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Hintonia latiflora 甲醇树皮提取物在致死性约氏疟原虫小鼠疟疾模型中的抗疟疗效、细胞毒性和遗传毒性。

Antimalarial efficacy, cytotoxicity, and genotoxicity of methanolic stem bark extract from Hintonia latiflora in a Plasmodium yoelii yoelii lethal murine malaria model.

机构信息

Laboratorio de Malariología, Departamento de Microbiología y Parasitología, Facultad de Medicina, Universidad Nacional Autónoma de México, México, DF, 04510, Mexico,

出版信息

Parasitol Res. 2014 Apr;113(4):1529-36. doi: 10.1007/s00436-014-3797-9. Epub 2014 Feb 19.

DOI:10.1007/s00436-014-3797-9
PMID:24549754
Abstract

Traditional medicines have been used to treat malaria for thousands of years and are the source of artemisinin and quinine derivatives. With the increasing levels of drug resistance, the high cost of artemisisnin-based combination therapies, and fake antimalarials drugs, traditional medicine have become an important and sustainable source of malaria treatment. For the benefit of those who use traditional medicine to treat malaria, there is an urgent need to study the efficacy and toxicity of herbal remedies. Hintonia latiflora stem bark infusions are use in Mexican traditional medicine to treat malaria, diabetes, and gastrointestinal diseases. Its efficacy in the treatment of complicated malaria and its ability to generate DNA damage to the host is not fully evaluated. In our search for antimalarial natural products, in the present study, we tested the efficacy of H. latiflora stem bark methanolic extract (HlMeOHe) in CD1 male mice infected with lethal Plasmodium yoelii yoelii and its in vivo cytotoxicity and genotoxicity. To assess the antimalarial activity, the extract was evaluated in a 4-day test scheme in oral doses of 1,200, 600, and 300 mg/kg prior acute toxicity test; oral chloroquine (15 mg/kg) was used as positive control. The ability of 1,200 mg/kg of HlMeOHe to induce cytotoxicity and DNA damage in the peripheral blood of mice was assessed using a fluorochrome-mediated viability test and the micronucleus (MN) assay; N-ethyl-N-nitrosourea (ENU) was used as a positive control. HlMeOHe median acute toxicity (LD₅₀) was 2,783.71 mg/kg and LD10 was 1,293.76 mg/kg (taken as the highest work dose). Plasmodium yoelii yoelii-infected mice in the untreated control group died between 6 and 7 days post-infection (PI) with parasitemia over 70%. Even though mice treated with 600 and 300 mg/kg showed a chemosuppression percentage of total parasitemia of 99.23 and 23.66, respectively, animals in both groups died 6 to 7 days PI with parasitemia over 45%. A 4-day dosage of 1,200 mg/kg of the extract showed, in the P. yoelii yoelii-infected mice, a 100% chemosuppression of total parasitemia on 5 days PI and a 23 days survival time with a mean parasitemia of 23.6% at the date of death. Only mice treated with chloroquine survived until the end of the experiment. Cell viability was not affected. The average number of micronuclei in the treated mice increased significantly (P < 0.05) to 4.8 MN when compared with the untreated control group (0.9 MN). The results obtained in this study showed that the infection outcome of P. yoelii yoelii-infected mice is affected by HlMeOHe. Although a concentration of 1,200 mg/kg of HlMeOHe is suitable to use in the treatment of malaria fever, slowed down the parasite replication, retarded the patency time, and increased the infected P. yoelii yoelii mice survival time, its chemical composition should be studied in detail in order to reduce its genotoxic potential.

摘要

传统医学已经使用了几千年,用来治疗疟疾,并且是青蒿素和奎宁衍生物的来源。随着耐药性水平的提高,青蒿素为基础的联合疗法的高成本,以及假冒的抗疟药物,传统医学已经成为治疗疟疾的重要和可持续的来源。为了使那些使用传统医学治疗疟疾的人受益,迫切需要研究草药的疗效和毒性。墨西哥传统医学中使用宽叶缬草茎皮浸剂来治疗疟疾、糖尿病和胃肠道疾病。其治疗复杂疟疾的疗效及其对宿主产生 DNA 损伤的能力尚未得到充分评估。在我们寻找抗疟天然产物的过程中,在本研究中,我们测试了宽叶缬草茎皮甲醇提取物(HlMeOHe)在感染致死性约氏疟原虫的 CD1 雄性小鼠中的疗效,以及其在体内的细胞毒性和遗传毒性。为了评估抗疟活性,在急性毒性试验之前,用 1,200、600 和 300 mg/kg 的口服剂量评估提取物在为期 4 天的试验方案中的疗效;口服氯喹(15 mg/kg)作为阳性对照。使用荧光染料介导的活力试验和微核(MN)试验评估 1,200 mg/kg 的 HlMeOHe 对小鼠外周血中诱导细胞毒性和 DNA 损伤的能力;N-乙基-N-亚硝脲(ENU)用作阳性对照。HlMeOHe 的中位急性毒性(LD₅₀)为 2,783.71mg/kg,LD10 为 1,293.76mg/kg(视为最高工作剂量)。未治疗的对照组感染约氏疟原虫的小鼠在感染后 6 至 7 天内死亡,寄生虫血症超过 70%。尽管 600 和 300 mg/kg 剂量的药物治疗组总寄生虫血症的化学抑制率分别为 99.23%和 23.66%,但两组动物均在感染后 6 至 7 天死亡,寄生虫血症超过 45%。在感染约氏疟原虫的小鼠中,用 1,200 mg/kg 的提取物进行为期 4 天的剂量治疗,在第 5 天寄生虫血症完全抑制,寄生虫血症为 23.6%时,存活时间为 23 天,在死亡日的平均寄生虫血症为 23.6%。只有接受氯喹治疗的小鼠存活到实验结束。细胞活力没有受到影响。与未处理的对照组(0.9 MN)相比,处理组的微核数平均增加了 4.8 MN(P<0.05)。本研究的结果表明,HlMeOHe 影响约氏疟原虫感染小鼠的感染结果。尽管 1,200mg/kg 的 HlMeOHe 浓度适合治疗疟疾发热,但它能减缓寄生虫的复制速度,延长潜伏时间,增加感染约氏疟原虫的小鼠的存活时间,但应详细研究其化学成分,以降低其遗传毒性。

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