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李斯特菌病的管理

Management of listeriosis.

作者信息

Hof H, Nichterlein T, Kretschmar M

机构信息

Institute of Medical Microbiology and Hygiene, Faculty of Clinical Medicine Mannheim, University of Heidelberg, Germany.

出版信息

Clin Microbiol Rev. 1997 Apr;10(2):345-57. doi: 10.1128/CMR.10.2.345.

Abstract

Determination of the MIC in vitro is often used as the basis for predicting the clinical efficacy of antibiotics. Listeriae are uniformly susceptible in vitro to most common antibiotics except cephalosporins and fosfomycin. However, the clinical outcome is poor. This is partially because listeriae are refractory to the bactericidal mechanisms of many antibiotics, especially to ampicillin-amoxicillin, which still is regarded as the drug of choice. A true synergism can be achieved by adding gentamicin. Another point is that listeriae are able to reside and multiply within host cells, e.g., macrophages, hepatocytes, and neurons, where they are protected from antibiotics in the extracellular fluid. Only a few agents penetrate, accumulate, and reach the cytosol of host cells, where the listeriae are found. Furthermore, certain host cells may exclude antibiotics from any intracellular compartment. Thus, determination of the antibacterial efficacy of a drug against listeriae in cell cultures may be a better approximation of potential therapeutic value. Certain host cells may have acquired the property of excluding certain antibiotics, for example macrolides, from intracellular spaces, which might explain therapeutic failures of antibiotic therapy in spite of low MICs. Animal models do not completely imitate human listeriosis, which is characterized by meningitis, encephalitis, soft tissue and parenchymal infections, and bacteremia. Meningitis produced in rabbits is a hyperacute disease, whereby most listeriae lie extracellularly, fairly accessible to antibiotics that can cross the blood-cerebrospinal fluid barrier. In the murine model of systemic infection, Listeria monocytogenes is located mainly within macrophages and parenchymal cells of the spleen and liver, hardly accessible to certain drugs, such as ampicillin and gentimicin. The therapeutic efficacy of drugs clearly depends on the model used. Thus, for example, the combination of ampicillin with gentamicin acts synergistically in the rabbit meningitis model but not in the mouse model. Since conventional antimicrobial therapy with antibiotics is not satisfactory, particularly in the immunocompromised host (about 30% of patients with listeriosis die in spite of a rational choice of antibiotics), other possibilities must be considered for therapy as well as prevention. Indeed, listeriae are highly susceptible to several endogenous antibiotics, such as defensins. Bacteriocins produced by related bacterial species, e.g., lactobacilli and enterococci, are rapidly bactericidal. However, unfortunately, the use of such alternative measures along with immunization and immunmodulation is not yet feasible.

摘要

体外最低抑菌浓度(MIC)的测定常被用作预测抗生素临床疗效的依据。李斯特菌在体外对除头孢菌素和磷霉素之外的大多数常用抗生素均敏感。然而,临床治疗效果却不佳。部分原因在于李斯特菌对许多抗生素的杀菌机制具有抗性,尤其是对仍被视为首选药物的氨苄西林 - 阿莫西林。添加庆大霉素可实现真正的协同作用。另一点是,李斯特菌能够在宿主细胞(如巨噬细胞、肝细胞和神经元)内生存和繁殖,在这些细胞内它们受到细胞外液中抗生素的保护。只有少数药物能够穿透、蓄积并到达发现李斯特菌的宿主细胞胞质溶胶。此外,某些宿主细胞可能会将抗生素排除在任何细胞内区室之外。因此,在细胞培养中测定药物对李斯特菌的抗菌效果可能更能近似潜在的治疗价值。某些宿主细胞可能获得了将某些抗生素(如大环内酯类)排除在细胞内空间之外的特性,这或许可以解释尽管最低抑菌浓度较低但抗生素治疗仍出现失败的情况。动物模型并不能完全模拟人类李斯特菌病,人类李斯特菌病的特征为脑膜炎、脑炎、软组织和实质感染以及菌血症。兔子身上诱发的脑膜炎是一种超急性疾病,其中大多数李斯特菌位于细胞外,能够穿过血脑屏障的抗生素相当容易作用于它们。在系统性感染的小鼠模型中,单核细胞增生李斯特菌主要位于脾脏和肝脏的巨噬细胞和实质细胞内,某些药物(如氨苄西林和庆大霉素)很难作用于它们。药物的治疗效果显然取决于所使用的模型。例如,氨苄西林与庆大霉素的组合在兔子脑膜炎模型中具有协同作用,但在小鼠模型中则不然。由于使用抗生素进行的传统抗菌治疗并不令人满意,尤其是在免疫功能低下的宿主中(约30%的李斯特菌病患者尽管合理选择了抗生素仍死亡),因此必须考虑其他治疗和预防的可能性。实际上,李斯特菌对几种内源性抗生素(如防御素)高度敏感。相关细菌物种(如乳酸杆菌和肠球菌)产生的细菌素具有快速杀菌作用。然而,不幸的是,将此类替代措施与免疫和免疫调节一起使用目前尚不可行。

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