Das Biswadeep, Sarkar Chayna, Schachter Jeffrey
Department of Pharmacology, Division of Pathology, School of Medicine, International Medical University (IMU), No. 126, Jalan Jalil Perkasa 19, Bukit Jalil, 57000 Kuala Lumpur, Malaysia.
Pak J Pharm Sci. 2013 Sep;26(5):1045-55.
Natural glycopeptide antibiotics like vancomycin and teicoplanin have played a significant role in countering the threat posed by Gram-positive bacterial infections. The emergence of resistance to glycopeptides among enterococci and staphylococci has prompted the search for second-generation drugs of this class and semi-synthetic derivatives are currently under clinical trials. Antimicrobial resistance among Gram-positive organisms has been increasing steadily during the past several decades and the current development of antibiotics falls short of meeting the needs. Oritavancin (LY-333328 diphosphate), a promising novel second-generation semisynthetic lipoglycopeptide, has a mechanism of action similar to that of other glycopeptides. It has concentration-dependent activity against a variety of Gram-positive organisms specially methicillin-resistant Staphylococcus aureus (MRSA), vancomycin-intermediate resistant Staphylococcus aureus (VISA), Streptococcus pneumoniae and vancomycin-resistant enterococcus. It is rapidly bactericidal against many species and in particular for enterococci where vancomycin and teicoplanin are only bacteriostatic even against susceptible strains. The pharmacokinetic profile of oritavancin has not been fully described; however, oritavancin has a long half-life of about 195.4 hours and is slowly eliminated by renal means. Oritavancin is not metabolized by the liver in animals. Oritavancin will most probably be prescribed as a once-daily dose and it demonstrates concentration-dependent bactericidal activity. Oritavancin has demonstrated preliminary safety and efficacy in Phase I and II clinical trials. In a Phase III clinical trial, oritavancin has achieved the primary efficacy end point in the treatment of complicated Gram-positive skin and skin-structure infections. To date, adverse events have been mild and limited; the most common being administration site complaints, headache, rhinitis, dry skin, pain, increases in liver transaminases and accumulation of free cholesterol and phospholipids in phagocytic (macrophages) and nonphagocytic (fibroblast) cells. Oritavancin appears to be a promising antimicrobial alternative to vancomycin (with additional activity against Staphylococcus and Enterococcus resistant to vancomycin) for the treatment of complicated Gram-positive skin and skin-structure infections. Additional clinical data are required to fully explore its use.
像万古霉素和替考拉宁这样的天然糖肽类抗生素在应对革兰氏阳性菌感染所带来的威胁方面发挥了重要作用。肠球菌和葡萄球菌中对糖肽类抗生素耐药性的出现促使人们寻找此类第二代药物,目前半合成衍生物正处于临床试验阶段。在过去几十年中,革兰氏阳性菌中的抗菌耐药性一直在稳步上升,而目前抗生素的研发无法满足需求。奥利万星(LY - 333328二磷酸盐)是一种有前景的新型第二代半合成脂糖肽,其作用机制与其他糖肽类抗生素相似。它对多种革兰氏阳性菌具有浓度依赖性活性,特别是对耐甲氧西林金黄色葡萄球菌(MRSA)、万古霉素中介耐药金黄色葡萄球菌(VISA)、肺炎链球菌和耐万古霉素肠球菌。它对许多菌种具有快速杀菌作用,尤其是对肠球菌,而万古霉素和替考拉宁即使对敏感菌株也仅具有抑菌作用。奥利万星的药代动力学特征尚未完全阐明;然而,奥利万星的半衰期约为195.4小时,且通过肾脏途径缓慢消除。在动物体内,奥利万星不会被肝脏代谢。奥利万星很可能会被规定为每日一次给药,并且它表现出浓度依赖性杀菌活性。奥利万星在I期和II期临床试验中已证明了初步的安全性和有效性。在一项III期临床试验中,奥利万星在治疗复杂性革兰氏阳性皮肤及皮肤结构感染方面达到了主要疗效终点。迄今为止,不良事件轻微且有限;最常见的是给药部位不适、头痛、鼻炎、皮肤干燥、疼痛、肝转氨酶升高以及吞噬细胞(巨噬细胞)和非吞噬细胞(成纤维细胞)中游离胆固醇和磷脂的蓄积。对于治疗复杂性革兰氏阳性皮肤及皮肤结构感染,奥利万星似乎是一种有前景的替代万古霉素的抗菌药物(对耐万古霉素的葡萄球菌和肠球菌具有额外活性)。需要更多临床数据来全面探索其用途。
