were also observed. OCT showed edema and unclear retinal structure in the necrotic area. ERG showed significant decrease of amplitude of Max-R, Cone-R and 30 Hz-R. After continuous IVG in high dose and low-dose experimental group, the amplitude of Max-R a wave (Z=-0.160, 0.000) and b wave (Z=-0.321, 0.000), Cone-R a wave (Z=-0.641,-0.641) and b wave (Z=-0.321, -0.160), and 30 Hz-R (Z=-0.321,-0.160) showed no difference compared to control group. No histologic evidences of retinal microstructure abnormalities were found in both groups. OCT and fundus photography before and after the intervention did not show any difference, either. ConclusionThere was no retinal toxicity of continuous 1 mg or 2 mg IVG recorded in albino rabbits.

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  • Research progress of hydroxychloroquine retinopathy

    Hydroxychloroquine is widely used in a variety of autoimmune diseases. However, long-term use of hydroxychloroquine can cause severe retinopathy, which has a complex pathogenic mechanism and diverse clinical manifestations, mainly manifested as photoreceptor and retinal pigment epithelial damage and irreversible vision loss. Identifying damage before retinitis pigment epithelium lesions preserve central vision, so early detection is crucial to slow disease progression and reduce vision loss. The development of multimodal imaging technology and the issuance of the latest treatment guidelines provide a powerful tool for the early screening and treatment of hydroxychloroquine retinopathy. Proficient in the latest guidelines for the treatment of hydroxychloroquine can better guide clinicians to do a good job in disease screening and management, recommend risks, safe dosages and appropriate screening procedures to patients and strengthen the prevention of hydroxychloroquine retinopathy, which will help save the vision of more patients and reduce the waste of medical resources.

    Release date:2023-06-16 05:21 Export PDF Favorites Scan
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