Nurul Aiezzah Z, Noor E, Hasidah M S
School of Biosciences and Biotechnology, Faculty of Science and Technology, Universiti Kebangsaan Malaysia, 43600 UKM Bangi, Selangor.
Trop Biomed. 2010 Dec;27(3):624-31.
Malaria, caused by the Plasmodium parasite is still a health problem worldwide due to resistance of the pathogen to current anti-malarials. The search for new anti-malarial agents has become more crucial with the emergence of chloroquine-resistant Plasmodium falciparum strains. Protein kinases such as mitogen-activated protein kinase (MAPK), MAPK kinase, cyclin-dependent kinase (CDK) and glycogen synthase kinase- 3(GSK-3) of parasitic protozoa are potential drug targets. GSK-3 is an enzyme that plays a vital role in multiple cellular processes, and has been linked to pathogenesis of several diseases such as type II diabetes and Alzheimer's disease. In the present study, the antiplasmodial property of LiCl, a known GSK-3 inhibitor, was evaluated in vivo for its antimalarial effect against mice infected with Plasmodium berghei. Infected ICR mice were intraperitoneally administered with LiCl for four consecutive days before (prophylactic test) and after (suppressive test) inoculation of P. berghei-parasitised erythrocytes. Results from the suppressive test (post-infection LiCl treatment) showed inhibition of erythrocytic parasitemia development by 62.06%, 85.67% and 85.18% as compared to nontreated controls for the 100 mg/kg, 300 mg/kg and 600 mg/kg dosages respectively. Both 300 mg/kg and 600 mg/kg LiCl showed similar significant (P<0.05) suppressive values to that obtained with chloroquine-treated mice (86% suppression). The prophylactic test indicated a significantly (P<0.05) high protective effect on mice pre-treated with LiCl with suppression levels relatively comparable to chloroquine (84.07% and 86.26% suppression for the 300 mg/kg and 600 mg/kg LiCl dosages respectively versus 92.86% suppression by chloroquine). In both the suppressive and prophylactic tests, LiCl-treated animals survived longer than their non-treated counterparts. Mortality of the non-treated mice was 100% within 6 to 7 days of parasite inoculation whereas mice administered with LiCl survived beyond 9 days. Healthy non-infected mice administered with 600 mg/ kg LiCl for four consecutive days also showed decreased mortality compared to animals receiving lower doses of LiCl; three of the seven mice intraperitoneally injected with the former dose of LiCl did not survive more than 24 h after administration of LiCl whereas animals given the lower LiCl doses survived beyond four days of LiCl administration. To date, no direct evidence of anti-malarial activity in vivo or in vitro has been reported for LiCl. Evidence of anti-plasmodial activity of lithium in a mouse infection model is presented in this study.
由疟原虫寄生虫引起的疟疾仍然是一个全球性的健康问题,因为该病原体对目前的抗疟疾药物产生了耐药性。随着耐氯喹恶性疟原虫菌株的出现,寻找新的抗疟疾药物变得更加关键。寄生原生动物的蛋白激酶,如丝裂原活化蛋白激酶(MAPK)、MAPK激酶、细胞周期蛋白依赖性激酶(CDK)和糖原合酶激酶-3(GSK-3)是潜在的药物靶点。GSK-3是一种在多种细胞过程中起关键作用的酶,并且与II型糖尿病和阿尔茨海默病等几种疾病的发病机制有关。在本研究中,对已知的GSK-3抑制剂LiCl的抗疟特性进行了体内评估,以观察其对感染伯氏疟原虫的小鼠的抗疟效果。在接种伯氏疟原虫寄生的红细胞之前(预防性试验)和之后(抑制性试验),对感染的ICR小鼠连续四天腹腔注射LiCl。抑制性试验(感染后LiCl治疗)的结果显示,与未治疗的对照组相比,100mg/kg、300mg/kg和600mg/kg剂量的LiCl分别使红细胞内疟原虫血症的发展受到62.06%、85.67%和85.18%的抑制。300mg/kg和600mg/kg的LiCl显示出与氯喹治疗的小鼠相似的显著(P<0.05)抑制值(86%的抑制率)。预防性试验表明,用LiCl预处理的小鼠具有显著(P<0.05)的高保护作用,其抑制水平与氯喹相对相当(300mg/kg和600mg/kg LiCl剂量的抑制率分别为84.07%和86.26%,而氯喹的抑制率为92.86%)。在抑制性试验和预防性试验中,用LiCl治疗的动物比未治疗的动物存活时间更长。未治疗的小鼠在接种寄生虫后的6至7天内死亡率为100%,而注射LiCl的小鼠存活超过9天。连续四天腹腔注射600mg/kg LiCl的健康未感染小鼠与接受较低剂量LiCl的动物相比,死亡率也有所降低;腹腔注射前一剂量LiCl的七只小鼠中有三只在注射LiCl后24小时内死亡,而给予较低LiCl剂量的动物在注射LiCl四天后仍存活。迄今为止,尚未有关于LiCl体内或体外抗疟活性的直接证据报道。本研究提供了锂在小鼠感染模型中的抗疟活性证据。
