Emerging Role of Sphingolipids in Amphotericin B Drug Resistance.

IF 2.3 4区 医学 Q3 INFECTIOUS DISEASES
Kashish Madaan, Vinay Kumar Bari
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引用次数: 1

Abstract

Invasive fungal infections in humans are common in people with compromised immune systems and are difficult to treat, resulting in high mortality. Amphotericin B (AmB) is one of the main antifungal drugs available to treat these infections. AmB binds with plasma membrane ergosterol, causing leakage of cellular ions and promoting cell death. The increasing use of available antifungal drugs to combat pathogenic fungal infections has led to the development of drug resistance. AmB resistance is not very common and is usually caused by changes in the amount or type of ergosterol or changes in the cell wall. Intrinsic AmB resistance occurs in the absence of AmB exposure, whereas acquired AmB resistance can develop during treatment. However, clinical resistance arises due to treatment failure with AmB and depends on multiple factors such as the pharmacokinetics of AmB, infectious fungal species, and host immune status. Candida albicans is a common opportunistic pathogen that can cause superficial infections of the skin and mucosal surfaces, thrush, to life-threatening systemic or invasive infections. In addition, immunocompromised individuals are more susceptible to systemic infections caused by Candida, Aspergillus, and Cryptococcus. Several antifungal drugs with different modes of action are used to treat systemic to invasive fungal infections and are approved for clinical use in the treatment of fungal diseases. However, C. albicans can develop a variety of defenses against antifungal medications. In fungi, plasma membrane sphingolipid molecules could interact with ergosterol, which can lead to the alteration of drug susceptibilities such as AmB. In this review, we mainly summarize the role of sphingolipid molecules and their regulators in AmB resistance.

鞘脂在两性霉素B耐药中的新作用。
侵袭性真菌感染在免疫系统受损的人群中很常见,难以治疗,导致高死亡率。两性霉素B (AmB)是治疗这些感染的主要抗真菌药物之一。AmB与质膜麦角甾醇结合,引起细胞离子渗漏,促进细胞死亡。越来越多地使用现有的抗真菌药物来对抗致病性真菌感染,导致了耐药性的发展。AmB抗性并不常见,通常是由麦角甾醇的量或类型的变化或细胞壁的变化引起的。内在耐药发生在没有AmB暴露的情况下,而获得性AmB耐药可以在治疗期间产生。然而,临床耐药是由于AmB治疗失败而产生的,并且取决于多种因素,如AmB的药代动力学、感染性真菌种类和宿主免疫状态。白色念珠菌是一种常见的机会性病原体,可引起皮肤和粘膜表面的浅表感染,鹅口疮,危及生命的全身或侵袭性感染。此外,免疫功能低下的个体更容易受到念珠菌、曲霉菌和隐球菌引起的全身感染。几种具有不同作用模式的抗真菌药物被用于治疗全身到侵袭性真菌感染,并被批准用于治疗真菌疾病的临床应用。然而,白色念珠菌可以对抗真菌药物产生多种防御。在真菌中,质膜鞘脂分子可以与麦角甾醇相互作用,从而导致AmB等药物敏感性的改变。本文就鞘脂分子及其调控因子在AmB耐药中的作用作一综述。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Microbial drug resistance
Microbial drug resistance 医学-传染病学
CiteScore
6.00
自引率
3.80%
发文量
118
审稿时长
6-12 weeks
期刊介绍: Microbial Drug Resistance (MDR) is an international, peer-reviewed journal that covers the global spread and threat of multi-drug resistant clones of major pathogens that are widely documented in hospitals and the scientific community. The Journal addresses the serious challenges of trying to decipher the molecular mechanisms of drug resistance. MDR provides a multidisciplinary forum for peer-reviewed original publications as well as topical reviews and special reports. MDR coverage includes: Molecular biology of resistance mechanisms Virulence genes and disease Molecular epidemiology Drug design Infection control.
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