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J Exp Med. 1948 Jul;88(1):99-131. doi: 10.1084/jem.88.1.99.
2
PERSISTENCE OF STAPHYLOCOCCUS AUREUS IN PENICILLIN IN VITRO.金黄色葡萄球菌在青霉素体外环境中的持续性
J Gen Microbiol. 1964 May;35:335-49. doi: 10.1099/00221287-35-2-335.
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Minimum fungicidal concentrations of amphotericin B for bloodstream Candida species.两性霉素B对血流感染念珠菌属的最低杀菌浓度
Diagn Microbiol Infect Dis. 2003 Mar;45(3):203-6. doi: 10.1016/s0732-8893(02)00525-4.
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In vivo pharmacodynamics of antifungal drugs in treatment of candidiasis.抗真菌药物治疗念珠菌病的体内药效学
Antimicrob Agents Chemother. 2003 Apr;47(4):1179-86. doi: 10.1128/AAC.47.4.1179-1186.2003.
5
Antifungal activity of the echinocandin anidulafungin (VER002, LY-303366) against yeast pathogens: a comparative study with M27-A microdilution method.棘白菌素类药物阿尼芬净(VER002,LY-303366)对酵母病原体的抗真菌活性:采用M27-A微量稀释法的比较研究。
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In vitro activity of micafungin (FK-463) against Candida spp.: microdilution, time-kill, and postantifungal-effect studies.米卡芬净(FK-463)对念珠菌属的体外活性:微量稀释法、时间杀菌法及抗真菌后效应研究
Antimicrob Agents Chemother. 2002 Dec;46(12):3846-53. doi: 10.1128/AAC.46.12.3846-3853.2002.
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Has antifungal susceptibility testing come of age?抗真菌药敏试验成熟了吗?
Clin Infect Dis. 2002 Oct 15;35(8):982-9. doi: 10.1086/342384. Epub 2002 Sep 24.
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Testing conditions for determination of minimum fungicidal concentrations of new and established antifungal agents for Aspergillus spp.: NCCLS collaborative study.测定新型及已确立的抗真菌药物对曲霉属最低杀菌浓度的试验条件:美国国家临床实验室标准委员会协作研究
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10
In vitro interaction of caspofungin acetate with voriconazole against clinical isolates of Aspergillus spp.醋酸卡泊芬净与伏立康唑对曲霉属临床分离株的体外相互作用
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针对酵母和霉菌的杀真菌活性测定:从杀菌测试中吸取的经验教训以及标准化的必要性。

Determination of fungicidal activities against yeasts and molds: lessons learned from bactericidal testing and the need for standardization.

作者信息

Pfaller M A, Sheehan D J, Rex J H

机构信息

Department of Pathology and Epidemiology, University of Iowa College of Medicine, Iowa City, Iowa 52242, USA.

出版信息

Clin Microbiol Rev. 2004 Apr;17(2):268-80. doi: 10.1128/CMR.17.2.268-280.2004.

DOI:10.1128/CMR.17.2.268-280.2004
PMID:15084501
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC387411/
Abstract

In certain unique clinical settings, the ability of the antimicrobial agent administered to kill the pathogen outright may be quite important. These situations invariably involve infection of a site not easily accessed by host defenses and/or of a structure with essential anatomic or physiologic function such as the heart (endocarditis), central nervous system (meningitis), or bone (osteomyelitis). Likewise, infections in immunosuppressed hosts, especially those who are neutropenic, are often thought to require microbicidal therapy. Proof of the cidal nature of an antimicrobial agent in vitro is tedious, complex, and fraught with error. Although several methods for assessing in vitro bactericidal activity have been standardized (NCCLS M26-A and M21-A), the clinical relevance of these determinations is questionable and the tests are performed infrequently in most laboratories. Most of the clinical data supporting the need for microbicidal therapy and testing have focused on bacterial infections. However, given the fact that most serious fungal infections occur in profoundly immunosuppressed individuals, it is generally assumed that a cidal regimen would be preferable in that setting as well. In view of this clinical concern and the perceived need to assess the fungicidal activity of a variety of agents, we considered that it would be useful to review what is known about the issues and problems in assessing bactericidal activity and the clinical utility of such measurements. Following this review, we discuss the issue of how one defines fungicidal activity in vitro and in vivo and how feasible it might be to determine the fungicidal activity of organism-drug combinations for purposes of both drug development and clinical care. Proposed methods for fungal time-kill determinations and minimal fungicidal concentration determinations are also discussed.

摘要

在某些独特的临床环境中,所使用的抗菌药物直接杀死病原体的能力可能非常重要。这些情况总是涉及宿主防御难以到达的部位的感染和/或具有重要解剖或生理功能的结构的感染,如心脏(心内膜炎)、中枢神经系统(脑膜炎)或骨骼(骨髓炎)。同样,免疫抑制宿主中的感染,尤其是中性粒细胞减少的宿主,通常被认为需要杀菌治疗。在体外证明抗菌药物的杀菌性质既繁琐又复杂,而且充满误差。尽管有几种评估体外杀菌活性的方法已经标准化(NCCLS M26 - A和M21 - A),但这些测定的临床相关性值得怀疑,并且在大多数实验室中很少进行这些测试。大多数支持杀菌治疗和测试必要性的临床数据都集中在细菌感染上。然而,鉴于大多数严重的真菌感染发生在深度免疫抑制的个体中,一般认为在这种情况下采用杀菌方案可能也是更可取的。鉴于这种临床关注以及评估各种药物杀菌活性的明显需求,我们认为回顾一下在评估杀菌活性方面已知的问题以及此类测量的临床实用性将是有用的。在这次回顾之后,我们讨论如何在体外和体内定义杀菌活性,以及为了药物开发和临床护理的目的确定生物体 - 药物组合的杀菌活性有多可行。还讨论了真菌时间 - 杀灭测定和最低杀菌浓度测定的建议方法。