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新型 Fks 热点导致酿酒酵母获得棘白菌素耐药性及其对枝顶孢属固有耐药性的影响。

New Fks hot spot for acquired echinocandin resistance in Saccharomyces cerevisiae and its contribution to intrinsic resistance of Scedosporium species.

机构信息

Department of Microbiology and Immunology, Drexel University College of Medicine, Philadelphia, PA 19129-1033, USA.

出版信息

Antimicrob Agents Chemother. 2011 Aug;55(8):3774-81. doi: 10.1128/AAC.01811-10. Epub 2011 May 16.

Abstract

Echinocandins represent a new antifungal group with potent activity against Candida species. These lipopeptides inhibit the synthesis of β-1,3-glucan, the major cell wall polysaccharide. Acquired resistance or reduced echinocandin susceptibility (RES) is rare and associated with mutations in two "hot spot" regions of Fks1 or Fks2, the probable β-1,3-glucan synthases. In contrast, many fungi demonstrate intrinsic RES for reasons that remain unclear. We are using Saccharomyces cerevisiae to understand the basis for RES by modeling echinocandin-Fks interaction. Previously characterized mutations confer cross-RES; we screened for mutations conferring differential RES, implying direct interaction of that Fks residue with a variable echinocandin side chain. One mutant (in an fks1Δ background) exhibited ≥16-fold micafungin and anidulafungin versus caspofungin RES. Sequencing identified a novel Fks2 mutation, W714L/Y715N. Equivalent W695L/Y696N and related W695L/F/C mutations in Fks1 generated by site-directed mutagenesis and the isolation of a W695L-equivalent mutation in Candida glabrata confirmed the role of the new "hot spot 3" in RES. Further mutagenesis expanded hot spot 3 to Fks1 residues 690 to 700, yielding phenotypes ranging from cross-RES to differential hypersusceptibility. Fks1 sequences from intrinsically RES Scedosporium species revealed W695F-equivalent substitutions; Fks1 hybrids expressing Scedosporium prolificans hot spot 3 confirmed that this substitution imparts RES.

摘要

棘白菌素类代表一类新的抗真菌药物,对念珠菌属具有强大的活性。这些脂肽抑制β-1,3-葡聚糖的合成,β-1,3-葡聚糖是主要的细胞壁多糖。获得性耐药或棘白菌素敏感性降低(RES)很少见,与 Fks1 或 Fks2 中两个“热点”区域的突变有关,这两个区域可能是β-1,3-葡聚糖合酶。相比之下,许多真菌由于某些原因表现出固有 RES,这些原因尚不清楚。我们正在使用酿酒酵母通过模拟棘白菌素-Fks 相互作用来了解 RES 的基础。以前表征的突变赋予交叉 RES;我们筛选了赋予差异 RES 的突变,这意味着该 Fks 残基与可变棘白菌素侧链的直接相互作用。一个突变体(在 fks1Δ 背景下)对米卡芬净和阿尼芬净的抗性比卡泊芬净高出 16 倍。测序确定了一个新的 Fks2 突变,W714L/Y715N。通过定点诱变产生的 Fks1 中相当于 W695L/Y696N 和相关的 W695L/F/C 突变,以及在 Candida glabrata 中分离到的相当于 W695L 的突变,证实了新的“热点 3”在 RES 中的作用。进一步的突变扩大了热点 3 到 Fks1 的残基 690 到 700,产生的表型从交叉 RES 到差异超敏性不等。从固有 RES 的 Scedosporium 种中分离到的 Fks1 序列显示出 W695F 等效取代;表达 Scedosporium prolificans 热点 3 的 Fks1 杂种证实了这种取代赋予了 RES。

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